TY  - JOUR
A1  - Beyer, Felix
A1  - Jadasz, Janusz
A1  - Samper Agrelo, Iria
A1  - Schira‐Heinen, Jessica
A1  - Groh, Janos
A1  - Manousi, Anastasia
A1  - Bütermann, Christine
A1  - Estrada, Veronica
A1  - Reiche, Laura
A1  - Cantone, Martina
A1  - Vera, Julio
A1  - Viganò, Francesca
A1  - Dimou, Leda
A1  - Müller, Hans Werner
A1  - Hartung, Hans‐Peter
A1  - Küry, Patrick
T1  - Heterogeneous fate choice of genetically modulated adult neural stem cells in gray and white matter of the central nervous system
JF  - Glia
N2  - Apart from dedicated oligodendroglial progenitor cells, adult neural stem cells (aNSCs) can also give rise to new oligodendrocytes in the adult central nervous system (CNS). This process mainly confers myelinating glial cell replacement in pathological situations and can hence contribute to glial heterogeneity. Our previous studies demonstrated that the p57kip2 gene encodes an intrinsic regulator of glial fate acquisition and we here investigated to what degree its modulation can affect stem cell‐dependent oligodendrogenesis in different CNS environments. We therefore transplanted p57kip2 knockdown aNSCs into white and gray matter (WM and GM) regions of the mouse brain, into uninjured spinal cords as well as in the vicinity of spinal cord injuries and evaluated integration and differentiation in vivo. Our experiments revealed that under healthy conditions intrinsic suppression of p57kip2 as well as WM localization promote differentiation toward myelinating oligodendrocytes at the expense of astrocyte generation. Moreover, p57kip2 knockdown conferred a strong benefit on cell survival augmenting net oligodendrocyte generation. In the vicinity of hemisectioned spinal cords, the gene knockdown led to a similar induction of oligodendroglial features; however, newly generated oligodendrocytes appeared to suffer more from the hostile environment. This study contributes to our understanding of mechanisms of adult oligodendrogenesis and glial heterogeneity and further reveals critical factors when considering aNSC mediated cell replacement in injury and disease.
KW  - glial fate modulation
KW  - myelin
KW  - neural stem cell
KW  - p57kip2
KW  - regional heterogeneity
KW  - spinal cord injury
KW  - transplantation
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-218566
VL  - 68
IS  - 2
SP  - 393
EP  - 406
ER  - 
TY  - JOUR
A1  - Berve, Kristina
A1  - West, Brian L.
A1  - Martini, Rudolf
A1  - Groh, Janos
T1  - Sex- and region-biased depletion of microglia/macrophages attenuates CLN1 disease in mice
JF  - Journal of Neuroinflammation
N2  - Background 
The neuronal ceroid lipofuscinoses (CLN diseases) are fatal lysosomal storage diseases causing neurodegeneration in the CNS. We have previously shown that neuroinflammation comprising innate and adaptive immune reactions drives axonal damage and neuron loss in the CNS of palmitoyl protein thioesterase 1-deficient (Ppt1\(^{-/-}\)) mice, a model of the infantile form of the diseases (CLN1). Therefore, we here explore whether pharmacological targeting of innate immune cells modifies disease outcome in CLN1 mice. 

Methods 
We applied treatment with PLX3397 (150 ppm in the chow), a potent inhibitor of the colony stimulating factor-1 receptor (CSF-1R) to target innate immune cells in CLN1 mice. Experimental long-term treatment was non-invasively monitored by longitudinal optical coherence tomography and rotarod analysis, as well as analysis of visual acuity, myoclonic jerks, and survival. Treatment effects regarding neuroinflammation, neural damage, and neurodegeneration were subsequently analyzed by histology and immunohistochemistry. 

Results 
We show that PLX3397 treatment attenuates neuroinflammation in CLN1 mice by depleting pro-inflammatory microglia/macrophages. This leads to a reduction of T lymphocyte recruitment, an amelioration of axon damage and neuron loss in the retinotectal system, as well as reduced thinning of the inner retina and total brain atrophy. Accordingly, long-term treatment with the inhibitor also ameliorates clinical outcomes in CLN1 mice, such as impaired motor coordination, visual acuity, and myoclonic jerks. However, we detected a sex- and region-biased efficacy of CSF-1R inhibition, with male microglia/macrophages showing higher responsiveness toward depletion, especially in the gray matter of the CNS. This results in a better treatment outcome in male Ppt1\(^{-/-}\) mice regarding some histopathological and clinical readouts and reflects heterogeneity of innate immune reactions in the diseased CNS. 

Conclusions 
Our results demonstrate a detrimental impact of innate immune reactions in the CNS of CLN1 mice. These findings provide insights into CLN pathogenesis and may guide in the design of immunomodulatory treatment strategies.
KW  - Neuronal ceroid lipofuscinosis
KW  - Microglia
KW  - Macrophages
KW  - T lymphocytes
KW  - Neurodegeneration
KW  - Axon degeneration
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-230234
VL  - 17
ER  - 
TY  - JOUR
A1  - Ben-Kraiem, Adel
A1  - Sauer, Reine-Solange
A1  - Norwig, Carla
A1  - Popp, Maria
A1  - Bettenhausen, Anna-Lena
A1  - Atalla, Mariam Sobhy
A1  - Brack, Alexander
A1  - Blum, Robert
A1  - Doppler, Kathrin
A1  - Rittner, Heike Lydia
T1  - Selective blood-nerve barrier leakiness with claudin-1 and vessel-associated macrophage loss in diabetic polyneuropathy
JF  - Journal of Molecular Medicine
N2  - Diabetic polyneuropathy (DPN) is the most common complication in diabetes and can be painful in up to 26% of all diabetic patients. Peripheral nerves are shielded by the blood-nerve barrier (BNB) consisting of the perineurium and endoneurial vessels. So far, there are conflicting results regarding the role and function of the BNB in the pathophysiology of DPN. In this study, we analyzed the spatiotemporal tight junction protein profile, barrier permeability, and vessel-associated macrophages in Wistar rats with streptozotocin-induced DPN. In these rats, mechanical hypersensitivity developed after 2 weeks and loss of motor function after 8 weeks, while the BNB and the blood-DRG barrier were leakier for small, but not for large molecules after 8 weeks only. The blood-spinal cord barrier remained sealed throughout the observation period. No gross changes in tight junction protein or cytokine expression were observed in all barriers to blood. However, expression of Cldn1 mRNA in perineurium was specifically downregulated in conjunction with weaker vessel-associated macrophage shielding of the BNB. Our results underline the role of specific tight junction proteins and BNB breakdown in DPN maintenance and differentiate DPN from traumatic nerve injury. Targeting claudins and sealing the BNB could stabilize pain and prevent further nerve damage.
KW  - macrophages
KW  - neuropathy
KW  - barrier
KW  - pain
Y1  - 2021
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-265237
VL  - 99
IS  - 9
ER  - 
TY  - JOUR
A1  - Bellut, Maximilian
A1  - Raimondi, Anthony T.
A1  - Haarmann, Axel
A1  - Zimmermann, Lena
A1  - Stoll, Guido
A1  - Schuhmann, Michael K.
T1  - NLRP3 inhibition reduces rt-PA induced endothelial dysfunction under ischemic conditions
JF  - Biomedicines
N2  - Thrombolysis with recombinant tissue plasminogen activator (rt-PA) is a mainstay of acute ischemic stroke treatment but is associated with bleeding complications, especially after prolonged large vessel occlusion. Recently, inhibition of the NLRP3 inflammasome led to preserved blood–brain barrier (BBB) integrity in experimental stroke in vivo. To further address the potential of NLRP3 inflammasome inhibition as adjunct stroke treatment we used immortalized brain derived endothelial cells (bEnd5) as an in vitro model of the BBB. We treated bEnd5 with rt-PA in combination with the NLRP3 specific inhibitor MCC950 or vehicle under normoxic as well as ischemic (OGD) conditions. We found that rt-PA exerted a cytotoxic effect on bEnd5 cells under OGD confirming that rt-PA is harmful to the BBB. This detrimental effect could be significantly reduced by MCC950 treatment. Moreover, under ischemic conditions, the Cell Index — a sensible indicator for a patent BBB — and the protein expression of Zonula occludens 1 stabilized after MCC950 treatment. At the same time, the extent of endothelial cell death and NLRP3 expression decreased. In conclusion, NLRP3 inhibition can protect the BBB from rt-PA-induced damage and thereby potentially increase the narrow time window for safe thrombolysis in stroke.
KW  - NLRP3
KW  - inflammasome
KW  - MCC950
KW  - rt-PA
KW  - blood–brain barrier
KW  - Cell Index
KW  - ASC
KW  - ischemic stroke
KW  - i.v. thrombolysis
Y1  - 2022
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-267261
SN  - 2227-9059
VL  - 10
IS  - 4
ER  - 
TY  - JOUR
A1  - Bellut, Maximilian
A1  - Papp, Lena
A1  - Bieber, Michael
A1  - Kraft, Peter
A1  - Stoll, Guido
A1  - Schuhmann, Michael K.
T1  - NLPR3 inflammasome inhibition alleviates hypoxic endothelial cell death in-vitro and protects blood-brain barrier integrity in murine stroke
JF  - Cell Death & Disease
N2  - In ischemic stroke (IS) impairment of the blood-brain barrier (BBB) has an important role in the secondary deterioration of neurological function. BBB disruption is associated with ischemia-induced inflammation, brain edema formation, and hemorrhagic infarct transformation, but the underlying mechanisms are incompletely understood. Dysfunction of endothelial cells (EC) may play a central role in this process. Although neuronal NLR-family pyrin domain-containing protein 3 (NLRP3) inflammasome upregulation is an established trigger of inflammation in IS, the contribution of its expression in EC is unclear. We here used brain EC, exposed them to oxygen and glucose deprivation (OGD) in vitro, and analyzed their survival depending on inflammasome inhibition with the NLRP3-specific drug MCC950. During OGD, EC death could significantly be reduced when targeting NLRP3, concomitant with diminished endothelial NLRP3 expression. Furthermore, MCC950 led to reduced levels of Caspase 1 (p20) and activated Gasdermin D as markers for pyroptosis. Moreover, inflammasome inhibition reduced the secretion of pro-inflammatory chemokines, cytokines, and matrix metalloproteinase-9 (MMP9) in EC. In a translational approach, IS was induced in C57Bl/6 mice by 60 mins transient middle cerebral artery occlusion and 23 hours of reperfusion. Stroke volume, functional outcome, the BBB integrity, and-in good agreement with the in vitro results-MMP9 secretion as well as EC survival improved significantly in MCC950-treated mice. In conclusion, our results establish the NLRP3 inflammasome as a critical pathogenic effector of stroke-induced BBB disruption by activating inflammatory signaling cascades and pyroptosis in brain EC.
KW  - inflammasome
KW  - preclinical research
KW  - stroke
Y1  - 2022
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-265693
VL  - 13
ER  - 
TY  - JOUR
A1  - Bellut, Maximilian
A1  - Bieber, Michael
A1  - Kraft, Peter
A1  - Weber, Alexander N. R.
A1  - Stoll, Guido
A1  - Schuhmann, Michael K.
T1  - Delayed NLRP3 inflammasome inhibition ameliorates subacute stroke progression in mice
JF  - Journal of Neuroinflammation
N2  - Background
Ischemic stroke immediately evokes a strong neuro-inflammatory response within the vascular compartment, which contributes to primary infarct development under vessel occlusion as well as further infarct growth despite recanalization, referred to as ischemia/reperfusion injury. Later, in the subacute phase of stroke (beyond day 1 after recanalization), further inflammatory processes within the brain parenchyma follow. Whether this second wave of parenchymal inflammation contributes to an additional/secondary increase in infarct volumes and bears the potential to be pharmacologically targeted remains elusive. We addressed the role of the NLR-family pyrin domain-containing protein 3 (NLRP3) inflammasome in the subacute phase of ischemic stroke.

Methods
Focal cerebral ischemia was induced in C57Bl/6 mice by a 30-min transient middle cerebral artery occlusion (tMCAO). Animals were treated with the NLRP3 inhibitor MCC950 therapeutically 24 h after or prophylactically before tMCAO. Stroke outcome, including infarct size and functional deficits as well as the local inflammatory response, was assessed on day 7 after tMCAO.

Results
Infarct sizes on day 7 after tMCAO decreased about 35% after delayed and about 60% after prophylactic NLRP3 inhibition compared to vehicle. Functionally, pharmacological inhibition of NLRP3 mitigated the local inflammatory response in the ischemic brain as indicated by reduction of infiltrating immune cells and reactive astrogliosis.

Conclusions
Our results demonstrate that the NLRP3 inflammasome continues to drive neuroinflammation within the subacute stroke phase. NLRP3 inflammasome inhibition leads to a better long-term outcome—even when administered with a delay of 1 day after stroke induction, indicating ongoing inflammation-driven infarct progression. These findings may pave the way for eagerly awaited delayed treatment options in ischemic stroke.
KW  - ischemic stroke
KW  - secondary infarct growth
KW  - neuroinflammation
KW  - middle cerebral artery occlusion
KW  - NLRP3
KW  - inflammasome
Y1  - 2023
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-300599
VL  - 20
IS  - 1
ER  - 
TY  - JOUR
A1  - Bellinger, Daniel
A1  - Altenmüller, Eckart
A1  - Volkmann, Jens
T1  - Perception of time in music in patients with Parkinson's disease - The processing of musical syntax compensates for rhythmic deficits
JF  - Frontiers in Neuroscience
N2  - Objective: Perception of time as well as rhythm in musical structures rely on complex brain mechanisms and require an extended network of multiple neural sources. They are therefore sensitive to impairment. Several psychophysical studies have shown that patients with Parkinson's disease (PD) have deficits in perceiving time and rhythms due to a malfunction of the basal ganglia (BG) network.

Method: In this study we investigated the time perception of PD patients during music perception by assessing their just noticeable difference (JND) in the time perception of a complex musical Gestalt. We applied a temporal discrimination task using a short melody with a clear beat-based rhythm. Among the subjects, 26 patients under L-Dopa administration and 21 age-matched controls had to detect an artificially delayed time interval in the range between 80 and 300 ms in the middle of the musical period. We analyzed the data by (a) calculating the detection threshold directly, (b) by extrapolating the JNDs, (c) relating it to musical expertise.

Results: Patients differed from controls in the detection of time-intervals between 220 and 300 ms (*p = 0.0200, n = 47). Furthermore, this deficit depended on the severity of the disease (*p = 0.0452; n = 47). Surprisingly, PD patients did not show any deficit of their JND compared to healthy controls, although the results showed a trend (*p = 0.0565, n = 40). Furthermore, no significant difference of the JND was found according to the severity of the disease. Additionally, musically trained persons seemed to have lower thresholds in detecting deviations in time and syntactic structures of music (*p = 0.0343, n = 39).

Conclusion: As an explanation of these results, we would like to propose the hypothesis of a time-syntax-congruency in music perception suggesting that processing of time and rhythm is a Gestalt process and that cortical areas involved in processing of musical syntax may compensate for impaired BG circuits that are responsible for time processing and rhythm perception. This mechanism may emerge more strongly as the deficits in time processing and rhythm perception progress. Furthermore, we presume that top-down-bottom-up-processes interfere additionally and interact in this context of compensation.
KW  - Parkinson disease
KW  - psychophysics
KW  - time perception
KW  - rhythm perception
KW  - musical syntax
KW  - just noticeable difference (JND)
Y1  - 2017
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-171805
VL  - 11
ER  - 
TY  - THES
A1  - Bellinger, Daniel
T1  - Zeitwahrnehmung in der Musik bei Morbus Parkinson - eine psychophysische Studie
T1  - Perception of Time in Music in Patients with Parkinson's Disease – A Psychophysical Study
N2  - Parkinson Patienten sind im Gegensatz zu gesunden Probanden in der kognitiven Verarbeitung zeitlicher Parameter, im Sinne einer Diskriminierungsfähigkeit für zeitliche Fehler innerhalb der Musikwahrnehmung beeinträchtigt. Dies betrifft lediglich die Zeiterkennung in höheren Intervallbereichen (> 600ms) und ist am ehesten durch Fluktuationen der Aufmerksamkeit, des Gedächtnisses, aber auch im Vergleich zu anderen Studien durch methodische Ansätze zu erklären. Durch die Koppelung des Audiostimulus an klare Rhythmusstrukturen weist diese Studie jedoch darauf hin, dass Überschneidungen zu anderen neuronalen Netzwerken existieren, die zur Kompensationsstrategie rekrutiert und nutzbar gemacht werden können. Dazu gehören etwa die Verarbeitung zeitlicher (Cerebellum) und musikperzeptiver Leistungen, wie etwa die Verarbeitung musikalischer Syntax (BA 6, 22, 44). Etwaige Wahrnehmungsdefizite können durch Mechanismen musiksyntaktischer Verarbeitung kompensiert werden, da zeitliche und syntaktische Strukturen in der Musik auf ihre Kongruenz hin abgeglichen und somit multineuronal mediiert werden (Paradigma der Zeit-Syntax-Kongruenz in der Musikwahrnehmung). Weiterhin sind vermutlich top-down-bottom-up-Prozesse als multimodale Interaktionen an diesem Kompensationsmechanismus beteiligt. Außerdem ist festzuhalten, dass das Krankheitsstadium nicht zwangsläufig mit einem stärkeren Wahrnehmungsdefizit für zeitliche Strukturen einhergehen muss, obwohl – wenn auch noch tolerabel – mit Progression der Erkrankung dieses Kompensationsmodell über Prinzipien der Gestaltwahrnehmung zusammenbricht und es hier zu schlechteren perzeptiven Leistungen kommen kann. 
Die Ergebnisse der OFF-Testungen und jener unter DBS-Therapie lassen weiterhin aufgrund der kleinen Stichprobe keine klare Aussage zu und machen weitere Untersuchungen notwendig. Das physiologische Alter korreliert außerdem mit der sensorischen Leistung, die allerdings starken, individuellen Unterschieden ausgesetzt ist und von multifaktoriellen Voraussetzungen abhängt. Auch zeigt die Studie, dass Menschen mit einem hohen Musikverständnis und einer musikalischen Ausbildung ein feineres Diskriminierungsvermögen in der zeitlichen Verarbeitung besitzen, welches v.a. im zeitlich niedrigen Intervallbereich (< 500ms) evident wird.
N2  - Objective: Perception of time as well as rhythm in musical structures rely on complex brain mechanisms and require an extended network of multiple neural sources. They are therefore sensitive to impairment. Several psychophysical studies have shown that patients with Parkinson's disease (PD) have deficits in perceiving time and rhythms due to a malfunction of the basal ganglia (BG) network.
Method: In this study we investigated the time perception of PD patients during music perception by assessing their just noticeable difference (JND) in the time perception of a complex musical Gestalt. We applied a temporal discrimination task using a short melody with a clear beat-based rhythm. Among the subjects, 26 patients under L-Dopa administration and 21 age-matched controls had to detect an artificially delayed time interval in the range between 80 and 300 ms in the middle of the musical period. We analyzed the data by (a) calculating the detection threshold directly, (b) by extrapolating the JNDs, (c) relating it to musical expertise.
Results: Patients differed from controls in the detection of time-intervals between 220 and 300 ms (*p = 0.0200, n = 47). Furthermore, this deficit depended on the severity of the disease (*p = 0.0452; n = 47). Surprisingly, PD patients did not show any deficit of their JND compared to healthy controls, although the results showed a trend (*p = 0.0565, n = 40). Furthermore, no significant difference of the JND was found according to the severity of the disease. Additionally, musically trained persons seemed to have lower thresholds in detecting deviations in time and syntactic structures of music (*p = 0.0343, n = 39).
Conclusion: As an explanation of these results, we would like to propose the hypothesis of a time-syntax-congruency in music perception suggesting that processing of time and rhythm is a Gestalt process and that cortical areas involved in processing of musical syntax may compensate for impaired BG circuits that are responsible for time processing and rhythm perception. This mechanism may emerge more strongly as the deficits in time processing and rhythm perception progress. Furthermore, we presume that top-down-bottom-up-processes interfere additionally and interact in this context of compensation.
KW  - Parkinson
KW  - Parkinson disease
KW  - psychophysics
KW  - Psychophysik
KW  - Musikwahrnehmung
KW  - Zeitwahrnehmung
KW  - Rhythmusperzeption
KW  - musikalische Syntax
KW  - time perception
KW  - rhythmperception
KW  - musical syntax
KW  - just noticeable difference (JND)
Y1  - 2020
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-198766
N1  - s. a. Frontiers of Neuroscience. 2017 Feb 23;11:68. doi: 10.3389/fnins.2017.00068. eCollection 2017
ER  - 
TY  - THES
A1  - Behnke, Jennifer Kim
T1  - Charakterisierung der Krankheitsprogression im genetischen hm\(^2\)α-SYN-39 Mausmodell des Morbus Parkinson
T1  - Characterization of disease progression in the genetic hm\(^2\)α-SYN-39 mouse model of Parkinson´s disease
N2  - In dieser Arbeit wurde die Krankheitsprogression im Parkinson-Mausmodell hm2α-SYN-39 mit zunehmendem Alter charakterisiert. Die Mäuse wurden in 4 Altersgruppen (2-3, 7-8, 11-12, 16-17 Monate) mit motorischen Verhaltenstests auf einen Parkinson-Phänotyp untersucht. Zudem erfolgten Untersuchungen des dopaminergen Systems zur Detektion von neurochemischen Veränderungen und einer Neurodegeneration im nigrostriatalen Trakt. Weiterhin wurden neuroinflammatorische Prozesse des adaptiven und angeborenen IS in der SN und im Striatum mittels immunhistochemischer Färbungen beurteilt.
Ein Parkinson-Phänotyp in diesem Mausmodell zeigte sich nur leicht ausgeprägt, sodass der Rotarod- und Zylinder-Test lediglich den Hinweis auf eine nicht-signifikante Einschränkung der Motorik erbrachte. Dennoch ergab die stereologische Quantifizierung TH- und Nissl-positiver Zellen in der SNpc der hm2α-SYN-39 Mäuse eine altersabhängige, signifikant-progrediente Reduktion der dopaminergen Neurone mit zunehmendem Alter. Eine signifikant niedrigere TH-positive Zellzahl dieser tg Mäuse zeigte sich ab einem Alter von 16-17 Monaten verglichen zu gleichaltrigen wt Tieren. Dagegen war die Neurodegeneration im Striatum etwas weniger ausgeprägt. Die tg Mäuse präsentierten im Alter von 16-17 Monaten eine nicht-signifikante Erniedrigung der dopaminergen Terminalen verglichen zu gleichaltrigen wt Tieren. Ein DA-Mangel im Striatum der tg Mäuse konnte mittels HPLC bestätigt werden. Bis zum Alter von 16-17 Monaten wurde eine signifikante Reduktion der DA-Level von 23,2 % verglichen zu gleichaltrigen wt Mäusen gezeigt. Außerdem erniedrigt waren die striatalen Level von NA und 5-HAT bei tg Mäusen, passend zu den bisherigen Ergebnissen bei Parkinson-Patienten.
Immunhistochemische Untersuchungen einer Neuroinflammation im nigrostriatalen Trakt ergaben eine tendenziell erhöhte Infiltration von CD4- und CD8-positiven T-Zellen bei hm2α-SYN-39 Mäusen mit zunehmendem Alter, wobei die Infiltration CD8-positiver Zellen ausgeprägter war als bei CD4-positiven Zellen. Eine noch deutlichere neuroinflammatorische Reaktion zeigte das angeborene IS. Hierbei ergab die immunhistologische Quantifizierung CD11b-positiver mikroglialer Zellen einen hochsignifikanten Anstieg im nigrostriatalen Trakt bei hm2α-SYN-39 Mäusen schon im jungen Alter. 
Zusammenfassend präsentierte dieses Parkinson-Mausmodell eine langsam-progrediente Parkinson-Pathologie mit begleitender Neuroinflammation im nigrostriatalen Trakt während des Alterns, wobei die Immunantwort der mikroglialen Zellen zu einem früheren Zeitpunkt einsetzte als die T-Zellinfiltration und Neurodegeneration. Dieses Mausmodell bietet zahlreiche Möglichkeiten zur zukünftigen Erforschung der Pathophysiologie beim MP. Generell weist diese Arbeit auf eine bedeutende Rolle neuroinflammatorischer Prozesse in der Krankheitsprogression der Parkinsonerkrankung hin und soll dazu ermutigen Neuroinflammation durchaus intensiver in tg Tiermodellen zu untersuchen.
N2  - In this doctoral thesis the progression of disease during ageing has been characterized in the mouse model of Parkinson´s disease hm2α-SYN-39. Mice in 4 age groups (2-3, 7-8, 11-12, 16-17 months of age) were tested for a Parkinson´s phenotype through motor performance analysis. Additionally, investigations of the dopaminergic system were performed to detect neurochemical changes and neurodegeneration in the nigrostriatal tract. Furthermore, neuroinflammatory processes of the adaptive and innate immune system in the SN and striatum were evaluated via immunohistochemical staining.
A Parkinson´s phenotype in this mouse model appeared only mildly, revealing a hint of non-significant motor impairment in the Rotarod and Cylinder test. However, stereological quantification of TH- and Nissl-positive cells in the SNpc of hm2α-SYN-39 mice resulted in an age-dependent, significant-progressive reduction of dopaminergic neurons with increased age. A significant lower TH-positive cell count of these tg mice was shown at an age of 16-17 months compared to wt mice of the same age. In contrast, the neurodegeneration in the striatum was less pronounced. At an age of 16-17 months tg mice presented with a non-significant reduction of dopaminergic terminals compared to wt mice of the same age. Loss of DA in the striatum of tg mice has been confirmed via HPLC. A significant reduction of DA-levels of 23,2 % was shown at the age of 16-17 months in comparison to same-aged wt mice. Striatal levels of NA and 5-HT of tg mice were reduced as well, matching previous results of Parkinson´s patients.
Immunohistochemical investigations of neuroinflammation in the nigrostriatal tract revealed a tendency of increased infiltration of CD4- and CD8-positive T cells in hm2α-SYN-39 mice with increased age, an infiltration of CD8-positive cells being more distinct though than of CD4-positive cells. The innate IS exposed an even stronger neuroinflammatory response. Immunohistochemical quantification of CD11b-positive microglial cells resulted in a highly significant surge in the nigrostriatal tract of hm2α-SYN-39 mice starting at a young age already.  
In summary, this mouse model of Parkinson´s disease presented with a slowly progressive Parkinson´s pathology accompanied by neuroinflammation in the nigrostriatal tract during the process of ageing, taking in account that an immune response of microglial cells was setting in earlier than T cell infiltration and neurodegeneration. This mouse model offers various opportunities for exploring Parkinson´s pathophysiology in the future. Generally, this work points to a substantial role of neuroinflammatory responses in the progression of Parkinson´s disease and should encourage to further investigate neuroinflammation in tg animal models.
KW  - Parkinson-Krankheit
KW  - Altern
KW  - Tiermodell
KW  - Neurodegeneration
KW  - Neuroinflammation
KW  - Mausmodell
Y1  - 2023
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-302040
ER  - 
TY  - THES
A1  - Behne, Robert Stefan Friedrich
T1  - Development Of A Human iPSC-Derived Cortical Neuron Model Of Adaptor- Protein-Complex-4-Deficiency
T1  - Entwicklung eines humanen iPSC-abgeleiteten kortikalen Neuronenmodells der Adaptor-Protein-Komplex-4-Defizienz
N2  - Adaptor-protein-4-deficiency (AP-4-deficiency) is an autosomal-recessive childhood- onset form of complicated hereditary spastic paraplegia (HSP) caused by bi-allelic loss- of-function mutations in one of the four subunits of the AP-4-complex. These four conditions are named SPG47 (AP4B1, OMIM #614066), SPG50 (AP4M1, OMIM #612936), SPG51 (AP4E1, OMIM #613744) and SPG52 (AP4S1, OMIM #614067), respectively and all present with global developmental delay, progressive spasticity and seizures. Imaging features include a thinning of the corpus callosum, ventriculomegaly and white matter changes. AP-4 is a highly conserved heterotetrameric complex, which is responsible for polarized sorting of transmembrane cargo including the autophagy- related protein 9 A (ATG9A). Loss of any of the four subunits leads to an instable complex and defective sorting of AP-4-cargo. ATG9A is implicated in autophagosome formation and neurite outgrowth. It is missorted in AP-4-deficient cells and CNS-specific knockout of Atg9a in mice results in a phenotype reminiscent of AP-4-deficiency. However, the AP-4-related cellular phenotypes including ATG9A missorting have not been investigated in human neurons.
Thus, the aim of this study is to provide the first human induced pluripotent stem cell- derived (iPSC) cortical neuron model of AP-4-deficiency to explore AP-4-related phenotypes in preparation for a high-content screening. Under the hypothesis that AP-4- deficiency leads to ATG9A missorting, elevated ATG9A levels, impaired autophagy and neurite outgrowth in human iPSC-derived cortical neurons, in vitro biochemical and imaging assays including automated high-content imaging and analysis were applied. First, these phenotypes were investigated in fibroblasts from three patients with compound heterozygous mutations in the AP4B1 gene and their sex-matched parental controls. The same cell lines were used to generate iPSCs and differentiate them into human excitatory cortical neurons.
This work shows that ATG9A is accumulating in the trans-Golgi-network in AP-4- deficient human fibroblasts and that ATG9A levels are increased compared to parental controls and wild type cells suggesting a compensatory mechanism. Protein levels of the AP4E1-subunit were used as a surrogate marker for the AP-4-complex and were decreased in AP-4-deficient fibroblasts with co-immunoprecipitation confirming the instability of the complex. Lentiviral re-expression of the AP4B1-subunit rescues this corroborating the fact that a stable AP-4-complex is needed for ATG9A trafficking. Surprisingly, autophagic flux was present in AP-4-deficient fibroblasts under nutrient- rich and starvation conditions. These phenotypic markers were evaluated in iPSC-derived cortical neurons and here, a robust accumulation of ATG9A in the juxtanuclear area was seen together with elevated ATG9A protein levels. Strikingly, assessment of autophagy markers under nutrient-rich conditions showed alterations in AP-4-deficient iPSC- derived cortical neurons indicating dysfunctional autophagosome formation. These findings point towards a neuron-specific impairment of autophagy and need further investigation. Adding to the range of AP-4-related phenotypes, neurite outgrowth and branching are impaired in AP-4-deficient iPSC-derived cortical neurons as early as 24h after plating and together with recent studies point towards a distinct role of ATG9A in neurodevelopment independent of autophagy.
Together, this work provides the first patient-derived neuron model of AP-4-deficiency and shows that ATG9A is sorted in an AP-4-dependent manner. It establishes ATG9A- related phenotypes and impaired neurite outgrowth as robust markers for a high-content screening. This disease model holds the promise of providing a platform to further study AP-4-deficiency and to search for novel therapeutic targets.
N2  - Die Adaptor-Protein-4-Defizienz (AP-4-Defizienz) ist eine autosomal-rezessiv vererbte, komplizierte Form hereditären spastischen Paraplegien (HSPs), welche durch biallelische Mutationen in einer der vier Untereinheiten des AP-4-Gens verursacht wird. Die vier resultierenden Erkrankungen werden SPG47 (AP4B1, OMIM #614066), SPG50 (AP4M1, OMIM #612936), SPG51 (AP4E1, OMIM #613744) und SPG52 (AP4S1, OMIM #614067) genannt und präsentieren sich mit globaler Entwicklungsverzögerung im frühen Säuglingsalter, progressiver Spastik sowie Krampfanfällen. Radiologische Zeichen beinhalten ein verschmälertes Corpus callosum, Ventrikulomegalie und Veränderungen der weißen Substanz. AP-4 ist ein hoch konservierter, heterotetramerer Proteinkomplex, welcher für die polarisierte Verteilung von Transmembranproteinen einschließlich des „autophagy-related protein 9 A“ (ATG9A) zuständig ist. Eine „lossof- function“ Mutation in einer der vier Untereinheiten führt zur Instabilität des gesamten Komplexes und zur Beeinträchtigung des AP-4-abhängigen Proteintransportes. ATG9A ist notwendig für die Bildung von Autophagosomen und das Neuritenwachstum. In AP- 4-defizienten Zellen ist der ATG9A-Transport beeinträchtigt und ein ZNS-spezifischer Knockout von ATG9A erzeugt in Mäusen einen Phenotyp, der große Überschneidungen mit dem der AP-4-Defizienz aufweist. Bisher sind diese AP-4-abhängigen zellulären Phenotypen nicht in humanen Neuronen untersucht worden. Daher ist die Entwicklung des ersten humanen aus induzierten pluripotenten Stammzellen (iPSC) abgeleiteten kortikalen Neuronenmodells der AP-4-Defizienz und die Identifikation AP-4-abhängiger Phenotypen für die Anwendung in einem Hochdurchsatzscreening das Ziel dieser Arbeit. Unter der Hypothese, dass AP-4- Defizienz in humanen iPSC-abgeleiteten kortikalen Neuronen zu ATG9A Fehltransport, erhöhtem ATG9A Protein, beeinträchtigter Autophagie und vermindertem Neuritenwachstum führt, wurden biochemische und automatisierte, Mikroskopie-basierte in vitro Assays entwickelt. Zunächst wurden primäre humane Fibroblasten von Patienten mit compound-heterozygoten Mutationen im AB4B1-Gen und geschlechtsangepasste, elterliche Kontrollzellen auf die genannten Phenotypen hin untersucht. Dieselben Zelllinien wurden anschließend für die Generierung von iPSCs und die Differenzierung in exzitatorische kortikale Neurone verwendet. 90 Diese Arbeit zeigt, dass ATG9A in AP-4-defizienten Fibroblasten im Bereich des Trans- Golgi-Netzwerkes akkumuliert und das ATG9A Proteinlevel erhöht sind, was auf eine kompensatorische Hochregulierung hindeutet. Die Proteinlevel der AP4E1-Untereinheit wurden als Surrogatparameter für einen stabilen AP-4-Komplex genutzt und waren in AP-4-defizienten Fibroblasten vermindert. In der Co-Immunpräzipitation konnte eine Instabilität des AP-4-Komplexes bestätigt werden. Die lentivirale Reexpression der AB4B1-Untereinheit führte zu einer Wiederherstellung des Wildtyp-Phänotyps und zeigt damit, dass ein stabiler AP-4-Komplex für die korrekte Verteilung von ATG9A notwendig ist. Trotz der bekannten Beteiligung von ATG9A an der Bildung von Autophagosomen, zeigte sich eine intakte Autophagosomenbildung und Degradation in AP-4-defizienten Fibroblasten. Die beschriebenen phänotypischen Marker wurden in iPSC-abgeleiteten kortikalen Neuronen evaluiert und auch hier konnten eine juxtanukleäre Akkumulation von ATG9A sowie erhöhte ATG9A Proteinlevel demonstriert werden. Im Gegensatz zu den Fibroblasten, zeigten AP-4-defiziente iPSCabgeleitete kortikale Neurone bereits unter nährstoffreichen Bedingungen eine Konstellation von Autophagiemarkern, die auf eine gestörte Autophagosomenbildung und damit auf eine Neuronen-spezifische Störung von Autophagie hindeuten und der weiteren Untersuchung bedürfen. Zusätzlich fand sich bei AP-4-defizienten kortikalen Neuronen bereits in den ersten 24 Stunden im Inkubator eine Störung des Neuritenwachstums und der -verzweigung, welche in Zusammenschau mit kürzlich erschienenen Arbeiten auf eine zusätzliche Autophagie-unabhängige Funktion von ATG9A hinweisen. Diese Arbeit stellt zusammenfassend die Entwicklung des ersten Patienten-abgeleiteten Neuronenmodells der AP-4-Defizienz dar und zeigt das ATG9A in einer AP-4-abhänigen Weise in der Zelle verteilt wird. Weiterhin etabliert diese Arbeit ATG9A-abhängige zelluläre Phänotypen und gestörtes Neuritenwachstum als robuste phänotypische Marker für ein High-Content Screening. Dieses zelluläre Krankheitsmodell trägt das Potential als Plattform für weitere Studien der AP-4-Defizienz zu dienen und damit neue therapeutische Möglichkeiten aufzudecken.
KW  - Adaptorproteine
KW  - hereditary spastic paraplegia
KW  - iPSC
Y1  - 2024
U6  - http://nbn-resolving.de/urn/resolver.pl?urn:nbn:de:bvb:20-opus-351390
ER  -