TY  - THES
A1  - Dang, Su-Yin Judith
T1  - Funktionelle Bedeutung der Neuroplastizität bei Multipler Sklerose
T1  - The functional relevance of neuronal plasticity in multiple sclerosis
N2  - Die Multiple Sklerose ist eine chronische neurologische Erkrankung, welche in der industrialisierten Welt einen der häufigsten Gründe für eine bleibende Behinderung bei jungen Erwachsenen darstellt. Obwohl die ZNS-Schädigung, charakterisiert durch Demyelinisierung und axonale Schädigung im Rahmen entzündlicher Vorgänge, durch verschiedene Reparaturmechanismen reduziert wird, akkumuliert die Läsionslast im zentralen Nervensystem mit der Zeit. T2-gewichtete MRT-Studien zeigen, dass die dargestellten Pathologien nur mäßig mit den motorischen Defiziten korrelieren. Diese Diskrepanz wird unter anderem auf Vorgänge der Neuroplastizität zurückgeführt, als deren Basismechanismen Langzeitpotenzierung (LTP) und -depression (LTD) gelten. In verschiedenen fMRT-Studien haben sich Hinweise ergeben, dass diese adaptiven Veränderungen zur Reorganisation kortikaler Repräsentationmuster führen können, so dass bei MS-Patienten eine ausgedehntere Aktivierung ipsilateraler sensomotorischer Areale bei motorischen Aufgaben zu beobachten ist. Die transkranielle Magnetstimulation (TMS) bietet die Möglichkeit, mittels virtueller Läsionstechniken eine direkte Aussage über die kausale Beziehung zwischen Struktur und Funktion zu liefern. Die funktionelle Rolle ipsilateraler Motorareale wurde an 26 MS-Patienten, in Relation zu ihrer motorischen Beeinträchtigung und ZNS-Schädigung, und an nach Alter, Geschlecht und Händigkeit zugeordneten Kontrollprobanden, untersucht. Die motorische Leistungsfähigkeit wurde durch verschiedene Tests zur Handfunktion erhoben. Die ZNS-Schädigung wurde mittels MR-Spektroskopie als NAA/Cr Quotient sowie durch die CML erhoben. Die Aufgabe zur einfachen Reaktionszeit (SRT) bestand aus einer isometrischen Abduktionsbewegung des rechten Daumens gegen einen Kraftaufnehmer auf ein akustisches Go-Signal. Mit TMS-Einzelreizen wurde mit Hilfe einer Neuronavigation eine reversible virtuelle Läsion über bestimmten Gehirnarealen, kontralateraler M1, ipsilateraler M1 und ipsilateraler PMd, erzeugt. Es wurde eine Kontrollstimulation über MO durchgeführt. Die TMS-Einzelreize wurden 100ms nach dem Go-Signal appliziert. Als SRT wurde der Zeitraum zwischen dem Go-Signal und EMG-Beginn im APB definiert. Die signifikanten SRT-Verlängerungen bei TMS über dem ipsilateralen M1 und dem ipsilateralen PMd zeigen, dass diese Regionen eine Rolle bei der motorischen Funktion bei MS spielen. Die fehlenden Korrelationen zwischen motorischen Funktionstest und NAA/Cr-Verhältnis sowie die inverse Korrelation zur kortikomuskulären Latenz sind durch strukturell von der krankheitsbedingten Pathologie betroffenen kompensierenden Gehirnregionen erklärbar. Bei dem Theta Burst Experiments (TBS) wurde ein virtueller Läsionseffekt durch eine repetitive TMS-Intervention über dem ipsilateralen M1 induziert. Die Ergebnisse zeigen ähnliche Veränderungen der Exzitabilität bei MS-Patienten und gesunden Kontrollprobanden, was schließen lässt, dass die LTD bei mild bis moderat betroffenen MS-Patienten weitestgehend unbeeinträchtigt ist. MS-Patienten zeigen im Vergleich zu den Kontrollen eine ähnliche Minderung der Verhaltensleistung, Trefferquote in ein Kraftfenster, der MS-Patienten im Kontrollvergleich. Die Ergebnisse zeigen, dass ipsilaterale motorische Areale in der Lage sind den primär motorischen Kortex soweit zu kompensieren, jedoch die Fähigkeit zur Kompensation in fortgeschrittenen Krankheitsstadien eingeschränkt ist. Abschließend kann man zusammenfassen, dass die funktionelle Rekrutierung von ipsilateralen Motorarealen eine adaptive Antwort auf chronische Gehirnschädigung bei MS-Patienten sein kann, allerdings mit Einschränkung der Kapazität in fortgeschrittenen Krankheitsstadien. Nachdem die synaptische Plastizität weitestgehend intakt scheint, sollte man besonders Mechanismen der späten Phase der Plastizität fördern, welche auf eine langfristige kortikale Plastizität abzielen. Weitere Studien in diesem Forschungszweig könnten einen Beitrag zur Entwicklung therapeutischer Konzepte der Neurorehabilitation bei Multipler Sklerose leisten.
N2  - Multiple Sclerosis is a chronic neurological disease, which is one of the common reasons in the industrial world causing a lasting disablement at young adults. Despite of reduction by several mechanisms the cns injury characterized by demyelinizing and axonal injury in order of inflammatory processes the lesion load of the cns accumulates over the years. T2-weighted MRI studies only show moderate correlations between the represented pathologies and the motoric deficits. This discrepancy is attributed i.a. to procedures of neuroplasticity whose basic mechanisms are considered as Long-term potentiation (LTP) and -depression (LTD). Several fMRI studies suggest a reogranization of cortical representative pattern due to these adaptive changes. Therefore an extended activation of ipilaterale sensomotoric areas is observed in MS patients performing motoric tasks. Transcranial Magnetic Stimulation (TMS) provides via lesional techniques the possibility of a direct conclusion causal link to structure and function. The functional role of ipsilateral motor areas has been examined in 26 MS patients in relation to their motor impairment and cns injury. Healthy controls were matched for age, sex and handedness. The motor performance was assessed by a test battery of hand function. The cns injury was evaluated using magnetic resonance spectroscopy (NAA/Cr Quotient) and TMS (CML). The Simple Reaction Time task (SRT) consisted of a brisk isometric abduction of the right thumb against a force transducer as a respond to an auditorily Go-Signal. With the help of a neuronavigational device a reversible virtual lesion, delivered by TMS single pulses, were applied to specific brain areas, contralateral M1, ipsilateral M1 and ipsilateral PMD. A control stimulation were assessed to MO??. TMS Single pulses were applied 100ms after Go-Signal. SRT were defined as the time between Go-Signal and EMG onset. Significant extention of SRT after TMS to ipsilateral M1 and ipsilateral PMd evidence the role of these regions in motoric function in MS. The missing correlation between motor performance and NAA/Cr Quotient as well as the inverse correlation to CML are explainable by compensation brain regions which are themselves structurally affected by disease pathologies. In the Thetaburs experiments (TBS) a virtual lesion was induced by a repetitive TMS intervention to ipsilateral M1. The results show a similar change of excitability in MS patients and healthy controls which concludes that LTD is not compromised in mild to moderate affected MS patients. MS patients presented in comparison to controlls a similiar discrease of behavioral performance, hit rate in a force range. The results evidence that ipsilateral motor areas have the ability to compensate the primary motor cortex. But the ability for compensation is limited in advanced stages of illness. The concluding summary is that functional recruitment of ipsilateral motor areas are adaptive response to chronic brain injury in MS patients but with limited capacity in advanced stages of illness. As the synaptic plasticity seem intact to the greatest possible extent mechanism of the late stadium of plasticity should be supported which aim at long term cortical plasticity. Further studies in this branch of research could contribute the development of therapeutic concepts of neurorehabilitation in MS.
KW  - Neuronale Plastizität
KW  - Multiple Sklerose
KW  - Transkranielle Magnetstimulation
KW  - neuronal plasticity
KW  - multiple sclerosis
KW  - transcranial magnetic stimulation
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-73817
ER  - 
TY  - JOUR
A1  - Chen, Y.
A1  - Palm, F.
A1  - Lesch, K. P.
A1  - Gerlach, M.
A1  - Moessner, R.
A1  - Sommer, C.
T1  - 5-hydroxyindolacetic acid (5-HIAA), a main metabolite of serotonin, is responsible for complete Freund's adjuvant-induced thermal hyperalgesia in mice
N2  - Background: The role of serotonin (5-hydroxytrptamine, 5-HT) in the modulation of pain has been widely studied. Previous work led to the hypothesis that 5-hydroxyindolacetic acid (5-HIAA), a main metabolite of serotonin, might by itself influence pain thresholds. Results: In the present study, we investigated the role of 5-HIAA in inflammatory pain induced by intraplantar injection of complete Freund’s adjuvant (CFA) into the hind paw of mice. Wild-type mice were compared to mice deficient of the 5-HT transporter (5-HTT-/- mice) using behavioral tests for hyperalgesia and high-performance liquid chromatography (HPLC) to determine tissue levels of 5-HIAA. Wild-type mice reproducibly developed thermal hyperalgesia and paw edema for 5 days after CFA injection. 5-HTT-/- mice treated with CFA had reduced thermal hyperalgesia on day 1 after CFA injection and normal responses to heat hereafter. The 5-HIAA levels in spinal cord and sciatic nerve as measured with HPLC were lower in 5-HTT-/- mice than in wild-type mice after CFA injection. Pretreatment of wild-type mice with intraperitoneal injection of para-chlorophenylalanine (p-CPA), a serotonin synthesis inhibitor, resulted in depletion of the 5-HIAA content in spinal cord and sciatic nerve and decrease in thermal hyperalgesia in CFA injected mice. The application of exogenous 5-HIAA resulted in potentiation of thermal hyperalgesia induced by CFA in 5-HTT-/- mice and in wild-type mice pretreated with p- CPA, but not in wild-type mice without p-CPA pretreatment. Further, methysergide, a broad-spectrum serotonin receptor antagonist, had no effect on 5-HIAA-induced potentiation of thermal hyperalgesia in CFA-treated wildtype mice. Conclusion: Taken together, the present results suggest that 5-HIAA plays an important role in modulating peripheral thermal hyperalgesia in CFA induced inflammation, probably via a non-serotonin receptor mechanism.
KW  - Medizin
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-68858
ER  - 
TY  - JOUR
A1  - Chen, Yong
A1  - Boettger, Michael K.
A1  - Reif, Andreas
A1  - Schmitt, Angelika
A1  - Ueceyler, Nurcan
A1  - Sommer, Claudia
T1  - Nitric oxide synthase modulates CFA-induced thermal hyperalgesia through cytokine regulation in mice
N2  - Background: Although it has been largely demonstrated that nitric oxide synthase (NOS), a key enzyme for nitric oxide (NO) production, modulates inflammatory pain, the molecular mechanisms underlying these effects remain to be clarified. Here we asked whether cytokines, which have well-described roles in inflammatory pain, are downstream targets of NO in inflammatory pain and which of the isoforms of NOS are involved in this process. Results: Intraperitoneal (i.p.) pretreatment with 7-nitroindazole sodium salt (7-NINA, a selective neuronal NOS inhibitor), aminoguanidine hydrochloride (AG, a selective inducible NOS inhibitor), L-N(G)-nitroarginine methyl ester (L-NAME, a non-selective NOS inhibitor), but not L-N(5)-(1-iminoethyl)-ornithine (L-NIO, a selective endothelial NOS inhibitor), significantly attenuated thermal hyperalgesia induced by intraplantar (i.pl.) injection of complete Freund’s adjuvant (CFA). Real-time reverse transcription-polymerase chain reaction (RT-PCR) revealed a significant increase of nNOS, iNOS, and eNOS gene expression, as well as tumor necrosis factor-alpha (TNF), interleukin-1 beta (IL-1b), and interleukin-10 (IL-10) gene expression in plantar skin, following CFA. Pretreatment with the NOS inhibitors prevented the CFA-induced increase of the pro-inflammatory cytokines TNF and IL-1b. The increase of the antiinflammatory cytokine IL-10 was augmented in mice pretreated with 7-NINA or L-NAME, but reduced in mice receiving AG or L-NIO. NNOS-, iNOS- or eNOS-knockout (KO) mice had lower gene expression of TNF, IL-1b, and IL-10 following CFA, overall corroborating the inhibitor data. Conclusion: These findings lead us to propose that inhibition of NOS modulates inflammatory thermal hyperalgesia by regulating cytokine expression.
KW  - Medizin
Y1  - 2010
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-68349
ER  - 
TY  - JOUR
A1  - Kraft, P.
A1  - Schwarz, T.
A1  - Pochet, L.
A1  - Stoll, G.
A1  - Kleinschnitz, Christoph
T1  - COU254, a specific 3-carboxamide-coumarin inhibitor of coagulation factor XII, does not protect mice from acute ischemic stroke
N2  - Background: Anticoagulation is an important means to prevent from acute ischemic stroke but is associated with a significant risk of severe hemorrhages. Previous studies have shown that blood coagulation factor XII (FXII)- deficient mice are protected from pathological thrombus formation during cerebral ischemia without bearing an increased bleeding tendency. Hence, pharmacological blockade of FXII might be a promising and safe approach to prevent acute ischemic stroke and possibly other thromboembolic disorders but pharmacological inhibitors selective over FXII are still lacking. In the present study we investigated the efficacy of COU254, a novel nonpeptidic 3-carboxamide-coumarin that selectively blocks FXII activity, on stroke development and post stroke functional outcome in mice. Methods: C57Bl/6 mice were treated with COU254 (40 mg/kg i.p.) or vehicle and subjected to 60 min transient middle cerebral artery occlusion (tMCAO) using the intraluminal filament method. After 24 h infarct volumes were determined from 2,3,5-Triphenyltetrazoliumchloride(TTC)-stained brain sections and functional scores were assessed. Hematoxylin and eosin (H&E) staining was used to estimate the extent of neuronal cell damage. Thrombus formation within the infarcted brain areas was analyzed by immunoblot. Results: Infarct volumes and functional outcomes on day 1 after tMCAO did not significantly differ between COU254 pre-treated mice or untreated controls (p > 0.05). Histology revealed extensive ischemic neuronal damage regularly including the cortex and the basal ganglia in both groups. COU254 treatment did not prevent intracerebral fibrin(ogen) formation. Conclusions: COU254 at the given concentration of 40 mg/kg failed to demonstrate efficacy in acute ischemic stroke in this preliminary study. Further preclinical evaluation of 3-carboxamide-coumarins is needed before the antithrombotic potential of this novel class of FXII inhibitors can be finally judged.
KW  - Schlaganfall
KW  - Maus
KW  - COU254
Y1  - 2010
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-68103
ER  - 
TY  - JOUR
A1  - Pham, Mirko
A1  - Helluy, X.
A1  - Braeuninger, S.
A1  - Jakob, P.
A1  - Stoll, G.
A1  - Kleinschnitz, Christoph
A1  - Bendszus, M.
T1  - Outcome of experimental stroke in C57Bl/6 and Sv/129 mice assessed by multimodal ultra-high field MRI
N2  - Transgenic mice bred on C57Bl/6 or Sv/129 genetic background are frequently used in stroke research. It is well established that variations in cerebrovascular anatomy and hemodynamics can influence stroke outcome in different inbred mouse lines. We compared stroke development in C57Bl/6 and Sv/129 mice in the widely used model of transient middle cerebral artery occlusion (tMCAO) by multimodal ultra-high field magnetic resonance imaging (MRI). C57Bl/6 and Sv/129 mice underwent 60 min of tMCAO and were analyzed by MRI 2 h and 24 h afterwards. Structural and functional images were registered to a standard anatomical template. Probability maps of infarction were rendered by automated segmentation from quantitative T2-relaxometric images. Whole-brain segmentation of infarction was accomplished manually on high-resolution T2-weighted (T2-w) RARE images. Cerebral perfusion (cerebral blood flow, CBF) was measured quantitatively by modified continuous arterial-spin-labeling (CASL) and apparent diffusion coefficients (ADC) by spin-echo diffusion-weighted imaging (DWI). Probabilities of cortical (95.1% ± 3.1 vs. 92.1% ± 2.5; p > 0.05) and subcortical (100% vs. 100%; p > 0.05) infarctions at 24 h were similar in both groups as was the whole-brain volumetric extent of cerebral infarction. In addition, CBF and ADC values did not differ between C57Bl/6 and Sv/129 mice at any time point or region of interest. The C57Bl/6 and Sv/129 genetic background is no major confounding factor of infarct size and cerebral perfusion in the tMCAO model.
KW  - NMR-Tomographie
Y1  - 2010
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-68115
ER  - 
TY  - JOUR
A1  - Ehling, P.
A1  - Bittner, S.
A1  - Bobak, N.
A1  - Schwarz, T.
A1  - Wiendl, H.
A1  - Budde, T.
A1  - Kleinschnitz, Christoph
A1  - Meuth, S. G.
T1  - Two pore domain potassium channels in cerebral ischemia: a focus on K2p9.1 (TASK3, KCNK9)
N2  - BACKGROUND: Recently, members of the two-pore domain potassium channel family (K2P channels) could be shown to be involved in mechanisms contributing to neuronal damage after cerebral ischemia. K2P3.1-/- animals showed larger infarct volumes and a worse functional outcome following experimentally induced ischemic stroke. Here, we question the role of the closely related K2P channel K2P9.1. METHODS: We combine electrophysiological recordings in brain-slice preparations of wildtype and K2P9.1-/- mice with an in vivo model of cerebral ischemia (transient middle cerebral artery occlusion (tMCAO)) to depict a functional impact of K2P9.1 in stroke formation. RESULTS: Patch-clamp recordings reveal that currents mediated through K2P9.1 can be obtained in slice preparations of the dorsal lateral geniculate nucleus (dLGN) as a model of central nervous relay neurons. Current characteristics are indicative of K2P9.1 as they display an increase upon removal of extracellular divalent cations, an outward rectification and a reversal potential close to the potassium equilibrium potential. Lowering extracellular pH values from 7.35 to 6.0 showed comparable current reductions in neurons from wildtype and K2P9.1-/- mice (68.31 +/- 9.80% and 69.92 +/- 11.65%, respectively). These results could be translated in an in vivo model of cerebral ischemia where infarct volumes and functional outcomes showed a none significant tendency towards smaller infarct volumes in K2P9.1-/- animals compared to wildtype mice 24 hours after 60 min of tMCAO induction (60.50 +/- 17.31 mm3 and 47.10 +/- 19.26 mm3, respectively). CONCLUSIONS: Together with findings from earlier studies on K2P2.1-/- and K2P3.1-/- mice, the results of the present study on K2P9.1-/- mice indicate a differential contribution of K2P channel subtypes to the diverse and complex in vivo effects in rodent models of cerebral ischemia.
KW  - Kaliumkanal
KW  - Ischemia
Y1  - 2010
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-68129
ER  - 
TY  - THES
A1  - Stenner, Max-Philipp
T1  - Diapedese und immuntolerogene Funktion regulatorischer T Zellen in der schubförmigen Multiplen Sklerose unter Therapie mit Natalizumab
T1  - Diapedesis and tolerogenic function of regulatory T cells under natalizumab therapy of relapsing-remitting multiple sclerosis
N2  - Die schubförmige Multiple Sklerose (MS) ist eine chronisch-entzündliche, demyelinisierende, multifokale Erkrankung des Zentralnervensystems (ZNS). Autoreaktive immunologische Prozesse, insbesondere der T-Zell vermittelten Immunität, leisten einen entscheidenden Beitrag zur Pathogenese der schubförmigen MS. Ein wesentlicher Schritt in immunpathogenetischen Modellen ist die transendotheliale Migration von Immunzellen über die Blut-Hirn-Schranke. Die Interaktion des very late antigen 4 (VLA-4) mit dem vascular cell adhesion molecule 1 (VCAM-1) und mit Fibronectin leistet einen wesentlichen Beitrag zur Extravasation von T Zellen in das ZNS. Auf dieser Schlüsselfunktion des VLA-4 gründet die Therapie mit Natalizumab, einem monoklonalen Antikörper gegen die α4 Integrinkette. Ziel der vorliegenden Studie war es, die Auswirkungen der Therapie der schubförmigen MS mit Natalizumab auf die transendotheliale Migration von CD4+CD25+FOXP3+ und CD4+HLA-G+ regulatorischen T Zellen (Treg) und auf die antiproliferative Funktion von FOXP3+ Treg zu untersuchen. Zentrale Hypothese war, dass Natalizumab über eine universelle Blockade der Immunzellinvasion in das ZNS hinaus immunmodulatorisch wirkt. Unter Verwendung eines prospektiven, longitudinalen Studiendesigns wurden die T Zellen von RR-MS Patienten unter Therapie mit Natalizumab (n=31) sowie von stabilen RR-MS Patienten ohne Therapie und gesunden Spendern in jeweils zwei in vitro Modellen der Blut-Hirn-Schranke sowie Treg vermittelter Immuntoleranz untersucht. FOXP3+ regulatorische T-Zellen banden weniger Natalizumab und exprimierten weniger VLA-4 als nicht-regulatorische T Helferzellen, bewahrten unter Therapie jedoch einen höheren Anteil ihrer ursprünglichen VLA-4 Expression. FOXP3+ Treg gesunder Spender wiesen in vitro höhere Migrationsraten über mikrovaskuläre humane Hirnendothelzellen als nicht-regulatorische T Helferzellen auf und akkumulierten innerhalb der T-Zell Population nach Migration. Dagegen reicherten sich FOXP3+ Treg von MS Patienten in Folge der Migration nur nach Vorbehandlung des Endothel mit inflammatorischen Zytokinen an, nicht jedoch ohne diese Vorbehandlung. Natalizumab beeinträchtigte die transendotheliale Migration von FOXP3+ Treg und nicht-regulatorischen T Helferzellen von MS Patienten in vergleichbaren Ausmaßen. HLA-G+ Treg zeigten in den Migrationsanalysen ein den FOXP3+ Treg entgegengesetztes Muster und wiesen ausschließlich in der MS, nicht jedoch im Gesunden, eine höhere Migrationsrate auf als HLA-G- T Helferzellen. Diese Akkumulation von HLA-G+ Treg in der migrierten Zellfraktion ließ sich nach Therapiebeginn nicht mehr nachweisen. Eine ergänzende Einzelfallstudie zu Auswirkungen des LFA-1 Antagonisten Efalizumab auf Treg ergab Hinweise auf eine Schlüsselfunktion dieses Integrins für die Migration von FOXP3+ Treg. Die Analyse der FOXP3+ Treg Suppressorfunktion zeigte eine schrittweise Zunahme des suppressiven Einflusses von FOXP3+ Treg auf die Reifung dendritischer Zellen unter Natalizumabtherapie. Zeitlich parallel kam es zu einem Ungleichgewicht in der Expression von LFA-1 auf der Oberfläche von FOXP3+ Treg und nicht-regulatorischen T Helferzellen. Zusammenfassend stützt die Studie die Hypothese immunmodulatorischer Effekte von Natalizumab in der schubförmigen Multiplen Sklerose, insbesondere auf den Antagonismus von regulatorischen und Effektor-T Zellen. Die Arbeit belegt, dass Natalizumab in vivo über die Blockade von VLA-4 hinaus modulatorisch in das Netzwerk von Adhäsionsmolekülen auf T Zellen eingreift. Die Studienergebnisse ergeben ein Überwiegen regulatorischer Einflüsse auf die Reifung dendritischer Zellen unter Therapie. Berichte zum Beitrag von LFA-1 zur Suppressorfunktion von FOXP3+ Treg werden durch Daten der vorliegenden Studie unterstützt und um Hinweise auf eine zusätzliche, spezifische Bedeutung des Integrins zur präferentiellen Diapedese dieser Treg über die Blut-Hirn-Schranke im Gesunden erweitert. Zudem liefert die Arbeit erstmals Hinweise auf einen Defekt der transendothelialen Migration von FOXP3+ Treg über die Blut-Hirn-Schranke in der schubförmigen Multiplen Sklerose, der zur Entstehung neuer Läsionen beitragen könnte.
N2  - Relapsing-remitting multiple sclerosis (MS) is a multifocal, chronic, inflammatory, demyelinating disease of the central nervous system (CNS). Autoreactive processes, in particular T-cell mediated immunity, are essential to the pathogenesis of MS. A pivotal step in immunopathogenetic models is the diapedesis of immune cells across the blood-brain barrier. Transendothalial migration of encephalitogenic T cells across the blood-brain barrier depends critically on the interaction between very late antigen 4 (VLA-4) and vascular cell adhesion molecule 1 (VCAM-1) as well as fibronectin. The therapeutic rationale for natalizumab, a monoclonal antibody against the α4 chain of VLA-4, is based on this pivotal role of VLA-4 for T-cell diapedesis. This study aimed to examine transendothelial migration of CD4+CD25+FOXP3+ and CD4+HLA-G+ regulatory T cells (Treg) as well as the suppressive capacity of FOXP3+ Treg in relapsing-remitting multiple sclerosis under natalizumab therapy. The study tested the hypothesis that natalizumab exerts immunmodulatory effects beyond a universal blockade of immune cell invasion into the CNS. T cells from MS patients under natalizumab therapy (n=31) were compared to T cells from stable MS patients without treatment and from healthy controls according to a prospective, longitudinal study design. Two in vitro models of the blood-brain barrier and two models of Treg-mediated tolerance were employed. FOXP3+ regulatory T cells exhibited reduced natalizumab binding and VLA-4 expression when compared to non-regulatory T helper cells but preserved a greater proportion of their initial VLA-4 expression under natalizumab therapy. FOXP3+ Treg from healthy controls showed enhanced migration across human brain microvascular endothelial cells when compared to non-regulatory T cells in vitro and accumulated within the T-cell population after migration. FOXP3+ Treg from MS patients, in contrast, accumulated only after pre-treatment of the endothelium with inflammatory cytokines. Natalizumab inhibited transendothelial migration of FOXP3+ Treg and non-regulatory T cells to a similar extent. HLA-G+ Treg showed a reverse pattern in these migration assays: HLA-G+ Treg from MS patients, but not from healthy controls, exhibited enhanced migratory rates when compared to non-regulatory, HLA-G- TH cells. This accumulation of HLA-G+ Treg within the fraction of migrated cells could no longer be detected any more after initiation of natalizumab therapy. The results of a supplementary single case study on the effects of the LFA-1 antagonist efalizumab on Treg pointed towards a pivotal role of this integrin for the preferential migration of FOXP3+ Treg. Suppression of the maturation of dendritic cells by FOXP3+ Treg gradually increased under natalizumab therapy. A growing imbalance in the surface distribution of LFA-1 among FOXP3+ Treg and non-regulatory TH cells parallelled this recovery of MS Treg suppression. In summary, this study supports the hypothesis of immunomodulatory effects of natalizumab in relapsing-remitting multiple sclerosis, particularly on the antagonism between regulatory and effector T cells. The study documents interference of natalizumab with the network of adhesion molecules on T cells in vivo that extends beyond its blockade of VLA-4. Furthermore, it demonstrates a dominance of Treg-mediated suppression on the maturation of dendritic cells under therapy. It supports recent reports on a pivotal role of LFA-1 for suppressive mechanisms of FOXP3+ Treg and points towards a similar relevance for preferential Treg migration across the blood-brain barrier. Lastly, the study provides the first evidence for deficient transendothelial migration of FOXP3+ Treg in multiple sclerosis, which could contribute to early lesion formation.
KW  - Neuroimmunologie
KW  - Multiple Sklerose
KW  - Natalizumab
KW  - regulatorische T Zellen
KW  - FOXP3
KW  - HLA-G
KW  - Diapedese
KW  - natalizumab
KW  - regulatory T cells
KW  - FOXP3
KW  - HLA-G
KW  - diapedesis
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-70573
ER  - 
TY  - JOUR
A1  - Sommer, Claudia
A1  - Richter, Helmut
A1  - Rogausch, Jan P.
A1  - Frettloh, Jule
A1  - Lungenhausen, Margitta
A1  - Maier, Christoph
T1  - A modified score to identify and discriminate neuropathic pain: a study on the German version of the neuropathic pain symptom inventory (NPSI)
N2  - Background: Neuropathic pain must be correctly diagnosed for optimal treatment. The questionnaire named Neuropathic Pain Symptom Inventory (NPSI) was developed in its original French version to evaluate the different symptoms of neuropathic pain. We hypothesized that the NPSI might also be used to differentiate neuropathic from non-neuropathic pain. Methods: We translated the NPSI into German using a standard forward-backward translation and administered it in a case-control design to patients with neuropathic (n = 68) and non-neuropathic pain (headache and osteoarthritis, n = 169) to validate it and to analyze its discriminant properties, its sensitivity to change, and to detect neuropathic pain subgroups with distinct profiles. Results: Using a sum score (the NPSI-G score), we found sensitivity to change (r between 0.37 and 0.5 for pain items of the graded chronic pain scale) and could distinguish between neuropathic and other pain on a group basis, but not for individual patients. Post hoc development of a discriminant score with optimized diagnostic properties to distinguish neuropathic pain from non-neuropathic pain resulted in an instrument with high sensitivity (91%) and acceptable specificity (70%). We detected six different pain profiles in the patient group with neuropathic pain; three profiles were found to be distinct. Conclusions: The NPSI-G potentially combines the properties of a diagnostic tool and an instrument to identify subtypes of neuropathic pain.
KW  - Neuralgie
KW  - NPSI
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-68716
ER  - 
TY  - JOUR
A1  - Kreissl, Michael C.
A1  - Stout, David B.
A1  - Wong, Koon-Pong
A1  - Wu, Hsiao-Ming
A1  - Caglayan, Evren
A1  - Ladno, Waldemar
A1  - Zhang, Xiaoli
A1  - Prior, John
A1  - Reiners, Christoph
A1  - Huang, Sung-Cheng
A1  - Schelbert, Heinrich R.
T1  - Influence of Dietary Interventions and Insulin on Myocardial, Skeletal Muscle and Brain [18F]-Fluorodeoxyglucose Kinetics in Mice
N2  - Background: We evaluated the effect of insulin stimulation and dietary changes on myocardial, skeletal muscle and brain [18F]-fluorodeoxyglucose (FDG) kinetics and uptake in vivo in intact mice. Methods: Mice were anesthetized with isoflurane and imaged under different conditions: non-fasted (n = 7; "controls"), non-fasted with insulin (2 IU/kg body weight) injected subcutaneously immediately prior to FDG (n = 6), fasted (n = 5), and fasted with insulin injection (n = 5). A 60-min small-animal PET with serial blood sampling and kinetic modeling was performed. Results: We found comparable FDG standardized uptake values (SUVs) in myocardium in the non-fasted controls and non-fasted-insulin injected group (SUV 45-60 min, 9.58 ± 1.62 vs. 9.98 ± 2.44; p = 0.74), a lower myocardial SUV was noted in the fasted group (3.48 ± 1.73; p < 0.001). In contrast, the FDG uptake rate constant (Ki) for myocardium increased significantly by 47% in non-fasted mice by insulin (13.4 ± 3.9 ml/min/100 g vs. 19.8 ± 3.3 ml/min/100 g; p = 0.030); in fasted mice, a lower myocardial Ki as compared to controls was observed (3.3 ± 1.9 ml/min/100 g; p < 0.001). Skeletal muscle SUVs and Ki values were increased by insulin independent of dietary state, whereas in the brain, those parameters were not influenced by fasting or administration of insulin. Fasting led to a reduction in glucose metabolic rate in the myocardium (19.41 ± 5.39 vs. 3.26 ± 1.97 mg/min/100 g; p < 0.001), the skeletal muscle (1.06 ± 0.34 vs. 0.34 ± 0.08 mg/min/100 g; p = 0.001) but not the brain (3.21 ± 0.53 vs. 2.85 ± 0.25 mg/min/100 g; p = 0.19). Conclusions: Changes in organ SUVs, uptake rate constants and metabolic rates induced by fasting and insulin administration as observed in intact mice by small-animal PET imaging are consistent with those observed in isolated heart/muscle preparations and, more importantly, in vivo studies in larger animals and in humans. When assessing the effect of insulin on the myocardial glucose metabolism of non-fasted mice, it is not sufficient to just calculate the SUV - dynamic imaging with kinetic modeling is necessary.
KW  - Insulin
KW  - Gehirn
KW  - Skelettmuskel
KW  - Maus
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-68775
ER  - 
TY  - JOUR
A1  - Puschmann, Anne-Katrin
A1  - Sommer, Claudia
T1  - Hypervigilance or avoidance of trigger related cues in migraineurs? - A case-control study using the emotional stroop task
N2  - Background: “Negative affect” is one of the major migraine triggers. The aim of the study was to assess attentional biases for negative affective stimuli that might be related to migraine triggers in migraine patients with either few or frequent migraine and healthy controls. Methods: Thirty-three subjects with frequent migraine (FM) or with less frequent episodic migraine, and 20 healthy controls conducted two emotional Stroop tasks in the interictal period. In task 1, general affective words and in task 2, pictures of affective faces (angry, neutral, happy) were used. For each task we calculated two emotional Stroop indices. Groups were compared using one-way ANOVAs. Results: The expected attentional bias in migraine patients was not found. However, in task 2 the controls showed a significant attentional bias to negative faces, whereas the FM group showed indices near zero. Thus, the FM group responded faster to negative than to positive stimuli. The difference between the groups was statistically significant. Conclusions: The findings in the FM group may reflect a learned avoidance mechanism away from affective migraine triggers.
KW  - Migräne
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-69103
ER  - 
TY  - THES
A1  - Subramanian, Narayan
T1  - Role of NaV1.9 in activity dependent axon growth in embryonic cultured motoneurons
T1  - Die Rolle der NaV1.9 in Aktivität abhängig Axonwachstum in embryonalen kultivierten Motoneuronen
N2  - Spontaneous neural activity has been shown to regulate crucial events in neurite growth including axonal branching and path finding. In animal models of spinal muscular atrophy (SMA) cultured embryonic mouse motoneurons show distinct defect in axon elongation and neural activity. This defect is governed by abnormal clustering of Ca2+ channels in the axonal regions and the protruding growth cone area. The mechanisms that regulate the opening of calcium channels in developing motoneurons are not yet clear. The question was addressed by blocking neural activity in embryonic cultured motoneurons by pharmacological inhibition of voltage-gated sodium channels (VGSC) by saxitoxin (STX) and tetrodotoxin (TTX). Low dosages of STX resulted in significant reduction of axon growth and neural activity in cultured motoneurons. This pharmacological treatment did not affect survival of motoneurons in comparison to control motoneurons that was grown in the presence of survival neurotrophic factors BDNF and CNTF. It was also found that STX was 10 times more potent than TTX a common inhibitor of VGSC with a reduced activity on the TTX-insensitive sodium channels NaV1.5, NaV1.8 and NaV1.9. Reverse Transcriptase-PCR experiments revealed the presence of NaV1.9 as the likely candidate that begins to express from embryonic stage sixteen in the mouse spinal cord. Immunolabelling experiments showed that the channel is expressed in the axonal compartments and axonal growth cones in cultured motoneurons. Suppression of NaV1.9 in cultured motoneurons by lentivirus mediated short hairpin-RNA (shRNA) resulted in shorter axon length in comparison with uninfected and scrambled constructs. Further, embryonic motoneurons cultured from NaV1.9 knockout mice also showed a significant reduction in neural activity and axon growth. The findings of this work highlight the role of NaV1.9 as an important contender in regulating activity dependent axon growth in embryonic cultured motoneurons. NaV1.9 could therefore be considered as a prospective molecule that could play an important role in regulating axon growth in motoneuron disease models like spinal muscular atrophy (SMA).
N2  - Spontane neuronale Aktivität reguliert essentielle Ereignisse im Neuritenwachstum, wie beispielsweise die axonale Verzweigung und die Erkennung des Wachstumspfades. Motoneurone, die aus Tiermodellen der Spinalen Muskelatrophie (SMA) gewonnen werden, zeigen einen auffälligen Defekt im Streckenwachstum von Axonen und in der neuronalen Aktivität. Dieser Defekt wird von anormaler Clusterbildung von Ca2+ Kanälen in axonalen Regionen und in Wachstumskegeln begleitet. Die Mechanismen, die das Öffnen von Kalziumkanälen in embryonalen Motoneuronen in der Entwicklung regulieren, und die für das aktivitätsabhängige Axonwachstum benötigt werden, sind nicht bekannt. Diese Frage wurde in dieser Studie bearbeitet, indem neuronale Aktivität in embryonalen Motoneuronen durch pharmakologische Inhibition von spannungsabhängigen Natriumkanälen durch Saxitoxin (STX) und Tetrodotoxin blockiert wurde. Geringe Dosen von Saxitoxin bewirkten eine deutliche Reduktion des Axonwachstums und der neuronalen Aktivität in kultivierten Motoneuronen. Diese pharmakologische Behandlung beeinflusste nicht das Überleben von Motoneuronen im Vergleich zu Kontroll-Motoneuronen, die in der Anwesenheit der neurotrophen Faktoren BDNF und CNTF kultiviert wurden. Saxitoxin war etwa 5-10-mal potenter als TTX, ein üblicher Blocker spannungsabhängiger Natriumkanäle mit einer verminderte Aktivität auf die TTX-insensitiven Natriumkanäle NaV1.5, NaV1.8, und NaV1.9. Reverse-Transkriptase-PCR Experimente bestätigten die Anwesenheit von NaV1.9 am Tag E16 (embryonaler Tag 16) im Rückenmark der Maus. NaV1.9 ist ein einzigartiger Typus von einem Natriumkanal welcher in der Lage ist neuronale Erregbarkeit in der Nähe des Ruhemembranpotentials zu steuern. Deshalb war NaV1.9 ein guter Kandidat für einen Kanal, der spontane Erregung in Motoneuronen vermittelt. Immunofärbungen zeigten, dass NaV1.9 in axonalen Kompartimenten und axonalen Wachstumskegeln von kultivierten Motoneuronen exprimiert ist. Die Unterdrückung von NaV1.9 in kultivierten Motoneuronen durch lentiviralexprimierte short hairpin-RNA (shRNA) resultierte in kürzerer Axonlänge, im Vergleich zu nicht-infizierten Motoneuronen oder Motoneuronen, die eine sinnlose Kontroll-shRNA Sequenz exprimierten. Embryonale, kultivierte Motoneurone von NaV1.9 knockout Mäusen zeigten eine signifikante Verringerung der neuronalen Aktivität und verkürzte Axone. Diese Ergebnisse weisen auf eine Bedeutung von NaV1.9 im aktivitätsabhängigen Axonwachstum hin
KW  - Axon
KW  - Embryonalentwicklung
KW  - Motoneuron
KW  - Natriumkanal
KW  - Motoneuronen
KW  - NaV1.9
KW  - motoneuron
KW  - Nav1.9
KW  - axon growth
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-57536
ER  - 
TY  - THES
A1  - Graulich, Michael
T1  - Spinale Effekte von TNF-α am Modell des tumorinduzierten Knochenschmerzes der Maus
T1  - Spinal effects of TNF-α in a mouse model of bone cancer pain
N2  - Am Modell des tumorinduzierten Schmerzes der Maus wurden sowohl das Schmerzverhalten der Tiere als auch spezifische morphologische Veränderungen im Hinterhorn des Rückenmarks (Aktivierung von Astrozyten) und im tumorbefallenen Knochen analysiert. Durch Analyse von Mäusen mit Defizienz für TNF-Rezeptor 1, TNF-Rezeptor 2 oder für beide Rezeptoren konnte die Rolle von TNF-α seiner Rezeptoren bei der Entstehung von tumorinduziertem Schmerz untersucht werden. Im Unterschied zu neuropathischen Schmerzmodellen konnte gezeigt werden, dass beide TNF-Rezeptoren ausgeschaltet werden müssen, um eine signifikante Schmerzreduktion zu erzielen. Die systemische Behandlung mit dem TNF-neutralisierenden Fusionsprotein Etanercept konnte die im genetischen Modell gezeigte Reduktion der mechanischen Allodynie teilweise, aber nicht vollständig reproduzieren. Eine Hemmung der Mikrogliaaktivierung mittels Minocyclin erbrachte im Tumor-schmerzmodell keinen Effekt auf das Schmerzverhalten der Tiere. Die histologische Analyse der tumoraffizierten Knochen zeigte eine signifikante Zunahme der Osteoklastenaktivität in tumortragenden Tieren. Die Behandlung mit Minocyclin war ohne erkennbaren Effekt auf die Differenzierung und die Aktivität der Osteoklasten. Es ergaben sich jedoch Hinweise, dass TNF-α einen hemmenden Einfluss auf die Osteoklastenaktivität im Knochentumormodell hat, da sowohl in den TNFR-KO-Tieren als auch unter Gabe von Etanercept eine Steigerung der Osteoklastenaktivität nachgewiesen werden konnte. Die Ergebnisse dieser Arbeit zeigen, dass TNF-α eine wichtige Rolle, sowohl in der Entstehung, als auch in der Aufrechterhaltung von tumorinduziertem Schmerz spielt. Hier liegt der Ansatzpunkt für weitere Studien mit dem Ziel, eine spezifische Pharmakotherapie zu entwickeln mit wirksamer TNF-α Blockade auch bei Patienten mit Tumorschmerzen. Nach den Erkenntnissen dieser Arbeit mit Etanercept sollte ein spezielles Augenmerk auf die ZNS-Gängigkeit dieser Substanzen gelegt werden und die Gefahr der Möglichkeit eines vermehrten Tumorwachstum bedacht werden.
N2  - Bone-cancer-related pain is one of the most disabling factors in patients suffering from primary bone cancer or bone metastases. Recent studies point toward an important role of proinflammatory cytokines, example tumor necrosis factor-alpha (TNF), for tumor growth and bone-cancer-associated pain. Mechanisms by which TNF, through its receptor subtypes, TNF receptor 1 (TNFR1) and -2 (TNFR2), elicits altered sensation and pain behavior, are still incompletely understood. To look for a potential role of TNF in bone cancer pain, cancer-related pain was analyzed in fibrosarcoma-bearing C57Bl/6J wild type mice after systemic antagonism of TNF. To further clarify the role of TNF receptor (TNFR) in bone-cancer pain, naive and fibrosarcoma-bearing C57Bl/ 6J wild type and transgenic mice with a deficiency of TNFR1 (TNFR1ko), TNFR2 (TNFR2ko), and TNFR1+2 (TNFR1+2ko) were compared regarding cancer-related pain and hyperalgesia, tumor growth, osteoclast activation, and spinal astrogliosis. Systemic antagonism of TNF significantly alleviated tactile hypersensitivity and spontaneous bone-cancer-related pain behavior. Most interestingly, combined deletion of the TNFR1 and TNFR2, but not of either gene alone, almost completely inhibited the development of tactile hypersensitivity, whereas spontaneous pain behavior was transiently increased. Accordingly, spinal astrogliosis was markedly reduced, whereas tumor growth was significantly increased in TNFR1+2ko mice. In contrast, deletion of the TNFR1 or TNFR2 gene alone did not change tumor growth or spinal astrogliosis. Our findings suggest that the combined absence of TNFR1 and TNFR2 is necessary for the attenuation of cancer-related tactile hypersensitivity and concomitant spinal astrogliosis, whereas tumor growth seems to be inhibited by combined TNFR activation. These findings support the hypothesis of cytokine-dependent pain development in cancer pain. Differential targeting of TNFR activation could be an interesting strategy in bone-cancer-related pain conditions.
KW  - Neuralgie
KW  - Schmerz
KW  - Schmerzforschung
KW  - Tumor-Nekrose-Faktor <alpha>
KW  - Tumor-Nekrose-Faktor <alpha>-Inhibitor
KW  - Experimentaltumor
KW  - Knochentumor
KW  - pain
KW  - tumor
KW  - bone
KW  - neuropathy
KW  - tnf
KW  - glia
KW  - minocycline
KW  - etanercept
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-54439
ER  - 
TY  - JOUR
A1  - Frerichs, K.
A1  - Sirèn, Anna-Leena
A1  - Feuerstein, G.
A1  - Hallenbeck, JM
T1  - The onset of postischemic hypoperfusion in rats is precipitous and may be controlled by local neurons
N2  - Background and Purpose: Reperfusion following transient global cerebral ischemia is characterized by an initial hyperemic phase, which precedes hypo perfusion. The pathogenesis of these flow derangements remains obscure. Our study investigates the dynamics of postischemic cerebral blood flow changes, with particular attention to the role of local neurons. Metho(Js: We assessed local cortical blood flow continuously by laser Doppler flowmetry to permit observation of any rapid flow changes after forebrain ischemia induced by four-vessel occlusion for 20 minutes in rats. To investigate the role of local cortical neurons in the regulation of any blood flow fluctuations, five rats received intracortical microinjections of a neurotoxin (10 p,g ibotenic acid in 1 p,1; 1.5-mm-depth parietal cortex) 24 hours before ischemia to induce selective and localized neuronal depletion in an area corresponding to the sampie volume of the laser Doppler probe (1 mm3 ). Local cerebral blood flow was measured within the injection site and at an adjacent control site. Results: Ischemia was followed by marked hyperemia (235 ±23% of control, n =7), followed by secondary hypoperfusion (45±3% of control, n=7). The transition from hyperemia to hypoperfusioo occurred not gradually but precipitously (maximal slope of flow decay: 66±6%/min; n=7). In ibotenic acid-injected rats, hyperemia was preserved at the injection site, but the sudden decline of blood flow was abolished (maximal slope of flow decay: 5±3%/min compared with 53±8%/min at the control site; n=5, p<O.OOI) and 00 significant hypoperfusion de\eloped (103±20% of control at 60 minutes). Conclusions: These data suggest that the rapid transition to cortical hypo perfusion after forebrain ischemia may be triggered locally by a neuronal mechanism but that this mechanism does not underlie the initial hyperemia.
KW  - Gehirn
KW  - Durchblutung
KW  - cerebral blood flow
KW  - cerebral ischemia
KW  - reperfusion
KW  - rats
Y1  - 1992
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-47980
ER  - 
TY  - RPRT
A1  - Magnus, Tim
A1  - Linker, Ralf A.
A1  - Meuth, Sven G.
A1  - Kleinschnitz, Christoph
A1  - Korn, Thomas
T1  - Report on the 2nd scientific meeting of the "Verein zur Foerderung des Wissenschaftlichen Nachwuchses in der Neurologie" (NEUROWIND e.V.) held in Motzen, Germany, Oct. 29'th - Oct. 31'st, 2010
N2  - Summary of the scientific contributions to the NEUROWIND meeting 2010: Contributions in the fields of neuroimmunology and neurodegeneration
KW  - Wissenschaftlicher Nachwuchs
KW  - Neurologie
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-68789
ER  - 
TY  - THES
A1  - Schubert, Andrea Julia
T1  - Vergleich der Ergebnisse von Karotis-Stenting und -TEA an der Universitätsklinik Würzburg
T1  - Comparing the results of carotid stenting and carotid endarterectomy at the university of Würzburg
N2  - Der Vergleich der Verfahren Karotisstenting und Karotis-TEA an der Universitätsklinik Würzburg zeigt, dass bei richtiger Indikationsstellung sowie ausreichender Erfahrung der Neuroradiologen, CAS eine ernstzunehmende Alternative zu CEA darstellt. Besonderes Augenmerk lag dabei auf periprozeduale Komplikationen sowie Langzeitergebnisse bezüglich Tod,Insult und Restenose.
N2  - Comparing carotid artery stenting and endarterectomy at the university of Würzburg, we showed that CAS is a serious alternative to CEA if the right indication is given and when interventionalists have enough experience. Our endpoints were periprocedual complications and long-term outcomes regarding stroke, death and recurrent stenosis.
KW  - Carotis
KW  - Arteria carotis interna
KW  - Carotisstenose
KW  - Carotischirurgie
KW  - Endarteriektomie
KW  - Würzburg / Universität Würzburg
KW  - Vergleich
KW  - Stent
KW  - CEA
KW  - CAS
KW  - versus
KW  - vs
KW  - CEA
KW  - CAS
KW  - versus
KW  - vs
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-67130
ER  - 
TY  - JOUR
A1  - Haarmann, Axel
A1  - Deiss, Annika
A1  - Prochaska, Juergen
A1  - Foerch, Christian
A1  - Weksler, Babette
A1  - Romero, Ignacio
A1  - Couraud, Pierre-Olivier
A1  - Stoll, Guido
A1  - Rieckmann, Peter
A1  - Buttmann, Mathias
T1  - Evaluation of Soluble Junctional Adhesion Molecule-A as a Biomarker of Human Brain Endothelial Barrier Breakdown
N2  - Background: An inducible release of soluble junctional adhesion molecule-A (sJAM-A) under pro-inflammatory conditions was described in cultured non-CNS endothelial cells (EC) and increased sJAM-A serum levels were found to indicate inflammation in non-CNS vascular beds. Here we studied the regulation of JAM-A expression in cultured brain EC and evaluated sJAM-A as a serum biomarker of blood-brain barrier (BBB) function. Methodology/Principal Findings: As previously reported in non-CNS EC types, pro-inflammatory stimulation of primary or immortalized (hCMEC/D3) human brain microvascular EC (HBMEC) induced a redistribution of cell-bound JAM-A on the cell surface away from tight junctions, along with a dissociation from the cytoskeleton. This was paralleled by reduced immunocytochemical staining of occludin and zonula occludens-1 as well as by increased paracellular permeability for dextran 3000. Both a self-developed ELISA test and Western blot analysis detected a constitutive sJAM-A release by HBMEC into culture supernatants, which importantly was unaffected by pro-inflammatory or hypoxia/reoxygenation challenge. Accordingly, serum levels of sJAM-A were unaltered in 14 patients with clinically active multiple sclerosis compared to 45 stable patients and remained unchanged in 13 patients with acute ischemic non-small vessel stroke over time. Conclusion: Soluble JAM-A was not suited as a biomarker of BBB breakdown in our hands. The unexpected non-inducibility of sJAM-A release at the human BBB might contribute to a particular resistance of brain EC to inflammatory stimuli, protecting the CNS compartment.
KW  - Biomarker
KW  - Gehirn
Y1  - 2010
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-68468
ER  - 
TY  - JOUR
A1  - Doerck, Sebastian
A1  - Goebel, Kerstin
A1  - Weise, Gesa
A1  - Schneider-Hohendorf, Tilman
A1  - Reinhardt, Michael
A1  - Hauff, Peter
A1  - Schwab, Nicholas
A1  - Linker, Ralf
A1  - Maeurer, Mathias
A1  - Meuth, Sven G.
A1  - Wiendl, Heinz
T1  - Temporal Pattern of ICAM-I Mediated Regulatory T Cell Recruitment to Sites of Inflammation in Adoptive Transfer Model of Multiple Sclerosis
N2  - Migration of immune cells to the target organ plays a key role in autoimmune disorders like multiple sclerosis (MS). However, the exact underlying mechanisms of this active process during autoimmune lesion pathogenesis remain elusive. To test if pro-inflammatory and regulatory T cells migrate via a similar molecular mechanism, we analyzed the expression of different adhesion molecules, as well as the composition of infiltrating T cells in an in vivo model of MS, adoptive transfer experimental autoimmune encephalomyelitis in rats. We found that the upregulation of ICAM-I and VCAM-I parallels the development of clinical disease onset, but persists on elevated levels also in the phase of clinical remission. However, the composition of infiltrating T cells found in the developing versus resolving lesion phase changed over time, containing increased numbers of regulatory T cells (FoxP3) only in the phase of clinical remission. In order to test the relevance of the expression of cell adhesion molecules, animals were treated with purified antibodies to ICAM-I and VCAM-I either in the phase of active disease or in early remission. Treatment with a blocking ICAM-I antibody in the phase of disease progression led to a milder disease course. However, administration during early clinical remission aggravates clinical symptoms. Treatment with anti-VCAM-I at different timepoints had no significant effect on the disease course. In summary, our results indicate that adhesion molecules are not only important for capture and migration of pro-inflammatory T cells into the central nervous system, but also permit access of anti-inflammatory cells, such as regulatory T cells. Therefore it is likely to assume that intervention at the blood brain barrier is time dependent and could result in different therapeutic outcomes depending on the phase of CNS lesion development.
KW  - Multiple Sklerose
Y1  - 2010
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-68565
ER  - 
TY  - JOUR
A1  - Kraft, Peter
A1  - Schwarz, Tobias
A1  - Meijers, Joost C. M.
A1  - Stoll, Guido
A1  - Kleinschnitz, Christoph
T1  - Thrombin-Activatable Fibrinolysis Inhibitor (TAFI) Deficient Mice Are Susceptible to Intracerebral Thrombosis and Ischemic Stroke
N2  - Background: Thrombus formation is a key step in the pathophysiology of acute ischemic stroke and results from the activation of the coagulation cascade. Thrombin plays a central role in this coagulation system and contributes to thrombus stability via activation of thrombin-activatable fibrinolysis inhibitor (TAFIa). TAFIa counteracts endogenous fibrinolysis at different stages and elevated TAFI levels are a risk factor for thrombotic events including ischemic stroke. Although substantial in vitro data on the influence of TAFI on the coagulation-fibrinolysis-system exist, investigations on the consequences of TAFI inhibition in animal models of cerebral ischemia are still lacking. In the present study we analyzed stroke development and post stroke functional outcome in TAFI-/- mice. Methodology/Principal Findings: TAFI-/- mice and wild-type controls were subjected to 60 min transient middle cerebral artery occlusion (tMCAO) using the intraluminal filament method. After 24 hours, functional outcome scores were assessed and infarct volumes weremeasured from 2,3,5-Triphenyltetrazoliumchloride (TTC)-stained brain slices. Hematoxylin and eosin (H&E) staining was used to estimate the extent of neuronal cell damage. Thrombus formation within the infarcted brain areas was analyzed by immunoblot. Infarct volumes and functional outcomes did not significantly differ between TAFI-/- mice and controls (p.0.05). Histology revealed extensive ischemic neuronal damage regularly including the cortex and the basal ganglia in both groups. TAFI deficiency also had no influence on intracerebral fibrin(ogen) formation after tMCAO. Conclusion: Our study shows that TAFI does not play a major role for thrombus formation and neuronal degeneration after ischemic brain challenge.
KW  - Thrombus
Y1  - 2010
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-68519
ER  - 
TY  - JOUR
A1  - Kraft, Peter
A1  - Benz, Peter Michael
A1  - Austinat, Madeleine
A1  - Brede, Marc Elmar
A1  - Schuh, Kai
A1  - Walter, Ulrich
A1  - Stoll, Guido
A1  - Kleinschnitz, Christoph
T1  - Deficiency of Vasodilator-Stimulated Phosphoprotein (VASP) Increases Blood-Brain-Barrier Damage and Edema Formation after Ischemic Stroke in Mice
N2  - Background: Stroke-induced brain edema formation is a frequent cause of secondary infarct growth and deterioration of neurological function. The molecular mechanisms underlying edema formation after stroke are largely unknown. Vasodilator-stimulated phosphoprotein (VASP) is an important regulator of actin dynamics and stabilizes endothelial barriers through interaction with cell-cell contacts and focal adhesion sites. Hypoxia has been shown to foster vascular leakage by downregulation of VASP in vitro but the significance of VASP for regulating vascular permeability in the hypoxic brain in vivo awaits clarification. Methodology/Principal Findings: Focal cerebral ischemia was induced in Vasp2/2 mice and wild-type (WT) littermates by transient middle cerebral artery occlusion (tMCAO). Evan’s Blue tracer was applied to visualize the extent of blood-brainbarrier (BBB) damage. Brain edema formation and infarct volumes were calculated from 2,3,5-triphenyltetrazolium chloride (TTC)-stained brain slices. Both mouse groups were carefully controlled for anatomical and physiological parameters relevant for edema formation and stroke outcome. BBB damage (p,0.05) and edema volumes (1.7 mm360.5 mm3 versus 0.8 mm360.4 mm3; p,0.0001) were significantly enhanced in Vasp2/2 mice compared to controls on day 1 after tMCAO. This was accompanied by a significant increase in infarct size (56.1 mm3617.3 mm3 versus 39.3 mm3610.7 mm3, respectively; p,0.01) and a non significant trend (p.0.05) towards worse neurological outcomes. Conclusion: Our study identifies VASP as critical regulator of BBB maintenance during acute ischemic stroke. Therapeutic modulation of VASP or VASP-dependent signalling pathways could become a novel strategy to combat excessive edema formation in ischemic brain damage.
KW  - Vasodilatator-stimuliertes Phosphoprotein
KW  - Vasodilator-Stimulated Phosphoprotein
Y1  - 2010
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-68522
ER  - 
TY  - JOUR
A1  - Kleinschnitz, Christoph
A1  - Grund, Henrike
A1  - Wingler, Kirstin
A1  - Armitage, Melanie E.
A1  - Jones, Emma
A1  - Mittal, Manish
A1  - Barit, David
A1  - Schwarz, Tobias
A1  - Geis, Christian
A1  - Kraft, Peter
A1  - Barthel, Konstanze
A1  - Schuhmann, Michael K.
A1  - Herrmann, Alexander M.
A1  - Meuth, Sven G.
A1  - Stoll, Guido
A1  - Meurer, Sabine
A1  - Schrewe, Anja
A1  - Becker, Lore
A1  - Gailus-Durner, Valerie
A1  - Fuchs, Helmut
A1  - Klopstock, Thomas
A1  - de Angelis, Martin Hrabe
A1  - Jandeleit-Dahm, Karin
A1  - Shah, Ajay M.
A1  - Weissmann, Norbert
A1  - Schmidt, Harald H. H. W.
T1  - Post-Stroke Inhibition of Induced NADPH Oxidase Type 4 Prevents Oxidative Stress and Neurodegeneration
N2  - Ischemic stroke is the second leading cause of death worldwide. Only one moderately effective therapy exists, albeit with contraindications that exclude 90% of the patients. This medical need contrasts with a high failure rate of more than 1,000 pre-clinical drug candidates for stroke therapies. Thus, there is a need for translatable mechanisms of neuroprotection and more rigid thresholds of relevance in pre-clinical stroke models. One such candidate mechanism is oxidative stress. However, antioxidant approaches have failed in clinical trials, and the significant sources of oxidative stress in stroke are unknown. We here identify NADPH oxidase type 4 (NOX4) as a major source of oxidative stress and an effective therapeutic target in acute stroke. Upon ischemia, NOX4 was induced in human and mouse brain. Mice deficient in NOX4 (Nox42/2) of either sex, but not those deficient for NOX1 or NOX2, were largely protected from oxidative stress, blood-brain-barrier leakage, and neuronal apoptosis, after both transient and permanent cerebral ischemia. This effect was independent of age, as elderly mice were equally protected. Restoration of oxidative stress reversed the stroke-protective phenotype in Nox42/2 mice. Application of the only validated low-molecular-weight pharmacological NADPH oxidase inhibitor, VAS2870, several hours after ischemia was as protective as deleting NOX4. The extent of neuroprotection was exceptional, resulting in significantly improved long-term neurological functions and reduced mortality. NOX4 therefore represents a major source of oxidative stress and novel class of drug target for stroke therapy.
KW  - Schlaganfall
Y1  - 2010
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-68416
ER  - 
TY  - THES
A1  - Fackelmann, Stefanie
T1  - Langzeitkorrelation evozierter Potentialparameter mit dem klinischen Verlauf bei Patienten mit Multipler Sklerose
T1  - Early abnormalities of evoked potentials and future disability in patients with multiple sclerosis
N2  - Evozierte Potenziale werden bereits als Hilfsmittel zur Diagnosestellung der Multiplen Sklerose herangezogen. Das Spektrum der Verläufe der Erkrankung ist sehr unterschiedlich. Ziel der Studie war es, zu prüfen, ob visuell (VEP), somatosensibel (SEP) und Magnet- (MEP) evozierte Potentiale durch das Aufdecken klinisch noch stummer Läsionen eine prognostische Bedeutung haben. Es wurden 94 Patienten bei Erstvorstellung sowie zum 5-Jahres- und 10-Jahresverlaufszeitpunkt untersucht. Es wurde ein Zusammenhang von MEP- und SEP-Scores mit dem späteren Behinderungsgrad, gemessen in Form der EDSS nach fünf und zehn jahren gefunden, sofern die elektrophysiologischen Untersuchungen in den ersten beiden Jahren nach Erstmanifestation klinischer Symptome durchgeführt worden waren (Gruppe 1, 44 Patienten). Für Gruppe 2 (50 Patienten), deren Erstuntersuchung später im Verlauf stattgefunden hatte (im Mittel 9,6a) konnte keine prognostische Bedeutung gesehen werden. Die Durchführung multimodaler evozierter Potenziale ist kann somit eine Hilfestellung zur frühzeitigen Therapieentscheidung geben.
N2  - Evoked potentials (EP) have a role in making the diagnosis of multiple sclerosis (MS) but their implication for predicting the future disease course in MS is under debate. EP data of 94 MS patients examined at first presentation, and after five and ten years were retrospectively analysed. Patients were divided into two groups in relation to the prior duration of disease at the time point of first examination: group 1 patients (n-44) were first examined within two years after disease onset, and group 2 patients (n-50) at later time points. As primary measures sum scores were calculated for abnormalities of single and combined EP (visual (VEP), somatosensory (SEP), magnetic motor evoked potentials (MEP)). In patients examined early after disease onset (group 1), a significant predictive value for abnormal EP was found with MEP and SEP sum scores at first presentation correlating significantly with Expanded Disability Status Scale (EDSS) values after five years, while the VEP sum score was not. The cumulative number of abnormal MEP, SEP and VEP results also indicated higher degrees of disability (EDSS≥ 3.5) after five years. Combined pathological SEP and MEP findings at first presentation best predicted clinical disability (EDSS≥ 3.5) after five years (odds ratio 11.0). EP data and EDSS at first presentation were not significantly linked suggesting that EP abnormalities at least in part represented clinically silent lesions not mirrored by EDSS. For patients in later disease phases (group 2), no significant associations between EP data at first presentation and EDSS at five and ten years were detected. Together with clinical findings and MR imaging, combined EP data may help to identify patients at high risk of long-term clinical deterioration and guide decisions as to immunomodulatory treatment.
KW  - Multiple Sklerose
KW  - Evozierte Potenziale
KW  - multiple sclerosis
KW  - evoked potentials
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-64840
ER  - 
TY  - THES
A1  - Ruschil, Christoph
T1  - Der Einfluss von Autoantikörpern gegen Aquaporin 4 bei der Pathogenese der Neuromyelitis optica
T1  - The function of autoantibodies targeting aquaporin-4 in the pathogenesis of neuromyelitis optica
N2  - Neuromyelitis optica (NMO) ist eine schwerwiegende Autoimmunerkrankung des zentralen Nervensystems, deren pathogene Ursache in Zusammenhang mit Autoantikörpern gegen Aquaporin 4 (AQP4) steht. In einem intrathekalen Passiv-Transfermodell der Ratte wurden die Auswirkungen von NMO-Immunglobulin (IgG) aus Plasmapheresematerial und rekombinanten Antikörpern gegen AQP4 sowie der Effekt von additiver Applikation von humanem Komplement untersucht. NMO-IgG, rekombinante Antikörper und modifizierte Antikörper ohne Fähigkeit zur Aktivierung der Komplementkaskade waren bei repetitiver Applikation in der Lage, auch ohne additives humanes Komplement NMO-ähnliche progrediente motorische Symptome zu induzieren. Durch Ko-Injektion von humanem Komplement konnte keine signifikante Exazerbation der Pathologie bewirkt werden. 
MRT-Studien zeigten lokale Schrankenstörungen am Ort der höchsten Antikörperkonzentration. In histologischen Aufarbeitungen von Rückenmarksschnitten zeigten sich lokale Deposition an humanem IgG, ein dazu korrelierender Verlust an AQP4 sowie eine darüber hinausgehende Reduktion des Glutamattransporters EAAT2, während GFAP-reaktive Astrozyten tendenziell hypertroph und vermehrt waren. Auch bei additiver Applikation von humanem Komplement wiesen die Läsionsareale im Gegensatz zu histopathologischen Befunden bei NMO-Patienten und anderen Tiermodellen nur eine geringe Ablagerung von aktivem Komplement und wenig Infiltration durch ED1-positive Makrophagen auf. Da in einem Kontrollexperiment mit intrazerebraler intraparenchymaler Applikation von NMO-IgG die beschriebene additive Zytotoxizität von humanem Komplement reproduziert werden konnte, erscheint die Verwendbarkeit des intrathkalen Modells zur Evaluation der Wirkung von humanem Komplement bei Autoimmunerkrankungen mit intraspinalen Zielepitopen nicht geeignet.
Die Ergebnisse lassen sich als Komplement-unabhängige intrinsische Wirkungen von Antikörpern gegen AQP4 deuten, die in einer Reduktion der Oberflächenexpresseion von AQP4 und EAAT2 resultieren und zu einer progredienten Myelopathie führen. Neben der bekannten Antikörper-induzierten Komplement-abhängigen Zytotoxizität könnten diese Effekte einen bislang nicht beschriebenen zusätzlichen Pathomechanismus bei der NMO darstellen.
N2  - Neuromyelitis optica (NMO) is a severe autoimmune disorder of the central nervous system that is causally linked to autoantibodies against aquaporin-4 (AQP4). In a intrathecal passive transfer rat model the effects of purified patient NMO-immunoglobuline (IgG) and recombinant anti-AQP4-antibodies were studied as well as those of additional application of human complement. Repetitive application of NMO-IgG, recombinant antibodies and modified antibodies without the ability of activation of the complement cascade caused NMO-like progressive symptoms. Additional application of human complement did not exacerbate the pathologic symptoms.
MRI-studies revealed local spinal cord lesions at the site of the highest antibody concentration. Histopathological analysis of the spinal cord showed local deposition of human IgG, a corresponding loss of AQP4 and - even more pronounced - of the excitatory amino acid transporter 2 (EAAT2), whereas immunoreactivity to the astrocytic marker glial fibrillary acid protein (GFAP) was increased. Even by additional application of human complement, only little deposition of activated complement und poor infiltration by ED1-positive macrophages was observed. However, direct intracerebral application of NMO-IgG revealed complement dependent cytotoxicity as described previously; therefore the intrathecal passive transfer model is not suited to evaluate the effects of human complement in autoimmune disorders with intraspinal targets.
The results can be interpreted as intrinsic effects of anti-AQP4-antibodies that are independent of complement activation and that reduce expressivity of AQP4 und EAAT2 and cause a progressive myelopathy. Additionally to the previously described antibody and complement dependent cytotoxicity, these effects might be a new pathogenic pathway in neuromyelitis optica.
KW  - Autoantikörper
KW  - AQP
KW  - Komplement
KW  - Neuromyelitis optica
KW  - Passiv-Transfer
KW  - autoantibodies
KW  - NMO
KW  - Aquaporin 4
KW  - AQP4
KW  - Komplement
KW  - EAAT2
KW  - passiv transfer
KW  - complement
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-105787
ER  - 
TY  - JOUR
A1  - Häuser, Winfried
A1  - Walitt, Brian
A1  - Fitzcharles, Mary-Ann
A1  - Sommer, Claudia
T1  - Review of pharmacological therapies in fibromyalgia syndrome
JF  - Arthritis Research & Therapy
N2  - This review addresses the current status of drug therapy for the management of fibromyalgia syndrome (FMS) and is based on interdisciplinary FMS management guidelines, meta-analyses of drug trial data, and observational studies. In the absence of a single gold-standard medication, patients are treated with a variety of drugs from different categories, often with limited evidence. Drug therapy is not mandatory for the management of FMS. Pregabalin, duloxetine, milnacipran, and amitriptyline are the current first-line prescribed agents but have had a mostly modest effect. With only a minority of patients expected to experience substantial benefit, most will discontinue therapy because of either a lack of efficacy or tolerability problems. Many drug treatments have undergone limited study and have had negative results. It is unlikely that these failed pilot trials will undergo future study. However, medications, though imperfect, will continue to be a component of treatment strategy for these patients. Both the potential for medication therapy to relieve symptoms and the potential to cause harm should be carefully considered in their administration.
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-121598
SN  - 1465-9913
VL  - 16
IS  - 201
ER  - 
TY  - JOUR
A1  - Weise, Gesa
A1  - Stoll, Guido
T1  - Magnetic resonance imaging of blood brain/nerve barrier dysfunction and leukocyte infiltration: closely related or discordant?
JF  - Frontiers in Neurology
N2  - Unlike other organs the nervous system is secluded from the rest of the organism by the blood brain barrier (BBB) or blood nerve barrier (BNB) preventing passive influx of fluids from the circulation. Similarly, leukocyte entry to the nervous system is tightly controlled. Breakdown of these barriers and cellular inflammation are hallmarks of inflammatory as well as ischemic neurological diseases and thus represent potential therapeutic targets. The spatiotemporal relationship between BBB/BNB disruption and leukocyte infiltration has been a matter of debate. We here review contrast-enhanced magnetic resonance imaging (MRI) as a non-invasive tool to depict barrier dysfunction and its relation to macrophage infiltration in the central and peripheral nervous system under pathological conditions. Novel experimental contrast agents like Gadofluorine M (Gf) allow more sensitive assessment of BBB dysfunction than conventional Gadolinium (Gd)-DTPA enhanced MRI. In addition, Gf facilitates visualization of functional and transient alterations of the BBB remote from lesions. Cellular contrast agents such as superparamagnetic iron oxide particles (SPIO) and perfluorocarbons enable assessment of leukocyte (mainly macrophage) infiltration by MR technology. Combined use of these MR contrast agents disclosed that leukocytes can enter the nervous system independent from a disturbance of the BBB, and vice versa, a dysfunctional BBB/BNB by itself is not sufficient to attract inflammatory cells from the circulation. We will illustrate these basic imaging findings in animal models of multiple sclerosis, cerebral ischemia, and traumatic nerve injury and review corresponding findings in patients.
KW  - contrast-enhanced MRI
KW  - neuroinflammation
KW  - gadolinium-DTPA
KW  - gadofluorine
KW  - iron oxide nanoparticles
KW  - blood brain barrier
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-123359
VL  - 3
IS  - 178
ER  - 
TY  - JOUR
A1  - Ablin, Jacob
A1  - Fitzcharles, Mary-Ann
A1  - Buskila, Dan
A1  - Shir, Yoram
A1  - Sommer, Claudia
A1  - Häuser, Winfried
T1  - Treatment of Fibromyalgia Syndrome: Recommendations of Recent Evidence-Based Interdisciplinary Guidelines with Special Emphasis on Complementary and Alternative Therapies
JF  - Evidence-Bayed Complementary and Alternative Medicine
N2  - Objective. Current evidence indicates that there is no single ideal treatment for fibromyalgia syndrome (FMS). First choice treatment options remain debatable, especially concerning the importance of complementary and alternative medicine (CAM) treatments. Methods. Three evidence-based interdisciplinary guidelines on FMS in Canada, Germany, and Israel were compared for their first choice and CAM-recommendations. Results. All three guidelines emphasized a patient-tailored approach according to the key symptoms. Aerobic exercise, cognitive behavioral therapy, and multicomponent therapy were first choice treatments. The guidelines differed in the grade of recommendation for drug treatment. Anticonvulsants (gabapentin, pregabalin) and serotonin noradrenaline reuptake inhibitors (duloxetine, milnacipran) were strongly recommended by the Canadian and the Israeli guidelines. These drugs received only a weak recommendation by the German guideline. In consideration of CAM-treatments, acupuncture, hypnosis/guided imagery, and Tai Chi were recommended by the German and Israeli guidelines. The Canadian guidelines did not recommend any CAM therapy. Discussion. Recent evidence-based interdisciplinary guidelines concur on the importance of treatment tailored to the individual patient and further emphasize the need of self-management strategies (exercise, and psychological techniques).
KW  - metaanalysis
KW  - management
KW  - care
Y1  - 2013
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-122235
SN  - 1741-427X
ER  - 
TY  - JOUR
A1  - Hansen, Niels
A1  - Seiler, Carola
A1  - Rumpf, Julian
A1  - Kraft, Peter
A1  - Dlaske, Henry
A1  - Abele-Horn, Marianne
A1  - Muellges, Wolfgang
T1  - Human Tuberculous Meningitis Caused by \(Mycobacterium\) \(caprae\)
JF  - Case Reports in Neurology
N2  - INTRODUCTION: Tuberculous meningitis (TM) causes substantial morbidity and mortality in humans. Human TM has been known to be induced by bacteria from the Mycobacterium tuberculosis complex (MTBC), such as M. tuberculosis and M. bovis.
CASE PRESENTATION: We describe a case of meningitis treated with fosfomycin, which showed partial effectiveness in an 80-year-old patient. After a lethal myocardial infarction, M. caprae (MC) was identified in cerebrospinal fluid culture. This isolated acid-fast organism was first identified as MTBC by MTBC-specific PCR (16S rDNA-PCR). Furthermore, species-specific identification of the isolate was done by gyrB PCR-restriction fragment length polymorphism analysis of a part of gyrB DNA. Colony morphology of the isolated MC strain showed dysgonic growth on Lowenstein-Jensen medium. The strain was susceptible to pyrazinamide (PZA).
CONCLUSION: This isolated strain was convincingly identified as MC according to the phenotypic and genotypic characteristics and PZA sensitivity. This is the first report of MC causing TM.
KW  - Mycobacterium caprae
KW  - Mycobacterium caprae
KW  - fosfomycin
KW  - Tuberkulose
KW  - Mycobacterium tuberculosis complex
KW  - tuberculous meningitis
KW  - cerebrospinal fluid culture
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-123425
VL  - 4
IS  - 1
ER  - 
TY  - JOUR
A1  - Boltze, Johannes
A1  - Kleinschnitz, Christoph
A1  - Reymann, Klaus G.
A1  - Reiser, Georg
A1  - Wagner, Daniel-Christoph
A1  - Kranz, Alexander
A1  - Michalski, Dominik
T1  - Neurovascular pathophysiology in cerebral ischemia, dementia and the ageing brain – current trends in basic, translational and clinical research
JF  - Experimental & Translational Stroke Medicine
N2  - The 7th International Symposium on Neuroprotection and Neurorepair was held from May 2nd to May 5th, 2012 in Potsdam, Germany. The symposium, which directly continues the successful Magdeburg meeting series, attracted over 330 colleagues from 29 countries to discuss recent findings and advances in the field. The focus of the 2012 symposium was widened from stroke and traumatic brain injury to neurodegenerative diseases, notably dementia, and more generally the ageing brain. Thereby, emphasis was given on neurovascular aspects of neurodegeneration and stroke including the blood–brain barrier, recent findings regarding the pathomechanism of Alzheimer’s disease, and brain imaging approaches. In addition, neurobiochemical aspects of neuroprotection, the role of astrogliosis, the clinical progress of cell-based approaches as well as translational hurdles and opportunities were discussed in-depth. This review summarizes some of the most stimulating discussions and reports from the meeting.
KW  - translational research
KW  - small vessel disease
KW  - Alzheimer’s disease
KW  - cerebral ischemia
KW  - neurorepair
KW  - neuroprotection
KW  - vascular dementia
KW  - mitochondria
KW  - astrogliosis
KW  - in vivo imaging
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-126679
VL  - 4
IS  - 14
ER  - 
TY  - JOUR
A1  - Kraft, Peter
A1  - De Meyer, Simon F.
A1  - Kleinschnitz, Christoph
T1  - Next-Generation Antithrombotics in Ischemic Stroke: Preclinical Perspective on ‘Bleeding-Free Antithrombosis’
JF  - Journal of Cerebral Blood Flow and Metabolism
N2  - The present antithrombotic drugs used to treat or prevent ischemic stroke have significant limitations: either they show only moderate efficacy (platelet inhibitors), or they significantly increase the risk for hemorrhages (thrombolytics, anticoagulants). Although most strokes are caused by thrombotic or embolic vessel occlusions, the pathophysiological role of platelets and coagulation is largely unclear. The introduction of novel transgenic mouse models and specific coagulation inhibitors facilitated a detailed analysis of molecular pathways mediating thrombus formation in models of acute ischemic stroke. Prevention of early platelet adhesion to the damaged vessel wall by blocking platelet surface receptors glycoprotein Ib alpha (GPIbα) or glycoprotein VI (GPVI) protects from stroke without provoking bleeding complications. In addition, downstream signaling of GPIbα and GPVI has a key role in platelet calcium homeostasis and activation. Finally, the intrinsic coagulation cascade, activated by coagulation factor XII (FXII), has only recently been identified as another important mediator of thrombosis in cerebrovascular disease, thereby disproving established concepts. This review summarizes the latest insights into the pathophysiology of thrombus formation in the ischemic brain. Potential clinical merits of novel platelet inhibitors and anticoagulants as powerful and safe tools to combat ischemic stroke are discussed.
KW  - von Willebrand factor
KW  - platelets
KW  - glycoprotein Ib
KW  - FXII
KW  - coagulation
KW  - Stim
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-126538
VL  - 32
IS  - 10
ER  - 
TY  - JOUR
A1  - Kraft, Peter
A1  - Drechsler, Christiane
A1  - Schuhmann, Michael K.
A1  - Gunreben, Ignaz
A1  - Kleinschnitz, Christoph
T1  - Characterization of Peripheral Immune Cell Subsets in Patients with Acute and Chronic Cerebrovascular Disease: A Case-Control Study
JF  - International Journal of Molecular Science
N2  - Immune cells (IC) play a crucial role in murine stroke pathophysiology. However, data are limited on the role of these cells in ischemic stroke in humans. We therefore aimed to characterize and compare peripheral IC subsets in patients with acute ischemic stroke/transient ischemic attack (AIS/TIA), chronic cerebrovascular disease (CCD) and healthy volunteers (HV). We conducted a case-control study of patients with AIS/TIA (n = 116) or CCD (n = 117), and HV (n = 104) who were enrolled at the University Hospital Würzburg from 2010 to 2013. We determined the expression and quantity of IC subsets in the three study groups and performed correlation analyses with demographic and clinical parameters. The quantity of several IC subsets differed between the AIS/TIA, CCD, and HV groups. Several clinical and demographic variables independently predicted the quantity of IC subsets in patients with AIS/TIA. No significant changes in the quantity of IC subsets occurred within the first three days after AIS/TIA. Overall, these findings strengthen the evidence for a pathophysiologic role of IC in human ischemic stroke and the potential use of IC-based biomarkers for the prediction of stroke risk. A comprehensive description of IC kinetics is crucial to enable the design of targeted treatment strategies.
KW  - chronic cerebrovascular disease
KW  - lymphocytes
KW  - leukocytes
KW  - immune cells
KW  - biomarker
KW  - monocytes
KW  - regulatory T cells
KW  - ischemic stroke
KW  - thromboinflammation
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-126319
VL  - 16
IS  - 10
ER  - 
TY  - JOUR
A1  - Fluri, Felix
A1  - Fleischer, Michael
A1  - Kleinschnitz, Christoph
T1  - Accidental Thrombolysis in a Stroke Patient Receiving Apixaban
JF  - Cerebrovascular Diseases Extra
N2  - No abstract available.
KW  - acute management of stroke
KW  - acute ischemic stroke
KW  - acute neurology
KW  - acute stroke imaging
KW  - acute stroke management
KW  - acute stroke outcome
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-126326
VL  - 5
ER  - 
TY  - JOUR
A1  - Üçeyler, Nurcan
A1  - Homola, György A.
A1  - González, Hans Guerrero
A1  - Kramer, Daniela
A1  - Wanner, Christoph
A1  - Weidemann, Frank
A1  - Solymosi, László
A1  - Sommer, Claudia
T1  - Increased Arterial Diameters in the Posterior Cerebral Circulation in Men with Fabry Disease
N2  - A high load of white matter lesions and enlarged basilar arteries have been shown in selected patients with Fabry disease, a disorder associated with an increased stroke risk. We studied a large cohort of patients with Fabry disease to differentially investigate white matter lesion load and cerebral artery diameters. We retrospectively analyzed cranial magnetic resonance imaging scans of 87 consecutive Fabry patients, 20 patients with ischemic stroke, and 36 controls. We determined the white matter lesion load applying the Fazekas score on fluid-attenuated inversion recovery sequences and measured the diameters of cerebral arteries on 3D-reconstructions of the time-of-flight-MR-angiography scans. Data of different Fabry patient subgroups (males – females; normal – impaired renal function) were compared with data of patients with stroke and controls. A history of stroke or transient ischemic attacks was present in 4/30 males (13%) and 5/57 (9%) females with Fabry disease, all in the anterior circulation. Only one man with Fabry disease showed confluent cerebral white matter lesions in the Fazekas score assessment (1%). Male Fabry patients had a larger basilar artery (p<0.01) and posterior cerebral artery diameter (p<0.05) compared to male controls. This was independent of disease severity as measured by renal function and did not lead to changes in arterial blood flow properties. A basilar artery diameter of >3.2 mm distinguished between men with Fabry disease and controls (sensitivity: 87%, specificity: 86%, p<0.001), but not from stroke patients. Enlarged arterial diameters of the posterior circulation are present only in men with Fabry disease independent of disease severity.
KW  - Arterial Diameters
KW  - ischemic stroke
KW  - magnetic resonance imaging
KW  - stroke
KW  - cerebral arteries
KW  - renal system
KW  - central nervous system
KW  - blood flow
KW  - lesions
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-112614
ER  - 
TY  - JOUR
A1  - Üçeyler, Nurcan
A1  - Sommer, Claudia
T1  - High-Dose Capsaicin for the Treatment of Neuropathic Pain: What We Know and What We Need to Know
JF  - Pain and Therapy
N2  - Neuropathic pain is a frequent and disabling condition with diverse underlying etiologies and is often difficult to treat. Systemic drug treatment is often limited in efficacy. Furthermore, adverse effects may be a limiting factor when trying to reach the necessary dose. Analgesics that can be applied topically have the potential to largely overcome this problem. They may be of particular advantage in localized neuropathic pain syndromes such as postherpetic neuralgia or small fiber neuropathy. Capsaicin, the pungent component of chili peppers, is a natural ligand of the transient receptor potential vanilloid 1 channel and has long been used as topically applicable cream with concentrations of 0.025 to 0.075%. In 2009, a high-concentration transdermal capsaicin 8% patch (Qutenza ; Acorda Therapeutics, Inc., Ardsley, NY, USA; Astellas Pharma Europe Ltd., Chertsey, Surrey, UK) was introduced for the treatment of peripheral neuropathic pain syndromes other than of diabetic origin in adults. It has since been widely used in diverse neuropathic pain disorders. In this review article, we summarize current knowledge on Qutenza, its advantages and problems, and expose unmet needs.
KW  - transient receptor potential vanilloid 1 (TRPV1)
KW  - analgesia
KW  - capsaicin
KW  - neuropathic pain
KW  - qutenza
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-120669
SN  - 2193-651X
VL  - 3
IS  - 2
ER  - 
TY  - JOUR
A1  - Niemann, Axel
A1  - Huber, Nina
A1  - Wagner, Konstanze M.
A1  - Somandin, Christian
A1  - Horn, Michael
A1  - Lebrun-Julien, Frédéric
A1  - Angst, Brigitte
A1  - Pereira, Jorge A.
A1  - Halfter, Hartmut
A1  - Welzl, Hans
A1  - Feltri, M. Laura
A1  - Wrabetz, Lawrence
A1  - Young, Peter
A1  - Wessig, Carsten
A1  - Toyka, Klaus V.
A1  - Suter, Ueli
T1  - The Gdap1 knockout mouse mechanistically links redox control to Charcot–Marie–Tooth disease
JF  - Brain
N2  - The ganglioside-induced differentiation-associated protein 1 (GDAP1) is a mitochondrial fission factor and mutations in GDAP1 cause Charcot–Marie–Tooth disease. We found that Gdap1 knockout mice (\(Gdap1^{−/−}\)), mimicking genetic alterations of patients suffering from severe forms of Charcot–Marie–Tooth disease, develop an age-related, hypomyelinating peripheral neuropathy. Ablation of Gdap1 expression in Schwann cells recapitulates this phenotype. Additionally, intra-axonal mitochondria of peripheral neurons are larger in \(Gdap1^{−/−}\) mice and mitochondrial transport is impaired in cultured sensory neurons of \(Gdap1^{−/−}\) mice compared with controls. These changes in mitochondrial morphology and dynamics also influence mitochondrial biogenesis. We demonstrate that mitochondrial DNA biogenesis and content is increased in the peripheral nervous system but not in the central nervous system of \(Gdap1^{−/−}\) mice compared with control littermates. In search for a molecular mechanism we turned to the paralogue of GDAP1, GDAP1L1, which is mainly expressed in the unaffected central nervous system. GDAP1L1 responds to elevated levels of oxidized glutathione by translocating from the cytosol to mitochondria, where it inserts into the mitochondrial outer membrane. This translocation is necessary to substitute for loss of GDAP1 expression. Accordingly, more GDAP1L1 was associated with mitochondria in the spinal cord of aged \(Gdap1^{−/−}\) mice compared with controls. Our findings demonstrate that Charcot–Marie–Tooth disease caused by mutations in GDAP1 leads to mild, persistent oxidative stress in the peripheral nervous system, which can be compensated by GDAP1L1 in the unaffected central nervous system. We conclude that members of the GDAP1 family are responsive and protective against stress associated with increased levels of oxidized glutathione.
KW  - animal models
KW  - Charcot-Marie-Tooth disease
KW  - mitochondria
KW  - axonal transport
KW  - demyelinating disease
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-120731
VL  - 137
IS  - 3
ER  - 
TY  - THES
A1  - Klein, Dennis
T1  - The pathogenic role of endogenous antibodies in a mouse model for Charcot-Marie-Tooth 1B neuropathy
T1  - Die pathogenetische Funktion von endogenen Antikörpern in einem Maus-Modell der Charcot-Marie-Tooth 1B Neuropathie
N2  - Charcot-Marie-Tooth (CMT) type 1 neuropathies are a genetically heterogeneous group of non-treatable inherited disorders affecting the peripheral nervous system that lead to sensory and motor dysfunction. Secondary low grade inflammation, implicating the innate and adaptive immune system, could previously be identified as a substantial disease modifier in two mouse models for CMT1, CMT1B and 1X, respectively. However, the exact mechanism how the adaptive immune system contributes to disease pathogenesis is not completely understood. Based on observations that the accumulation of endogenous antibodies to myelin components is important for rapid myelin clearance after nerve injury during Wallerian degeneration, a possibly similar mechanism was considered for endogenous antibodies as disease amplifier in mice heterozygously deficient for P0 (P0het), mimicking some typical features of CMT1B.
In this study an increased antibody deposition was detected in the affected peripheral nerves of P0het myelin mutant mice. By crossbreeding P0het mutants with mice specifically lacking B-lymphocytes, and therefore antibodies (JHD-/-), a decline of endoneurial macrophages together with a substantially ameliorated demyelination could be demonstrated in 6-month-old mutant mice. Moreover, reconstitution with murine IgGs reverted the neuropathic phenotype, substantiating that endogenous antibodies are potentially pathogenic at this early stage of disease. Unexpectedly, in 12-months-old P0het mutants, JHD deficiency resulted in disease aggravation accompanied by an increased inflammatory reaction and M2-polarized macrophage response.
These observations suggest that in a mouse model for CMT1B, the lack of endogenous antibodies has a dichotomous effect: ameliorating early macrophage-mediated demyelination, as opposed to increasing inflammatory reactions leading to disease aggravation at older ages.
N2  - Als Charcot-Marie-Tooth (CMT) Typ 1 Erkrankungen bezeichnet man eine genetisch heterogene Gruppe von nicht behandelbaren, erblichen Neuropathien, die das periphere Nervensystem betreffen und letztendlich zu starken motorischen und sensorischen Defiziten führen. Anhand verschiedener Studien konnte gezeigt werden, dass sekundäre Entzündungsreaktionen, insbesondere des angeborenen und adaptiven Immunsystems, eine entscheidende Rolle bei der Pathogenese von zwei verschiedenen CMT1-Mausmodellen (CMT1B und CMT1X) spielen. Jedoch ist der genaue Mechanismus, in dem das adaptive Immunsystem zur Pathogenese beiträgt, nicht komplett bekannt. In einer veröffentlichten Studie wurden gebundenen endogenen Antiköpern eine wichtige Rolle beim raschen Myelinabbau nach Nervläsion während der Waller´schen Degeneration zugeschrieben. In Mäusen, die heterozygot defizient für P0 (P0het) sind und einige typische Merkmale der CMT1B Neuropathie aufweisen, sollte ein möglicherweise ähnlicher Mechanismus von endogenen Antikörpern untersucht werden, der zur Verstärkung der Krankheitsentwicklung führt.
In dieser Studie konnte eine vermehrte Antikörperbindung in den betroffenen peripheren Nerven von P0het Myelinmutanten beobachtet werden. Anhand von Verkreuzungs-Experimenten von P0het Mutanten mit Mäusen, die keine B-Lymphozyten besitzen und daher keine Antikörper bilden können (JHD-/-), konnte zudem in den untersuchten 6 Monate alten Doppelmutanten eine verringerte Anzahl endoneuraler Makrophagen und eine deutliche Verbesserung der Demyelinisierung aufgezeigt werden. Zusätzlich konnte anhand von Rekonstitutions-Experimenten mit mausspezifischen-IgGs der neuropathische Phänotyp in peripheren Nerven wiederhergestellt werden, was die mögliche pathogenetische Rolle endogener Antikörper im frühen Stadium der Erkrankung bekräftigt. Unerwarteterweise führte die JHD-Defizienz jedoch in 12 Monate alten P0het Mausmutanten eher zu einer Verschlechterung der Neuropathie, zusammen mit einer verstärkten Entzündungsreaktion und M2-polarisierten Makrophagen-Aktivierung.
Diese Beobachtungen deuten darauf hin, dass das Fehlen von Antikörpern in einem etablierten Mausmodell für CMT1B unterschiedliche Folgen hat, da dies zu einer verringerten Makrophagen-vermittelten Demyelinisierung im frühen Erkrankungsverlauf führt, gleichzeitig aber im späteren Alter in einer verstärkten Entzündungsreaktion und einem vermehrten Nervschaden resultiert.
KW  - Charcot-Marie-Tooth
KW  - Demyelinisierung
KW  - Adaptives Immunsystem
KW  - Antikörper
KW  - Makrophagen
KW  - B-Lymphocyten
KW  - Fc-Rezeptor
KW  - Komplement
KW  - demyelination
KW  - antibodies
KW  - macrophages
KW  - adaptive immune system
KW  - B-lymphocytes
KW  - Fc-receptor
KW  - complement
KW  - Maus
KW  - Charcot-Marie-Syndrom
KW  - Immunsystem
KW  - Antikörper
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-121941
ER  - 
TY  - JOUR
A1  - Albert-Weissenberger, Christiane
A1  - Mencl, Stine
A1  - Schuhmann, Michael K.
A1  - Salur, Irmak
A1  - Göb, Eva
A1  - Langhauser, Friederike
A1  - Hopp, Sarah
A1  - Hennig, Nelli
A1  - Meuth, Sven G.
A1  - Nolte, Marc W.
A1  - Sirén, Anna-Leena
A1  - Kleinschnitz, Christoph
T1  - C1-Inhibitor protects from focal brain trauma in a cortical cryolesion mice model by reducing thrombo-inflammation
JF  - Frontiers in Cellular Neuroscience
N2  - Traumatic brain injury (TBI) induces a strong inflammatory response which includes blood-brain barrier damage, edema formation and infiltration of different immune cell subsets. More recently, microvascular thrombosis has been identified as another pathophysiological feature of TBI. The contact-kinin system represents an interface between inflammatory and thrombotic circuits and is activated in different neurological diseases. C1-Inhibitor counteracts activation of the contact-kinin system at multiple levels. We investigated the therapeutic potential of C1-Inhibitor in a model of TBI. Male and female C57BL/6 mice were subjected to cortical cryolesion and treated with C1-Inhibitor after 1 h. Lesion volumes were assessed between day 1 and day 5 and blood-brain barrier damage, thrombus formation as well as the local inflammatory response were determined post TBI. Treatment of male mice with 15.0 IU C1-Inhibitor, but not 7.5 IU, 1 h after cryolesion reduced lesion volumes by ~75% on day 1. This protective effect was preserved in female mice and at later stages of trauma. Mechanistically, C1-Inhibitor stabilized the blood-brain barrier and decreased the invasion of immune cells into the brain parenchyma. Moreover, C1-Inhibitor had strong antithrombotic effects. C1-Inhibitor represents a multifaceted anti-inflammatory and antithrombotic compound that prevents traumatic neurodegeneration in clinically meaningful settings.
KW  - thrombosis
KW  - traumatic brain injury
KW  - C1-inhibitor
KW  - blood-brain barrier
KW  - contact-kinin system
KW  - edema
KW  - inflammation
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-119263
SN  - 1662-5102
VL  - 8
ER  - 
TY  - JOUR
A1  - Mencacci, Niccoló E.
A1  - Isaias, Ioannis U.
A1  - Reich, Martin M.
A1  - Ganos, Christos
A1  - Plagnol, Vincent
A1  - Polke, James M.
A1  - Bras, Jose
A1  - Hersheson, Joshua
A1  - Stamelou, Maria
A1  - Pittman, Alan M.
A1  - Noyce, Alastair J.
A1  - Mok, Kin Y.
A1  - Opladen, Thomas
A1  - Kunstmann, Erdmute
A1  - Hodecker, Sybille
A1  - Münchau, Alexander
A1  - Volkmann, Jens
A1  - Samnick, Samuel
A1  - Sidle, Katie
A1  - Nanji, Tina
A1  - Sweeney, Mary G.
A1  - Houlden, Henry
A1  - Batla, Amit
A1  - Zecchinelli, Anna L.
A1  - Pezzoli, Gianni
A1  - Marotta, Giorgio
A1  - Lees, Andrew
A1  - Alegria, Paulo
A1  - Krack, Paul
A1  - Cormier-Dequaire, Florence
A1  - Lesage, Suzanne
A1  - Brice, Alexis
A1  - Heutink, Peter
A1  - Gasser, Thomas
A1  - Lubbe, Steven J.
A1  - Morris, Huw R.
A1  - Taba, Pille
A1  - Koks, Sulev
A1  - Majounie, Elisa
A1  - Gibbs, J. Raphael
A1  - Singleton, Andrew
A1  - Hardy, John
A1  - Klebe, Stephan
A1  - Bhatia, Kailash P.
A1  - Wood, Nicholas W.
T1  - Parkinson’s disease in GTP cyclohydrolase 1 mutation carriers
JF  - Brain
N2  - GTP cyclohydrolase 1, encoded by the GCH1 gene, is an essential enzyme for dopamine production in nigrostriatal cells. Loss-of-function mutations in GCH1 result in severe reduction of dopamine synthesis in nigrostriatal cells and are the most common cause of DOPA-responsive dystonia, a rare disease that classically presents in childhood with generalized dystonia and a dramatic long-lasting response to levodopa. We describe clinical, genetic and nigrostriatal dopaminergic imaging ([(123)I]N-ω-fluoropropyl-2β-carbomethoxy-3β-(4-iodophenyl) tropane single photon computed tomography) findings of four unrelated pedigrees with DOPA-responsive dystonia in which pathogenic GCH1 variants were identified in family members with adult-onset parkinsonism. Dopamine transporter imaging was abnormal in all parkinsonian patients, indicating Parkinson's disease-like nigrostriatal dopaminergic denervation. We subsequently explored the possibility that pathogenic GCH1 variants could contribute to the risk of developing Parkinson's disease, even in the absence of a family history for DOPA-responsive dystonia. The frequency of GCH1 variants was evaluated in whole-exome sequencing data of 1318 cases with Parkinson's disease and 5935 control subjects. Combining cases and controls, we identified a total of 11 different heterozygous GCH1 variants, all at low frequency. This list includes four pathogenic variants previously associated with DOPA-responsive dystonia (Q110X, V204I, K224R and M230I) and seven of undetermined clinical relevance (Q110E, T112A, A120S, D134G, I154V, R198Q and G217V). The frequency of GCH1 variants was significantly higher (Fisher's exact test P-value 0.0001) in cases (10/1318 = 0.75%) than in controls (6/5935 = 0.1%; odds ratio 7.5; 95% confidence interval 2.4-25.3). Our results show that rare GCH1 variants are associated with an increased risk for Parkinson's disease. These findings expand the clinical and biological relevance of GTP cycloydrolase 1 deficiency, suggesting that it not only leads to biochemical striatal dopamine depletion and DOPA-responsive dystonia, but also predisposes to nigrostriatal cell loss. Further insight into GCH1-associated pathogenetic mechanisms will shed light on the role of dopamine metabolism in nigral degeneration and Parkinson's disease.
KW  - DOPA-responsive-dystonia
KW  - GCH1
KW  - Parkinson's disease
KW  - dopamine
KW  - exome sequencing
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-121268
VL  - 137
IS  - 9
ER  - 
TY  - JOUR
A1  - Hohnmann, Christopher
A1  - Milles, Bianca
A1  - Schinke, Michael
A1  - Schroeter, Michael
A1  - Ulzheimer, Jochen
A1  - Kraft, Peter
A1  - Kleinschnitz, Christoph
A1  - Lehmann, Paul V.
A1  - Kuerten, Stefanie
T1  - Categorization of multiple sclerosis relapse subtypes by B cell profiling in the blood
JF  - Acta Neuropathologica Communications
N2  - Introduction
B cells are attracting increasing attention in the pathogenesis of multiple sclerosis (MS). B cell-targeted therapies with monoclonal antibodies or plasmapheresis have been shown to be successful in a subset of patients. Here, patients with either relapsing-remitting (n = 24) or secondary progressive (n = 6) MS presenting with an acute clinical relapse were screened for their B cell reactivity to brain antigens and were re-tested three to nine months later. Enzyme-linked immunospot technique (ELISPOT) was used to identify brain-reactive B cells in peripheral blood mononuclear cells (PBMC) directly ex vivo and after 96 h of polyclonal stimulation. Clinical severity of symptoms was determined using the Expanded Disability Status Scale (EDSS).

Results
Nine patients displayed B cells in the blood producing brain-specific antibodies directly ex vivo. Six patients were classified as B cell positive donors only after polyclonal B cell stimulation. In 15 patients a B cell response to brain antigens was absent. Based on the autoreactive B cell response we categorized MS relapses into three different patterns. Patients who displayed brain-reactive B cell responses both directly ex vivo and after polyclonal stimulation (pattern I) were significantly younger than patients in whom only memory B cell responses were detectable or entirely absent (patterns II and III; p = 0.003). In one patient a conversion to a positive B cell response as measured directly ex vivo and subsequently also after polyclonal stimulation was associated with the development of a clinical relapse. The evaluation of the predictive value of a brain antigen-specific B cell response showed that seven of eight patients (87.5%) with a pattern I response encountered a clinical relapse during the observation period of 10 months, compared to two of five patients (40%) with a pattern II and three of 14 patients (21.4%) with a pattern III response (p = 0.0005; hazard ratio 6.08 (95% confidence interval 1.87-19.77).

Conclusions
Our data indicate actively ongoing B cell-mediated immunity against brain antigens in a subset of MS patients that may be causative of clinical relapses and provide new diagnostic and therapeutic options for a subset of patients.
KW  - predictive value
KW  - MS
KW  - ELISPOT
KW  - B cells
KW  - relapse
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-126124
VL  - 2
IS  - 138
ER  - 
TY  - JOUR
A1  - Doppler, Kathrin
A1  - Appeltshauser, Luise
A1  - Krämer, Heidrun H.
A1  - King Man Ng, Judy
A1  - Meinl, Edgar
A1  - Villmann, Carmen
A1  - Brophy, Peter
A1  - Dib-Hajj, Sulayman D.
A1  - Waxman, Stephen G.
A1  - Weishaupt, Andreas
A1  - Sommer, Claudia
T1  - Contactin-1 and Neurofascin-155/-186 Are Not Targets of Auto-Antibodies in Multifocal Motor Neuropathy
JF  - PLoS One
N2  - Multifocal motor neuropathy is an immune mediated disease presenting with multifocal muscle weakness and conduction block. IgM auto-antibodies against the ganglioside GM1 are detectable in about 50% of the patients. Auto-antibodies against the paranodal proteins contactin-1 and neurofascin-155 and the nodal protein neurofascin-186 have been detected in subgroups of patients with chronic inflammatory demyelinating polyneuropathy. Recently, auto-antibodies against neurofascin-186 and gliomedin were described in more than 60% of patients with multifocal motor neuropathy. In the current study, we aimed to validate this finding, using a combination of different assays for auto-antibody detection. In addition we intended to detect further auto-antibodies against paranodal proteins, specifically contactin-1 and neurofascin-155 in multifocal motor neuropathy patients’ sera. We analyzed sera of 33 patients with well-characterized multifocal motor neuropathy for IgM or IgG anti-contactin-1, anti-neurofascin-155 or -186 antibodies using enzyme-linked immunosorbent assay, binding assays with transfected human embryonic kidney 293 cells and murine teased fibers. We did not detect any IgM or IgG auto-antibodies against contactin-1, neurofascin-155 or -186 in any of our multifocal motor neuropathy patients. We conclude that auto-antibodies against contactin-1, neurofascin-155 and -186 do not play a relevant role in the pathogenesis in this cohort with multifocal motor neuropathy.
KW  - motor proteins
KW  - enzyme-linked immunoassays
KW  - binding analysis
KW  - neuropathy
KW  - nerve fibers
KW  - cell binding assay
KW  - antibodies
KW  - enzyme assays
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-126156
VL  - 10
IS  - 7
ER  - 
TY  - THES
A1  - Ebert, Sönke
T1  - Small- und Large-fiber-Beteiligung bei Morbus Parkinson
T1  - Small- and large-fiber-neuropathy in Parkinson's disease
N2  - Die hier vorliegende Forschungsarbeit überprüfte eine mögliche Beteiligung des peripheren Nervensystems bei M. Parkinson und den atypischen Parkinson-Syndromen. 31 Patienten mit einem idiopathischen Parkinson-Syndrom (IPD-Patienten) und neun Patienten mit einem atypischen Parkinson-Syndrom (APD-Patienten) sowie 35 altersentsprechende Kontrollprobanden wurden zwischen 2011 und 2012 für diese Studie rekrutiert. Neben der Eigenanamnese und der neurologischen Untersuchung erhielten die Patienten eine Suralisneurographie zur Überprüfung der large fibers und eine Quantitative sensorische Testung (QST) zur Detektion einer möglichen Small-fiber-Dysfunktion. Die Vitamin-Bestimmung diente der Untersuchung möglicher Zusammenhänge zwischen der Levodopa-Therapie, eventuell daraus resultierenden Vitamin-Mangelzuständen und einer reduzierten intraepidermalen Nervenfaser-Dichte (IENF-Dichte) beim M. Parkinson. Für die histologische Auswertung der IENF-Dichte und der dermalen, myelinisierten Nervenfaserbündel (PGP 9.5- / MBP- Doppelfärbung) sowie für die immunohistochemische Untersuchung der Nervenfasersubtypen (anti-alpha-CGRP- und anti-Substanz P-Antikörper) wurden bei jedem Probanden vier Hautbiopsien von den Extremitäten und dem Körperstamm entnommen. 
Sieben IPD-Patienten und ein Proband mit einem atypischen Parkinson-Syndrom wiesen ein vermindertes sensorisches Nervenaktionspotenzial (SNAP) in der Suralisneurographie auf. Dagegen war eine pathologisch reduzierte Nervenleitgeschwindigkeit nur bei einem IPD-Patienten nachweisbar. Auffällig war zudem eine negative Korrelation zwischen der Erkrankungsdauer und dem SNAP (Korrelationskoeffizient -0,367, p<0,03). In der Auswertung der Hautbiopsien konnte eine statistisch signifikante Reduktion der myelinisierten Bündel am Unterschenkel der IPD-Patienten festgestellt werden. 
Bei zehn von 30 IPD-Patienten, jedoch bei keinem der Probanden mit einem atypischen Parkinson-Syndrom, konnte eine verminderte IENF-Dichte nachgewiesen werden. In der statistischen Überprüfung wurde außerdem am Unterschenkel ein signifikanter Unterschied zwischen den IPD-Patienten und der Kontrollkohorte sowie eine negative Korrelation zwischen der Krankheitsdauer und der IENF-Dichte (Korrelationskoeffizient -0,320, p<0,05) festgestellt. Die QST konnte dagegen keinen statistisch signifikanten Unterschied zwischen den einzelnen Kohorten aufzeigen. 
Im Kontrast dazu fand sich eine längenunabhängige Reduktion der CGRP-positiven und der Substanz P-positiven IENF-Dichte bei den Patienten mit einem idiopathischen Parkinson-Syndrom. Bemerkenswert war zudem eine signifikante Verminderung der Substanz P-positiven intraepidermalen Nervenfasern am Oberschenkel und Rücken bei den APD-Patienten. Eine statistisch signifikante Abweichung der CGRP- und Substanz P-positiven Bündel konnte dagegen nicht festgestellt werden. 
In der laborchemischen Untersuchung war ein Zusammenhang zwischen den bestimmten Vitamin-Spiegeln und der kumulativen Levodopa-Dosis sowie zwischen den Vitaminen und der IENF-Dichte lediglich bei dem Vitamin B6 nachweisbar. 
Zusammengefasst erscheint eine Beteiligung des peripheren Nervensystems beim idiopathischen Parkinson als wahrscheinlich, wohingegen bei den atypischen Parkinson-Syndromen vor allem von einer zentralen Genese ausgegangen werden kann. Basierend auf den Ergebnissen der Suralisneurographie und der Bestimmung der myelinisierten Bündel erscheint eine krankheitsbedingte Large-fiber-Beeinträchtigung beim M.Parkinson möglich. Die nachgewiesene längenabhängige Small-fiber-Reduktion bei IPD-Patienten wird vermutlich durch eine axonale Transportstörung verursacht. Einen krankheitsbedingten Erklärungsansatz für die längenunabhängige Reduktion der CGRP-positiven und der Substanz P-positiven IENF-Dichte bei IPD-Patienten liefert der Nachweis von neurotoxischem α-Synuclein in den sensiblen Spinatganglien mit einem daraus resultierenden Untergang von sensorischen Nervenfasern. Aufgrund der geringen Anzahl an Parkinson-Patienten mit sensiblen Symptomen und dem fehlenden Nachweis eines statistisch signifikanten Unterschiedes in der QST liegt der Verdacht nahe, dass die ermittelte intraepidermale Nervenfaserreduktion der IPD-Patienten nicht stark genug ausgeprägt ist, um eine signifikante Abweichung der QST-Ergebnisse zu verursachen. Weiterhin konnte kein Zusammenhang zwischen der kumulativen Levodopa-Menge, den Vitaminen B12, Methylmalonsäure sowie Homocystein und dem Auftreten einer Nervenfaserverminderung nachgewiesen werden, was gegen eine iatrogene Beteiligung des peripheren Nervensystems als Nebenwirkung der Levodopa-Therapie spricht. Das idiopathische Parkinson-Syndrom geht mit einer Reduktion der kleinen Nervenfasern einher, welche vermutlich auf die Grunderkrankung selbst zurückzuführen ist. Die Untersuchung der Haut erscheint somit vielversprechend für die Erforschung der Pathogenese und für die Differentialdiagnostik des M. Parkinson.
N2  - Small- and large-fiber-neuropathy in Parkinson's disease
KW  - Parkinson-Krankheit
KW  - Parkinson
KW  - Nervenfaser
KW  - Biopsie
KW  - Fluoreszenzmikroskopie
KW  - Hautbiopsie
KW  - Quantitative Sensorische Testung
KW  - Suralisneurographie
KW  - Neuropathie
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-124647
ER  - 
TY  - JOUR
A1  - Langhauser, Friederike L.
A1  - Heiler, Patrick M.
A1  - Grudzenski, Saskia
A1  - Lemke, Andreas
A1  - Alonso, Angelika
A1  - Schad, Lothar R.
A1  - Hennerici, Michael G.
A1  - Meairs, Stephen
A1  - Fata, Marc
T1  - Thromboembolic stroke in C57BL/6 mice monitored by 9.4 T MRI using a 1H cryo probe
JF  - Experimental and Translational Stroke Medicine
N2  - Background
A new thromboembolic animal model showed beneficial effects of t-PA with an infarct volume reduction of 36.8% in swiss mice. Because knock-out animal experiments for stroke frequently used C57BL76 mice we evaluated t-PA effects in this mouse strain and measured infarct volume and vascular recanalisation in-vivo by using high-field 9.4 T MRI and a 1H surface cryo coil.
Methods
Clot formation was triggered by microinjection of murine thrombin into the right middle cerebral artery (MCA). Animals (n = 28) were treated with 10 mg/kg, 5 mg/kg or no tissue plasminogen activator (t-PA) 40 min after MCA occlusion. For MR-imaging a Bruker 9.4 T animal system with a 1H surface cryo probe was used and a T2-weighted RARE sequence, a diffusion weighted multishot EPI sequence and a 3D flow-compensated gradient echo TOF angiography were performed.
Results
The infarct volume in animals treated with t-PA was significantly reduced (0.67 ± 1.38 mm3 for 10 mg/kg and 10.9 ± 8.79 mm3 for 5 mg/kg vs. 19.76 ± 2.72 mm3 ; p < 0.001) compared to untreated mice. An additional group was reperfused with t-PA inside the MRI. Already ten minutes after beginning of t-PA treatment, reperfusion flow was re-established in the right MCA. However, signal intensity was lower than in the contralateral MCA. This reduction in cerebral blood flow was attenuated during the first 60 minutes after reperfusion. 24 h after MCA occlusion and reperfusion, no difference in signal intensity of the contralateral and ipsilateral MCAs was observed.
Conclusions
We confirm a t-Pa effect using this stroke model in the C57BL76 mouse strain and demonstrate a chronological sequence MRI imaging after t-PA using a 1H surface cryo coil in a 9.4 T MRI. This setting will allow testing of new thrombolytic strategies for stroke treatment in-vivo in C57BL76 knock-out mice.
KW  - animal models
KW  - MRI
KW  - experimental
KW  - embolic stroke
KW  - T-PA
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-124218
VL  - 4
IS  - 18
ER  - 
TY  - JOUR
A1  - Üçeyler, Nurcan
A1  - Kewenig, Susanne
A1  - Kittel-Schneider, Sarah
A1  - Fallgatter, Andreas J.
A1  - Sommer, Claudia
T1  - Increased cortical activation upon painful stimulation in fibromyalgia syndrome
JF  - BMC Neurology
N2  - Background
Fibromyalgia syndrome (FMS) is a chronic condition characterized by widespread pain and associated symptoms. We investigated cerebral activation in FMS patients by functional near-infrared spectroscopy (fNIRS).

Methods
Two stimulation paradigms were applied: a) painful pressure stimulation at the dorsal forearm; b) verbal fluency test (VFT). We prospectively recruited 25 FMS patients, ten patients with unipolar major depression (MD) without pain, and 35 healthy controls. All patients underwent neurological examination and all subjects were investigated with questionnaires (pain, depression, FMS, empathy).

Results
FMS patients had lower pressure pain thresholds than patients with MD and controls (p < 0.001) and reported higher pain intensity (p < 0.001). Upon unilateral pressure pain stimulation fNIRS recordings revealed increased bilateral cortical activation in FMS patients compared to controls (p < 0.05). FMS patients also displayed a stronger contralateral activity over the dorsolateral prefrontal cortex in direct comparison to patients with MD (p < 0.05). While all three groups performed equally well in the VFT, a frontal deficit in cortical activation was only found in patients with depression (p < 0.05). Performance and cortical activation correlated negatively in FMS patients (p < 0.05) and positively in patients with MD (p < 0.05).

Conclusion
Our data give further evidence for altered central nervous processing in patients with FMS and the distinction between FMS and MD.
KW  - fibromyalgia syndrome
KW  - depression
KW  - cortical activation
KW  - pain
KW  - near-infrared spectroscopy
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-125230
VL  - 15
IS  - 210
ER  - 
TY  - JOUR
A1  - Horn, Michael
A1  - Baumann, Reto
A1  - Pereira, Jorge A.
A1  - Sidiropoulos, Páris N. M.
A1  - Somandin, Christian
A1  - Welzl, Hans
A1  - Stendel, Claudia
A1  - Lühmann, Tessa
A1  - Wessig, Carsten
A1  - Toyka, Klaus V.
A1  - Relvas, João B.
A1  - Senderek, Jan
A1  - Suter, Ueli
T1  - Myelin is dependent on the Charcot–Marie–Tooth Type 4H disease culprit protein FRABIN/FGD4 in Schwann cells
JF  - Brain
N2  - Studying the function and malfunction of genes and proteins associated with inherited forms of peripheral neuropathies has provided multiple clues to our understanding of myelinated nerves in health and disease. Here, we have generated a mouse model for the peripheral neuropathy Charcot–Marie–Tooth disease type 4H by constitutively disrupting the mouse orthologue of the suspected culprit gene FGD4 that encodes the small RhoGTPase Cdc42-guanine nucleotide exchange factor Frabin. Lack of Frabin/Fgd4 causes dysmyelination in mice in early peripheral nerve development, followed by profound myelin abnormalities and demyelination at later stages. At the age of 60 weeks, this was accompanied by electrophysiological deficits. By crossing mice carrying alleles of Frabin/Fgd4 flanked by loxP sequences with animals expressing Cre recombinase in a cell type-specific manner, we show that Schwann cell-autonomous Frabin/Fgd4 function is essential for proper myelination without detectable primary contributions from neurons. Deletion of Frabin/Fgd4 in Schwann cells of fully myelinated nerve fibres revealed that this protein is not only required for correct nerve development but also for accurate myelin maintenance. Moreover, we established that correct activation of Cdc42 is dependent on Frabin/Fgd4 function in healthy peripheral nerves. Genetic disruption of Cdc42 in Schwann cells of adult myelinated nerves resulted in myelin alterations similar to those observed in Frabin/Fgd4-deficient mice, indicating that Cdc42 and the Frabin/Fgd4–Cdc42 axis are critical for myelin homeostasis. In line with known regulatory roles of Cdc42, we found that Frabin/Fgd4 regulates Schwann cell endocytosis, a process that is increasingly recognized as a relevant mechanism in peripheral nerve pathophysiology. Taken together, our results indicate that regulation of Cdc42 by Frabin/Fgd4 in Schwann cells is critical for the structure and function of the peripheral nervous system. In particular, this regulatory link is continuously required in adult fully myelinated nerve fibres. Thus, mechanisms regulated by Frabin/Fgd4–Cdc42 are promising targets that can help to identify additional regulators of myelin development and homeostasis, which may crucially contribute also to malfunctions in different types of peripheral neuropathies.
KW  - Frabin/Fgd4
KW  - myelination
KW  - hereditary motor and sensory neuropathy
KW  - Charcot–Marie–Tooth disease
KW  - Rho-GTPase Cdc42
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-125390
VL  - 135
ER  - 
TY  - JOUR
A1  - Walter, Maggie C.
A1  - Reilich, Peter
A1  - Thiele, Simone
A1  - Schessl, Joachim
A1  - Schreiber, Herbert
A1  - Reiners, Karlheinz
A1  - Kress, Wolfram
A1  - Müller-Reible, Clemens
A1  - Vorgerd, Matthias
A1  - Urban, Peter
A1  - Schrank, Bertold
A1  - Deschauer, Marcus
A1  - Schlotter-Weigel, Beate
A1  - Kohnen, Ralf
A1  - Lochmüller, Hans
T1  - Treatment of dysferlinopathy with deflazacort: a double-blind, placebo-controlled clinical trial
JF  - Orphanet Journal of Rare Diseases
N2  - Background: Dysferlinopathies are autosomal recessive disorders caused by mutations in the dysferlin (DYSF) gene encoding the dysferlin protein. DYSF mutations lead to a wide range of muscular phenotypes, with the most prominent being Miyoshi myopathy (MM) and limb girdle muscular dystrophy type 2B (LGMD2B). 
Methods: We assessed the one-year-natural course of dysferlinopathy, and the safety and efficacy of deflazacort treatment in a double-blind, placebo-controlled cross-over trial. After one year of natural course without intervention, 25 patients with genetically defined dysferlinopathy were randomized to receive deflazacort and placebo for six months each (1 mg/kg/day in month one, 1 mg/kg every 2nd day during months two to six) in one of two treatment sequences. Results: During one year of natural course, muscle strength declined about 2% as measured by CIDD (Clinical Investigation of Duchenne Dystrophy) score, and 76 Newton as measured by hand-held dynamometry. Deflazacort did not improve muscle strength. In contrast, there is a trend of worsening muscle strength under deflazacort treatment, which recovers after discontinuation of the study drug. During deflazacort treatment, patients showed a broad spectrum of steroid side effects. 
Conclusion: Deflazacort is not an effective therapy for dysferlinopathies, and off-label use is not warranted. This is an important finding, since steroid treatment should not be administered in patients with dysferlinopathy, who may be often misdiagnosed as polymyositis.
KW  - Deflazacort
KW  - muscle strength
KW  - gridle muscular-dystrophy
KW  - Duchenne dystrphy
KW  - Miyoshi myopathy
KW  - mutation
KW  - prednisone
KW  - gene
KW  - 2B
KW  - children
KW  - design
KW  - steroids
KW  - therapy
KW  - dysferlinopathy
KW  - Limb girdle muscular dystrophy (LGMD)
Y1  - 2013
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-125663
SN  - 1750-1172
VL  - 8
IS  - 26
ER  - 
TY  - JOUR
A1  - Karle, Kathrin N.
A1  - Schüle, Rebecca
A1  - Klebe, Stephan
A1  - Otto, Susanne
A1  - Frischholz, Christian
A1  - Liepelt-Scarfone, Inga
A1  - Schöls, Ludger
T1  - Electrophysiological characterisation of motor and sensory tracts in patients with hereditary spastic paraplegia (HSP)
JF  - Orphanet Journal of Rare Diseases
N2  - Background: Hereditary spastic paraplegias (HSPs) are characterised by lower limb spasticity due to degeneration of the corticospinal tract. We set out for an electrophysiological characterisation of motor and sensory tracts in patients with HSP. 
Methods: We clinically and electrophysiologically examined a cohort of 128 patients with genetically confirmed or clinically probable HSP. Motor evoked potentials (MEPs) to arms and legs, somato-sensory evoked potentials of median and tibial nerves, and nerve conduction studies of tibial, ulnar, sural, and radial nerves were assessed. 
Results: Whereas all patients showed clinical signs of spastic paraparesis, MEPs were normal in 27% of patients and revealed a broad spectrum with axonal or demyelinating features in the others. This heterogeneity can at least in part be explained by different underlying genotypes, hinting for distinct pathomechanisms in HSP subtypes. In the largest subgroup, SPG4, an axonal type of damage was evident. Comprehensive electrophysiological testing disclosed a more widespread affection of long fibre tracts involving peripheral nerves and the sensory system in 40%, respectively. Electrophysiological abnormalities correlated with the severity of clinical symptoms. 
Conclusions: Whereas HSP is primarily considered as an upper motoneuron disorder, our data suggest a more widespread affection of motor and sensory tracts in the central and peripheral nervous system as a common finding in HSP. The distribution patterns of electrophysiological abnormalities were associated with distinct HSP genotypes and could reflect different underlying pathomechanisms. Electrophysiological measures are independent of symptomatic treatment and may therefore serve as a reliable biomarker in upcoming HSP trials.
KW  - motor evoked potential (MEP)
KW  - amyotrophic-lateral-sclerosis
KW  - somatosensory-evoked-potentials
KW  - Silver-syndrome
KW  - gene mutations
KW  - SPG4
KW  - mouse model
KW  - ALSIN gene
KW  - neuropathy
KW  - paraparesis
KW  - protein
KW  - electrophysiology
KW  - hereditary spastic paraplegia (HSP)
Y1  - 2013
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-124763
SN  - 1750-1172
VL  - 8
IS  - 158
ER  - 
TY  - JOUR
A1  - Hansen, Niels
A1  - Kahn, Ann-Kathrin
A1  - Zeller, Daniel
A1  - Katsarava, Zaza
A1  - Sommer, Claudia
A1  - Üçeyler, Nurcan
T1  - Amplitudes of pain-related evoked potentials are useful to detect small fiber involvement in painful mixed fiber neuropathies in addition to quantitative sensory testing – an electrophysiological study
JF  - Frontiers in Neurology
N2  - To investigate the usefulness of pain-related evoked potentials (PREP) elicited by electrical stimulation for the identification of small fiber involvement in patients with mixed fiber neuropathy (MFN). Eleven MFN patients with clinical signs of large fiber impairment and neuropathic pain and ten healthy controls underwent clinical and electrophysiological evaluation. Small fiber function, electrical conductivity and morphology were examined by quantitative sensory testing (QST), PREP, and skin punch biopsy. MFN was diagnosed following clinical and electrophysiological examination (chronic inflammatory demyelinating neuropathy: n = 6; vasculitic neuropathy: n = 3; chronic axonal ­neuropathy: n = 2). The majority of patients with MFN characterized their pain by descriptors that mainly represent C-fiber-mediated pain. In QST, patients displayed elevated cold, warm, mechanical, and vibration detection thresholds and cold pain thresholds indicative of MFN. PREP amplitudes in patients correlated with cold (p < 0.05) and warm detection thresholds (p < 0.05). Burning pain and the presence of par-/dysesthesias correlated negatively with PREP amplitudes (p < 0.05). PREP amplitudes correlating with cold and warm detection thresholds, burning pain, and par-/dysesthesias support employing PREP amplitudes as an additional tool in conjunction with QST for detecting small fiber impairment in patients with MFN.
KW  - burning pain
KW  - quantitative sensory testing
KW  - mixed fiber neuropathy
KW  - pain-related evoked potentials
KW  - Aδ- and C-fibers
KW  - neuropathic pain
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-124824
VL  - 6
ER  - 
TY  - JOUR
A1  - Westermaier, Thomas
A1  - Koehler, Stefan
A1  - Linsenmann, Thomas
A1  - Kinderlen, Michael
A1  - Pakos, Paul
A1  - Ernestus, Ralf-Ingo
T1  - Intraoperative Myelography in Cervical Multilevel Stenosis Using 3D Rotational Fluoroscopy: Assessment of Feasibility and Image Quality
JF  - Radiology Research and Practice
N2  - Background. Intraoperative myelography has been reported for decompression control in multilevel lumbar disease. Cervical myelography is technically more challenging. Modern 3D fluoroscopy may provide a new opportunity supplying multiplanar images. This study was performed to determine the feasibility and image quality of intraoperative cervical myelography using a 3D fluoroscope. Methods. The series included 9 patients with multilevel cervical stenosis. After decompression, 10 mL of water-soluble contrast agent was administered via a lumbar drainage and the operating table was tilted. Thereafter, a 3D fluoroscopy scan (O-Arm) was performed and visually evaluated. Findings. The quality of multiplanar images was sufficient to supply information about the presence of residual stenosis. After instrumentation, metal artifacts lowered image quality. In 3 cases, decompression was continued because myelography depicted residual stenosis. In one case, anterior corpectomy was not completed because myelography showed sufficient decompression after 2-level discectomy. Interpretation. Intraoperative myelography using 3D rotational fluoroscopy is useful for the control of surgical decompression in multilevel spinal stenosis providing images comparable to postmyelographic CT. The long duration of contrast delivery into the cervical spine may be solved by preoperative contrast administration. The method is susceptible to metal artifacts and, therefore, should be applied before metal implants are placed.
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-125779
VL  - 2015
ER  - 
TY  - JOUR
A1  - Klein, Dennis
A1  - Groh, Janos
A1  - Weishaupt, Andreas
A1  - Martini, Rudolf
T1  - Endogenous antibodies contribute to macrophage-mediated demyelination in a mouse model for CMT1B
JF  - Journal of Neuroinflammation
N2  - Background
We could previously identify components of both the innate and the adaptive immune system as disease modifiers in the pathogenesis of models for Charcot-Marie-Tooth (CMT) neuropathies type 1B and 1X. As part of the adaptive immune system, here we investigated the role of antibodies in a model for CMT1B.

Methods
Antibodies were localized and characterized in peripheral nerves of the CMT1B model by immunohistochemistry and Western blot analysis. Experimental ablation of antibodies was performed by cross breeding the CMT1B models with mutants deficient in B-lymphocytes (JHD−/− mutants). Ameliorated demyelination by antibody deficiency was reverted by intravenous injection of mouse IgG fractions. Histopathological analysis was performed by immunocytochemistry and light and quantitative electron microscopy.

Results
We demonstrate that in peripheral nerves of a mouse model for CMT1B, endogenous antibodies strongly decorate endoneurial tubes of peripheral nerves. These antibodies comprise IgG and IgM subtypes and are preferentially, but not exclusively, associated with nerve fiber aspects nearby the nodes of Ranvier. In the absence of antibodies, the early demyelinating phenotype is substantially ameliorated. Reverting the neuropathy by reconstitution with murine IgG fractions identified accumulating antibodies as potentially pathogenic at this early stage of disease.

Conclusions
Our study demonstrates that in a mouse model for CMT1B, endogenous antibodies contribute to early macrophage-mediated demyelination and disease progression. Thus, both the innate and adaptive immune system are mutually interconnected in a genetic model for demyelination. Since in Wallerian degeneration antibodies have also been shown to be involved in myelin phagocytosis, our study supports our view that inherited demyelination and Wallerian degeneration share common mechanisms, which are detrimental when activated under nonlesion conditions.
KW  - adaptive immune system
KW  - macrophages
KW  - antibodies
KW  - demyelination
KW  - Charcot-Marie-Tooth
KW  - B-lymphocytes
KW  - Fc-receptor
KW  - complement
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-125036
VL  - 12
IS  - 49
ER  - 
TY  - JOUR
A1  - Kleinschnitz, Christoph
A1  - Linker, Ralf A.
A1  - Magnus, Tim
A1  - Korn, Thomas
A1  - Meuth, Sven G.
T1  - Report on the 6th scientific meeting of the “Verein zur Förderung des Wissenschaftlichen Nachwuchses in der Neurologie” (NEUROWIND e.V.) held in Motzen, Germany, Oct. 31th – Nov. 2nd, 2014
JF  - Experimental & Translational Stroke Medicine
N2  - From October 31th – November 2nd, 2014, the 6th NEUROWIND e.V. meeting was held in Motzen, Brandenburg, Germany. 70 doctoral students and postdocs from over 25 different groups working in German and Swiss university hospitals or research institutes attended the meeting to discuss their latest experiments and findings in the fields of neuroimmunology, neurodegeneration and neurovascular research. The meeting was regarded as a very well organized platform to support research of young investigators in Germany and all participants enjoyed the stimulating environment for lively in depth discussions.

According to the major aim of NEUROWIND e.V. to support younger researchers in Germany the 4th NEUROWIND YOUNG SCIENTIST AWARD for experimental neurology was awarded to Michael Breckwoldt on his work in the group of Thomas Misgeld (Institute of Neuronal Cell Biology, Technische Universität München, Germany). The successful project was published in Nature Medicine entitled “Multiparametric optical analysis of mitochondrial redox signals during neuronal physiology and pathology in vivo”. This outstanding paper deals with a molecular imaging approach in living mice to optically analyze the role of mitochondrial redox signals in axons in health and disease. The award is endowed with 20.000 Euro sponsored by Merck Serono GmbH, Darmstadt, Germany (unrestricted educational grant).

This year’s keynote lecture was given by Bernhard Hemmer, Head of the Department of Neurology at the Klinikum rechts der Isar, Technische Universität München. Dr. Hemmer highlighted the particular role of B cells and (auto)antibodies in multiple sclerosis (MS). As a new highlight Dr. Urbahns, head of global discovery technologies at Merck research laboratories, gave insights from research practice in the pharmaceutical industry and introduced a shift in the view on present-day drug discovery paradigms.
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-125049
VL  - 7
IS  - 1
ER  - 
TY  - JOUR
A1  - Albert-Weissenberger, Christiane
A1  - Stetter, Christian
A1  - Meuth, Sven G.
A1  - Göbel, Kerstin
A1  - Bader, Michael
A1  - Sirén, Anna-Leena
A1  - Kleinschnitz, Christoph
T1  - Blocking of Bradykinin Receptor B1 Protects from Focal Closed Head Injury in Mice by Reducing Axonal Damage and Astroglia Activation
JF  - Journal of Cerebral Blood Flow and Metabolism
N2  - The two bradykinin receptors B1R and B2R are central components of the kallikrein–kinin system with different expression kinetics and binding characteristics. Activation of these receptors by kinins triggers inflammatory responses in the target organ and in most situations enhances tissue damage. We could recently show that blocking of B1R, but not B2R, protects from cortical cryolesion by reducing inflammation and edema formation. In the present study, we investigated the role of B1R and B2R in a closed head model of focal traumatic brain injury (TBI; weight drop). Increased expression of B1R in the injured hemispheres of wild-type mice was restricted to the later stages after brain trauma, i.e. day 7 (P<0.05), whereas no significant induction could be observed for the B2R (P>0.05). Mice lacking the B1R, but not the B2R, showed less functional deficits on day 3 (P<0.001) and day 7 (P<0.001) compared with controls. Pharmacological blocking of B1R in wild-type mice had similar effects. Reduced axonal injury and astroglia activation could be identified as underlying mechanisms, while inhibition of B1R had only little influence on the local inflammatory response in this model. Inhibition of B1R may become a novel strategy to counteract trauma-induced neurodegeneration.
KW  - R-715
KW  - kinin receptors
KW  - closed head injury
KW  - β-APP
KW  - astrocytes
KW  - TNF-α
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-125903
VL  - 32
IS  - 9
ER  - 
TY  - JOUR
A1  - Isaias, Ioannis Ugo
A1  - Spiegel, Jörg
A1  - Brumberg, Joachim
A1  - Cosgrove, Kelly P.
A1  - Marotta, Giorgio
A1  - Oishi, Naoya
A1  - Higuchi, Takahiro
A1  - Küsters, Sebastian
A1  - Schiller, Markus
A1  - Dillmann, Ulrich
A1  - van Dyck, Christopher H.
A1  - Buck, Andreas
A1  - Herrmann, Ken
A1  - Schloegl, Susanne
A1  - Volkmann, Jens
A1  - Lassmann, Michael
A1  - Fassbender, Klaus
A1  - Lorenz, Reinhard
A1  - Samnick, Samuel
T1  - Nicotinic acetylcholine receptor density in cognitively intact subjects at an early stage of Parkinson's disease
JF  - Frontiers in Aging Neuroscience
N2  - We investigated in vivo brain nicotinic acetylcholine receptor (nAChR) distribution in cognitively intact subjects with Parkinson's disease (PD) at an early stage of the disease. Fourteen patients and 13 healthy subjects were imaged with single photon emission computed tomography and the radiotracer 5-[(123)I]iodo-3-[2(S)-2-azetidinylmethoxy]pyridine ([(123)I]5IA). Patients were selected according to several criteria, including short duration of motor signs (<7 years) and normal scores at an extensive neuropsychological evaluation. In PD patients, nAChR density was significantly higher in the putamen, the insular cortex and the supplementary motor area and lower in the caudate nucleus, the orbitofrontal cortex, and the middle temporal gyrus. Disease duration positively correlated with nAChR density in the putamen ipsilateral (ρ = 0.56, p < 0.05) but not contralateral (ρ = 0.49, p = 0.07) to the clinically most affected hemibody. We observed, for the first time in vivo, higher nAChR density in brain regions of the motor and limbic basal ganglia circuits of subjects with PD. Our findings support the notion of an up-regulated cholinergic activity at the striatal and possibly cortical level in cognitively intact PD patients at an early stage of disease.
KW  - nicotinic receptors
KW  - Parkinson disease
KW  - 5IA-SPECT
KW  - dopamine acetylcholine
KW  - cognitive decline
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-119351
VL  - 6
ER  - 
TY  - JOUR
A1  - Albert-Weissenberger, Christiane
A1  - Mencl, Stine
A1  - Hopp, Sarah
A1  - Kleinschnitz, Christoph
A1  - Siren, Anna-Leena
T1  - Role of the kallikrein-kinin system in traumatic brain injury
JF  - Frontiers in Cellular Neuroscience
N2  - Traumatic brain injury (TBI) is a major cause of mortality and morbidity worldwide. Despite improvements in acute intensive care, there are currently no specific therapies to ameliorate the effects of TBI. Successful therapeutic strategies for TBI should target multiple pathophysiologic mechanisms that occur at different stages of brain injury. The kallikrein-kinin system is a promising therapeutic target for TBI as it mediates key pathologic events of traumatic brain damage, such as edema formation, inflammation, and thrombosis. Selective and specific kinin receptor antagonists and inhibitors of plasma kallikrein and coagulation factor XII have been developed, and have already shown therapeutic efficacy in animal models of stroke and TBI. However, conflicting preclinical evaluation, as well as limited and inconclusive data from clinical trials in TBI, suggests that caution should be taken before transferring observations made in animals to humans. This review summarizes current evidence on the pathologic significance of the kallikrein-kinin system during TBI in animal models and, where available, the experimental findings are compared with human data.
KW  - bradykinin
KW  - factor XII
KW  - kallikrein–kinin system
KW  - kinin receptor
KW  - traumatic brain injury
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-118226
SN  - 1662-5102
VL  - 8
ER  - 
TY  - JOUR
A1  - Hohmann, Christopher
A1  - Milles, Bianca
A1  - Schinke, Michael
A1  - Schroeter, Michael
A1  - Ulzheimer, Jochen
A1  - Kraft, Peter
A1  - Kleinschnitz, Christoph
A1  - Lehmann, Paul V.
A1  - Kuerten, Stefanie
T1  - Categorization of multiple sclerosis relapse subtypes by B cell profiling in the blood
JF  - Acta Neuropathologica Communications
N2  - INTRODUCTION:
B cells are attracting increasing attention in the pathogenesis of multiple sclerosis (MS). B cell-targeted therapies with monoclonal antibodies or plasmapheresis have been shown to be successful in a subset of patients. Here, patients with either relapsing-remitting (n = 24) or secondary progressive (n = 6) MS presenting with an acute clinical relapse were screened for their B cell reactivity to brain antigens and were re-tested three to nine months later. Enzyme-linked immunospot technique (ELISPOT) was used to identify brain-reactive B cells in peripheral blood mononuclear cells (PBMC) directly ex vivo and after 96 h of polyclonal stimulation. Clinical severity of symptoms was determined using the Expanded Disability Status Scale (EDSS).

RESULTS:
Nine patients displayed B cells in the blood producing brain-specific antibodies directly ex vivo. Six patients were classified as B cell positive donors only after polyclonal B cell stimulation. In 15 patients a B cell response to brain antigens was absent. Based on the autoreactive B cell response we categorized MS relapses into three different patterns. Patients who displayed brain-reactive B cell responses both directly ex vivo and after polyclonal stimulation (pattern I) were significantly younger than patients in whom only memory B cell responses were detectable or entirely absent (patterns II and III; p = 0.003). In one patient a conversion to a positive B cell response as measured directly ex vivo and subsequently also after polyclonal stimulation was associated with the development of a clinical relapse. The evaluation of the predictive value of a brain antigen-specific B cell response showed that seven of eight patients (87.5%) with a pattern I response encountered a clinical relapse during the observation period of 10 months, compared to two of five patients (40%) with a pattern II and three of 14 patients (21.4%) with a pattern III response (p = 0.0005; hazard ratio 6.08 (95% confidence interval 1.87-19.77).

CONCLUSIONS:
Our data indicate actively ongoing B cell-mediated immunity against brain antigens in a subset of MS patients that may be causative of clinical relapses and provide new diagnostic and therapeutic options for a subset of patients.
KW  - ELISPOT
KW  - MS
KW  - predictive value
KW  - relapse
KW  - B cells
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-120580
SN  - 2051-5960
VL  - 2
IS  - 138
ER  - 
TY  - JOUR
A1  - Isaias, Ioannis Ugo
A1  - Dipaola, Mariangela
A1  - Michi, Marlies
A1  - Marzegan, Alberto
A1  - Volkmann, Jens
A1  - Rodocanachi Roidi, Mariana L.
A1  - Frigo, Carlo Albino
A1  - Cavallari, Paolo
T1  - Gait Initiation in Children with Rett Syndrome
JF  - PLoS ONE
N2  - Rett syndrome is an X-linked neurodevelopmental condition mainly characterized by loss of spoken language and a regression of purposeful hand use, with the development of distinctive hand stereotypies, and gait abnormalities. Gait initiation is the transition from quiet stance to steady-state condition of walking. The associated motor program seems to be centrally mediated and includes preparatory adjustments prior to any apparent voluntary movement of the lower limbs. Anticipatory postural adjustments contribute to postural stability and to create the propulsive forces necessary to reach steady-state gait at a predefined velocity and may be indicative of the effectiveness of the feedforward control of gait. In this study, we examined anticipatory postural adjustments associated with gait initiation in eleven girls with Rett syndrome and ten healthy subjects. Muscle activity (tibialis anterior and soleus muscles), ground reaction forces and body kinematic were recorded. Children with Rett syndrome showed a distinctive impairment in temporal organization of all phases of the anticipatory postural adjustments. The lack of appropriate temporal scaling resulted in a diminished impulse to move forward, documented by an impairment in several parameters describing the efficiency of gait start: length and velocity of the first step, magnitude and orientation of centre of pressure-centre of mass vector at the instant of (swing-)toe off. These findings were related to an abnormal muscular activation pattern mainly characterized by a disruption of the synergistic activity of antagonistic pairs of postural muscles. This study showed that girls with Rett syndrome lack accurate tuning of feedforward control of gait.
KW  - syndrome
KW  - ankles  
KW  - biological locomotion
KW  - kinematics
KW  - rett
KW  - soleus muscles
KW  - walking
KW  - velocity
KW  - children
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-119789
SN  - 1932-6203
VL  - 9
IS  - 4
ER  - 
TY  - JOUR
A1  - Kraft, Peter
A1  - Drechsler, Christiane
A1  - Gunreben, Ignaz
A1  - Nieswandt, Bernhard
A1  - Stoll, Guido
A1  - Heuschmann, Peter Ulrich
A1  - Kleinschnitz, Christoph
T1  - Von Willebrand Factor Regulation in Patients with Acute and Chronic Cerebrovascular Disease: A Pilot, Case-Control Study
JF  - PLoS ONE
N2  - Background and Purpose

In animal models, von Willebrand factor (VWF) is involved in thrombus formation and propagation of ischemic stroke. However, the pathophysiological relevance of this molecule in humans, and its potential use as a biomarker for the risk and severity of ischemic stroke remains unclear. This study had two aims: to identify predictors of altered VWF levels and to examine whether VWF levels differ between acute cerebrovascular events and chronic cerebrovascular disease (CCD).

Methods

A case–control study was undertaken between 2010 and 2013 at our University clinic. In total, 116 patients with acute ischemic stroke (AIS) or transitory ischemic attack (TIA), 117 patients with CCD, and 104 healthy volunteers (HV) were included. Blood was taken at days 0, 1, and 3 in patients with AIS or TIA, and once in CCD patients and HV. VWF serum levels were measured and correlated with demographic and clinical parameters by multivariate linear regression and ANOVA.

Results

Patients with CCD (158±46%) had significantly higher VWF levels than HV (113±36%, P<0.001), but lower levels than AIS/TIA patients (200±95%, P<0.001). Age, sex, and stroke severity influenced VWF levels (P<0.05).

Conclusions

VWF levels differed across disease subtypes and patient characteristics. Our study confirms increased VWF levels as a risk factor for cerebrovascular disease and, moreover, suggests that it may represent a potential biomarker for stroke severity, warranting further investigation.
KW  - cerebrovascular diseases
KW  - sex addiction
KW  - biomarkers
KW  - ischemic stroke
KW  - blood
KW  - stroke
KW  - platelets
KW  - demography
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-119588
SN  - 1932-6203
VL  - 9
IS  - 6
ER  - 
TY  - JOUR
A1  - Wurmb, Thomas Erik
A1  - Schlereth, Stefan
A1  - Kredel, Markus
A1  - Muellenbach, Ralf M.
A1  - Wunder, Christian
A1  - Brederlau, Jörg
A1  - Roewer, Norbert
A1  - Kenn, Werner
A1  - Kunze, Ekkehard
T1  - Routine Follow-Up Cranial Computed Tomography for Deeply Sedated, Intubated, and Ventilated Multiple Trauma Patients with Suspected Severe Head Injury
JF  - BioMed Research International
N2  - Background. Missed or delayed detection of progressive neuronal damage after traumatic brain injury (TBI) may have negative impact on the outcome. We investigated whether routine follow-up CT is beneficial in sedated and mechanically ventilated trauma patients. Methods. The study design is a retrospective chart review. A routine follow-up cCT was performed 6 hours after the admission scan. We defined 2 groups of patients, group I: patients with equal or recurrent pathologies and group II: patients with new findings or progression of known pathologies. Results. A progression of intracranial injury was found in 63 patients (42%) and 18 patients (12%) had new findings in cCT 2 (group II). In group II a change in therapy was found in 44 out of 81 patients (54%). 55 patients with progression or new findings on the second cCT had no clinical signs of neurological deterioration. Of those 24 patients (44%) had therapeutic consequences due to the results of the follow-up cCT. Conclusion. We found new diagnosis or progression of intracranial pathology in 54% of the patients. In 54% of patients with new findings and progression of pathology, therapy was changed due to the results of follow-up cCT. In trauma patients who are sedated and ventilated for different reasons a routine follow-up CT is beneficial.
KW  - Computertomographie
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-120084
IS  - 361949
ER  - 
TY  - THES
A1  - Schwab, Nicholas
T1  - The importance of CD8\(^+\) T cells and antigen-presenting cells in the immune reaction of primary inflammatory versus degenerative diseases
T1  - Die Bedeutung CD8\(^+\) T-Zellen und Antigen-präsentierender Zellen in der Immunreaktion primär inflammatorischer gegenüber degenerativen Erkrankungen
N2  - The bidirectional influence of parenchymal cells and cells of the immune system, especially of antigen-presenting and CD8\(^+\) T cells, in situations of putative auto- immune pathogenicity and degeneration was the main topic of this thesis. In the first part, the influence of human muscle cells on antigen-presenting cells was investigated. In inflammatory myopathies prominent infiltrates of immune cells containing T cells and antigen-presenting cells like macrophages and dendritic cells are present. The hypothesis was that human myoblasts have an inhibiting influence on these antigen-presenting cells under homeostatic conditions. A dysfunction or impairment under inflammatory circumstances might contribute to the development of myopathic conditions. The surface analysis of dendritic cells cocultured with myoblasts showed that immature dendritic cells could be driven into a reversible semi- mature state with significantly elevated levels of CD80. These dendritic cells were additionally characterized by their inhibiting function on T-cell proliferation. It was also shown that the lysates of healthy myoblasts could strongly enhance the phagocytic ability of macrophages, which could help with muscle regeneration and which might be disturbed in myositis patients. The second part of this thesis was about the clonal specificity of CD8\(^+\) T cells in a mouse model with genetically induced over-expression of PLP in oligodendrocytes. Here, we could show that the cytotoxic T lymphocytes, which had previously been shown to be pathogenic, were clonally expanded in the CNS of the transgenic mice. The amino acid sequences of the corresponding receptor chains were not identical, yet showed some similarities, which could mean that these clones recognize similar antigens (or epitopes of the same antigen). The knockout of PD-1 in this setting allowed for an analysis of the importance of tissue immune regulation. It became evident that the absence of PD-1 induced a larger number of clonal expansions in the CNS, hinting towards a reduced threshold for clonal disturbance and activation in these T cells. The expansions were, however, not pathogenic by themselves. Only in the presence of tissue damage and an antigenic stimulus (in our case the overexpression of PLP), the PD-1 limitation exacerbated the immune pathogenicity. Therefore, only in the presence of a “tissue damage signal”, the dyshomeostasis of T cells lacking PD-1 achieved high pathogenetic relevance. Finally, we investigated the pathogenetic role of CD8 T cells in Rasmussen encephalitis, a rare and chronic neurological disease mainly affecting children. The analysis of the T-cell receptor repertoire in Rasmussen encephalitis patients in the peripheral CD4\(^+\) and CD8\(^+\) T-cell compartments as well as the brain revealed the involvement of T cells in the pathogenicity of this disease. Many clonal expansions in the brain matched CD8\(^+\) T-cell expansions in the periphery on the sequence level. These putatively pathogenic clones could be visualized by immunohistochemistry in the brain and were found in close proximity to astrocytes and neurons. Additionally, the expanded clones could be found in the periphery of patients for at least one year.
N2  - Der Einfluss von Parenchymzellen auf Immunzellen und umgekehrt, im Besonderen von Antigen-präsentierenden Zellen und CD8\(^+\) T-Zellen, im Zusammenhang von auto- immuner Pathogenese und Degeneration war das Hauptthema dieser Dissertation. Im ersten Teil wurde der Einfluss menschlicher Muskelzellen auf Antigen- präsentierende Zellen untersucht. In entzündlichen Myopathien kommt es zu massiven Infiltraten von Immunzellen, die T-Zellen und auch Antigen-präsentierende Zellen wie Makrophagen und dendritische Zellen enthalten. Die Hypothese war, dass menschliche Myoblasten einen hemmenden Einfluss auf die Antigen-präsentierenden Zellen unter homöostatischen Bedingungen haben. Eine Störung dieses Einflusses oder eine Beeinträchtigung unter entzündlichen Rahmenbedingungen könnte eventuell zur Entwicklung eines myopathischen Zustands beitragen. In der Oberflächenanalyse der dendritischen Zellen, die mit Myoblasten kultiviert wurden, zeigte sich, dass unreife dendritische Zellen in einen halb-reifen Zustand versetzt werden konnten, der sich beispielsweise durch stark erhöhte CD80 Expression kennzeichnet. Diese dendritischen Zellen wurden weiterhin charakterisiert über ihre hemmende Funktion auf die T-Zell Proliferation. Außerdem wurde gezeigt, dass Zelllysate gesunder Myoblasten die Phagozytoserate von Makrophagen enorm verstärken, was die Regeneration des Muskelgewebes erhöhen und möglicherweise in Myositispatienten gestört sein könnte. Im zweiten Teil der Dissertation ging es um die klonale Spezifität von CD8\(^+\) T-Zellen in einem Mausmodell mit genetisch induzierter Überexpression von PLP in Oligodendrozyten. Hier konnte gezeigt werden, dass die zytotoxischen T-Zellen, deren Pathogenität Gegenstand früherer Arbeiten war, im ZNS der transgenen Mäuse klonal expandiert waren. Die Aminosäuresequenzen der TCR&#946; Kette der expandierten Klone waren nicht identisch, zeigten jedoch einige Ähnlichkeiten, die darauf hinweisen könnten, dass diese Klone ähnliche Antigene (oder Epitope des gleichen Antigens) erkennen. Die genetisch induzierte Abwesenheit von PD-1 ermöglichte es, in diesem Zusammenhang den Einfluss von spezifischer Immunregulation im Gewebe zu untersuchen. Es zeigte sich, dass die Deletion von PD-1 eine erhöhte Anzahl von klonalen Expansionen im ZNS der Mäuse erzeugte, was auf eine herabgesetzte Schwelle für klonale Störungen und Aktivierung schließen lässt. Diese Expansionen &#8233; waren jedoch für sich genommen nicht pathogen. Nur in der Anwesenheit eines Gewebeschadens und eines zusätzlicher Antigenstimulus (in unserem Fall in Form der PLP Überexpression) konnte man die erhöhte Pathogenität durch die PD-1 Deletion erkennen. Deswegen erreichten die PD-1 deletierten T-Zellen nur in der Gegenwart eines „Gewebeschaden-Signals“ hohe pathogenetische Relevanz. Schließlich untersuchten wir die pathogenetische Rolle von CD8\(^+\) T-Zellen in der Rasmussen Enzephalitis, einer seltenen, chronischen Erkrankung des Gehirns, die hauptsächlich in Kindern vorkommt. Die Analyse des T-Zell-Rezeptor Repertoires in Rasmussen Enzephalitis Patienten in peripheren CD4\(^+\) und CD8\(^+\) T-Zell Populationen und im Gehirn zeigte die Beteiligung von T-Zellen in der Pathogenese dieser Krankheit auf. Viele klonale Expansionen waren zwischen Gehirn und der peripheren CD8\(^+\) Population bis hin zur Aminosäuresequenz identisch. Diese vermutlich pathogenen Klone konnten in Gehirnbiopsien von Rasmussenpatienten histochemisch nachgewiesen werden und wurden in enger Nachbarschaft zu Astrozyten und Neuronen gefunden. Zusätzlich konnten diese expandierten Kone in der Peripherie von Patienten für die beobachteten Zeiträume (mindestens ein Jahr) nachgewiesen werden.
KW  - T-Lymphozyt
KW  - Entzündung
KW  - Degeneration
KW  - Immunsystem
KW  - Rasmussen-Syndrom
KW  - T lymphocyte
KW  - inflammation
KW  - degeneration
KW  - immune system
KW  - rasmussen encephalitis
Y1  - 2009
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-37330
ER  - 
TY  - THES
A1  - Fischer, Cindy Erika Elisabeth
T1  - Expression des fetalen Acetylcholinrezeptors im Muskel bei experimenteller Nervenläsion der Ratte und bei Neuropathien des Menschen
N2  - No abstract available
KW  - Acetylcholinrezeptor
KW  - Nicotinischer Acetylcholinrezeptor
KW  - Denervierung
KW  - Nervenregeneration
KW  - Muskel
KW  - Muskelhypertonie
KW  - Motorische Endplatte
KW  - Alkoholische Polyneuropathie
KW  - Diabetische Polyneuropathie
KW  - Polyneuropathie
KW  - Atrophie
KW  - neurogen
KW  - fetal
KW  - SMA
Y1  - 2009
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-36619
ER  - 
TY  - THES
A1  - Hirschmann, Anna
T1  - microRNA-Genexpressionsprofile in Blut-, Haut- und Nervenproben von Patienten mit Polyneuropathien
T1  - microRNA gene expression profiles in blood, skin and nerve samples of patients with polyneuropathy
N2  - Die Polyneuropathie (PNP) ist die häufigste Störung des peripheren Nervensystems bei Erwachsenen. Die Suche nach der Ursache bleibt in vielen Fällen erfolglos, ist aber unverzichtbar, da die Therapiewahl von der Ätiologie der Erkrankung abhängt. Geeignete Biomarker könnten die Differentialdiagnose unter Umständen erleichtern. microRNAs (miRNAs) sind in dieser Hinsicht vielversprechend, da in vielen Studien bei Nervende- und  regenerationsprozessen sowie in neuropathischen Schmerzmodellen eine Dysregulation beschrieben wurde.
In dieser Studie wurde die Expression zweier miRNAs, miR-103a und miR-let-7d, sowie eines Zielmoleküls der miR-103a, des Kalziumkanals Cav1,2, in einer großen Kohorte von PNP-Patienten unterschiedlicher Ätiologie in Blut, Haut- und Nervenbiopsien untersucht. Insgesamt wurden 116 Patienten und 22 Kontroll-probanden in die Studie eingeschlossen. Nach der Isolation von RNA aus weißen Blutzellen (WBC), Haut- und Nervenbiopsien folgte die Expressionsbestimmung mittels qRT-PCR.
Während sich jeweils Unterschiede zwischen PNP-Patienten und Kontrollen und zwischen Patienten mit entzündlicher und solchen mit nicht-entzündlicher PNP zeigten, wurden keine Unterschiede in der Expression zwischen den ätiologischen Subgruppen oder zwischen Patienten mit schmerzhafter und schmerzloser PNP festgestellt. In den Nervenbiopsien der Patientenkohorte ergab sich eine inverse Korrelation der miR-103a und ihrem Zielgen Cacna1c, die darauf hinweisen könnte, dass Cacna1c von der miR-103a negativ reguliert wird.
Da in unserer Patientenkohorte keine Unterschiede zwischen den PNP-Subgruppen auftraten, scheint der Einsatz der miR-103a und miR-let-7d als diagnostische Biomarker zur ätiologischen Einordnung einer PNP nicht gerechtfertigt. Dennoch deuten unsere Ergebnisse auf eine mögliche Rolle der untersuchten miRNAs bei Entstehung und Verlauf von PNP hin. Für ein tieferes pathophysiologisches Verständnis der miRNAs vor allem bei entzündlichen Neuropathien, könnte die Untersuchung von weiteren miRNAs und Zielgenen Aufschluss geben.
N2  - Polyneuropathies (PNP) are the most frequent disorder of the peripheral nervous system in adults. Since the choice of therapy depends on it, the etiological diagnostic  is essential but often remains without results so far. The differential diagnosis could be facilitated by a suitable biomarker. In this respect, microRNA (miRNA) are promising because their dysregulation has been described in processes of nerve degeneration and regeneration as well as in neuropathic pain models.
This study investigated the expression of two miRNA, miR-103a and miR-let-7d, and the calcium channel Cav1.2, a target of miR-103a, in a large cohort of PNP patients with different etiology in blood, skin and nerve samples. Altogether, 116 patients and 22 controls have been included in the study. Expressional analysis via qRT-PCR succeeded the isolation of RNA out of white blood cells (WBC), skin and nerve biopsies.
Differences have been found between PNP patients and controls and between patients with inflammatory and non-inflammatory PNP. No differences have been recorded between the etiological subgroups or between painful and painless PNP. miR-103a and its target Cacna1c correlated inversely in nerve which could be an indication for Cacna1c being negatively regulated by miR-103a.
miR-103a and miR-let-7d do not seem to be appropriate diagnostic biomarkers for the etiological classification of PNP as there have not been found any differences between the PNP subgroups. Nevertheless, our results suggest that miRNA may play a part in the development and the progression of PNP. The investigation of further miRNA and targets could provide insight into a deeper pathophysiological understanding of miRNA, especially in inflammatory neuropathies.
KW  - miRNS
KW  - Polyneuropathie
KW  - Genexpression
KW  - microRNA
KW  - miRNA
KW  - PNP
KW  - Neuropathischer Schmerz
KW  - neuropathic pain
KW  - gene expression
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-217010
ER  - 
TY  - THES
A1  - Pozzi, Nicoló Gabriele
T1  - Parkinson’s disease revisited: multiple circuitopathies
T1  - Neuinterpretation des Morbus Parkinson als multiple Netzwerkerkrankung
N2  - Parkinson’s disease (PD) is among the most common neurodegenerative conditions, and it is characterized by the progressive loss of dopaminergic neurons and a great variability in clinical expression. Despite several effective medications, it still causes disability as all patients show treatment-resistant symptoms and complications.
A possible reason for this therapeutic-burden and great clinical variability lies in a probable misconception about its pathophysiology, one that focuses on neurodegeneration, while largely neglecting its functional consequences and the related compensatory changes. In this thesis, I expand on the hypothesis that some PD symptoms have a dysfunctional origin and reflect derangements of neural network dynamics, the means by which brain coordination supports any motor behaviour. In particular, I have investigated resting tremor and freezing of gait, two common symptoms with an enigmatic mechanism and suboptimal management.
In the case of tremor, I predicted a pathological change in response to dopamine loss, which included the activation of noradrenergic (NA) neurons of the locus coeruleus (LC) projecting to the cerebellum. This compensatory LC activation that supports dopaminergic neurons might indeed come at the expense of tremor development. To assess the role of LC-NA in tremor development, I recorded tremor occurrence in the reserpinized rat model of PD, one of very few showing tremor, after selective lesioning (with the neurotoxin DSP-4) of the LC-NA terminal axons. DSP-4 induced a severe reduction of LC-NA terminal axons in the cerebellar cortex and this was associated with a significant reduction in tremor development. Unlike its development, tremor frequency and the akinetic rigid signs did not differ between the groups, thus suggesting a dopaminergic dependency. These findings suggest that the LC-NA innervation of the cerebellum has a critical role for PD tremor, possibly by exerting a network effect, which gates the cerebello-thalamic-cortical circuit into pathological oscillations upon a dopaminergic loss in the basal ganglia.
In contrast, for the study of freezing of gait, I worked with human PD subjects and deep brain stimulation, a therapeutic neuromodulation device that in some prototypes also allows the recording of neural activity in freely-moving subjects. Gait freezing is a disabling PD symptom that suddenly impairs effective stepping, thus causing falls and disability. Also in this study, I hypothesized that the underlying pathophysiology may be represented by dysfunctional neural network dynamics that abruptly impair locomotor control by affecting the communication in the supraspinal locomotor network. To test this hypothesis, I investigated the coupling between the cortex and the subthalamic nucleus, two main nodes of the supraspinal locomotor network, in freely-moving subjects PD patients and also performed molecular brain imaging of striatal dopamine receptor density and kinematic measurements. I found that in PD patients, walking is associated with cortical-subthalamic stable coupling in a low-frequency band (i.e. θ-α rhythms). In contrast, these structures decoupled when gait freezing occurred in the brain hemisphere with less dopaminergic innervation. These findings suggest that freezing of gait is a “circuitopathy”, with dysfunctional cortical-subcortical communication.
Altogether the results of my experiments support the hypothesis that the pathophysiology of PD goes beyond neurodegenerative (loss-of-function) processes and that derangement of neural network dynamics coincides with some disabling PD symptoms, thus suggesting that PD can be interpreted as the combination of multiple circuitopathies.
N2  - Die Parkinson-Krankheit ist eine neurodegenerative Erkrankung mit einem progressiven Verlust dopaminerger Neurone, die trotz wirksamer Medikamente zur Einschränkung in der Lebensqualität führen kann.
Eine mögliche Ursache für diese unzureichende Behandlung der Symptome liegt in einem möglichen Missverständnis über die Pathophysiologie der Krankheit, die sich auf die Neurodegeneration konzentriert. Bei der Parkinson-Krankheit können jedoch funktionelle Veränderungen aufgrund der Neurodegeneration sowie die damit verbundenen kompensatorischen Modifikationen sehr wichtig sein. Der Fokus meiner Dissertation liegt in der Bearbeitung der Hypothese, dass einige Symptome der Parkinson-Krankheit einen dysfunktionellen Ursprung haben können. Insbesodere habe ich den Ruhetremor und das Freezing-Phänomen, das eine Blockade des Gehens bedeutet, untersucht, um zu erklären, ob ein Störung der neuronalen Netzwerkdynamik diese Symptome verursachen kann.
In dieser Arbeit wurde zuerst die Entwicklung des Ruhetremors bei der Parkinson-Krankheit untersucht. Meine Hypothese war, dass eine Aktivierung von projizierenden noradrenergen Fasern des Locus-Coeruleus zum Cerebellum das Auftreten des Tremors verursachen kann, welches durch den Verlust dopaminerger Neurone verursacht wird. Da die Aktivität des Locus-Coeruleus bei Patienten mit Parkisnon-Krankheit nicht messbar ist, wurde dies in einem Parkinson-Rattenmodell untersucht. Die Ratten wurden etweder mit Reserpin oder mit Reserpine plus eine Neurotoxin gegen noradrenerger Neuronen (DSP-4) behandelt. Diese Behandlung mit DSP-4 führte zur Degeneration noradrenerger Terminalen im Locus-Coeruleus. Das Auftreten von Tremor zwischen die beiden Gruppen von Ratten war unterschiedlich. Insbesondere entwickelten DSP-4 behandelte Ratten einen niedrigen Ruhetremor. Dieses Ergebnis deutet darauf hin, dass die noradrenerge Innervation des Cerebellums vom Locus-Ceruleus für das Auftreten des Ruhetremors eine große Rolle spielt. In der Frequenz des Tremors sowie in den akinetischen Symptomen konnte kein Unterschied zwischen den Gruppen festgestellt werden. Das zeigt, dass diese akinetischen Symptome vom Dopaminverlust abhängig sind. Die Kombination von Tremor und akinetischen Symptomen kann aufgrund eines patologischen Netzwerkeffekts entstehen, welche vom Verlust dopaminerger Neurone in den Basalganglien im Zusammenspiel mit der kompensatorischen Aktivierung noradrenerger Neurone des Locus-Coeruleus verursacht werden kann.
Des Weiteren wurde der Ursprung des Freezing-Phänomens bei Patienten, die an der Parkinson-Krankheit leiden und eine therapeutische Behandlung mittels Tiefer Hirnstimulation (THS) bekommen haben, untersucht. Insbesodere konnten mittels neuer THS-Prototypen Messungen neuronaler Aktivität von Bewegungen durchgeführt werden. In dieser Studie stellte ich die Hypothese auf, dass die Pathophysiologie des Freezings durch eine fehlerhafte neuronale Dynamik der Bewegungsnetzwerke erklärt werden kann. Um dies zu testen, wurde die Kommunikation zwischen den zwei Hauptknoten des Bewegungsnetzwerkes, dem Kortex und dem Nucleus Subthalamicus, bei THS behandelten Parkinson-Patienten während des Gehens und den Freezing-Episoden untersucht. Zudem wurde bei diesen Patienten eine molekulare Darstellung der dopaminergen Rezeptoren in den Basalganglien durchgeführt. Zusätzlich wurden kinematischen Messungen der Bewegungen vorgenommen, die eine präzise Beschreibung des Freezings ermöglichen. Es konnte gezeigt werden, dass bei Patienten mit der Parkinson-Krankheit ein Zusammenhang von stabiler Kommunikation zwischen dem Kortex und dem Nucleus Subthalamicus bei einer bestimten Frequenz (d.h. θ-α-Rhythmen) beim Gehen besteht. Beim Auftreten des Freezing-Phänomens konnte diese Kommunikation in der Gehirnhemisphäre mit weniger dopaminerger Innervation nicht mehr nachgewiesen werden. Diese Ergebnisse deuten darauf hin, dass das Freezing-Phänomen eine „Circuitopathie“ ist, in der eine fehlerhafte Kommunikation zwischen kortikalen und subkortikalen Arealen zur Bewegungsblockade führen kann.
Insgesamt stützen die Ergebnisse meiner Experimente die Hypothese, dass die Pathophysiologie der Parkinson-Krankheit sowohl über neurodegenerative Prozesse (Zellverlust) als auch über Störungen der neuronalen Netzwerkdynamik (Funktionsverlust) hinausgeht. Das deutet darauf hin, dass die Parkison-Krankheit als „Circuitopathie“ interpretiert werden kann.
KW  - Parkinson-Krankheit
KW  - freezing of gait
KW  - resting tremor
KW  - circuitopathies
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-216715
ER  - 
TY  - THES
A1  - Beaucamp, Marcel
T1  - Prädiktion des Verschlusses großer intrakranieller Arterien anhand präklinischer Schlaganfallscores
T1  - Prediction of large vessel oclusions by using preclinical stroke scores
N2  - 2015 konnte in mehreren Studien ESCAPE, EXTENDED IA, MR CLEAN, REVASCAT, SWIFT-PRIME eine signifikante Überlegenheit der mechanischen Thrombektomie verglichen mit der alleinigen i. v. Lysetherapie mit rtPA bezogen auf Revaskularisierung bei Patienten mit einer LVO (large vessel occlusion) nachgewiesen werden. Diese neue Therapiemöglichkeit erforderte eine Aufteilung der Patienten die von einer Thrombektomie profitieren (LVO) und der Patienten, die keiner Thrombektomie zugeführt werden können (nLVO). Die zentrale Fragestellung der Studie ist: Kann ein symptomorientierter Schlaganfallscore die Wahrscheinlichkeit eines großen intrakraniellen Gefäßverschlusses mit hinreichender Präzision vorhersagen und kann auf Basis dieser Vorhersage ein Patient direkt in ein übergeordnetes Schlagfanfallzentrum gebracht werden, obwohl sich dadurch eine Bridging Lysetherapie verzögern würde?
Um diesen Fragen auf den Grund zu gehen führten wir eine monozentrische Querschnittstudie durch, in deren Rahmen 215 Patienten rekrutiert wurden. Die Rekrutierung erfolgte mittels eines aus Subitems bereits etablierter Schlafanfallscores (FAST, CPSS, LAPSS, 3ISS, RACE), zusammengesetzten Fragebogens. Die ausgefüllten Fragebögen wurde in Excel digitalisiert und mittels SPSS, Signifikanz und Odds Ratio berechnet. Anschließend wurde aus den signifikanten Subitems mit der höchsten Odds Ratio ein neuer einfach anzuwendender Schlaganfallscore, bestehend aus den präklinisch erhobenen Daten gebildet (Würzburg Score of Large Vessel Occlusions, WOLVE- Score). Weiter wurden Signifikanz, Odds Ratio, Sensitivität und Spezifität des WOLVE-Score mit denen der oben genannten etablieren Scores verglichen.
N2  - 2015 several publications ESCAPE, EXTENDED IA, MR CLEAN, REVASCAT, SWIFT-PRIME proofed a significant superiority of the mechanical thrombectomy in Patients suffering from a LVO (large vessel occlusion) concerning revascularization rates compared to i. v. thrombolysis with rtPA, alone. This newly discovered therapy required a new distribution of patients who could profit from a thrombectomy (LVO) and those who would not profit from a thrombectomy (nLVO). The key question is: Can a symptom related stroke score predict the probability of a large vessel occlusion with a sufficient precision and is it possible to admit a patient to a comprehensive stroke center based on this prediction, even though an early bridging thrombolysis is delayed. To answer this question we performed a cross-sectional study in which 215 patients were recruited by using a composite questionnaire consisting of subitems from established stroke scores (FAST, CPSS, LAPSS, 3ISS, RACE). The questionnaire was digitalized in Ecxel. Statistical calculations of the significancy and the odds ratio were conducted in SPSS. The significant subitems with the highest odds ratio were used to construct a new simple stroke score for LVO recognition in the field (Würzburg Score of Large Vessel Occlusions, WOLVE- Score). Eventually the significancy, odds ratio sensitivity and specificity of the WOLVE-Score were calculated and compared to the ones of the established scores.
KW  - Schlaganfall
KW  - Gefäßverschluss
KW  - Score
KW  - Thrombektomie
KW  - Revaskularisierung
KW  - Stroke
KW  - Score
KW  - LVO
Y1  - 2021
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-215117
ER  - 
TY  - THES
A1  - Frank, Franziska
T1  - Veränderung der Ranvier’schen Schnürringarchitektur bei Patienten mit diabetischer Neuropathie
T1  - Disruption of the nodal architecture in patients with diabetic neuropathy
N2  - In der Krankheitsentstehung der diabetischen Neuropathie wird die paranodale Demyelinisierung als ein möglicher Pathomechanismus diskutiert, wobei Studien mit Gewebeproben von Patienten aufgrund der Invasivität limitiert sind. In der vorliegenden Studie wurden periphere Nervenfasern in Hautbiopsien von Patienten mit diabetischer Neuropathie und in Patienten mit Diabetes mellitus ohne Neuropathie untersucht. Ziel war es, nodale und paranodale Veränderungen, wie eine Dispersion der paranodalen Proteine Caspr und Neurofascin oder der nodalen Na-Kanäle, zu detektieren und die Proben auf verlängerte Ranvier`sche Schnürringe zu untersuchen. 
Es wurde die Hypothese überprüft, dass paranodale Demyelinisierungen bei Patienten mit diabetischer Neuropathie in Hautbiopsien, als minimal-invasive Methode, nachweisbar sind. Hautproben von Patienten mit Diabetes mellitus ohne Neuropathie sollten zudem in einem frühen Krankheitsstadium untersucht werden. 
Für die Untersuchung konnten 35 Patienten mit einer diabetischen Neuropathie, 17 Patienten mit Diabetes mellitus und 31 Kontrollen eingeschlossen werden. Immunfluoreszenzfärbungen mit Antikörpern gegen Caspr, Neurofascin und Natrium-Kanälen wurden zur Analyse der Ranvier`schen Schnürringarchitektur durchgeführt und ausgewertet. 
Eine erhöhte Anzahl an verlängerten Schnürringen, als Zeichen einer segmentalen Demyelinisierung, konnte in den Patienten mit diabetischer Neuropathie aber auch in Patienten mit Diabetes mellitus nachgewiesen werden. Weiterhin waren vermehrt Veränderungen der paranodalen Proteine, wie eine Dispersion von Caspr und Neurofascin in den Proben des Fingers der Patienten mit diabetischer Neuropathie sowie eine Dispersion von Neurofascin im Unterschenkel in beiden Patientengruppen nachweisbar. Interessanterweise waren einzelne Veränderungen auch in den gesunden Kontrollen auffindbar. 
Veränderungen der Schnürringarchitektur lassen sich mithilfe der Hautbiopsie nachweisen und quantifizieren. Nodale und paranodale Veränderungen weisen auf demyelinisierende Prozesse in Patienten mit diabetischer Neuropathie hin und finden sich auch bereits in einem frühen Krankheitsstadium.
N2  - During the course of diabetic neuropathy, paranodal demyelination has been discussed as a possible mechanism, although studies with tissue samples from patients are limited due to its invasiveness. In the present study, peripheral nerve fibers were examined in skin biopsies from patients with diabetic neuropathy and in patients with diabetes mellitus without neuropathy. The aim was to detect nodal and paranodal changes, such as a dispersion of the paranodal proteins Caspr and Neurofascin or the nodal sodium channels, and to examine the samples for elongated nodes of Ranvier.
The hypothesis was tested that paranodal demyelination in patients with diabetic neuropathy can be detected in skin biopsies as a minimally invasive method. Skin samples from patients with diabetes mellitus without neuropathy should also be examined at an early stage of the disease.
35 patients with diabetic neuropathy, 17 patients with diabetes mellitus and 31 controls could be included in the study. Immunofluorescence staining with antibodies against Caspr, Neurofascin and sodium channels were carried out and evaluated in order to analyze the architecture of nodes of Ranvier. 
An increased number of elongated nodes, as a sign of segmental demyelination, could be demonstrated in patients with diabetic neuropathy, but also in patients with diabetes mellitus. An increased number of changes in paranodal proteins, such as a dispersion of Caspr and Neurofascin in the samples of the finger of the patients with diabetic neuropathy and a dispersion of Neurofascin in the lower leg in both patient groups, were detectable. Interestingly, alterations of the nodal architecture could also be found in healthy controls.
A disruption of the architecture of the node of Ranvier can be detected and quantified using skin biopsies. Nodal and paranodal alterations indicate demyelinating processes in patients with diabetic neuropathy and are also found at an early stage of the disease.
KW  - Ranvier-Schnürring
KW  - Diabetische Neuropathie
KW  - Diabetes mellitus
KW  - Hautbiopsie
KW  - skin biopsy
KW  - Caspr
KW  - Neurofascin
KW  - Caspr
KW  - Neurofascin
KW  - node of Ranvier
KW  - diabetic neuropathy
Y1  - 2021
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-219668
ER  - 
TY  - THES
A1  - Kohl, Bianca Dorothea
T1  - PMP22-overexpressing mice as a model for Charcot-Marie-Tooth 1A neuropathy implicate a role of immune-related cells
T1  - PMP22-überexprimierende Mäuse als Modell einer Charcot-Marie-Tooth 1A Neuropatie.
N2  - Charcot-Marie-Tooth disease (CMT) is a cohort of human hereditary disorders of the peripheral nervous system (PNS) which exhibit symptoms like sensory dysfunction, muscle weakness and gait disturbances. Different mutations are described as causation for this neuropathy, such as a duplication of chromosome 17 comprising the gene for the peripheral myelin protein-22 (PMP22). Based on different animal models former studies identified immune cells, i.e. macrophages and T-lymphocytes, as crucial mediators of pathology in these neuropathies. In this study, PMP22-overexpressing mice (PMP22tg, C61), serving as a model for a specific type of CMT – CMT1A – were crossbred with immune-deficient mutant mice to examine the impact of the immune system on nerve pathology. Crossbreeding of PMP22tg mice with recombination activating gene-1 (RAG-1) deficient mice, lacking mature T- and B-lymphocytes, caused no striking alterations of pathogenesis in peripheral nerves of mutant mice. In contrast, crossbreeding of PMP22tg myelin mutants with mice deficient in the chemokine monocyte chemoattractant protein-1 (MCP-1, CCL2) caused an amelioration of the demyelinating phenotype of peripheral nerves when MCP-1 was either reduced or completely absent. Furthermore, functional investigations, i.e. neurographic recordings and examinations of the grip strength of the extremities, revealed an amelioration in PMP22tg/MCP-1-/- mice in regard to a symptomatic improvement in the compound action muscle potential (CMAP) and stronger grip strength of the hindlimbs. Interestingly, peripheral nerves of PMP22tg mice showed an irregular distribution of potassium channels in presence of MCP-1, whereas the absence of MCP-1 in the myelin mutants rescued the ion channel distribution and resulted in a more wild type-like phenotype. Having shown the impact of MCP-1 as an important mediator of nerve pathology in PMP22/MCP-1 double mutants, the regulation of this chemokine became an important target for potential treatment strategies. We found that the signaling cascade MEK1/2/ERK1/2 was more strongly activated in peripheral nerves of PMP22tg mice compared to nerves of wild type mice. This activation corresponded to an increase in MCP-1 mRNA expression in peripheral nerves at the same age. Furthermore, a MEK1/2-inhibitor was used in vivo to confirm the regulation of MCP-1 by the MEK1/2/ERK1/2 pathway. After a treatment period of three weeks, a clear reduction of ERK1/2-phosphorylation as well as a reduction of MCP-1 mRNA expression was observed, accompanied by a decline in macrophage number in peripheral nerves of PMP22tg mice. These observations suggest that the expression of MCP-1 is crucial for the neuropathological progression in a mouse model for CMT1A. Therefore, this chemokine could provide a basis for a putative treatment strategy of inherited neuropathies.
N2  - Die Charcot-Marie-Tooth Erkrankungen (CMT) sind eine Gruppe von humanen, erblichen Erkrankungen des peripheren Nervensystems (PNS), welche Symptome wie sensible Störungen, Muskelschwäche und Gangstörungen verursachen können. Verschiedene Mutationen, z.B. eine Duplikation des Chromosoms 17, welches das Gen für das periphere Myelinprotein-22 (PMP22) enthält, sind als Ursache für diese Neuropathie beschrieben. Anhand verschiedener Tiermodelle wurde in früheren Studien gezeigt, dass Immunzellen, insbesondere Makrophagen und T-Lymphozyten, maßgeblich an der Pathogenese dieser Neuropathien beteiligt sind. In der vorliegenden Studie wurden PMP22-überexprimierende Mäuse (PMP22tg, C61) als Modell einer spezifischen CMT-Form – CMT1A – mit immun-defizienten Mutanten verkreuzt, um die modulierende Rolle des Immunsystems innerhalb der Pathogenese peripherer Nerven untersuchen zu können. Die Verkreuzung von PMP22tg Mäusen mit „recombination activating gene-1“-defizienten Mutanten (RAG-1-/-), die keine reifen T- und B-Lymphozyten besitzen, resultierte in keiner deutlich veränderten Pathologie der peripheren Nerven. Im Gegensatz hierzu führte die Verkreuzung der Myelinmutanten mit Mäusen, defizient für das Chemokin „monocyte chemoattractant protein-1“ (MCP-1), zu einer Abschwächung des demyelinisierenden Phänotyps in peripheren Nerven, wenn MCP-1 reduziert war oder völlig fehlte. Funktionelle Analysen, wie elektrophysiologische Messungen und Untersuchungen der Kraft in den Extremitäten, zeigten zudem in PMP22tg/MCP-1-/- Mäusen eine symptomatische Verbesserung, was sich in einer höheren Amplitude (compound muscle action potential, CMAP) und einer erhöhten Kraft in den Hinterpfoten der Mäuse widerspiegelte. Interessanterweise zeigten periphere Nerven der PMP22tg Mäuse eine abnorme Verteilung von Kalium-Kanälen, wohingegen das Fehlen von MCP-1 in den Myelinmutanten zu einer Verteilung dieser Ionenkanäle führte, die ähnlich zu Wildtyp-Mäusen war. Da MCP-1 in den PMP22/MCP-1 Doppelmutanten einen deutlichen Einfluss auf die Pathogenese aufwies, wurde die Regulation dieses Chemokins im Hinblick auf mögliche Therapie-Ansätze untersucht. Diese Untersuchung zeigte, dass die MEK1/2/ERK1/2-Signalkaskade in peripheren Nerven von PMP22tg Mäusen stärker aktiviert wird als in Nerven von Wildtyp-Tieren. Die Aktivierung dieser Signalkaskade ging dabei mit einer erhöhten MCP-1 mRNA Expression in peripheren Nerven von Tieren des gleichen Alters einher. Ergänzend wurde ein MEK1/2-Inhibitor in vivo verwendet, um die Regulation von MCP-1 durch die MEK1/2/ERK1/2 Kaskade zu bestätigen. Nach einer Behandlungszeit von drei Wochen wurde eine deutliche Reduktion der ERK1/2-Phosphorylierung, sowie eine Reduktion der MCP-1 mRNA Expression und eine geringere Makrophagen-Anzahl in peripheren Nerven von PMP22tg Mäusen detektiert. Diese Untersuchungen zeigen, dass die Expression von MCP-1 entscheidend für den neuropathologischen Verlauf in einem Mausmodell für CMT1A ist. Somit bietet dieses Chemokin eine Basis für die Entwicklung neuer Behandlungsstrategien peripherer Neuropathien.
KW  - Myelin
KW  - Makrophage
KW  - Entmarkung
KW  - Schwann Zellen
KW  - PMP22
KW  - MCP-1
KW  - Immunzellen
KW  - Periphere Nerven
KW  - Schwann cells
KW  - PMP22
KW  - MCP-1
KW  - immune cells
KW  - peripheral nerves
Y1  - 2009
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-43066
ER  - 
TY  - THES
A1  - Raban, Rebecca Emmi Hildegard
T1  - Sicherheit und Wirksamkeit von intrathekalem Triamcinolon bei Patienten mit chronisch-progredienter Multipler Sklerose : eine retrospektive Longitudinalstudie
T1  - Safety and efficacy of intrathecal triamcinolone in chronic progressive multiple sclerosis - a retrospective longitudinal study
N2  - Im Zeitraum von 2004 bis 2016 erhielten an der Neurologischen Universitätsklinik Würzburg Patienten mit einer chronisch progredienten Multiplen Sklerose insgesamt 595 Injektionen von intrathekalem Triamcinolonacetonid. Diese Arbeit befasst sich mit Sicherheit, Nebenwirkungen und Wirksamkeit der intrathekalen Therapieform.
N2  - In the period from 2004 to 2016 patients with chronic progressive multiple sclerosis at the Neurological University Clinic Würzburg received a total of 595 injections of intrathecal triamcinolone acetonide. This work deals with safety, side effects and effectiveness of intrathecal therapy.
KW  - Intrathekale Applikation
KW  - Triamcinolon
KW  - Multiple Sklerose
KW  - intrathekal
KW  - intrathecal
KW  - Volon A
KW  - chronische Multiple Sklerose
KW  - triamcinolone acetonide
KW  - progressive multiple sclerosis
Y1  - 2021
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-220478
ER  - 
TY  - THES
A1  - Küttner [geb. Weber], Sarah-Lucia
T1  - Der Optikusnervenscheidendurchmesser als Instrument zur Prognoseeinschätzung bei Patienten mit hypoxischer Enzephalopathie nach erfolgreicher Reanimation
T1  - Optic nerve sheath diameter for prognostication in resuscitated patients with hypoxic-ischemic encephalopathy
N2  - Eine Prognoseeinschätzung bei Patienten mit hypoxischer Enzephalopathie (HIE) nach Reanimation wird frühestens 72 Stunden nach Reanimation empfohlen. Bis zu diesem Zeitpunkt besteht eine für Ärzte und Angehörige belastende prognostische Lücke. Und auch nach 72 Stunden bestehen nur ungenaue Angaben zum weiteren Vorgehen, sodass eine fundierte Prognoseeinschätzung aktuell eine deutliche Herausforderung im Alltag klinisch tätiger Ärzte darstellt.

Der Nervus opticus ist als Bestandteil des zentralen Nervensystems mit dem Liquorsystem verbunden. Intrazerebrale Druckerhöhungen wirken sich daher unmittelbar auf die ihn ummantelnde Nervenscheide und deren Durchmesser aus, sodass sich die Bestimmung des Optikusnervenscheidendurchmessers (ONSD) mittels transorbitaler Sonographie in der Diagnostik unterschiedlicher intrakranieller Erkrankungen bereits bewährt hat. Das Krankheitsbild der HIE wurde als weiteres mögliches Einsatzgebiet des ONSD jedoch bisher nicht untersucht.


Ziel dieser Dissertation war es daher, den ONSD grundsätzlich auf seine Verlässlichkeit als Prognoseparameter bei HIE nach Reanimation zu überprüfen. Besonderes Augenmerk lag hierbei auf der Ermöglichung einer frühzeitigen Prognoseeinschätzung innerhalb von 24 Stunden sowie auf der Definition eines prognostischen Cut-Off-Wertes als klare Entscheidungshilfe für weitere therapeutische Strategien.

24, 48 und 72 Stunden nach Reanimation werden signifikant unterschiedliche ONSD unter überlebenden und verstorbenen Patienten nachgewiesen. Letztere weisen dabei im Vergleich sowohl höhere als auch im zeitlichen Verlauf signifikant ansteigende ONSD-Werte auf. Als prognostischer Cut-Off-Wert konnte eine Grenze bei 5,75mm festgelegt werden.

Zusammenfassend stellt die sonographische Bestimmung des ONSD eine sinnvolle Zusatzdiagnostik in der Prognoseeinschätzung bei Patienten mit HIE nach Reanimation dar.
N2  - Prognostication of neurological outcome in resuscitated patients with hypoxic-ischemic encephalopathy (HIE) is recommended 72 hours after cardiac arrest. Until this time, there is a prognostic gap that is burdensome for physicians and relatives. And even after 72 hours, there is only imprecise information on the further course of action, so that a well-founded prognostication remains challenging in the everyday life of physicians. 

As a component of the central nervous system, the optic nerve is connected to the cerebrospinal fluid system. Increase in intracerebral pressure therefore directly affects the optic nerve sheath and its diameter, so that measurement of the optic nerve sheath diameter (ONSD) by means of transorbital sonography has already proven its worth in the diagnosis of various intracranial diseases. However, HIE has not yet been investigated as another possible field of application of ONSD.


Therefore, the aim of this dissertation was to evaluate the reliability of ONSD as a prognostic parameter in HIE after resuscitation. Particular emphasis was placed on enabling early prognostication within 24 hours and on defining a prognostic cut-off-value as a clear decision aid for further therapeutic strategies.

Significantly different ONSD are demonstrated among surviving and deceased patients 24, 48, and 72 hours after resuscitation. The latter show both higher ONSD values and significantly increasing ONSD values over time. A prognostic cut-off value of 5.75mm could be established.

In conclusion, sonographic measurement of ONSD is a useful additional diagnostic tool for prognostication in patients with HIE after resuscitation.
KW  - Wiederbelebung
KW  - Prognostik
KW  - Ultraschalldiagnostik
KW  - Optikusnervenscheidendurchmesser
KW  - hypoxische Enzephalopathie
KW  - optic nerve sheath diameter
KW  - hypoxic-ischemic encephalopathy
Y1  - 2021
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-237669
ER  - 
TY  - THES
A1  - Auchter, Antonia
T1  - Schlafassoziierte Veränderung der lokalen Feldpotential Aktivität im Nucleus subthalamicus bei Patienten mit Morbus Parkinson
T1  - Sleep-associated changes in local field potential activity in the nucleus subthalamicus in patients with Parkinson's disease
N2  - Die tiefe Hirnstimulation ist eine etablierte und hocheffiziente operative Behandlungsmethode für Patienten mit idiopathischem Parkinson- Syndrom (IPS). Als Zielgebiet dient in den meisten Fällen der Nucleus subthalamicus. Die Indikationen zur Implantation einer tiefen Hirnstimulation (THS) sind medikamentös nicht behandelbare motorische Fluktuationen und Dyskinesien oder ein medikamentös nicht kontrollierbarer Tremor.
Bislang erfolgt eine kontinuierliche Stimulation. Little et al. konnten jedoch bereits in ihrer 2013 veröffentlichen Studie zeigen, dass eine adaptive Stimulation, gemessen am UPDRS, um 27 % effektiver war und entsprechend die Stimulationszeit um 56 % gesenkt werden konnte.
Voraussetzung für die Anwendbarkeit einer adaptiven Stimulation im klinischen Alltag ist der Nachweis eines oder mehrerer Physiomarker, welche als Rückkopplungssignal für den Stimulationsbeginn dienen. Diese Marker müssen verlässlich mit dem Auftreten und der Ausprägung der Bewegungsstörungen korrelieren. Die Systeme müssen die Signale auslesen und entsprechend darauf reagieren können, damit ein sogenanntes Closed- loop- Verfahren entstehen kann. Bei diesen Markern handelt es sich um sogenannte lokale Feldpotenzialaktivitäten, das heißt niederfrequente Potentialänderungen von Zellen in subkortikalen Arealen des Gehirns, welche über Elektroden der THS abgeleitet werden können. Der Stimulator Activa PC+S (Medtronic) ermöglicht es erstmalig Aufzeichnungen von LFP- Daten, außerhalb eines experimentellen Laboraufbaus, mittels dauerhaft implantiertem Gerät vorzunehmen und damit auch Langzeitanalysen durchzuführen.
Erkenntnisse vergangener Studien ergaben, dass die synchronisierte, pathologisch gesteigerte oszillatorische Aktivität im Beta-Frequenzband (13- 35 Hz) eine bedeutende Rolle im Bezug auf die Pathophysiologie des IPS spielt und als krankheitsspezifische Aktivität gilt.  Es konnte bereits belegt werden, dass die Verbesserung der motorischen Symptome (Bradykinese und Rigor) mit dem Ausmaß der Suppression der Betaband- Aktivität korreliert. Die Betabandaktivität als lokale Feldpotentialaktivität kann als Physiomarker einer adaptiven Stimulation dienen.
Unser Hauptaugenmerk galt daher der Analyse der Betabandaktivität oder anderer Frequenzbereiche während des Schlafes um hier die THS bedarfsgerecht einzusetzen. Hierfür wurden nächtliche subkortikale LFP- Aufzeichnungen parallel zur Schlaf- Polysomnographie durchgeführt. Zudem erfolgte in der vorliegenden Arbeit sowohl in unserem Vorversuch als auch in unserem Hauptversuch die Anwendung des UPDRS Teil III zur Erfassung der motorischen Symptome, sowie die Durchführung von Fragebögen zur Erfassung der nicht- motorischen Symptome, insbesondere des Schlafes vor und nach Implantation der tiefen Hirnstimulation.
Wir konnten belegen, dass es nach Implantation der THS zu einer Erhöhung der Schlafeffizienz und zu einer Erhöhung des Anteils der Schlafstadien II und III und damit einhergehend zu einer Steigerung der Schlafqualität kommt. Übereinstimmend mit anderen Studien konnten wir zeigen, dass sich die Motorik unter Stimulation deutlich verbessert. Im Vorversuch reduzierte sich der mittlere präoperative MDS- UPDRS III im MedsOFF verglichen mit dem mittleren postoperativ MDS- UPDRS III im MedsOFF/StimON um 37 %. In der PC+S- Studie imponierte eine Reduktion um 67%. Zudem zeigte sich eine Reduktion der nicht- motorischen Symptome durch die THS, insbesondere in der Kategorie Schlaf.  Die Ergebnisse der vorliegenden Arbeit ergaben außerdem, dass die Betabandaktivität im Schlafstadium II und vor allem im Schlafstadium III am geringsten ist. Im Schlafstadium I und REM ist die Betabandaktivität höher als im Schlafstadium II und III. Hierbei war entscheidend, dass die Patienten eine klar abgrenzbare Betabandaktivität im Wachstadium aufwiesen und die Elektrodenkontakte im dorsolateralen Kerngebiet des STN lokalisiert waren.
Gegenläufig dazu verhält sich die Deltaaktivität. Sie ist im Schlafstadium II und besonders im Stadium III am höchsten. Stadium I ist mit durchschnittlich um 7,3 % niedriger als im Wachstadium. Am geringsten ist sie jedoch im REM-Schlafstadium. 
Indem wir mit der Betabandaktivität und Deltaaktivität in den einzelnen Schlafstadien einen stabilen und reproduzierbaren Physiomarker finden konnten, sind wir unserem Ziel der adaptiven THS ein Stück näher gekommen.
N2  - Deep brain stimulation is an established and highly efficient surgical treatment modality for patients with idiopathic Parkinson's syndrome (IPS). The target area in most cases is the subthalamic nucleus. The indications for implantation of deep brain stimulation (THS) are motor fluctuations and dyskinesias that cannot be treated with medication or tremor that cannot be controlled with medication.
To date, continuous stimulation has been used. However, Little et al. were already able to show in their study published in 2013 that adaptive stimulation was 27% more effective, as measured by UPDRS, and that the stimulation time could be reduced by 56% accordingly.
A prerequisite for the applicability of adaptive stimulation in clinical practice is the detection of one or more physiomarkers that serve as feedback signals for the onset of stimulation. These markers must correlate reliably with the occurrence and severity of movement disorders. The systems must be able to read out the signals and react to them accordingly, so that a so-called closed-loop procedure can be created. These markers are so-called local field potential activities, i.e. low-frequency potential changes of cells in subcortical areas of the brain, which can be derived via electrodes of the THS. The Activa PC+S stimulator (Medtronic) makes it possible for the first time to record LFP data outside of an experimental laboratory setup using a permanently implanted device and thus also to perform long-term analyses.
Findings of past studies revealed that synchronized, pathologically enhanced oscillatory activity in the beta frequency band (13- 35 Hz) plays a significant role in relation to the pathophysiology of IPS and is considered disease-specific activity.  It has already been demonstrated that the improvement of motor symptoms (bradykinesia and rigor) correlates with the extent of suppression of beta-band activity. Beta-band activity as local field potential activity may serve as a physiomarker of adaptive stimulation.
Therefore, our main focus was on the analysis of beta-band activity or other frequency ranges during sleep in order to apply THS as needed. For this purpose, nocturnal subcortical LFP recordings were performed in parallel to sleep polysomnography. In addition, the UPDRS Part III was used to record motor symptoms in our preliminary trial as well as in our main trial, and questionnaires were administered to record nonmotor symptoms, especially sleep before and after implantation of deep brain stimulation.
We were able to prove that after implantation of THS there is an increase in sleep efficiency and an increase in the proportion of sleep stages II and III and thus an associated increase in sleep quality. Consistent with other studies, we demonstrated that motor function improves significantly under stimulation. In the preliminary trial, the mean preoperative MDS- UPDRS III in MedsOFF was reduced by 37% compared with the mean postoperative MDS- UPDRS III in MedsOFF/StimON. In the PC+S- study, a reduction of 67% was impressive. In addition, THS showed a reduction in non-motor symptoms, especially in the sleep category.  The results of the present work also revealed that beta-band activity is lowest in sleep stage II and especially in sleep stage III. In sleep stage I and REM, beta-band activity is higher than in sleep stage II and III. Here, it was crucial that the patients showed a clearly delineable beta-band activity in the waking stage and that the electrode contacts were localized in the dorsolateral nucleus area of the STN.
Opposite to this is the delta activity. It is highest in sleep stage II and especially in stage III. Stage I is lower than in the waking stage, with an average of 7.3%. However, it is lowest in the REM sleep stage. 
By finding a stable and reproducible physiomarker with beta band activity and delta activity in the individual sleep stages, we have come a step closer to our goal of adaptive THS.
KW  - Parkinson
KW  - Lokale Feldpotentialaktivität
KW  - Nucleus subthalamicus
Y1  - 2021
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-237822
ER  - 
TY  - THES
A1  - Köberle, Philipp
T1  - High-resolution ultrasound for the identification of pathological patterns in patients with polyneuropathies and amyotrophic lateral sclerosis
T1  - Hochauflösender Ultraschall zur Identifizierung von pathologischen Mustern bei Patienten mit Polyneuropathien und amyotropher Lateralsklerose
N2  - Neuropathies are a group of potentially treatable diseases with an often disabling and restricting course. Amyotrophic lateral sclerosis (ALS) is a lethal disease without causal treatment possibilities. The objective of this study was to examine the diagnostic utility of HRUS for the differentiation of subtypes of axonal and demyelinating neuropathies and to investigate its utility for the sonological differentiation of ALS. 
The hypothetical statement that neuropathy causes enlargement of peripheral nerves compared to healthy controls proved to be right, but the adjunctive assumption that ALS does not cause enlargement of peripheral nerves proved to be wrong – in patients with ALS slight enlargement of peripheral nerves was visible as well. The statement that nerve enlargement can be detected by measurement of the cross-sectional area (CSA) and the longitudinal diameter (LD) with comparable results proved to be right, but the enlargement was slightly less present by measurement of the LD. The statement that axonal and demyelinating neuropathies show distinct patterns of nerve enlargement must be answered differentiated: The comparison between axonal and demyelinating neuropathies showed a stronger nerve enlargement in patients with demyelinating neuropathies than in patients with axonal neuropathies at proximal nerve segments of upper extremities. In the comparison of diagnose-defined subgroups of inflammatory demyelinating neuropathies a respective specific pattern of nerve enlargement was visible. However, remarkable in this context was the strong nerve enlargement found in patients with NSVN, which is classified as an axonal neuropathy. Stratification for specific findings in nerve biopsy did not lead to constructive differences in comparison between the different groups. 
To sum up, HRUS showed to provide a useful contribution in the diagnostic process of neuropathies and ALS but needs to be integrated in a multimodal diagnostic approach.
N2  - Neuropathien stellen eine Gruppe potenziell behandelbarer Erkrankungen mit häufig behinderndem und einschränkendem Verlauf dar. Die amyotrophe Lateralsklerose (ALS) ist eine tödliche Erkrankung ohne Möglichkeiten der kausalen Behandlung. Das Ziel dieser Studie war es, den diagnostischen Nutzen von hochauflösendem Ultraschall für die Differenzierung von Subtypen axonaler und demyelinisierender Neuropathien, sowie der amyotrophen Lateralsklerose zu untersuchen. Die hypothetische Aussage, dass durch Neuropathien eine Vergrößerung von peripheren Nerven im Vergleich zu gesunden Kontrollen nachgewiesen werden kann, erwies sich als richtig. Entgegen der hiermit verknüpften Aussage, dass es bei amyotropher Lateralsklerose zu keiner Größenzunahme peripherer Nerven kommt, konnte bei diesen Patienten ebenfalls eine leichte Kaliberzunahme der Nerven nachgewiesen werden. Die Aussage, dass eine Nervenvergrößerung durch die Messung von Querschnittsfläche und longitudinalem Durchmesser mit vergleichbaren Ergebnissen erfolgen kann, erwies sich als richtig, jedoch zeigte sich die Nervenvergrößerung bei der Messung des longitudinalen Durchmessers etwas geringer ausgeprägt. Die Aussage, dass axonale und demyelinisierende Neuropathien unterschiedliche Muster der Nervenvergrößerung aufweisen, muss differenziert beantwortet werden: Der Vergleich axonalen und demyelinisierenden Neuropathien zeigte bei Patienten mit demyelinisierenden Neuropathien, insbesondere an proximalen Nervensegmenten der oberen Extremitäten, eine stärkere Nervenvergrößerung als bei Patienten mit axonalen Neuropathien. Im Vergleich diagnose-definierter Subgruppen demyelinisierender Neuropathien zeigte sich ein jeweils spezifisches Verteilungsmuster der Nervenvergrößerung. In diesem Zusammenhang bemerkenswert war jedoch die starke Nervenvergrößerung bei Patienten mit nicht-systemischer vaskulitischer Polyneuropahie, welche als axonale Neuropathie klassifiziert wird. Die Stratifikation nach spezifischen Befunden in der Nervenbiopsie führte nicht zu konstruktiven Unterschieden im Vergleich der Untergruppen. 
Zusammenfassend zeigte sich, dass der hochauflösende Nervenultraschall einen nützlichen Beitrag im diagnostischen Prozess von Neuropathien und ALS leisten kann, jedoch in eine multimodale diagnostische Herangehensweise integriert werden muss.
KW  - Polyneuropathie
KW  - Ultraschall
KW  - HRUS
KW  - polyneuropathy
KW  - ALS
KW  - pattern
KW  - biopsy
KW  - Nervenultraschall
KW  - Muster
KW  - Nervenbiopsie
KW  - Polyneuropathie
KW  - amyotrophe Lateralsklerose
Y1  - 2021
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-245800
ER  - 
TY  - THES
A1  - Christ, Nicolas
T1  - Die Auswirkung zerebraler Mikroblutungen auf die kognitive Leistungsfähigkeit nach ischämischem Schlaganfall
T1  - The impact of cerebral microbleeds on the Cognition after ischemic stroke
N2  - In der vorliegenden Studie wurde untersucht, ob zerebrale Mikroblutungen (CMB) bereits im frühen Verlauf nach ischämischem Schlaganfall (IS) oder Transitorisch-Ischämischer Attacke (TIA) mit kognitivem Abbau assoziiert sind und ob spezifische kognitive Domänen besonders betroffen sind. Der Vergleich zweier Probandengruppen mit IS/TIA und CMB bzw. IS/TIA ohne CMB hinsichtlich ihrer Ergebnisse in der neuropsychologischen Testbatterie CERAD ergab, dass CMB bereits sechs Monate nach dem zerebrovaskulären Ereignis mit einem kognitiven Abbau assoziiert sind. Multilokuläre CMB zeigen eine stärkere Auswirkung auf die Kognition als solche CMB, die in einer einzigen Hirnregion gefunden wurden. Zudem wurde eine signifikante Korrelation zwischen dem Grad der kognitiven Einschränkung und der Anzahl der CMB errechnet. Die separate Betrachtung derjenigen Testungen, welche das episodische Gedächtnis erfassen, zeigte eine Beeinträchtigung der Testpersonen beim Wiedererkennen von zuvor gelernten Wörtern. Bei der Untersuchung des semantischen Gedächtnisses der ProbandInnen fiel eine signifikant eingeschränkte phonematische Wortflüssigkeit auf, die semantische Flüssigkeit und das Benennen jedoch waren weniger betroffen. Die Domäne „Visuokonstruktive Fähigkeiten“ wurde ebenfalls in drei Untertests beurteilt. Hierbei zeigten sich keine Defizite der Testgruppe beim Abzeichnen der dargebotenen Figuren, die Reproduktion hingegen war signifikant gestört. Es zeigte sich keine CMB-bedingte Einschränkung der exekutiven Funktionen.
N2  - In this study, we aimed to investigate (1) whether cerebral microbleeds (CMB) are associated with cognitive decline 6 months after ischemic stroke and if so (2) whether there are some cognitive domains that are affected more preferentially by CMB. In a prospective cohort study, cognitive function was investigated in 33 patients with ischemic stroke or transient ischemic attack (TIA) and ≥ 1 CMB valuated by the Consortium to Establish a Registry for Alzheimer’s Diseases (CERAD)-plus test battery. The cognitive performance of these patients was compared with 33 stroke survivors without CMB . Both groups were matched for age, gender, clinical and radiological characteristics. This study yielded the following main findings: (1) within 6 months after ischemic stroke or TIA, CMB-positive patients revealed cognitive decline in more than one cognitive domain; (2) among tested domains, memory and phonemic fluency were most affected in CMB-positive patients, and (3) an occurrence of CMB in more than one of the predefined brain regions was associated with more pronounced cognitive deficits.
KW  - Hirnblutung
KW  - Kognition
KW  - Schlaganfall
KW  - Neuropsychologischer Test
KW  - Consortium to Establish a Registry for Alzheimer's Disease
KW  - Mikroblutung
Y1  - 2021
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-243679
ER  - 
TY  - JOUR
A1  - Schrewe, L.
A1  - Lill, C. M.
A1  - Liu, T.
A1  - Salmen, A.
A1  - Gerdes, L. A.
A1  - Guillot-Noel, L.
A1  - Akkad, D. A.
A1  - Blaschke, P.
A1  - Graetz, C.
A1  - Hoffjan, S.
A1  - Kroner, A.
A1  - Demir, S.
A1  - Böhme, A.
A1  - Rieckmann, P.
A1  - El Ali, A.
A1  - Hagemann, N.
A1  - Hermann, D. M.
A1  - Cournu-Rebeix, I.
A1  - Zipp, F.
A1  - Kümpfel, T.
A1  - Buttmann, M.
A1  - Zettl, U. K.
A1  - Fontaine, B.
A1  - Bertram, L.
A1  - Gold, R.
A1  - Chan, A.
T1  - Investigation of sex-specific effects of apolipoprotein E on severity of EAE and MS
JF  - Journal of Neuroinflammation
N2  - Background: Despite pleiotropic immunomodulatory effects of apolipoprotein E (apoE) in vitro, its effects on the clinical course of experimental autoimmune encephalomyelitis (EAE) and multiple sclerosis (MS) are still controversial. As sex hormones modify immunomodulatory apoE functions, they may explain contentious findings. This study aimed to investigate sex-specific effects of apoE on disease course of EAE and MS. 
Methods: MOG\(_{35-55}\) induced EAE in female and male apoE-deficient mice was assessed clinically and histopathologically. apoE expression was investigated by qPCR. The association of the MS severity score (MSSS) and APOE rs429358 and rs7412 was assessed across 3237 MS patients using linear regression analyses. 
Results: EAE disease course was slightly attenuated in male apoE-deficient (apoE\(^{-/-}\)) mice compared to wildtype mice (cumulative median score: apoE\(^{-/-}\) = 2 [IQR 0.0-4.5]; wildtype = 4 [IQR 1.0-5.0]; n = 10 each group, p = 0.0002). In contrast, EAE was more severe in female apoE\(^{-/-}\) mice compared to wildtype mice (cumulative median score: apoE\(^{-/-}\) = 3 [IQR 2.0-4.5]; wildtype = 3 [IQR 0.0-4.0]; n = 10, p = 0.003). In wildtype animals, apoE expression during the chronic EAE phase was increased in both females and males (in comparison to naive animals; p < 0.001). However, in MS, we did not observe a significant association between MSSS and rs429358 or rs7412, neither in the overall analyses nor upon stratification for sex. 
Conclusions: apoE exerts moderate sex-specific effects on EAE severity. However, the results in the apoE knock-out model are not comparable to effects of polymorphic variants in the human APOE gene, thus pinpointing the challenge of translating findings from the EAE model to the human disease.
KW  - immune
KW  - apoE
KW  - gender
KW  - inflammation
KW  - association studies in genetics
KW  - apoe
KW  - CNS disease
KW  - system
KW  - multiple sclerosis
KW  - MSSS
KW  - experimental autoimmune encephalomyelitis
KW  - disease severity
KW  - cognitive function
KW  - Alzheimer disease
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-136252
VL  - 12
IS  - 234
ER  - 
TY  - THES
A1  - Reymann, Stephan Andreas
T1  - Pathophysiologische Rolle und therapeutische Relevanz von Plasmakallikrein beim experimentellen Schlaganfall
T1  - Pathophysiological role and therapeutic relevance of plasma kallikrein in experimental stroke
N2  - Die Rolle thromboinflammatorischer Vorgänge in der Pathogenese des ischämischen Schlaganfalls ist in den letzten Jahren immer mehr in den wissenschaftlichen Fokus gerückt. Plasmakallikrein (PK) spaltet von hochmolekularem Kininogen (KNG) Bradykinin (BK) ab und ist dadurch Ausgangspunkt des proinflammatorischen Kallikrein-Kinin-Systems (KKS). Zum anderen kann es den Gerinnungsfaktor XII (FXII) aktivieren, den Ausgangspunkt der intrinsischen Gerinnungskaskade. Es initiiert also sowohl inflammatorische als auch thrombotische Vorgänge. Daher wurde in dieser Arbeit der Effekt einer Blockade PKs in einem Mausmodell der fokalen zerebralen Ischämie untersucht – und zwar sowohl durch genetische Depletion als auch durch pharmakologische Blockade. Beide Ansätze brachten einen nachhaltigen protektiven Effekt in Bezug auf Infarktgrößen und funktionelles Outcome, ohne die Blutungsgefahr zu erhöhen.
N2  - Recent scientific evidence raises the question whether ischemic stroke is a thromboinflammatory disease. Plasma kallikrein (PK) cleaves high–molecular-weight kininogen to release bradykinin (BK) and is a key constituent of the proinflammatory contact-kinin system. In addition, PK can activate coagulation factor XII, the origin of the intrinsic coagulation cascade. Thus, PK triggers 2 important pathological pathways of stroke formation, thrombosis and inflammation. 
Therefore we investigated the consequences of both genetic and pharmacological PK inhibition in a model of ischemic stroke and found out that PK-inhibition leads to significantly smaller brain infarctions and less severe neurological deficits compared with controls without an increase in infarct-associated hemorrhage.
KW  - Plasmakallikrein
KW  - Schlaganfall
KW  - Plasmakallikrein ischämischer Schlaganfall
Y1  - 2016
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-135834
ER  - 
TY  - JOUR
A1  - Minnerup, Jens
A1  - Sutherland, Brad A.
A1  - Buchan, Alastair M.
A1  - Kleinschnitz, Christoph
T1  - Neuroprotection for Stroke: Current Status and Future Perspectives
JF  - International Journal of Molecular Science
N2  - Neuroprotection aims to prevent salvageable neurons from dying. Despite showing efficacy in experimental stroke studies, the concept of neuroprotection has failed in clinical trials. Reasons for the translational difficulties include a lack of methodological agreement between preclinical and clinical studies and the heterogeneity of stroke in humans compared to homogeneous strokes in animal models. Even when the international recommendations for preclinical stroke research, the Stroke Academic Industry Roundtable (STAIR) criteria, were followed, we have still seen limited success in the clinic, examples being NXY-059 and haematopoietic growth factors which fulfilled nearly all the STAIR criteria. However, there are a number of neuroprotective treatments under investigation in clinical trials such as hypothermia and ebselen. Moreover, promising neuroprotective treatments based on a deeper understanding of the complex pathophysiology of ischemic stroke such as inhibitors of NADPH oxidases and PSD-95 are currently evaluated in preclinical studies. Further concepts to improve translation include the investigation of neuroprotectants in multicenter preclinical Phase III-type studies, improved animal models, and close alignment between clinical trial and preclinical methodologies. Future successful translation will require both new concepts for preclinical testing and innovative approaches based on mechanistic insights into the ischemic cascade.
KW  - free radical scavenger
KW  - ischemic cascade
KW  - acute ischemic stroke
KW  - trial
KW  - focal cerebral-ischemia
KW  - interleukin-1 receptor antagonist
KW  - colony-stimulating factor
KW  - tissue-plasminogen activator
KW  - traumatic brain injury
KW  - placebo-controlled
KW  - alias pilot trial
KW  - damage cool aid
KW  - neuroprotection
KW  - ischemic stroke
KW  - translation
KW  - STAIR
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-134730
VL  - 13
IS  - 9
ER  - 
TY  - JOUR
A1  - Golombeck, Stefanie Kristin
A1  - Wessig, Carsten
A1  - Monoranu, Camelia-Maria
A1  - Schütz, Ansgar
A1  - Solymosi, Laszlo
A1  - Melzer, Nico
A1  - Kleinschnitz, Christoph
T1  - Fatal atypical reversible posterior leukoencephalopathy syndrome: a case report
JF  - Journal of Medical Case Reports
N2  - Introduction: Reversible posterior leukoencephalopathy syndrome – a reversible subacute global encephalopathy clinically presenting with headache, altered mental status, visual symptoms such as hemianopsia or cortical blindness, motor symptoms, and focal or generalized seizures – is characterized by a subcortical vasogenic edema symmetrically affecting posterior brain regions. Complete reversibility of both clinical signs and magnetic resonance imaging lesions is regarded as a defining feature of reversible posterior leukoencephalopathy syndrome. Reversible posterior leukoencephalopathy syndrome is almost exclusively seen in the setting of a predisposing clinical condition, such as pre-eclampsia, systemic infections, sepsis and shock, certain autoimmune diseases, various malignancies and cytotoxic chemotherapy, transplantation and concomitant immunosuppression (especially with calcineurin inhibitors) as well as episodes of abrupt hypertension. We describe for the first time clinical, radiological and histological findings in a case of reversible posterior leukoencephalopathy syndrome with an irreversible and fatal outcome occurring in the absence of any of the known predisposing clinical conditions except for a hypertensive episode.
Case presentation: A 58-year-old Caucasian woman presented with a two-week history of subacute and progressive occipital headache, blurred vision and imbalance of gait and with no evidence for raised arterial blood pressure during the two weeks previous to admission. Her past medical history was unremarkable except for controlled arterial hypertension. Cerebral magnetic resonance imaging demonstrated cortical and subcortical lesions with combined vasogenic and cytotoxic edema atypical for both venous congestion and arterial infarction. Routine laboratory and cerebrospinal fluid parameters were normal. The diagnosis of reversible posterior leukoencephalopathy syndrome was established. 
Within hours after admission the patient showed a rapidly decreasing level of consciousness, extension and flexion synergisms, bilaterally extensor plantar responses and rapid cardiopulmonary decompensation requiring ventilatory and cardiocirculatory support. Follow-up cerebral imaging demonstrated widespread and confluent cytotoxic edematous lesions in different arterial territories, global cerebral swelling, and subsequent upper and lower brainstem herniation. Four days after admission, the patient was declared dead because of brain death.
Conclusion: This case demonstrates that fulminant and fatal reversible posterior leukoencephalopathy syndrome may occur spontaneously, that is, in the absence of any of the known predisposing systemic conditions.
KW  - reversible posterior leukoencephalopathy syndrome
KW  - generalized cerebral edema
KW  - cerebral autoregulation
KW  - blood pressure
Y1  - 2013
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-135517
VL  - 7
IS  - 14
ER  - 
TY  - JOUR
A1  - Bittner, Stefan
A1  - Bobak, Nicole
A1  - Feuchtenberger, Martin
A1  - Herrmann, Alexander M
A1  - Göbel, Kerstin
A1  - Kinne, Raimund W
A1  - Hansen, Anker J
A1  - Budde, Thomas
A1  - Kleinschnitz, Christoph
A1  - Frey, Oliver
A1  - Tony, Hans-Peter
A1  - Wiendl, Heinz
A1  - Meuth, Sven G
T1  - Expression of K\(_2\)\(_P\)5.1 potassium channels on CD4\(^+\)T lymphocytes correlates with disease activity in rheumatoid arthritis patients
JF  - Arthritis Research & Therapy
N2  - Introduction

CD4+ T cells express K2P5.1 (TWIK-related acid-sensitive potassium channel 2 (TASK2); KCNK5), a member of the two-pore domain potassium channel family, which has been shown to influence T cell effector functions. Recently, it was shown that K2P5.1 is upregulated upon (autoimmune) T cell stimulation. The aim of this study was to correlate expression levels of K2P5.1 on T cells from patients with rheumatoid arthritis (RA) to disease activity in these patients.

Methods

Expression levels of K2P5.1 were measured by RT-PCR in the peripheral blood of 58 patients with RA and correlated with disease activity parameters (C-reactive protein levels, erythrocyte sedimentation rates, disease activity score (DAS28) scores). Twenty patients undergoing therapy change were followed-up for six months. Additionally, synovial fluid and synovial biopsies were investigated for T lymphocytes expressing K2P5.1.

Results

K2P5.1 expression levels in CD4+ T cells show a strong correlation to DAS28 scores in RA patients. Similar correlations were found for serological inflammatory parameters (erythrocyte sedimentation rate, C-reactive protein). In addition, K2P5.1 expression levels of synovial fluid-derived T cells are higher compared to peripheral blood T cells. Prospective data in individual patients show a parallel behaviour of K2P5.1 expression to disease activity parameters during a longitudinal follow-up for six months.

Conclusions

Disease activity in RA patients correlates strongly with K2P5.1 expression levels in CD4+ T lymphocytes in the peripheral blood in cross-sectional as well as in longitudinal observations. Further studies are needed to investigate the exact pathophysiological mechanisms and to evaluate the possible use of K2P5.1 as a potential biomarker for disease activity and differential diagnosis.
KW  - neurology
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-139334
VL  - 13
IS  - R21
ER  - 
TY  - JOUR
A1  - Puschmann, Anne-Katrin
A1  - Sommer, Claudia
T1  - Hypervigilance or avoidance of trigger related cues in migraineurs? - A case-control study using the emotional stroop task
JF  - BMC Neurology
N2  - Background

"Negative affect" is one of the major migraine triggers. The aim of the study was to assess attentional biases for negative affective stimuli that might be related to migraine triggers in migraine patients with either few or frequent migraine and healthy controls.

Methods

Thirty-three subjects with frequent migraine (FM) or with less frequent episodic migraine, and 20 healthy controls conducted two emotional Stroop tasks in the interictal period. In task 1, general affective words and in task 2, pictures of affective faces (angry, neutral, happy) were used. For each task we calculated two emotional Stroop indices. Groups were compared using one-way ANOVAs.

Results

The expected attentional bias in migraine patients was not found. However, in task 2 the controls showed a significant attentional bias to negative faces, whereas the FM group showed indices near zero. Thus, the FM group responded faster to negative than to positive stimuli. The difference between the groups was statistically significant.

Conclusions

The findings in the FM group may reflect a learned avoidance mechanism away from affective migraine triggers.
KW  - migraineur
KW  - cue
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-137750
VL  - 11
IS  - 141
ER  - 
TY  - JOUR
A1  - Weise, Gesa
A1  - Basse-Lüsebrink, Thomas C.
A1  - Kleinschnitz, Christoph
A1  - Kampf, Thomas
A1  - Jakob, Peter M.
A1  - Stoll, Guido
T1  - In Vivo Imaging of Stepwise Vessel Occlusion in Cerebral Photothrombosis of Mice by \(^{19}\)F MRI
JF  - PLoS One
N2  - Background
\(^{19}\)F magnetic resonance imaging (MRI) was recently introduced as a promising technique for in vivo cell tracking. In the present study we compared \(^{19}\)F MRI with iron-enhanced MRI in mice with photothrombosis (PT) at 7 Tesla. PT represents a model of focal cerebral ischemia exhibiting acute vessel occlusion and delayed neuroinflammation.

Methods/Principal Findings
Perfluorocarbons (PFC) or superparamagnetic iron oxide particles (SPIO) were injected intravenously at different time points after photothrombotic infarction. While administration of PFC directly after PT induction led to a strong \(^{19}\)F signal throughout the entire lesion, two hours delayed application resulted in a rim-like \(^{19}\)F signal at the outer edge of the lesion. These findings closely resembled the distribution of signal loss on T2-weighted MRI seen after SPIO injection reflecting intravascular accumulation of iron particles trapped in vessel thrombi as confirmed histologically. By sequential administration of two chemically shifted PFC compounds 0 and 2 hours after illumination the different spatial distribution of the \(^{19}\)F markers (infarct core/rim) could be visualized in the same animal. When PFC were applied at day 6 the fluorine marker was only detected after long acquisition times ex vivo. SPIO-enhanced MRI showed slight signal loss in vivo which was much more prominent ex vivo indicative for neuroinflammation at this late lesion stage.

Conclusion
Our study shows that vessel occlusion can be followed in vivo by \(^{19}\)F and SPIO-enhanced high-field MRI while in vivo imaging of neuroinflammation remains challenging. The timing of contrast agent application was the major determinant of the underlying processes depicted by both imaging techniques. Importantly, sequential application of different PFC compounds allowed depiction of ongoing vessel occlusion from the core to the margin of the ischemic lesions in a single MRI measurement.
KW  - in vivo imaging
KW  - magnetic resonance imaging
KW  - macrophages
KW  - emulsions
KW  - infarction
KW  - fluorine
KW  - prefrontal cortex
KW  - developmental signaling
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-137792
VL  - 6
IS  - 12
ER  - 
TY  - JOUR
A1  - Üçeyler, Nurcan
A1  - Topuzoğlu, Tengü
A1  - Schießer, Peter
A1  - Hahnenkamp, Saskia
A1  - Sommer, Claudia
T1  - IL-4 Deficiency Is Associated with Mechanical Hypersensitivity in Mice
JF  - PLoS One
N2  - Interleukin-4 (IL-4) is an anti-inflammatory and analgesic cytokine that induces opioid receptor transcription. We investigated IL-4 knockout (ko) mice to characterize their pain behavior before and after chronic constriction injury (CCI) of the sciatic nerve as a model for neuropathic pain. We investigated opioid responsivity and measured cytokine and opioid receptor gene expression in the peripheral and central nervous system (PNS, CNS) of IL-4 ko mice in comparison with wildtype (wt) mice. Naïve IL-4 ko mice displayed tactile allodynia (wt: 0.45 g; ko: 0.18 g; p<0.001), while responses to heat and cold stimuli and to muscle pressure were not different. No compensatory changes in the gene expression of tumor necrosis factor-alpha (TNF), IL-1β, IL-10, and IL-13 were found in the PNS and CNS of naïve IL-4 ko mice. However, IL-1β gene expression was stronger in the sciatic nerve of IL-4 ko mice (p<0.001) 28 days after CCI and only IL-4 ko mice had elevated IL-10 gene expression (p = 0.014). Remarkably, CCI induced TNF (p<0.01), IL-1β (p<0.05), IL-10 (p<0.05), and IL-13 (p<0.001) gene expression exclusively in the ipsilateral spinal cord of IL-4 ko mice. The compensatory overexpression of the anti-inflammatory and analgesic cytokines IL-10 and IL-13 in the spinal cord of IL-4 ko mice may explain the lack of genotype differences for pain behavior after CCI. Additionally, CCI induced gene expression of μ, κ, and δ opioid receptors in the contralateral cortex and thalamus of IL-4 ko mice, paralleled by fast onset of morphine analgesia, but not in wt mice. We conclude that a lack of IL-4 leads to mechanical sensitivity; the compensatory hyperexpression of analgesic cytokines and opioid receptors after CCI, in turn, protects IL-4 ko mice from enhanced pain behavior after nerve lesion.
KW  - mouse models
KW  - animal behavior
KW  - sciatic nerves
KW  - spinal cord
KW  - opioids
KW  - cytokines
KW  - gene expression
KW  - mice
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-137924
VL  - 6
IS  - 12
ER  - 
TY  - JOUR
A1  - Ruck, Tobias
A1  - Bittner, Stefan
A1  - Afzali, Ali Maisam
A1  - Göbel, Kerstin
A1  - Glumm, Sarah
A1  - Kraft, Peter
A1  - Sommer, Claudia
A1  - Kleinschnitz, Christoph
A1  - Preusse, Corinna
A1  - Stenzel, Werner
A1  - Wiendl, Heinz
A1  - Meuth, Sven G.
T1  - The NKG2D-IL-15 signaling pathway contributes to T-cell mediated pathology in inflammatory myopathies
JF  - Oncotarget
N2  - NKG2D is an activating receptor on T cells, which has been implicated in the pathogenesis of autoimmune diseases. T cells are critically involved in idiopathic inflammatory myopathies (IIM) and have been proposed as specific therapeutic targets. However, the mechanisms underlying T cell-mediated progressive muscle destruction in IIM remain to be elucidated. We here determined the involvement of the NKG2D - IL-15 signaling pathway. Primary human myoblasts expressed NKG2D ligands, which were further upregulated upon inflammatory stimuli. In parallel, shedding of the soluble NKG2D ligand MICA (sMICA) decreased upon inflammation potentially diminishing inhibition of NKG2D signaling. Membrane-related expression of IL-15 by myoblasts induced differentiation of naive CD8\(^+\) T cells into highly activated, cytotoxic \(CD8^+NKG2D^{high}\) T cells demonstrating NKG2D-dependent lysis of myoblasts in vitro. \(CD8^+NKG2D^{high}\) T cell frequencies were increased in the peripheral blood of polymyositis (PM) patients and correlated with serum creatinine kinase concentrations, while serum sMICA levels were not significantly changed. In muscle biopsy specimens from PM patients expression of the NKG2D ligand MICA/B was upregulated, IL-15 was expressed by muscle cells, CD68\(^+\) macrophages as well as CD4\(^+\) T cells, and \(CD8^+NKG2D^+\) cells were frequently detected within inflammatory infiltrates arguing for a local signaling circuit in the inflammatory muscle milieu. In conclusion, the NKG2D - IL-15 signaling pathway contributes to progressive muscle destruction in IIM potentially opening new therapeutic avenues.
KW  - MIC ligands
KW  - pathology section
KW  - T cell activation
KW  - idiopathic inflammatory myopathies
KW  - polymyositis
KW  - IL-15
KW  - NKG2D
KW  - receptor
KW  - expression
KW  - lymphokine-activated killer
KW  - human muscle-cells
KW  - multiple sclerosis
KW  - celiac disease
KW  - tumor immunity
KW  - NKG2D ligands
KW  - cutting edge
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-136047
VL  - 6
IS  - 41
ER  - 
TY  - JOUR
A1  - Volkmann, Jens
A1  - Albanese, Alberto
A1  - Antonini, Angelo
A1  - Chaudhuri, K. Ray
A1  - Clarke, Karl E.
A1  - de Bie, Rob M. A.
A1  - Deuschl, Günther
A1  - Eggert, Karla
A1  - Houeto, Jean-Luc
A1  - Kulisevsky, Jaime
A1  - Nyholm, Dag
A1  - Odin, Per
A1  - Ostergaard, Karen
A1  - Poewe, Werner
A1  - Pollak, Pierre
A1  - Rabey, Jose Martin
A1  - Rascol, Olivier
A1  - Ruzicka, Evzen
A1  - Samuel, Michael
A1  - Speelman, Hans
A1  - Sydow, Olof
A1  - Valldeoriola, Francesc
A1  - van der Linden, Chris
A1  - Oertel, Wolfgang
T1  - Selecting deep brain stimulation or infusion therapies in advanced Parkinson’s disease: an evidence-based review
JF  - Journal of Neurology
N2  - Motor complications in Parkinson’s disease (PD) result from the short half-life and irregular plasma fluctuations of oral levodopa. When strategies of providing more continuous dopaminergic stimulation by adjusting oral medication fail, patients may be candidates for one of three device-aided therapies: deep brain stimulation (DBS), continuous subcutaneous apomorphine infusion, or continuous duodenal/jejunal levodopa/carbidopa pump infusion (DLI). These therapies differ in their invasiveness, side-effect profile, and the need for nursing care. So far, very few comparative studies have evaluated the efficacy of the three device-aided therapies for specific motor problems in advanced PD. As a result, neurologists currently lack guidance as to which therapy could be most appropriate for a particular PD patient. A group of experts knowledgeable in all three therapies reviewed the currently available literature for each treatment and identified variables of clinical relevance for choosing one of the three options such as type of motor problems, age, and cognitive and psychiatric status. For each scenario, pragmatic and (if available) evidence-based recommendations are provided as to which patients could be candidates for either DBS, DLI, or subcutaneous apomorphine.
KW  - Parkinson’s disease
KW  - apomorphine
KW  - deep brain stimulation
KW  - duodenal levodopa infusion
Y1  - 2013
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-132373
VL  - 260
ER  - 
TY  - JOUR
A1  - Isaias, Ioannis U.
A1  - Marzegan, Alberto
A1  - Pezzoli, Gianni
A1  - Marotta, Giorgio
A1  - Canesi, Margherita
A1  - Biella, Gabriele E. M.
A1  - Volkmann, Jens
A1  - Cavallari, Paolo
T1  - A role for locus coeruleus in Parkinson tremor
JF  - Frontiers in Human Neuroscience
N2  - We analyzed rest tremor, one of the etiologically most elusive hallmarks of Parkinson disease(PD), in 12 consecutive PD patients during a specific task activating the locus coeruleus (LC) to investigate a putative role of noradrenaline (NA) in tremor generation and suppression. Clinical diagnosis was confirmed in all subjects by reduced dopamine reuptake transporter (DAT) binding values investigated by single photon computed tomography imaging (SPECT) with [\(^{123}\)I] N-\(\omega\)-fluoropropyl-2 \(\beta\)-carbomethoxy-3 \(\beta\)-(4-iodophenyl) tropane (FP-CIT). The intensity of tremor (i.e., the power of Electromyography [EMG] signals), but not its frequency, significantly increased during the task. In six subjects, tremor appeared selectively during the task. In a second part of the study, we retrospectively reviewed SPECT with FP-CIT data and confirmed the lack of correlation between dopaminergic loss and tremor by comparing DAT binding values of 82 PD subjects with bilateral tremor (n = 27), unilateral tremor (n = 22), and no tremor (n = 33). This study suggests a role of the LC in Parkinson tremor.
KW  - locus coeruleus
KW  - disease
KW  - basal ganglia
KW  - resting tremor
KW  - functional neuroanatomy
KW  - dopamine
KW  - norepinephrine
KW  - progression
KW  - binding
KW  - rat
KW  - noradrenalin
KW  - parkinson disease
KW  - tremor
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-133955
VL  - 5
IS  - 179
ER  - 
TY  - JOUR
A1  - Isaias, Ioannis U.
A1  - Volkmann, Jens
A1  - Marzegan, Alberto
A1  - Marotta, Giorgio
A1  - Cavallari, Paolo
A1  - Pezzoli, Gianni
T1  - The Influence of Dopaminergic Striatal Innervation on Upper Limb Locomotor Synergies
JF  - PLoS One
N2  - To determine the role of striatal dopaminergic innervation on upper limb synergies during walking, we measured arm kinematics in 13 subjects with Parkinson disease. Patients were recruited according to several inclusion criteria to represent the best possible in vivo model of dopaminergic denervation. Of relevance, we included only subjects with normal spatio-temporal parameters of the stride and gait speed to avoid an impairment of upper limbs locomotor synergies as a consequence of gait impairment per se. Dopaminergic innervation of the striatum was measured by FP-CIT and SPECT. All patients showed a reduction of gait-associated arms movement. No linear correlation was found between arm ROM reduction and contralateral dopaminergic putaminal innervation loss. Still, a partition analysis revealed a 80% chance of reduced arm ROM when putaminal dopamine content loss was >47%. A significant correlation was described between the asymmetry indices of the swinging of the two arms and dopaminergic striatal innervation. When arm ROM was reduced, we found a positive correlation between upper-lower limb phase shift modulation ( at different gait velocities) and striatal dopaminergic innervation. These findings are preliminary evidence that dopaminergic striatal tone plays a modulatory role in upper-limb locomotor synergies and upper-lower limb coupling while walking at different velocities.
KW  - pet
KW  - Parkinsons disease
KW  - basal ganglia
KW  - spinal-cord
KW  - walking
KW  - gait
KW  - arm
KW  - coordination
KW  - movements
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-133976
VL  - 7
IS  - 12
ER  - 
TY  - JOUR
A1  - Brandt, Alexander U.
A1  - Zimmermann, Hanna
A1  - Kaufhold, Falko
A1  - Promesberger, Julia
A1  - Schippling, Sven
A1  - Finis, David
A1  - Aktas, Orhan
A1  - Geis, Christian
A1  - Ringelstein, Marius
A1  - Ringelstein, E. Bernd
A1  - Hartung, Hans-Peter
A1  - Paul, Friedemann
A1  - Kleffner, Ilka
A1  - Dörr, Jan
T1  - Patterns of Retinal Damage Facilitate Differential Diagnosis between Susac Syndrome and MS
JF  - PLoS One
N2  - Susac syndrome, a rare but probably underdiagnosed combination of encephalopathy, hearing loss, and visual deficits due to branch retinal artery occlusion of unknown aetiology has to be considered as differential diagnosis in various conditions. Particularly, differentiation from multiple sclerosis is often challenging since both clinical presentation and diagnostic findings may overlap. Optical coherence tomography is a powerful and easy to perform diagnostic tool to analyse the morphological integrity of retinal structures and is increasingly established to depict characteristic patterns of retinal pathology in multiple sclerosis. Against this background we hypothesised that differential patterns of retinal pathology facilitate a reliable differentiation between Susac syndrome and multiple sclerosis. In this multicenter cross-sectional observational study optical coherence tomography was performed in nine patients with a definite diagnosis of Susac syndrome. Data were compared with age-, sex-, and disease duration-matched relapsing remitting multiple sclerosis patients with and without a history of optic neuritis, and with healthy controls. Using generalised estimating equation models, Susac patients showed a significant reduction in either or both retinal nerve fibre layer thickness and total macular volume in comparison to both healthy controls and relapsing remitting multiple sclerosis patients. However, in contrast to the multiple sclerosis patients this reduction was not distributed over the entire scanning area but showed a distinct sectorial loss especially in the macular measurements. We therefore conclude that patients with Susac syndrome show distinct abnormalities in optical coherence tomography in comparison to multiple sclerosis patients. These findings recommend optical coherence tomography as a promising tool for differentiating Susac syndrome from MS.
KW  - optical coherence tomography
KW  - vasculopathy
KW  - artery occlusion
KW  - hearing loss
KW  - microangiopathy
KW  - brain
KW  - endotheliopathy
KW  - antibodies
KW  - multiple-sclerosis
KW  - retinocochleocerebral
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-134013
VL  - 7
IS  - 6
ER  - 
TY  - JOUR
A1  - Jarius, Sven
A1  - Ruprecht, Klemens
A1  - Wildemann, Brigitte
A1  - Kuempfel, Tania
A1  - Ringelstein, Marius
A1  - Geis, Christian
A1  - Kleiter, Ingo
A1  - Kleinschnitz, Christoph
A1  - Berthele, Achim
A1  - Brettschneider, Johannes
A1  - Hellwig, Kerstin
A1  - Hemmer, Bernhard
A1  - Linker, Ralf A.
A1  - Lauda, Florian
A1  - Hayrettin, Christoph A.
A1  - Tumani, Hayrettin
A1  - Melms, Arthur
A1  - Trebst, Corinna
A1  - Stangel, Martin
A1  - Marziniak, Martin
A1  - Hoffmann, Frank
A1  - Schippling, Sven
A1  - Faiss, Jürgen H.
A1  - Neuhaus, Oliver
A1  - Ettrich, Barbara
A1  - Zentner, Christian
A1  - Guthke, Kersten
A1  - Hofstadt-van Oy, Ulrich
A1  - Reuss, Reinhard
A1  - Pellkofer, Hannah
A1  - Ziemann, Ulf
A1  - Kern, Peter
A1  - Wandinger, Klaus P.
A1  - Bergh, Florian Then
A1  - Boettcher, Tobias
A1  - Langel, Stefan
A1  - Liebetrau, Martin
A1  - Rommer, Paulus S.
A1  - Niehaus, Sabine
A1  - Münch, Christoph
A1  - Winkelmann, Alexander
A1  - Zettl, Uwe K
A1  - Metz, Imke
A1  - Veauthier, Christian
A1  - Sieb, Jörn P.
A1  - Wilke, Christian
A1  - Hartung, Hans P.
A1  - Aktas, Orhan
A1  - Paul, Friedemann
T1  - Contrasting disease patterns in seropositive and seronegative neuromyelitis optica: A multicentre study of 175 patients
JF  - Journal of Neuroinflammation
N2  - Background: The diagnostic and pathophysiological relevance of antibodies to aquaporin-4 (AQP4-Ab) in patients with neuromyelitis optica spectrum disorders (NMOSD) has been intensively studied. However, little is known so far about the clinical impact of AQP4-Ab seropositivity. 
Objective: To analyse systematically the clinical and paraclinical features associated with NMO spectrum disorders in Caucasians in a stratified fashion according to the patients' AQP4-Ab serostatus. 
Methods: Retrospective study of 175 Caucasian patients (AQP4-Ab positive in 78.3%). 
Results: Seropositive patients were found to be predominantly female (p < 0.0003), to more often have signs of co-existing autoimmunity (p < 0.00001), and to experience more severe clinical attacks. A visual acuity of <= 0.1 during acute optic neuritis (ON) attacks was more frequent among seropositives (p < 0.002). Similarly, motor symptoms were more common in seropositive patients, the median Medical Research Council scale (MRC) grade worse, and MRC grades <= 2 more frequent, in particular if patients met the 2006 revised criteria (p < 0.005, p < 0.006 and p < 0.01, respectively), the total spinal cord lesion load was higher (p < 0.006), and lesions >= 6 vertebral segments as well as entire spinal cord involvement more frequent (p < 0.003 and p < 0.043). By contrast, bilateral ON at onset was more common in seronegatives (p < 0.007), as was simultaneous ON and myelitis (p < 0.001); accordingly, the time to diagnosis of NMO was shorter in the seronegative group (p < 0.029). The course of disease was more often monophasic in seronegatives (p < 0.008). Seropositives and seronegatives did not differ significantly with regard to age at onset, time to relapse, annualized relapse rates, outcome from relapse (complete, partial, no recovery), annualized EDSS increase, mortality rate, supratentorial brain lesions, brainstem lesions, history of carcinoma, frequency of preceding infections, oligoclonal bands, or CSF pleocytosis. Both the time to relapse and the time to diagnosis was longer if the disease started with ON (p < 0.002 and p < 0.013). Motor symptoms or tetraparesis at first myelitis and > 1 myelitis attacks in the first year were identified as possible predictors of a worse outcome.
KW  - cerebrospinal-fluid
KW  - intractable hiccup
KW  - extensiv transverse myelitis
KW  - multiple sclerosis
KW  - anti-aquaporin-4 antibody
KW  - NMO-IGG
KW  - aquaporin-4 autoantibodies
KW  - immune-response
KW  - myasthenia gravis
KW  - immunoglobulin-G
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-133636
VL  - 9
IS  - 14
ER  - 
TY  - THES
A1  - Oehler, Steffen Claus
T1  - Deeskalation der Immuntherapie bei Patienten mit Multipler Sklerose
T1  - Deescalation of Immuntherapy in patients with Multiple Sclerosis
N2  - Die vorliegende Arbeit ist die erste, die sich mit der Frage beschäftigt, mit welcher zur Deeskalation eingesetzten Therapie nach Beendigung einer Eskalationstherapie mit Mitoxantron am besten Krankheitsstabilität erreicht werden kann bzw. ob Patienten-/Krankheitscharakteristika existieren, die eine bestimmte Nachfolge-Therapie favorisieren.
Trotz neuer Behandlungsmöglichkeiten der hochaktiven MS mit Fingolimod, Natalizumab und Alemtuzumab hat Mitoxantron im klinischen Alltag nach wie vor einen hohen Stellenwert, so dass die Fragestellung dieser Studie weiter relevant ist. 
Es zeigten sich keine Patientencharakteristika, die auf eine erfolgsversprechende Therapie in der Deeskalationsphase nach Mitoxantron schließen ließen.
Bei Patienten, bei denen während der Eskalation mit Mitoxantron die Dosis reduziert werden konnte, wurden während der Deeskalationstherapie ein stabilerer Verlauf und weniger Therapiewechsel beobachtet. Bei Patienten, die wegen einer rein chronischen Krankheitsprogredienz eskaliert wurden, trat eine Verschlechterung nach Deeskalation häufiger auf als bei denjenigen, welche wegen Schubaktivität eskaliert wurden.
Die Aussagekraft der Daten wird durch die nur niedrige Anzahl der in diese Studie eingeschlossenen Patienten limitiert. Rekrutierungsprobleme stellten die Hauptursache für die geringe Anzahl der Studienteilnehmer dar.
N2  - Deescalation of Immuntherapy in patients with Multiple Sclerosis
KW  - Multiple Sklerose
KW  - Mitoxantron
KW  - Deeskalation
KW  - MS
KW  - Deeskalationstherapie
Y1  - 2015
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-133666
ER  - 
TY  - JOUR
A1  - Ehling, Petra
A1  - Göb, Eva
A1  - Bittner, Stefan
A1  - Budde, Thomas
A1  - Ludwig, Andreas
A1  - Kleinschnitz, Christoph
A1  - Meuth, Sven G.
T1  - Ischemia-induced cell depolarization: does the hyperpolarization-activated cation channel HCN2 affect the outcome after stroke in mice?
JF  - Experimental & Translational Stroke Medicine
N2  - Background
Brain ischemia is known to include neuronal cell death and persisting neurological deficits. A lack of oxygen and glucose are considered to be key mediators of ischemic neurodegeneration while the exact mechanisms are yet unclear. In former studies the expression of two different two-pore domain potassium \((K_{2P})\) channels (TASK1, TREK1) were shown to ameliorate neuronal damage due to cerebral ischemia. In neurons, TASK channels carrying hyperpolarizing \(K^+\) leak currents, and the pacemaker channel HCN2, carrying depolarizing \(I_h\), stabilize the membrane potential by a mutual functional interaction. It is assumed that this ionic interplay between TASK and HCN2 channels enhances the resistance of neurons to insults accompanied by extracellular pH shifts.

Methods
In C57Bl/6 (wildtype, WT), \(hcn2^{+/+}\) and \(hcn2^{-/-}\) mice we used an in vivo model of cerebral ischemia (transient middle cerebral artery occlusion (tMCAO)) to depict a functional impact of HCN2 in stroke formation. Subsequent analyses comprise behavioural tests and hcn2 gene expression assays.

Results
After 60 min of tMCAO induction in WT mice, we collected tissue samples at 6, 12, and 24 h after reperfusion. In the infarcted neocortex, hcn2 expression analyses revealed a nominal peak of hcn2 expression 6 h after reperfusion with a tendency towards lower expression levels with longer reperfusion times. Hcn2 gene expression levels in infarcted basal ganglia did not change after 6 h and 12 h. Only at 24 h after reperfusion, hcn2 expression significantly decreases by ~55%. However, 30 min of tMCAO in hcn2-/- as well as hcn2+/+ littermates induced similar infarct volumes. Behavioural tests for global neurological function (Bederson score) and motor function/coordination (grip test) were performed at day 1 after surgery. Again, we found no differences between the groups.

Conclusions
Here, we hypothesized that the absence of HCN2, an important functional counter player of TASK channels, affects neuronal survival during stroke-induced tissue damage. However, together with a former study on TASK3 these results implicate that both TASK3 and HCN2 which were supposed to be neuroprotective due to their pH-dependency, do not influence ischemic neurodegeneration during stroke in the tMCAO model.
KW  - ischemia
Y1  - 2013
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-131887
VL  - 5
IS  - 16
ER  - 
TY  - JOUR
A1  - Brecht, Isabel
A1  - Weissbrich, Benedikt
A1  - Braun, Julia
A1  - Toyka, Klaus Viktor
A1  - Weishaupt, Andreas
A1  - Buttmann, Mathias
T1  - Intrathecal, Polyspecific Antiviral Immune Response in Oligoclonal Band Negative Multiple Sclerosis
JF  - PLoS One
N2  - Background: Oligoclonal bands (OCB) are detected in the cerebrospinal fluid (CSF) in more than 95% of patients with multiple sclerosis (MS) in the Western hemisphere. Here we evaluated the intrathecal, polyspecific antiviral immune response as a potential diagnostic CSF marker for OCB-negative MS patients. 
Methodology/Principal Findings: We tested 46 OCB-negative German patients with paraclinically well defined, definite MS. Sixteen OCB-negative patients with a clear diagnosis of other autoimmune CNS disorders and 37 neurological patients without evidence for autoimmune CNS inflammation served as control groups. Antibodies against measles, rubella, varicella zoster and herpes simplex virus in paired serum and CSF samples were determined by ELISA, and virus-specific immunoglobulin G antibody indices were calculated. An intrathecal antibody synthesis against at least one neurotropic virus was detected in 8 of 26 (31%) patients with relapsing-remitting MS, 8 of 12 (67%) with secondary progressive MS and 5 of 8 (63%) with primary progressive MS, in 3 of 16 (19%) CNS autoimmune and 3 of 37 (8%) non-autoimmune control patients. Antibody synthesis against two or more viruses was found in 11 of 46 (24%) MS patients but in neither of the two control groups. On average, MS patients with a positive antiviral immune response were older and had a longer disease duration than those without. 
Conclusion: Determination of the intrathecal, polyspecific antiviral immune response may allow to establish a CSF-supported diagnosis of MS in OCB-negative patients when two or more of the four virus antibody indices are elevated.
KW  - MS
KW  - cerebrospinal fluid
KW  - differential diagnosis
KW  - nervous-system
KW  - criteria
KW  - serum
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-134426
VL  - 7
IS  - 7
ER  - 
TY  - JOUR
A1  - Ip, Chi Wang
A1  - Kroner, Antje
A1  - Groh, Janos
A1  - Huber, Marianne
A1  - Klein, Dennis
A1  - Spahn, Irene
A1  - Diem, Ricarda
A1  - Williams, Sarah K.
A1  - Nave, Klaus-Armin
A1  - Edgar, Julia M.
A1  - Martini, Rudolf
T1  - Neuroinflammation by Cytotoxic T-Lymphocytes Impairs Retrograde Axonal Transport in an Oligodendrocyte Mutant Mouse
JF  - PLoS One
N2  - Mice overexpressing proteolipid protein (PLP) develop a leukodystrophy-like disease involving cytotoxic, CD8+ T-lymphocytes. Here we show that these cytotoxic T-lymphocytes perturb retrograde axonal transport. Using fluorogold stereotactically injected into the colliculus superior, we found that PLP overexpression in oligodendrocytes led to significantly reduced retrograde axonal transport in retina ganglion cell axons. We also observed an accumulation of mitochondria in the juxtaparanodal axonal swellings, indicative for a disturbed axonal transport. PLP overexpression in the absence of T-lymphocytes rescued retrograde axonal transport defects and abolished axonal swellings. Bone marrow transfer from wildtype mice, but not from perforin- or granzyme B-deficient mutants, into lymphocyte-deficient PLP mutant mice led again to impaired axonal transport and the formation of axonal swellings, which are predominantly located at the juxtaparanodal region. This demonstrates that the adaptive immune system, including cytotoxic T-lymphocytes which release perforin and granzyme B, are necessary to perturb axonal integrity in the PLP-transgenic disease model. Based on our observations, so far not attended molecular and cellular players belonging to the immune system should be considered to understand pathogenesis in inherited myelin disorders with progressive axonal damage.
KW  - myelin
KW  - experimental autoimmune encephalomyelitis
KW  - degeneration
KW  - axonopathic changes
KW  - neural apoptosis
KW  - nervous system
KW  - motor function
KW  - proteolipid protein gene
KW  - retinal ganglion cells
KW  - granzyme B
KW  - multiple sclerosis
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-134982
VL  - 7
IS  - 8
ER  - 
TY  - THES
A1  - Hullin, Marcus
T1  - Zusammenhang zwischen Raumwahrnehmung, Körperselbstgefühl und Puppenhandillusion bei gesunden Älteren und Patienten mit kortikobasalem Syndrom
T1  - Relationship between spatial attention, the feeling of bodily self and the rubber hand illusion in the healthy elderly and patients with corticobasal syndrome
N2  - Das Körperselbstgefühl (KSG) bezeichnet das Gefühl, einen bestimmten Kör-perteil als dem eigenen Körper zugehörig zu empfinden. Es erscheint stabil und nicht störbar, lässt sich jedoch bei den meisten Menschen experimentell beein-flussen. Ein Beispiel hierfür ist die Puppenhandillusion (PHI), bei der die nicht sichtbare eigene Hand des Probanden und eine sichtbare Plastikhand in glei-cher Stellung an den gleichen Fingerstellen synchron mit zwei Pinseln bestri-chen wird, wodurch die Wahrnehmung entsteht, die Plastikhand sei die eigene. Veränderungen des KSG können jedoch auch im Rahmen neurodegenerativer Erkrankungen vorkommen. So nimmt beim kortikobasalen Syndrom (CBS) etwa die Hälfte der Patienten im Krankheitsverlauf einen Arm und seine Bewegungen als fremd war ("Alien-limb“-Phänomen). Das CBS beginnt oft einseitig und ist durch eine rasch fortschreitende, akinetisch-rigide Parkinson-Symptomatik, aber auch durch kortikale Funktionsstörungen gekennzeichnet, so dass es ne-ben einer Störung des KSG auch zu einer Störung der räumlichen Aufmerk-samkeit (Hemineglect) kommt. Bislang wurde der Zusammenhang zwischen Raumwahrnehmung, KSG und PHI bei gesunden älteren Menschen noch nicht systematisch untersucht. Ebenso wenig war bisher bekannt, inwieweit das KSG bei CBS-Patienten durch die PHI modulierbar ist. Wir untersuchten 65 gesunde ältere Probanden (60 - 90 Jahre) ohne neurologi-sche Vorerkrankungen sowie zehn Patienten zwischen 59 und 77 Jahren mit wahrscheinlichem oder möglichem CBS. Den kognitiven und orientierend seeli-schen Zustand eruierten wir mit Hilfe des PANDA- und des Uhrentests, die Raumwahrnehmung testeten wir mittels des Milner-Landmark-Tests sowie des Letter-Cancellation-Tests, das spontane Körperselbstgefühl wurde mittels eines Fragebogens erfasst. Der PHI-Versuch wurde mit synchroner sowie asynchro-ner taktiler Stimulation durchgeführt, das Auftreten eines Selbstgefühls für die Plastikhand wurde subjektiv über spontane Äußerungen und einen etablierten Fragebogen, objektiv über den sog. propriozeptiven Drift der stimulierten Hand erfasst. Unter den Kontrollprobanden fanden sich 12% mit einer wahrscheinlichen De-menz, wohingegen dies bei 80% der CBS-Patienten der Fall war. Im Milner-Landmark-Test zeigte sich bei den Kontrollprobanden eine Überschätzung des rechten Segmentes einer mittig geteilten Linie, entsprechend einem milden Hemineglect, bei den CBS-Patienten konnte keine einheitliche Tendenz festge-stellt werden. Das spontane Körperselbstgefühl stellte sich bei nahezu allen Probanden als intakt dar, während sich bei vier Patienten mit CBS Hinweise auf aktuelle oder intermittierende Störungen desselben ergaben. Die Puppenhandil-lusion war in der Gruppe gesunder Älterer bei synchroner Stimulation auslös-bar, nicht jedoch bei asynchroner Stimulation. Eine Lateralisierungstendenz zeigte sich nicht. Darüber hinaus konnte bei den Probanden eine positive Korre-lation zwischen dem propriozeptiven Drift der linken Hand nach synchroner Stimulation und dem Hemineglect nach links gefunden werden. Bei den CBS-Patienten fand sich unabhängig von der Stimulationsart (synchron oder asyn-chron) eine erhöhte Bereitschaft, die linke Puppenhand ins eigene Körperbild zu integrieren. Das Auftreten der PHI bei gesunden älteren Probanden ist vergleichbar mit den Daten jüngerer Probandengruppen. Hinweise auf eine hemisphärische Laterali-sierungstendenz der PHI ergaben sich nicht, jedoch scheint der in dieser Grup-pe festgestellte leichtgradige Hemineglect nach links den multisensorischen Prozess zu beeinflussen, eine künstliche Hand in das eigene Körperschema zu integrieren. Bei den CBS-Patienten war die PHI unabhängig vom Stimulations-modus links besser auslösbar als rechts, was mit vorwiegend rechtshemisphä-rischen krankheitsbedingten Veränderungen des multisensorischen Integrati-onsprozesses vereinbar ist.
N2  - The feeling of bodily self describes the perception of a particular body part as belonging to the own body. While it appears stable and nearly undisturbable to us, it can be easily modulated experimentally in most people. During the “rubber hand illusion” (RHI) paradigm, a well-known example for such an experimental manipulation, synchronous brushstrokes are applied to a subject´s hidden real hand and an aligned plastic hand. This results in the perception that the plastic hand is one´s own hand. An impairment of the feeling of bodily self can also occur spontaneously in the course of neurodegenerative diseases. About half of the patients with corticobasal syndrome (CBS) perceive one arm, including its movements, as strange ("alien-limb" phenomenon). CBS usually starts unilaterally and is characterized by progressive akinetic-rigid symptoms as well as cortical dysfunction. This may result in an impairment of the feeling of bodily self and of spatial attention (hemineglect). So far, the relationship between spatial attention, the feeling of bodily self and the rubber hand illusion in the healthy elderly has not been assessed systematically. Moreover, it was unknown whether the RHI may be used to modulate the feeling of bodily self in CBS patients. Sixty-five elderly subjects (age 60 to 90 years) without neurological history and ten patients aged between 59 and 77 years with a diagnosis of probable or possible CBS were assessed in this study. We used the PANDA and the clock-drawing test to assess the cognitive condition. The PANDA also includes a rough assessment for depressive symptoms. Spatial attention was assessed by the Milner landmark task as well as by the letter cancellation test; the spontaneous feeling of limb ownership was inquired by a questionnaire. The RHI experiment was conducted with synchronous and asynchronous tactile stimlation, respectively. The appearance of the illusion was assessed both subjectively by spontaneous statements and by a well established questionnaire, and objectively by the so-called proprioceptive drift of the stimulated hand. We found probable dementia in 12% of healthy controls, but in 80% of CBS-patients. The Milner's landmark test showed an asymmetry of spatial attention in the control group, with overestimation of the right segment of the mid-bisected line, according to a mild hemineglect, whereas there was no clear trend in CBS patients. In all healthy subjects except for one, the spontaneous feeling of limb-ownership was unimpaired, whereas we found evidence of an impairment in most CBS patients. In the control group, subjective responses indicated an experience of the RHI during synchronous, but not asynchronous stimulation, without lateralization. The proprioceptive drift towards the plastic hand following synchronous stroking was comparable between sides. With the left hand, however, the proprioceptive drift correlated with the rightward bias of spatial attention. In CBS patients, we found an increased disposition to integrate the left rubber hand into their body schema irrespective of the kind of stimulation (synchronous or asynchronous). The occurrence of the RHI in healthy, elderly subjects is comparable with data of younger subject groups. Neither subjective nor objective measures of the RHI were lateralized on group level. However, asymmetric spatial attention may influence the multisensory process of embodiment of an artificial hand into one's body schema. In CBS patients, the RHI was perceived stronger with left hand stimulation, which is in line with a pronounced right-hemispheric dysfunction of multisensory integration caused by CBS pathology.
KW  - Raumwahrnehmung
KW  - Körperwahrnehmung
KW  - Raumwahrnehmung
KW  - Körperselbstgefühl
KW  - Puppenhandillusion
KW  - Ältere
KW  - Kortikobasales Syndrom
KW  - spatial attention
KW  - feeling of bodily self
KW  - rubber hand illusion
KW  - elderly
KW  - corticobasal syndrome
Y1  - 2016
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-134291
ER  - 
TY  - JOUR
A1  - Burlina, Alessandro P.
A1  - Sims, Katherine B.
A1  - Politei, Juan M.
A1  - Bennett, Gary J.
A1  - Baron, Ralf
A1  - Sommer, Claudia
A1  - Moller, Anette Torvin
A1  - Hilz, Max J.
T1  - Early diagnosis of peripheral nervous system involvement in Fabry disease and treatment of neuropathic pain: the report of an expert panel
JF  - BMC Neurology
N2  - Background: 

Fabry disease is an inherited metabolic disorder characterized by progressive lysosomal accumulation of lipids in a variety of cell types, including neural cells. Small, unmyelinated nerve fibers are particularly affected and small fiber peripheral neuropathy often clinically manifests at young age. Peripheral pain can be chronic and/or occur as provoked attacks of excruciating pain. Manifestations of dysfunction of small autonomic fibers may include, among others, impaired sweating, gastrointestinal dysmotility, and abnormal pain perception. Patients with Fabry disease often remain undiagnosed until severe complications involving the kidney, heart, peripheral nerves and/or brain have arisen. 

Methods: 

An international expert panel convened with the goal to provide guidance to clinicians who may encounter unrecognized patients with Fabry disease on how to diagnose these patients early using simple diagnostic tests. A further aim was to offer recommendations to control neuropathic pain. 

Results: 

We describe the neuropathy in Fabry disease, focusing on peripheral small fiber dysfunction - the hallmark of early neurologic involvement in this disorder. The clinical course of peripheral pain is summarized, and the importance of medical history-taking, including family history, is highlighted. A thorough physical examination (e. g., angiokeratoma, corneal opacities) and simple non-invasive sensory perception tests could provide clues to the diagnosis of Fabry disease. Reported early clinical benefits of enzyme replacement therapy include reduction of neuropathic pain, and adequate management of residual pain to a tolerable and functional level can substantially improve the quality of life for patients. 

Conclusions: 

Our recommendations can assist in diagnosing Fabry small fiber neuropathy early, and offer clinicians guidance in controlling peripheral pain. This is particularly important since management of pain in young patients with Fabry disease appears to be inadequate.
KW  - Enzyme replacement therapy
KW  - Quality of life
KW  - Small-fiber neuropathy
KW  - Rochester diabetic neuropathy
KW  - Randomized controlled trial
KW  - Agalsidase beta therapy
KW  - Outcome survey
KW  - Pharmacological management
KW  - Clinical manifestations
KW  - Alpha galactosidase
KW  - Diagnosis
KW  - Fabry
KW  - Disease
KW  - Neuropathy
KW  - Pain
KW  - Treatment
Y1  - 2011
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-135309
VL  - 11
IS  - 61
ER  - 
TY  - JOUR
A1  - Dupuis, Luc
A1  - Dengler, Reinhard
A1  - Heneka, Michael T.
A1  - Meyer, Thomas
A1  - Zierz, Stephan
A1  - Kassubek, Jan
A1  - Fischer, Wilhelm
A1  - Steiner, Franziska
A1  - Lindauer, Eva
A1  - Otto, Markus
A1  - Dreyhaupt, Jens
A1  - Grehl, Torsten
A1  - Hermann, Andreas
A1  - Winkler, Andrea S.
A1  - Bogdahn, Ulrich
A1  - Benecke, Reiner
A1  - Schrank, Bertold
A1  - Wessig, Carsten
A1  - Grosskreutz, Julian
A1  - Ludolph, Albert C.
T1  - A Randomized, Double Blind, Placebo-Controlled Trial of Pioglitazone in Combination with Riluzole in Amyotrophic Lateral Sclerosis
JF  - PLoS One
N2  - Background: Pioglitazone, an oral anti-diabetic that stimulates the PPAR-gamma transcription factor, increased survival of mice with amyotrophic lateral sclerosis (ALS). 
Methods/Principal Findings: We performed a phase II, double blind, multicentre, placebo controlled trial of pioglitazone in ALS patients under riluzole. 219 patients were randomly assigned to receive 45 mg/day of pioglitazone or placebo (one: one allocation ratio). The primary endpoint was survival. Secondary endpoints included incidence of non-invasive ventilation and tracheotomy, and slopes of ALS-FRS, slow vital capacity, and quality of life as assessed using EUROQoL EQ-5D. The study was conducted under a two-stage group sequential test, allowing to stop for futility or superiority after interim analysis. Shortly after interim analysis, 30 patients under pioglitazone and 24 patients under placebo had died. The trial was stopped for futility; the hazard ratio for primary endpoint was 1.21 (95% CI: 0.71-2.07, p = 0.48). Secondary endpoints were not modified by pioglitazone treatment. Pioglitazone was well tolerated. 
Conclusion/Significance: Pioglitazone has no beneficial effects on the survival of ALS patients as add-on therapy to riluzole.
KW  - ALS
KW  - transgenic mouse model
KW  - central nervous system
KW  - nonalcoholic steatohepatitis
KW  - PPAR-gamme
KW  - hexanucleotide repeat
KW  - disease progression
KW  - delays progression
KW  - SOD1 mutations
KW  - monocycline
Y1  - 2012
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-130255
VL  - 7
IS  - 6
ER  - 
TY  - JOUR
A1  - Golombeck, Stefanie Kristin
A1  - Wessig, Carsten
A1  - Monoranu, Camelia-Maria
A1  - Schütz, Ansgar
A1  - Solymosi, Laszlo
A1  - Melzer, Niko
A1  - Kleinschnitz, Christoph
T1  - Fatal atypical reversible posterior leukoencephalopathy syndrome: a case report
JF  - Journal of Medical Case Reports
N2  - Introduction: Reversible posterior leukoencephalopathy syndrome – a reversible subacute global encephalopathy clinically presenting with headache, altered mental status, visual symptoms such as hemianopsia or cortical blindness, motor symptoms, and focal or generalized seizures – is characterized by a subcortical vasogenic edema symmetrically affecting posterior brain regions. Complete reversibility of both clinical signs and magnetic resonance imaging lesions is regarded as a defining feature of reversible posterior leukoencephalopathy syndrome. Reversible posterior leukoencephalopathy syndrome is almost exclusively seen in the setting of a predisposing clinical condition, such as pre-eclampsia, systemic infections, sepsis and shock, certain autoimmune diseases, various malignancies and cytotoxic chemotherapy, transplantation and concomitant immunosuppression (especially with calcineurin inhibitors) as well as episodes of abrupt hypertension. We describe for the first time clinical, radiological and histological findings in a case of reversible posterior leukoencephalopathy syndrome with an irreversible and fatal outcome occurring in the absence of any of the known predisposing clinical conditions except for a hypertensive episode.
Case presentation: A 58-year-old Caucasian woman presented with a two-week history of subacute and progressive occipital headache, blurred vision and imbalance of gait and with no evidence for raised arterial blood pressure during the two weeks previous to admission. Her past medical history was unremarkable except for controlled arterial hypertension. Cerebral magnetic resonance imaging demonstrated cortical and subcortical lesions with combined vasogenic and cytotoxic edema atypical for both venous congestion and arterial infarction. Routine laboratory and cerebrospinal fluid parameters were normal. The diagnosis of reversible posterior leukoencephalopathy syndrome was established. Within hours after admission the patient showed a rapidly decreasing level of consciousness, extension and flexion synergisms, bilaterally extensor plantar responses and rapid cardiopulmonary decompensation requiring ventilatory and cardiocirculatory support. Follow-up cerebral imaging demonstrated widespread and confluent cytotoxic edematous lesions in different arterial territories, global cerebral swelling, and subsequent upper and lower brainstem herniation. Four days after admission, the patient was declared dead because of brain death.
Conclusion: This case demonstrates that fulminant and fatal reversible posterior leukoencephalopathy syndrome may occur spontaneously, that is, in the absence of any of the known predisposing systemic conditions.
KW  - reversible posterior leukoencephalopathy syndrome
KW  - generalized cerebral edema
KW  - cerebral autoregulation
KW  - blood pressure
Y1  - 2013
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-129456
VL  - 7
IS  - 14
ER  - 
TY  - JOUR
A1  - Fluri, Felix
A1  - Heinen, Florian
A1  - Kleinschnitz, Christoph
T1  - Intravenous Thrombolysis in a Stroke Patient Receiving Rivaroxaban
JF  - Cerebrovascular Disease Extra
N2  - No abstract available.
KW  - anticoagulants
KW  - intravenous thrombolysis
KW  - acute ischemic stroke
Y1  - 2013
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-128816
VL  - 2013
IS  - 3
ER  - 
TY  - JOUR
A1  - Linker, Ralf A.
A1  - Magnus, Tim
A1  - Korn, Thomas
A1  - Kleinschnitz, Christoph
A1  - Meuth, Sven G.
T1  - Report on the 5‘th scientific meeting of the “Verein zur Förderung des Wissenschaftlichen Nachwuchses in der Neurologie” (NEUROWIND e.V.) held in Motzen, Germany, Oct. 25th – Oct. 27th, 2013
JF  - Experimental & Translational Stroke Medicine
N2  - From october 25th - 27th 2013, the 5th NEUROWIND e.V. meeting was held in Motzen, Brandenburg, Germany. This year more than 60 doctoral students and postdocs from over 25 different groups working in German university hospitals or research institutes attended the meeting to discuss their latest findings in the fields of neuroimmunology, neurodegeneration and neurovascular research. All participants appreciated the stimulating environment in Motzen, Brandenburg, and people took the opportunity for scientific exchange, discussion about ongoing projects and already started further collaborations. Like in the previous years, the symposium was regarded as a very well organized platform to support research of young investigators in Germany.
According to the major aim of NEUROWIND e.V. to support younger researchers in Germany the 3rd NEUROWIND YOUNG SCIENTIST AWARD for experimental neurology was awarded to Ruth Stassart working in the group of Klaus Armin Nave and Wolfgang Brück (MPI Göttingen and Department of Neuropathology, Göttingen Germany). The successful work was published in Nature Neuroscience entitled “A role for Swann cell-derived neuregulin-1 in remyelination”. This outstanding paper deals with the function of Schwann cell neuregulin as an endogenous factor for myelin repair. The award is endowed with 20.000 Euro sponsored by Merck Serono GmbH, Darmstadt, Germany (unrestricted educational grant). This year’s keynote lecture was given by Albert Ludolph, Head of the Department of Neurology at the University Clinic of Ulm. Dr. Ludolph highlighted the particular role of individual scientists for the development of research concepts in Alzheimer´s disease (AD) and frontotemporal dementia (FTD).
KW  - NEUROWIND
Y1  - 2013
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-129230
VL  - 5
IS  - 15
ER  - 
TY  - JOUR
A1  - Ehling, Petra
A1  - Göb, Eva
A1  - Bittner, Stefan
A1  - Budde, Thomas
A1  - Ludwig, Andreas
A1  - Kleinschnitz, Christoph
A1  - Meuth, Sven G.
T1  - Ischemia-induced cell depolarization: does the hyperpolarization-activated cation channel HCN2 affect the outcome after stroke in mice?
JF  - Experimental & Translational Stroke Medicine
N2  - Background
Brain ischemia is known to include neuronal cell death and persisting neurological deficits. A lack of oxygen and glucose are considered to be key mediators of ischemic neurodegeneration while the exact mechanisms are yet unclear. In former studies the expression of two different two-pore domain potassium \((K_{2P})\) channels (TASK1, TREK1) were shown to ameliorate neuronal damage due to cerebral ischemia. In neurons, TASK channels carrying hyperpolarizing \(K^+\) leak currents, and the pacemaker channel HCN2, carrying depolarizing Ih, stabilize the membrane potential by a mutual functional interaction. It is assumed that this ionic interplay between TASK and HCN2 channels enhances the resistance of neurons to insults accompanied by extracellular pH shifts.

Methods
In C57Bl/6 (wildtype, WT), \(hcn2^{+/+}\) and \(hcn2^{-/-}\) mice we used an in vivo model of cerebral ischemia (transient middle cerebral artery occlusion (tMCAO)) to depict a functional impact of HCN2 in stroke formation. Subsequent analyses comprise behavioural tests and hcn2 gene expression assays.

Results
After 60 min of tMCAO induction in WT mice, we collected tissue samples at 6, 12, and 24 h after reperfusion. In the infarcted neocortex, hcn2 expression analyses revealed a nominal peak of hcn2 expression 6 h after reperfusion with a tendency towards lower expression levels with longer reperfusion times. Hcn2 gene expression levels in infarcted basal ganglia did not change after 6 h and 12 h. Only at 24 h after reperfusion, hcn2 expression significantly decreases by ~55%. However, 30 min of tMCAO in hcn2-/- as well as hcn2+/+ littermates induced similar infarct volumes. Behavioural tests for global neurological function (Bederson score) and motor function/coordination (grip test) were performed at day 1 after surgery. Again, we found no differences between the groups.

Conclusions
Here, we hypothesized that the absence of HCN2, an important functional counter player of TASK channels, affects neuronal survival during stroke-induced tissue damage. However, together with a former study on TASK3 these results implicate that both TASK3 and HCN2 which were supposed to be neuroprotective due to their pH-dependency, do not influence ischemic neurodegeneration during stroke in the tMCAO model.
KW  - neurology
Y1  - 2013
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-129240
VL  - 5
IS  - 16
ER  - 
TY  - THES
A1  - Stallforth, Sabine
T1  - Unterschiedliche Wirkungen der TNF-alpha-Rezeptoren auf De- und Regeneration peripherer NervenEine Studie an TNF-alpha-Rezeptor-Knockoutmäusen in zwei verschiedenen Tiermodellen für Nervenläsionen
T1  - Different effects of TNF-alpha-receptors on de- and regeneration of the peripheral nerveA study in TNF-alpha-receptor-knockout-mice in two different models of nerve injury
N2  - Noch immer ist die Behandlung von Neuropathien mit den gängigen therapeutischen Mitteln für viele Patienten sehr unbefriedigend. Als erfolgsversprechender therapeutischer Ansatz werden zur Zeit Wege erforscht, welche direkt in die molekularen Entstehungsmechanismen pathologischer Veränderungen und regenerationsfördernder Mechanismen eingreifen, um dadurch eine Heilung von Nervenschäden zu ermöglichen. Bisher sind die Erkenntnisse über diese Mechanismen nicht vollständig genug, um daraus eine sichere Behandlungsmöglichkeit abzuleiten. Wegweisende Erkenntnisse deuten sich allerdings durch Studien von unterschiedlichen Vertretern des Zytokinnetzwerkes an - darunter auch TNF-alpha - welche als molekulare Ursache neuropathischer Veränderungen diskutiert werden. In dieser Studie wurde an Knockoutmäusen der Einfluss des jeweiligen TNF-alpha-Rezeptors auf morphologische Veränderungen nach CCI (Chronic constriction injury) und Crush-Verletzung des N. ischiadicus untersucht. Nach 3,7,15 und 36 Tagen (CCI) bzw. 3,7 und 28 Tagen (Crush) wurden in Methylenblau gefärbten Semidünnschnitten intakte und degenerierte Nervenfasern, Makrophagen, Angioproliferation, Ödembildung udn Veränderung des Anteils nicht neuronaler Zellen lichtmikroskopisch beurteilt. Zusätzlich wurden Mac-1+ Makrophagen immunzytochemisch erfasst. Die Ergebnisse zeigten in beiden Modellen und bei beiden Knockouttypen eine starke axonale Schädigung, die von einer großen endoneuroalen Makrophagenansammlung begleitet war. Bei TNF-R1-/- Mäusen war eine stärkere und verlängerte Degeneration mit entsprechend höheren Makrophagenzahlen sichtbar. In den Immunzytochemischen Färbungen wiesen die TNF-R1-/- Mäuse hingegen den geringsten Makropahgenanteil auf.Trotz der starken Schädigung war die anschließende Regeneration im Gegensatz zu WT und TNF-R2-/- Mäusen besser. Die Ödembildung war bei den TNF-R2-/- nach CCI besonders stark ausgeprägt und von einer schlechten Regeneration gefolgt. Während die gefundenen Daten auf eine Beteiligung beider Rezeptoren während degenerativer Prozesse hindeuten, scheint insbesondere TNF-R2 regenerationsfördernde Effekte zu vermitteln.
N2  - Current Treatment of neuropathic disorders is still dissatisfactory for many patients. A promising approach is the investigation of agents that directly interfere with molecular development of pathologic changes and regeneration. Up to now, consolidated findings of the underlying mechanisms are not yet sufficent to allow therapeutic intervention. Pathbreaking findings come from studies investigating different agents of the cytokine network - as e.g. TNF-alpha - that are discussed as molecular cause of neuropathic changes. This study investigated the influence of both TNF-alpha-receptors on morphologic changes after CCI (chronic constriction injury) and crush-injury of the sciatic nerve of TNF-R-knockoutmice. After 3,7,15 and 36 days (CCI), and 3,7 and 28 respectively (Crush),intact and degenerating nerve fibers, macrophages, angioproliferation, development of edema and changes in the amount of non-neuronal cells were acquired by light microscopy of toluidin-stained semithin sections. Additionally Mac-1+ macrophages were acquired via immuncytochemically stained sections. The results showed strong axonal damage in both knockout-types accompanied by large amounts of endoneurial macrophages. TNF-R1-/-mice showed a longer degeneration phase including respectively higher amounts of macrophages. In contrast the TNF-R1-/-mice revealed the fewest amount of macrophages in immunocytochemical sections. Despite the strong damage better nerve regeneration was observed compared to WT and TNF-R2-/-mice. Formation of edema was pronounced in TNF-R2-/- after CCI and followed by poorly regeneration. Whereas these findings point to a participation of both receptors in degeneration, TNF-R2 seems to support regeneration.
KW  - peripheral nerve
KW  - TNF
KW  - TNF-R1
KW  - TNF-R2
KW  - TNF-receptors
KW  - knockout
KW  - Crush
KW  - CCI
KW  - sciatic nerve injury
KW  - Cytokines
KW  - regeneration
KW  - degeneration
KW  - Degeneration
KW  - Regeneration
KW  - TNF-Rezeptor-1
KW  - TNF-Rezeptor-2
KW  - degeneration
KW  - regeneration
KW  - TNF-receptor-1
KW  - TNF-receptor-2
Y1  - 2007
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-24808
ER  - 
TY  - THES
A1  - He, Lan
T1  - Small fiber involvement in Fabry's disease
N2  - Aim of Investigation: The neurological manifestations of Fabry’s disease, a rare, X-linked, multisystem disorder caused by alpha-galactosidase A deficiency and globotriosylceramide (Gb3) accumulation, include both peripheral and central nervous system symptoms. Here we evaluated a prospectively recruited cohort of patients with Fabry’s disease for pain, small nerve fiber function, and skin innervation. Methods: 66 patients (31 male and 35 female) were enrolled&#65292;31 patients were on ERT. All patients underwent quantitative sensory testing (QST), electrophysiological examination, and extra- and transcranial Doppler sonography. For pain and mood assessment standardized questionnaires were used. Skin biopsies were performed at the left distal leg in 38 patients for intraepidermal nerve fiber density (IENFD) assessment. Results: Age at examination did not differ significantly between women (40.2+/-16.2 years) and men (38.9+/-13.8; n.s.). 29/31 male and 19/35 female patients complained of acroparesthesias or neuropathic pain. QST abnormalities indicative of small fiber impairment were found in 26/31 male and 28/35 female patients. Electrophysiological examination of large fibers and autonomic fibers revealed pathological findings in 11/31 male and 3/35 female patients. All patients had normal Doppler sonography results. Indicators for depression were present in 14/31 male and 10/35 female patients. 20/31 male and 18/35 female patients had a skin biopsy, the IENFD was significantly reduced in male (2.0+/-2.8 fibers/mm) compared with female patients (6.7 +/- 4.4 fibers/mm). In 10 patients free from neurological symptoms, QST and IENFD abnormalities were still detected. Follow up examination after one year in 12 patients under ERT (2.1+/-1.7 years) showed improvement in some symptoms and in QST and neurophysiology in six patients with normal renal function. 20/35 female patients older than 40 y had concomitant diseases, while none of the 18 younger female patients did. The corresponding radio in male patients was 5/19 (>=40y) and 2/13 (<40y) respectively. Conclusions: Neuropathic pain and sensory deficits of the distal extremities are common in patients with Fabry’s disease. QST and IENFD analysis are important for early diagnosis of nerve involvement in Fabry’s disease. Small fiber function may improve under ERT in patients without severe renal impairment.
KW  - Fabry’s disease
KW  - neuropathic pain
KW  - QST
KW  - IENFD
KW  - ERT
KW  - Fabry’s disease
KW  - neuropathic pain
KW  - QST
KW  - IENFD
KW  - ERT
Y1  - 2009
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-32844
ER  - 
TY  - THES
A1  - Yu-Hwa, Huang
T1  - The Role of HLA-G-expressing Regulatory T cells in Multiple Sclerosis: A Perspective of Beneficial Inflammation in the Central Nervous System Inflammation
T1  - Die Rolle HLA-G-exprimierender regulatorischer T-Zellen in multipler Sklerose: Möglichkeit einer hilfreichen Entzündung bei Entzündungserkrankung des zentralen  Nervensystems
N2  - Die Regulation von Effektor-T-Zellen ist ein wichtiger Mechanismus zur Kontrolle organspezifischer Entzündungen. Dabei sind regulatorische T-Zellen (Treg) maßgeblich an der Aufrechterhaltung peripherer Immuntoleranz und parenchymaler Immunhomöostase beteiligt. Eine neue Population von humanen, natürlich vorkommenden Treg Zellen wurde durch ihre konstitutive Expression des immuntolerogenen Moleküls HLA-G identifiziert. Im ersten Teil dieser Arbeit wurden die Mechanismen, durch die CD4+ HLA-Gpos Treg Zellen ihre Zielzellen (autologe HLA-Gneg T-Zellen) modulieren, aufgeklärt. Unter Verwendung eines Suppressionsansatzes in Abwesenheit von antigenpräsentierenden Zellen (APC) wurden T-T-Zell-Interaktionen, die die Proliferation von HLA-Gneg T-Zellen hemmen, demonstriert. Diese Suppression, die durch die Stimulierung des T-Zell-Rezeptors auf HLA-Gpos Treg Zellen verstärkt wurde, war unabhängig vom Zell-Zell-Kontakt. Die HLA-Gneg T-Zellen erlangten nach Entfernung der HLA-Gpos Treg Zellen und einer erneuten Stimulierung ihrer T-Zell- Rezeptoren ihre Fähigkeit zur Proliferation wieder. Dies wies auf die Umkehrbarkeit dieser Suppression hin. Darüber hinaus war die HLA-Gpos Treg-vermittelte Suppression entscheidend von der IL-10- Sekretion, nicht jedoch von TGF-&#946; abhängig. Zusammengefasst beschreibt dieser Teil der Arbeit eine detaillierte Charakterisierung der Mechanismen, wie HLA-Gpos Treg HLA-Gneg TZellen supprimieren. Das tiefere Verständnis der Wirkmechanismen von HLA-Gpos Treg könnte in therapeutischen Strategien verwendet werden, in denen die regulatorische Funktion der T-Zell-Suppression verstärkt oder moduliert werden soll. Im zweiten Teil dieser Arbeit wurde die potenzielle Rolle von HLA-Gpos Treg bei der Multiplen Sklerose (MS) untersucht, einer klassischen Autoimmunerkrankung des Zentralnervensystems (ZNS). Im Gegensatz zu Vergleichspatienten mit nicht-entzündlichen Erkrankungen konnte im Liquor von MS Patienten eine erhöhte Anzahl von HLA-Gpos Treg gefunden werden. Diese aus dem Liquor isolierten HLA-Gpos Treg wiesen phänotypische Merkmale von zentralen Gedächtnis-T-Zellen (CD45RA- CD27+) auf, exprimierten den Aktivierungsmarker ICOS sowie deutlich höhere Level des Chemokinrezeptors (CCR) CCR5 und agierten als starke Suppressoren der autologen CD4+ T-Zellproliferation. Durch Verwendung eines in vitro Modells der humanen Bluthirnschranke konnte demonstriert werden, dass HLA-Gpos Treg eine starke Neigung zur Migration haben, die durch die CCR5- Liganden MIP1&#945; und RANTES, nicht jedoch durch MIP3&#946; (Ligand von CCR7) unterstützt wird. Diese Chemokin-induzierte Migration von HLA-Gpos Treg war auch mit einer Steigerung der suppressiven Kapazität nach Zelltransmigration assoziiert. Im Gegensatz zu CD4+CD25+, FoxP3-exprimierenden Treg zeigten HLA-Gpos Treg von MS-Patienten keine beeinträchtigte Funktionalität. Dies deutet auf eine selektive Rekrutierung von HLA-Gpos Treg zu Entzündungsherden im ZNS und ihre Beteiligung an der Bekämpfung der destruktiven Entzündung hin. Die Ergebnisse dieser Studien tragen zum weitergehenden Verständnis der Rolle und Funktion HLA-Gpos Treg Zellen bei und stellen somit ein wichtiges pathophysiologisches Beispiel „gutartiger“ T-Zell-Entzündung während der ZNS Autoimmunität dar, das sowohl aus pathophysiologischer als auch therapeutischer Sicht interessant ist.
N2  - Regulation of effector T cells is an important mechanism to control organ-specific inflammation. Thereby regulatory T cells (Treg cells) are essential for maintaining peripheral immune tolerance and for establishing parenchyma immune homeostasis. A novel population of natural human Treg characterized by the constitutive expression of the immune-tolerogenic human HLA-G molecule has been identified. In the first part of the study, we elucidated the mechanism(s) by which CD4+ HLA-Gpos Treg modulates their cellular targets namely autologous HLA-G negative responder T cells (HLAGneg Tresp). Using a suppression system free of antigen-presenting cells (APC), we demonstrate a T-T cell interaction resulting in suppression of HLA-Gneg Tresp. We could also show that this suppression was independent of cell-cell contact. Importantly, stimulus of T cell receptor (TCR) on HLA-Gpos Treg facilitated their suppressive capacity. We also observed that removal of HLA-Gpos Treg from the established co-cultures could restore the ability of HLA-Gneg Tresp to proliferate upon TCR re-stimulation, indicating that the suppression was reversible. Further, HLA-Gpos Treg–mediated suppression was critically depending on the secretion of IL-10 but not TGF-&#946;. Taken together, this part of the work provides an in-depth characterization of the mechanisms of how HLA-Gpos Treg suppresses T responder cells in direct T-T interactions. Understanding the suppressive mechanism used by HLA-Gpos Treg may help to develop therapeutic strategies to modulate regulatory arms of T-cell suppression. In the second part of this study, the potential role of HLA-Gpos Treg in the pathophysiological process of Multiple Sclerosis (MS), a prototypic autoimmune inflammatory central nervous system (CNS), has been investigated. We found that HLA-Gpos Treg are enriched in the cerebrospinal fluid (CSF) from MS patients, but not in non-inflammatory controls. CSFderived HLA-Gpos Treg showed predominance of central memory (CD45RA-CD27+) phenotype, exhibited markers of activation (ICOS), and had significantly higher expression of the inflammatory chemokine receptor CCR5. Importantly, these cells demonstrated as potent suppressors to autologous CD4+ T-cell proliferation. Using an in vitro model of human blood brain barrier, we showed that HLA-Gpos Treg have a strong propensity to migrate, which could be facilitated by MIP1&#945; and RANTES (ligands of CCR5) but not MIP3&#946; (a ligand of CCR7). The HLA-Gpos Treg migration triggered by chemokines was also associated with a gain of suppressive capacity upon cellular transmigration. In contrast to CD4+CD25+ naturally occurring FoxP3-expressing Treg, HLA-Gpos Treg from patients with MS did not exhibit impaired function, suggesting that HLA-Gpos Treg are selectively recruited to the sites of CNS inflammation in an effort to combat destructive inflammation during MS. Our results contribute to the understanding of the role and function of HLA-Gpos Treg and provide an important example of “beneficial” T-cell inflammation in CNS autoimmunity- interesting both from a patho/-physiological and a therapeutically point of view.
KW  - Regulatorische T-Zellen
KW  - Multiplen Sklerose
KW  - HLA-G
KW  - Zentralnervensystems
KW  - Chemokinrezeptors
KW  - Regulatory T cells
KW  - Multiple Sclerosis
KW  - HLA-G
KW  - Central Nervous System
KW  - Chemokine Receptor
Y1  - 2009
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-39957
ER  - 
TY  - JOUR
A1  - Giordano, Rosaria
A1  - Canesi, Margherita
A1  - Isalberti, Maurizio
A1  - Isaias, Ioannis Ugo
A1  - Montemurro, Tiziana
A1  - Viganò, Mariele
A1  - Montelatici, Elisa
A1  - Boldrin, Valentina
A1  - Benti, Riccardo
A1  - Cortelezzi, Agostino
A1  - Fracchiolla, Nicola
A1  - Lazzari, Lorenza
A1  - Pezzoli, Gianni
T1  - Autologous mesenchymal stem cell therapy for progressive supranuclear palsy: translation into a phase I controlled, randomized clinical study
JF  - Journal of Translational Medicine
N2  - Background: Progressive Supranuclear Palsy (PSP) is a sporadic and progressive neurodegenerative disease which belongs to the family of tauopathies and involves both cortical and subcortical structures. No effective therapy is to date available. 
Methods/design: Autologous bone marrow (BM) mesenchymal stem cells (MSC) from patients affected by different type of parkinsonisms have shown their ability to improve the dopaminergic function in preclinical and clinical models. It is also possible to isolate and expand MSC from the BM of PSP patients with the same proliferation rate and immuphenotypic profile as MSC from healthy donors. BM MSC can be efficiently delivered to the affected brain regions of PSP patients where they can exert their beneficial effects through different mechanisms including the secretion of neurotrophic factors. Here we propose a randomized, placebo-controlled, double-blind phase I clinical trial in patients affected by PSP with MSC delivered via intra-arterial injection. 
Discussion: To our knowledge, this is the first clinical trial to be applied in a no-option parkinsonism that aims to test the safety and to exploit the properties of autologous mesenchymal stem cells in reducing disease progression. The study has been designed to test the safety of this " first-in-man" approach and to preliminarily explore its efficacy by excluding the placebo effect. 
Trial registration: NCT01824121
KW  - Parkinson's disease
KW  - cellular therapy
KW  - deep brain-stimulation
KW  - bone-marrow
KW  - transplantation
KW  - receptor tyrosine kinase
KW  - Richardson-Olszewski-Syndrome
KW  - multiple system atrophy
KW  - advanced therapy medicinal products
KW  - mesenchymal stem and stromal cells
KW  - progressive supranuclear palsy
KW  - treatment options
KW  - adrenal medulla
KW  - stromal cells
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-117594
VL  - 12
IS  - 14
ER  - 
TY  - JOUR
A1  - Norrmen, Camilla
A1  - Figlia, Gianluca
A1  - Lebrun-Julien, Frederic
A1  - Pereira, Jorge A.
A1  - Trötzmüller, Martin
A1  - Köfeler, Harald C.
A1  - Rantanen, Ville
A1  - Wessig, Carsten
A1  - van Deijk, Anne-Lieke F.
A1  - Smit, August B.
A1  - Verheijen, Mark H. G.
A1  - Rüegg, Markus A.
A1  - Hall, Michael N.
A1  - Suter, Ueli
T1  - mTORC1 Controls PNS Myelination along the mTORC1-RXR gamma-SREBP-Lipid Biosynthesis Axis in Schwann Cells
JF  - Cell Reports
N2  - Myelin formation during peripheral nervous system (PNS) development, and reformation after injury and in disease, requires multiple intrinsic and extrinsic signals. Akt/mTOR signaling has emerged as a major player involved, but the molecular mechanisms and downstream effectors are virtually unknown. Here, we have used Schwann-cell-specific conditional gene ablation of raptor and rictor, which encode essential components of the mTOR complexes 1 (mTORC1) and 2 (mTORC2), respectively, to demonstrate that mTORC1 controls PNS myelination during development. In this process, mTORC1 regulates lipid biosynthesis via sterol regulatory element-binding proteins (SREBPs). This course of action is mediated by the nuclear receptor RXRg, which transcriptionally regulates SREBP1c downstream of mTORC1. Absence of mTORC1 causes delayed myelination initiation as well as hypomyelination, together with abnormal lipid composition and decreased nerve conduction velocity. Thus, we have identified the mTORC1-RXR gamma-SREBP axis controlling lipid biosynthesis as a major contributor to proper peripheral nerve function.
KW  - axonal integrity
KW  - peripheral nervous-system
KW  - COMPLEX 1
KW  - rat hepatocytes
KW  - SREBP
KW  - mice
KW  - growth
KW  - protein
KW  - element
KW  - CNS Myelination
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-114847
SN  - 2211-1247
VL  - 9
IS  - 2
ER  - 
TY  - JOUR
A1  - Cruccu, Giorgio
A1  - Pennisi, Elena M.
A1  - Antonini, Giovanni
A1  - Biasiotta, Antonella
A1  - Di Stefano, Giulia
A1  - La Cesa, Silvia
A1  - Leone, Caterina
A1  - Raffa, Salvatore
A1  - Sommer, Claudia
A1  - Truini, Andrea
T1  - Trigeminal isolated sensory neuropathy (TISN) and FOSMN syndrome: despite a dissimilar disease course do they share common pathophysiological mechanisms?
JF  - BMC Neurology
N2  - Background: Patients presenting with bilateral trigeminal hypoesthesia may go on to have trigeminal isolated sensory neuropathy, a benign, purely trigeminal neuropathy, or facial-onset sensory motor neuronopathy (FOSMN), a malignant life-threatening condition. No diagnostic criteria can yet differentiate the two conditions at their onset. Nor is it clear whether the two diseases are distinct entities or share common pathophysiological mechanisms. 
Methods: Seeking pathophysiological and diagnostic information to distinguish these two conditions at their onset, in this neurophysiological and morphometric study we neurophysiologically assessed function in myelinated and unmyelinated fibres and histologically examined supraorbital nerve biopsy specimens with optic and electron microscopy in 13 consecutive patients with recent onset trigeminal hypoesthesia and pain. 
Results: The disease course distinctly differed in the 13 patients. During a mean 10 year follow-up whereas in eight patients the disease remained relatively stable, in the other five it progressed to possibly life-threatening motor disturbances and extra-trigeminal spread. From two to six years elapsed between the first sensory symptoms and the onset of motor disorders. In patients with trigeminal isolated sensory neuropathy (TISN) and in those with FOSMN neurophysiological and histological examination documented a neuronopathy manifesting with trigeminal nerve damage selectively affecting myelinated fibres, but sparing the Ia-fibre-mediated proprioceptive reflex. 
Conclusions: Although no clinical diagnostic criteria can distinguish the two conditions at onset, neurophysiological and nerve-biopsy findings specify that in both disorders trigeminal nerve damage manifests as a dissociated neuronopathy affecting myelinated and sparing unmyelinated fibres, thus suggesting similar pathophysiological mechanisms.
KW  - amyotrophic-lateral-sclerosis
KW  - atrophy Kennedys-disease
KW  - trigeminal nerve
KW  - neuronopathy
KW  - trigeminal neuropathy
KW  - FOSMN
KW  - facial pain
KW  - Sjorgens-syndrome
KW  - reflex
KW  - afferents
KW  - neuralgia
KW  - pathways
KW  - humans
KW  - fibers
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-114249
SN  - 1471-2377
VL  - 14
ER  - 
TY  - JOUR
A1  - Bischoff, Joakim M.
A1  - Ringsted, Thomas K.
A1  - Petersen, Marian
A1  - Sommer, Claudia
A1  - Üçeyler, Nurcan
A1  - Werner, Mads U.
T1  - A Capsaicin (8%) Patch in the Treatment of Severe Persistent Inguinal Postherniorrhaphy Pain: A Randomized, Double-Blind, Placebo-Controlled Trial
JF  - PLOS ONE
N2  - Background: Persistent pain after inguinal herniorrhaphy is a disabling condition with a lack of evidence-based pharmacological treatment options. This randomized placebo-controlled trial investigated the efficacy of a capsaicin 8% cutaneous patch in the treatment of severe persistent inguinal postherniorrhaphy pain. Methods: Forty-six patients with persistent inguinal postherniorrhaphy pain were randomized to receive either a capsaicin 8% patch or a placebo patch. Pain intensity (Numerical Rating Scale [NRS 0-10]) was evaluated under standardized conditions (at rest, during movement, and during pressure) at baseline and at 1, 2 and 3 months after patch application. Skin punch biopsies for intraepidermal nerve fiber density (IENFD) measurements were taken at baseline and 1 month after patch application. Quantitative sensory testing was performed at baseline and at 1, 2, and 3 months after patch application. The primary outcome was comparisons of summed pain intensity differences (SPIDs) between capsaicin and placebo treatments at 1, 2 and 3 months after patch application (significance level P<0.01). Results: The maximum difference in SPID, between capsaicin and placebo treatments, was observed at 1 month after patch application, but the pain reduction was not significant (NRS, mean difference [95% CI]: 5.0 [0.09 to 9.9]; P=0.046). No differences in SPID between treatments were observed at 2 and 3 months after patch application. Changes in IENFD on the pain side, from baseline to 1 month after patch application, did not differ between capsaicin and placebo treatment: 1.9 [-0.1 to 3.9] and 0.6 [-1.2 to 2.5] fibers/mm, respectively (P=0.32). No significant changes in sensory function, sleep quality or psychological factors were associated with capsaicin patch treatment. Conclusions: The study did not demonstrate significant differences in pain relief between capsaicin and placebo treatment, although a trend toward pain improvement in capsaicin treated patients was observed 1 month after patch application.
KW  - postherpetic neuralgia
KW  - long-term pain
KW  - crossover trial
KW  - neuropathic pain
KW  - risk factors
KW  - cutaneous patch
KW  - scale
KW  - hernia repair
KW  - interference
KW  - validation
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-115198
SN  - 1932-6203
VL  - 9
IS  - 10
ER  - 
TY  - JOUR
A1  - Meyer zu Hörste, Gerd
A1  - Cordes, Steffen
A1  - Mausberg, Anne K.
A1  - Zozulya, Alla L.
A1  - Wessig, Carsten
A1  - Sparwasser, Tim
A1  - Mathys, Christian
A1  - Wiendl, Heinz
A1  - Hartung, Hans-Peter
A1  - Kieseier, Bernd C.
T1  - FoxP3+Regulatory T Cells Determine Disease Severity in Rodent Models of Inflammatory Neuropathies
JF  - PLOS ONE
N2  - Inflammatory neuropathies represent disabling human autoimmune disorders with considerable disease variability. Animal models provide insights into defined aspects of their disease pathogenesis. Forkhead box P3 (FoxP3)+ regulatory T lymphocytes (Treg) are anti-inflammatory cells that maintain immune tolerance and counteract tissue damage in a variety of immune-mediated disorders. Dysfunction or a reduced frequency of Tregs have been associated with different human autoimmune disorders. We here analyzed the functional relevance of Tregs in determining disease manifestation and severity in murine models of autoimmune neuropathies. We took advantage of the DEREG mouse system allowing depletion of Treg with high specificity as well as anti-CD25 directed antibodies to deplete Tregs in mice in actively induced experimental autoimmune neuritis (EAN). Furthermore antibody-depletion was performed in an adoptive transfer model of chronic neuritis. Early Treg depletion increased clinical EAN severity both in active and adoptive transfer chronic neuritis. This was accompanied by increased proliferation of myelin specific T cells and histological signs of peripheral nerve inflammation. Late stage Treg depletion after initial disease manifestation however did not exacerbate inflammatory neuropathy symptoms further. We conclude that Tregs determine disease severity in experimental autoimmune neuropathies during the initial priming phase, but have no major disease modifying function after disease manifestation. Potential future therapeutic approaches targeting Tregs should thus be performed early in inflammatory neuropathies.
KW  - Guillain-Barre-Syndrome
KW  - regulatory cells
KW  - C57BL/6 mice
KW  - demyelinating polyradiculoneuropathy
KW  - cytokines
KW  - pathogenesis
KW  - polyneuropathy
KW  - enteropathy
KW  - peptide
KW  - experimental autoimmune neuritis
Y1  - 2014
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-115239
VL  - 9
IS  - 10
ER  -