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Institute
- Medizinische Klinik und Poliklinik I (46) (remove)
Background
Fabry disease is an inborn lysosomal storage disorder which is associated with small fiber neuropathy. We set out to investigate small fiber conduction in Fabry patients using pain-related evoked potentials (PREP).
Methods
In this case–control study we prospectively studied 76 consecutive Fabry patients for electrical small fiber conduction in correlation with small fiber function and morphology. Data were compared with healthy controls using non-parametric statistical tests. All patients underwent neurological examination and were investigated with pain and depression questionnaires. Small fiber function (quantitative sensory testing, QST), morphology (skin punch biopsy), and electrical conduction (PREP) were assessed and correlated. Patients were stratified for gender and disease severity as reflected by renal function.
Results
All Fabry patients (31 men, 45 women) had small fiber neuropathy. Men with Fabry disease showed impaired cold (p < 0.01) and warm perception (p < 0.05), while women did not differ from controls. Intraepidermal nerve fiber density (IENFD) was reduced at the lower leg (p < 0.001) and the back (p < 0.05) mainly of men with impaired renal function. When investigating A-delta fiber conduction with PREP, men but not women with Fabry disease had lower amplitudes upon stimulation at face (p < 0.01), hands (p < 0.05), and feet (p < 0.01) compared to controls. PREP amplitudes further decreased with advance in disease severity. PREP amplitudes and warm (p < 0.05) and cold detection thresholds (p < 0.01) at the feet correlated positively in male patients.
Conclusion
Small fiber conduction is impaired in men with Fabry disease and worsens with advanced disease severity. PREP are well-suited to measure A-delta fiber conduction.
Nach einem Myokardinfarkt werden ventrikuläres Remodeling und myokardiale Funktion unter anderem durch die ablaufenden Reaktionen des angeborenen Immunsystems beeinflusst. Von zentraler Bedeutung für die Regulation dieser Immunreaktion ist der Transkriptionsfaktor Nuclear Factor kappa B. Tiere, bei denen NF-κB durch das Fehlen seiner Untereinheit p50 global inaktiv ist, wei- sen einen Schutz vor linksventrikulärem Remodeling auf. Bisher ist jedoch un- klar, welche Zellen für diesen protektiven Effekt verantwortlich sind. Vorange- gangene Studien konnten zeigen, dass die Protektion nicht auf die fehlende NF- κB Aktivierung in Kardiomyozyten zurückzuführen ist. Aus Ischämie- Reperfusions-Experimenten an NF-κB-defizienten Tieren ergaben sich Hinwei- se, dass v.a. die Hemmung von NF-κB in Entzündungszellen die protektiven Effekte vermittelt.
Durch Kreuzung von LysMCre- mit lox-IKKβ-Tieren erzeugten wir Tiere, denen makrophagenspezifisch IκB-Kinase β (IKKβ) fehlt. IKK deaktiviert den Inhibitor von NF-κB und ist somit essentiell für eine NF-κB-Aktivierung. Als Modell der Herzinsuffizienz diente der chronische Myokardinfarkt. Die Nachbeobachtung erfolgte über 56 Tage.
Die Knockout-Tiere (KO) hatten im Vergleich zu den Wildtyp-Tiere (WT) eine signifikant bessere Überlebensrate (KO vs. WT, 100% vs. 49%, p < 0,01). Präoperativ sowie postoperativ an den Tagen 1, 21 und 56 wurden transthora- kale Echokardiographien durchgeführt. Bei gleicher Infarktgröße zeigten die KO-Tiere eine deutlich geringere linksventrikuläre Dilatation. Es konnte moleku- larbiologisch keine Reduktion der humoralen Entzündungsreaktion nachgewie- sen werden, ebenso blieb das Entzündungszellinfiltrat immunhistochemisch unverändert. Auch bezüglich Apoptoserate und Neovaskularisation zeigte sich kein Unterschied zwischen den Gruppen. Allerdings zeigten die LysM-IKKβ-KO-Tiere 56 Tage nach Myokardinfarkt einen deutlich erhöhten septalen Kollagen- gehalt als Hinweis auf ein verändertes extrazelluläres Remodeling.
Aus diesen Ergebnissen kann geschlossen werden, dass die protektiven Effek- te der globalen NF-κB-Hemmung durch die fehlende NF-κB-Aktivierung in Ma- krophagen und Granulozyten, nicht aber in Kardiomyozyten vermittelt wurden. Die durch die makrophagenspezifische NF-κB-Hemmung vermittelten Verände- rungen im Remodeling der extrazellulären Matrix führen zu einer Verbesserung der Überlebensrate, besseren funktionellen Ergebnissen und einem insgesamt verminderten linksventrikulären Remodeling nach Myokardinfarkt.
Background
The aortic pulse-wave velocity (PWV) is an important indicator of cardiovascular risk. In recent studies MRI methods have been developed to measure this parameter noninvasively in mice. Present techniques require additional hardware for cardiac and respiratory gating. In this work a robust self-gated measurement of the local PWV in mice without the need of triggering probes is proposed.
Methods
The local PWV of 6-months-old wild-type C57BL/6J mice (n=6) was measured in the abdominal aorta with a retrospectively triggered radial Phase Contrast (PC) MR sequence using the flow-area (QA) method. A navigator signal was extracted from the CMR data of highly asymmetric radial projections with short repetition time (TR=3 ms) and post-processed with high-pass and low-pass filters for retrospective cardiac and respiratory gating. The self-gating signal was used for a reconstruction of high-resolution Cine frames of the aortic motion. To assess the local PWV the volume flow Q and the cross-sectional area A of the aorta were determined. The results were compared with the values measured with a triggered Cartesian and an undersampled triggered radial PC-Cine sequence.
Results
In all examined animals a self-gating signal could be extracted and used for retrospective breath-gating and PC-Cine reconstruction. With the non-triggered measurement PWV values of 2.3±0.2 m/s were determined. These values are in agreement with those measured with the triggered Cartesian (2.4±0.2 m/s) and the triggered radial (2.3±0.2 m/s) measurement. Due to the strong robustness of the radial trajectory against undersampling an acceleration of more than two relative to the prospectively triggered Cartesian sampling could be achieved with the retrospective method.
Conclusion
With the radial flow-encoding sequence the extraction of a self-gating signal is feasible. The retrospective method enables a robust and fast measurement of the local PWV without the need of additional trigger hardware.
Das Nebennierenrindenkarzinom ist eine hochmaligne Erkrankung und hat eine schlechte Prognose. Mitotane ist bis heute die einzige hierfür zugelassene Therapie. Um die molekularen Mechanismen der Mitotanetherapie besser zu verstehen, wurde die Nebennierenkarzinom-Zelllinie NCI-H295 mit unterschiedlichen Konzentrationen von Mitotane inkubiert und die Wirkung auf mehreren Ebenen untersucht. Dabei kam der Untersuchung der Steroidogenese und apoptotischer Vorgänge ein besonderer Fokus zu. In den Hormonanalysen via Immunoassay zeigte sich eine zeit- und konzentrationsabhängige Hemmung der adrenalen Steroidsekretion. So kam es unter 24-stündiger Inkubation mit 100µM Mitotane zu einer Reduktion der Cortisolsekretion um 89%. Diese Hormonsuppression geht einher mit einer Herabregulation von steroidogenen Enzymen in den durchgeführten Microarray-basierten Genexpressionsanalysen. So konnte gezeigt werden, dass vor allem Steroidbiosynthese-Enzyme der Zona fasciculata und reticularis betroffen sind. Als weitere wichtige Gene im Zusammenhang mit der Beeinflussung des Steroidhaushalts unter Mitotanetherapie konnten SQLE, LDLR, SCD, SREBF1 und ABCG1 identifiziert werden.
Gleichzeitig konnte durch Durchflusszytometrie und Zelltod-ELISA die proapoptotische Wirkung von Mitotane gezeigt werden (FACS: 100µM Mitotane, 24 Stunden; Zunahme der Apoptose um den Faktor 2,13). Dies bestätigte sich beispielsweise auch in der Überexpression des Apoptosegens BAX in der Real-Time-PCR. Weiterhin zeigte der RNA-Microarray eine starke Expressionszunahme bei Genen, die mit dem programmierten Zelltod zusammenhängen wie GDF15, DUSP4, TRIB3 und CHOP.
Ausgehend von den klinischen Effekten und bestätigt durch die oben genannten in vitro Ergebnisse bewirkt Mitotane auch molekular folgende Änderungen in Nebennierenrindenzellen: Hemmung der Steroidogenese und Induktion von Apotose. Es stellt sich damit die Frage, ob diese Mechanismen parallel und separat voneinander ablaufen oder ob es einen gemeinsamen Nenner gibt.
Interessanterweise ergab die Analyse der Genexpressionsdaten, dass viele der proapoptotischen Gene mit dem sogenannten ER-Stress zusammenhängen. Einerseits könnte Mitotane durch direkte Inhibition der Hormonsekretion wirken, andererseits könnte ER-Stress durch Mitotane-induzierte-Bildung toxischer Lipide, wie Cholesterol, ausgelöst werden. Um den genauen Wirkmechanismus endgültig zu klären, werden weitere Experimente benötigt.
Mitotane-induzierter ER-Stress liefert einen vollständig neuen Blickwinkel auf die molekulare Wirkweise von Mitotane auf Nebennierenrindenkarzinomzellen. Gerade da die Mediatoren des ER-Stresses gut definiert und ER-Stress spezifisch sind, könnten sie sinnvolle Ziele in der Therapie darstellen. Die Beobachtung, dass Mitotane ER-Stress hervorruft, könnte in Zukunft somit zur Entwicklung wirksamerer und spezifischerer Therapien des Nebennierenrindenkarzinoms führen und so die infauste Prognose dieser malignen Krankheit verbessern.
Vaskuläre Komplikationen wie Atherosklerose sind bei Diabetikern weit verbreitet. Eine erhöhte Produktion reaktiver Sauerstoffspezies trägt zu einer Dysfunktion des Endothels bei Diabetes und hohen Glukosespiegeln bei. Glutathion (GSH) ist das häufigste zelluläre Thiol und stellt ein bedeutendens Antioxidans des menschlichen Organismus dar. Das Multidrug Resistance Protein 1 (MRP 1) ist im Endothel der Haupttransporter von oxidiertem GSH. Blockiert man MRP 1, so wird unter oxidativem Stress der intrazelluläre GSH-Spiegel erhalten.
In dieser Arbeit wird der Einfluss von MRP 1 auf die endotheliale Funktion und Produktion reaktiver Sauerstoffspezies bei Diabetes und erhöhten Glukosespiegeln anhand von MRP 1-/- -Mäusen und Wildtyp-FVB-Tieren untersucht.
Acht Wochen nach Injektion von STZ wurde die endothelabhängige Vasorelaxation an den isolierten thorakalen Aorten bestimmt. Diabetische Wildtyp-Tiere wiesen eine signifikant verminderte endothelabhängige Vasorelaxation auf. In MRP 1-/- -Tieren hingegen kam es zu keiner Beeinträchtigung der Endothelfunktion. Die endothelunabhängige Vasorelaxation war nicht signifikant unterschiedlich. STZ-induzierter Diabetes führte zu einer signifikant erhöhten Produktion von Superoxidanionen sowie Wasserstoffperoxid in Wildtyp-Tieren. Diabetische MRP 1-/- -Mäuse hingegen zeigten keinen Anstieg der Produktion reaktiver Sauerstoffspezies. Erhöhte Glukosekonzentrationen führten in vitro in humanen aortalen Endothelzellen ebenso zur erhöhten Superoxidanion-Produktion. In Zellen, in denen MRP 1 mittels siRNA herunterreguliert war, zeigte sich keine Erhöhung von Superoxidanionen. In Wildtyp-Mäusen führte Diabetes zu einer Verminderung des vaskulären GSH-Spiegels, wohingegen bei MRP 1-/- -Tieren keine Veränderung auftrat.
Diese Daten weisen auf die wichtige Rolle von MRP 1 bei der unter hohen Glukosekonzentrationen auftretenden endothelialen Dysfunktion hin. MRP 1 stellt somit einen neuen Ansatzpunkt in der Behandlung der durch Diabetes ausgelösten vaskulären Dysfunktion dar.
Fabry disease is a rare X-linked hereditary disease caused by mutations in the AGAL gene encoding the lysosomal enzyme alpha-galactosidase A. Enzyme replacement therapy (ERT) is the current cornerstone of Fabry disease management. Involvement of kidney, heart and the central nervous system shortens life span, and fibrosis of these organs is a hallmark of the disease. Fibrosis was initially thought to result from tissue ischemia secondary to endothelial accumulation of glycosphingolipids in the microvasculature. However, despite ready clearance of endothelial deposits, ERT is less effective in patients who have already developed fibrosis. Several potential explanations of this clinical observation may impact on the future management of Fabry disease. Alternative molecular pathways linking glycosphingolipids and fibrosis may be operative; tissue injury may recruit secondary molecular mediators of fibrosis that are unresponsive to ERT, or fibrosis may represent irreversible tissue injury that limits the therapeutic response to ERT. We provide an overview of Fabry disease, with a focus on the assessment of fibrosis, the clinical consequences of fibrosis, and recent advances in understanding the cellular and molecular mechanisms of fibrosis that may suggest novel therapeutic approaches to Fabry disease.
The long-term effects of enzyme-replacement therapy (ERT) in Fabry disease are unknown. Thus, the aim of this study was to determine whether ERT in patients with advanced Fabry disease affects progression towards 'hard' clinical end-points in comparison with the natural course of the disease.
METHODS:
A total of 40 patients with genetically proven Fabry disease (mean age 40 ± 9 years; n = 9 women) were treated prospectively with ERT for 6 years. In addition, 40 subjects from the Fabry Registry, matched for age, sex, chronic kidney disease stage and previous transient ischaemic attack (TIA), served as a comparison group. The main outcome was a composite of stroke, end-stage renal disease (ESRD) and death. Secondary outcomes included changes in myocardial left ventricular (LV) wall thickness and replacement fibrosis, change in glomerular filtration rate (GFR), new TIA and change in neuropathic pain.
RESULTS:
During a median follow-up of 6.0 years (bottom and top quartiles: 5.1, 7.2), 15 events occurred in 13 patients (n = 7 deaths, n = 4 cases of ESRD and n = 4 strokes). Sudden death occurred (n = 6) only in patients with documented ventricular tachycardia and myocardial replacement fibrosis. The annual progression of myocardial LV fibrosis in the entire cohort was 0.6 ± 0.7%. As a result, posterior end-diastolic wall thinning was observed (baseline, 13.2 ± 2.0 mm; follow-up, 11.4 ± 2.1 mm; P < 0.01). GFR decreased by 2.3 ± 4.6 mL min(-1) per year. Three patients experienced a TIA. The major clinical symptom was neuropathic pain (n = 37), and this symptom improved in 25 patients. The event rate was not different between the ERT group and the untreated (natural history) group of the Fabry Registry.
CONCLUSION:
Despite ERT, clinically meaningful events including sudden cardiac death continue to develop in patients with advanced Fabry disease.
Beim akuten Herzinfarkt beträgt die 30-Tages-Mortalität immer noch rund 50%. Die Hälfte dieser Todesfälle geschieht in den ersten 2 Stunden nach Symptombeginn. Zielführend in der Therapie ist die schnelle Wiedereröffnung der verschlossenen Coronararterie. Die Leitlinien der ESC (European Society of Cardiology) empfehlen die primäre perkutane Coronarintervention (PPCI) in einem Zeitfenster von weniger als 120 bzw. 90 Minuten nach first medical contact (FMC) durchzuführen. Eine Optimierung der akuten Infarktversorgung erscheint vor diesem Hintergrund dringend erforderlich. Primäre Zielgröße des Projekts ist die Verkürzung der Contact-to-ballon-Zeit (C2B), also die Zeit zwischen FMC bis zur Ballondilatation. Voraussetzung für schnelle Reaktionszeiten und damit auch für schnelle C2B-Zeiten ist eine sichere und schnelle EKG-Diagnose bereits am präklinischen Einsatzort. Aber, Unsicherheiten bei der STEMI-Diagnostik sind gegenwärtig. Um eine Verbesserung der STEMI-Versorgung zu gewährleisten, wurde im Herzinfarktnetz Mainfranken die telemetrische 12-Kanal-EKG-Übertragung im Pilotversuch eingeführt. In der vorliegenden Arbeit wurde mit Hilfe eines prospektiv erhobenen Patientenregisters untersucht, welchen Einfluss die Etablierung telemetrischer Verfahren in der Akutversorgung von STEMI-Patienten hat. Sowohl die strukturellen Abläufe im Rahmen des Herzinfarktnetzwerkes als auch der klinische Outcome der Patienten wurden untersucht und dokumentiert. Insgesamt erfüllten über sechs Studienquartale (vom 01.01.2009 bis 30.09.2010) hinweg 310 Patienten die Einschlusskriterien. Die Ergebnisse zeigen, dass durch eine sichere, präklinische EKG-Diagnose mit Hilfe telemetrischer Verfahren, die C2B-Intervalle im Studienzeitraum signifikant reduziert wurden. Auch die innerklinische Behandlung wurde merklich beschleunigt. Zusammenfassend können mit Hilfe der telemetrischen EKG-Übertragung vier wesentliche Punkte verbessert werden. 1. die sichere Diagnosestellung des STEMI; 2. der gezielte Primärtransport in das nächstgelegene, geeignete Interventionszentrum; 3. das organsierte Bypassing der nächstgelegenen Nicht-Interventionsklinik und somit die Vermeidung von Sekundärtransporten; 4. das Bypassing der Notaufnahme und der Intensivstation der Interventionsklinik und somit die Direktübergabe im HKL.
Die Nierentransplantation ist neben den verschiedenen Formen der Dialyse die wichtigste Therapieform für Patienten mit terminaler Niereninsuffizienz.
In dieser retrospektiven, monozentrischen Analyse wurden 204 Patienten erfasst, die von 2000 bis 2007 eine Nierentransplantation im Universitätsklinikum Würzburg erhalten hatten. Die Patienten wurden an Hand ihrer Nierenfunktion in vier Gruppen eingeteilt und miteinander verglichen. Ziel dieser Studie war es, Einflussfaktoren auf die Nierenfunktion, Komplikationen und Kosten im ersten Jahr nach Nierentransplantation zu untersuchen.
Wir konnten zeigen, dass eine längere Wartezeit auf ein Spenderorgan und ein hoher präoperativer BMI mit einer schlechteren Nierenfunktion nach Transplantation assoziiert waren. Außerdem fiel auf, dass in den Gruppen mit besserer Nierenfunktion nach Transplantation häufiger Lebendspenden durchgeführt worden waren.
Zu den häufigsten Komplikationen im ersten Jahr nach Nierentransplantation gehörten Anämien, akute Abstoßungsreaktionen, die verzögerte Funktionsaufnahme des Organs, Infektionen, arterielle Hypertonie und Verschlechterungen der Transplantatfunktion. Eine höhere Komplikationsrate war mit einer schlechteren Nierenfunktion und höheren Kosten assoziiert. Der Kostenmehraufwand ergab sich aus der Zunahme an ambulanten Interventionen sowie verlängerten bzw. zusätzlichen stationären Aufenthalten. In unserer Studie hatte die Gruppe mit der schlechtesten Nierenfunktion die meisten Komplikationen und verursachte so die höchsten Kosten.
Wir errechneten einen Gesamtkostenbetrag von 43.000€ im ersten Jahr nach Nierentransplantation pro Patient. 48 % der Gesamtkosten entfielen dabei auf die DRG-Pauschale der Transplantation selbst, 28% auf die immunsuppressive Therapie sowie 10 % auf die Therapie und Prophylaxe von Infektionen.
Somit lagen unsere Kosten für eine Nierentransplantation im ersten Jahr verglichen mit den Kosten für die Hämodialyse in anderen, aktuellen Studien gleich oder höher. Im Vergleich zu den Kosten der Peritonealdialyse anderer Studien waren sie durchgehend höher. Die Kosten für einen transplantierten Patienten reduzierten sich laut Studien jedoch deutlich ab dem zweiten Jahr auf durchschnittlich 12.000€. Die Kosten einer Hämodialyse beliefen sich je nach Studie auf 28.000-43.000 € pro Jahr. Eine Peritonealdialyse kostete ca. 25.000€.
Damit ist die Transplantation mittel- und langfristig die günstigste Therapieform. Aus finanzieller Sicht sollten mehr dialysepflichtige Patienten mittels Peritonealdialyse behandelt und die Transplantationszahlen möglichst gesteigert werden.
Da die Anzahl an Nierentransplantationen von Risikopatienten weiter steigen wird, ist mit einer Zunahme von behandlungsbedürftigen Komplikationen und nachfolgend mit einer Kostensteigerung zu rechnen. Zukünftig sollte versucht werden, Wartezeiten zu reduzieren, die Anzahl der Lebendspenden zu steigern und möglichst Normalgewicht vor Transplantation zu erreichen.
Um dem Kostenanstieg entgegenzuwirken, sollten Kosteneinsparungen durch Optimierung der immunsuppressiven Schemata und verstärkten Einsatz von Generika realisiert werden. Auch eine bessere Infektionsprophylaxe sowie ein frühzeitiges Erkennen und Behandeln von manifesten Infektionen könnten die Kosten weiter reduzieren und die Transplantation ökonomisch noch attraktiver werden lassen.
Dialysepatienten weisen eine hohe Anzahl kardiovaskulärer Ereignisse auf. Betrachtet man die häufigsten Todesursachen von Dialysepatienten, so fällt ein großer Teil in den kardiovaskulären Bereich. In dieser Arbeit wurde der Einfluss von Aldosteron und Cortisol auf kardiale und vaskuläre Ereignisse bei Dialysepatienten mit Diabetes mellitus untersucht. Dazu wurden Daten von 1255 Dialysepatienten mit Diabetes mellitus aus der Deutschen Diabetes Dialyse Studie analysiert.
In der vorliegenden Arbeit konnte gezeigt werden, dass mit erhöhten Aldosteronkonzentrationen ein signifikanter Anstieg des Risikos für plötzlichen Herztod (HR: 1.69; 95% CI: 1.06–2.69) einhergeht. Das Risiko an plötzlichem Herztod zu versterben war bei hohen Konzentrationen von Aldosteron und gleichzeitig vorliegenden hohen Konzentrationen von Cortisol noch deutlicher erhöht (HR: 2.86, 95% CI: 1.32–6.21). Ebenso war die Gesamtsterblichkeit signifikant erhöht bei Patienten, die hohe Aldosteron- und Cortisolkonzentrationen aufwiesen im Vergleich zu Patienten mit niedrigen Spiegeln beider Hormone (HR: 1.62, 95% CI: 1.01–2.62).
In dieser Arbeit konnte somit ein deutlicher Zusammenhang hoher Aldosteron- und Cortisolkonzentrationen mit plötzlichem Herztod und Gesamtsterblichkeit gezeigt werden.
Background: Resistance to ESAs (erythropoietin stimulating agents) is highly prevalent in hemodialysis patients with diabetes and associated with an increased mortality. The aim of this study was to identify predictors for ESA resistance and to develop a prediction model for the risk stratification in these patients.
Methods: A post-hoc analysis was conducted of the 4D study, including 1015 patients with type 2 diabetes undergoing hemodialysis. Determinants of ESA resistance were identified by univariate logistic regression analyses. Subsequently, multivariate models were performed with stepwise inclusion of significant predictors from clinical parameters, routine laboratory and specific biomarkers.
Results: In the model restricted to clinical parameters, male sex, shorter dialysis vintage, lower BMI, history of CHF, use of ACE-inhibitors and a higher heart rate were identified as independent predictors of ESA resistance. In regard to routine laboratory markers, lower albumin, lower iron saturation, higher creatinine and higher potassium levels were independently associated with ESA resistance. With respect to specific biomarkers, higher ADMA and CRP levels as well as lower Osteocalcin levels were predictors of ESA resistance.
Conclusions: Easily obtainable clinical parameters and routine laboratory parameters can predict ESA resistance in diabetic hemodialysis patients with good discrimination. Specific biomarkers did not meaningfully further improve the risk prediction of ESA resistance. Routinely assessed data can be used in clinical practice to stratify patients according to the risk of ESA resistance, which may help to assign appropriate treatment strategies.
DHEA is a precursor for the male and female sex hormones testosterone and estradiol, which are mainly secreted from the testes and the ovary, respectively. In addition, epidemiological studies showed that low serum levels of DHEA and DHEAS correlate with the incidence of autoimmune disease, cancer and cardiovascular disease. In vitro, DHEA and DHEAS influenced glucose metabolism in a favourable manner. However, positive effects of DHEA substitution were only significant adrenal insufficiency in women.
Steroid sulphotransferase 2A1 (SULT2A1) is the responsible enzyme for sulphonation of DHEA to DHEAS which is thought to be the inactive form of DHEA. In this role, SULT2A1 acts as a central regulator of steroid synthesis because sulphonation of DHEA withdraws the substrate for further downstream conversion. Another essential cofactor for sulphonation is PAPS, which is produced by the enzyme PAPS synthase (PAPSS) from ATP and anorganic sulphate. PAPSS exists in the different isoforms PAPSS1 and PAPSS2 and splice variants PAPSS2a and PAPSS2b. Changes in PAPSS activity are thought to influence sulphonation of DHEA significantly. However, neither regulation of PAPSS nor its influence on SULT2A1 have been investigated in human cell lines or humans.
The main goal of this thesis was to analyze the enzyme expression of the DHEA/DHEA shuttle, i.e. mRNA and protein of SULT2A1, PAPSS1 and PAPSS2, in various human cell lines. Furthermore, I investigated which cell line could serve as a suitable model for further research regarding regulation of SULT2A1, PAPSS1 and PAPSS2.
Here, I could show that the enzymes of the DHEA/DHEAS shuttle were expressed in the human adrenal cell line NCI-h295R as both mRNA and protein. In enzyme assays, I was able to prove conversion of DHEA to DHEAS as well as to different other steroids. However, applying Trilostane, a potent inhibitor of CYP3B, effectively directed conversion of DHEA to DHEAS. Using these findings, future experiments can investigate for example the influence of certain cytokines or endocrine disruptors on expression and activity of PAPSS1/2 and on sulphonation of DHEA. In particular, the relatively equal expression of PAPSS1 and PAPSS2 will enable us to do knock down experiments with siRNA to elucidate how the activity of one enzyme changes when the other one fails.
Sulphonation of DHEA by SULT2A1 is thought to happen in the cytoplasm or more precisely in the Golgi apparatus. However, experiments in transfected cells have shown both a cytoplasmatic and a nuclear localisation when both enzymes were expressed at the same time. Immunocytochemistry revealed the same results in the adrenal cell line NCI-h295R, where both enzymes were expressed strongly in the nucleus. The physiological role is not clear and requires further research. Presumably, sulphate is activated in the nucleus. However, one could also speculate that a shift of PAPSS to the nucleus could generate a reservoir, which can be activated by re-localisation to the cytoplasm when more PAPS is needed.
Expression of SULT2A1 in some foetal tissues has been investigated earlier. Whilst in adult human cartilage PAPSS1 is predominant, in newly born hamsters PAPSS2 is more abundantly expressed. The expression of PAPSS isoforms in highly sulphonating tissue has not been investigated in humans, so far. This work demonstrated a differential expression of SULT2A1, PAPSS1 and PAPSS2 in adult and foetal liver, adrenal and foetal cartilage tissue. In adult and foetal adrenal expression was similar. However, foetal and adult liver differed in the expression of SULT2A1, which was expressed much more in adult tissue. Most importantly, in foetal cartilage there was only a low expression of SULT2A1 and PAPS seems to mostly provided by PAPSS1, which was considerably higher expressed in cartilage than in other tissues. In contrast, PAPSS2 was mainly expressed in adult and foetal adrenal.
Additionally, we reported a case of a female patient who had been investigated for hyperandrogenism. Two mutations in the PAPSS2 gene had led to massively reduced serum levels of DHEAS. One heterozygous mutation in the domain of the APS kinase of the PAPSS2 protein leads to substitution of one amino acid at position 48 (T48R). In vitro experiments showed a residual activity of 6% for this mutation. A second mutation in the ATP sulphurylase domain of PAPSS2 was found. The introduction of thymidine instead of cytidine leads to a stop codon, which is presumed to truncate the protein at position 329 (R329X). In vitro, no residual activity was seen for this mutation. The lack of PAPS reduces sulphonation of DHEA but also sulphonation of proteoglycanes, which leads to skeletal abnormalities. The abundance of DHEA enables massive downstream conversion to androgens leading to clinical features of hyperandrogenism. Regarding the bone abnormalities, it is interesting and surprising that activity of PAPSS1 compensated to a great extent in cartilage but was not able to keep up a more considerable sulphonation of DHEA. Possibly, the subcellular localisation might play a role in this scenario.
Adrenocortical tumors consist of benign adenomas and highly malignant carcinomas with a still incompletely understood pathogenesis. A total of 46 adrenocortical tumors (24 adenomas and 22 carcinomas) were investigated aiming to identify novel genes involved in adrenocortical tumorigenesis. High-resolution single nucleotide polymorphism arrays (Affymetrix) were used to detect copy number alterations (CNAs) and copy neutral losses of heterozygosity (cnLOH). Genomic clustering showed good separation between adenomas and carcinomas, with best partition including only chromosome 5, which was highly amplified in 17/22 malignant tumors. The malignant tumors had more relevant genomic aberrations than benign tumors, such as a higher median number of recurrent CNA (2631 vs 94), CNAs >100 Kb (62.5 vs 7) and CN losses (72.5 vs 5.5), and a higher percentage of samples with cnLOH (91% vs 29%). Within the carcinoma cohort, a precise genetic pattern (i.e. large gains at chr 5, 7, 12, and 19, and losses at chr 1, 2, 13, 17, and 22) was associated with a better prognosis (overall survival: 72.2 vs 35.4 months, P=0.063). Interestingly, >70% of gains frequent in beningn were also present in malignant tumors. Notch signaling was the most frequently involved pathway in both tumor entities. Finally, a CN gain at imprinted “IGF2” locus chr 11p15.5 appeared to be an early alteration in a multi-step tumor progression, followed by the loss of one or two alleles, associated with increased IGF2 expression, only in carcinomas. Our study serves as database for the identification of genes and pathways, such as Notch signaling, which could be involved in the pathogenesis of adrenocortical tumors. Using these data, we postulate an adenoma-carcinoma sequence for these tumors.
Background: The clinical signs of adrenal cortical insufficiency (incidence, ca. 25 per million per year; prevalence, ca. 400 per million) are nonspecific, and misdiagnoses are therefore common. Glucocorticoid substitution therapy has been in use for 50 years but is not a wholly adequate treatment. Our understanding of this disease remains incomplete in many ways.
Methods: We selectively searched the Medline database for publications on adrenal cortical insufficiency, with particular attention to studies from the year 2000 onward (search terms: "adrenal insufficiency" or "Addison's disease" or "hypopituitarism"). Results: Hydrocortisone substitution therapy is often given in doses of 10-25 mg/day, timed according to the circadian rhythm. Gastrointestinal and other, febrile infections account for 30-50% of life-threatening adrenocortical crises. Such crises affect 8 of 100 persons with adrenal cortical insufficiency per year and must be treated by the immediate administration of glucocorticoids and fluids. When persons with adrenal cortical insufficiency are acutely ill or are otherwise under unusual stress, they may need additional amounts of hydrocortisone, often in the range of 5-10 mg but occasionally as high as 200 mg. The sustained administration of excessive amounts of steroid can shorten patients' lives by several years. Inappropriate substitution therapy can cause other major medical conditions, such as metabolic syndrome and osteoporosis.
Conclusion: Important measures for the prevention of adrenocortical crises include improved care by treating physicians, education of patients and their families, the provision of emergency identifying documents, and the prescription of glucocorticoid emergency kits.
The effect of mild chronic renal failure (CRF) induced by 4/6-nephrectomy (4/6NX) on central neuronal activations was investigated by c-Fos immunohistochemistry staining and compared to sham-operated rats. In the 4/6 NX rats also the effect of the angiotensin receptor blocker, losartan, and the central sympatholyticum moxonidine was studied for two months. In serial brain sections Fos-immunoreactive neurons were localized and classified semiquantitatively. In 37 brain areas/nuclei several neurons with different functional properties were strongly affected in 4/6NX. It elicited a moderate to high Fos-activity in areas responsible for the monoaminergic innervation of the cerebral cortex, the limbic system, the thalamus and hypothalamus (e.g. noradrenergic neurons of the locus coeruleus, serotonergic neurons in dorsal raphe, histaminergic neurons in the tuberomamillary nucleus). Other monoaminergic cell groups (A5 noradrenaline, C1 adrenaline, medullary raphe serotonin neurons) and neurons in the hypothalamic paraventricular nucleus (innervating the sympathetic preganglionic neurons and affecting the peripheral sympathetic outflow) did not show Fos-activity. Stress- and pain-sensitive cortical/subcortical areas, neurons in the limbic system, the hypothalamus and the circumventricular organs were also affected by 4/6NX. Administration of losartan and more strongly moxonidine modulated most effects and particularly inhibited Fos-activity in locus coeruleus neurons. In conclusion, 4/6NX elicits high activity in central sympathetic, stress- and pain-related brain areas as well as in the limbic system, which can be ameliorated by losartan and particularly by moxonidine. These changes indicate a high sensitivity of CNS in initial stages of CKD which could be causative in clinical disturbances.
Background: Tumor necrosis factor-like weak inducer of apoptosis (TWEAK) and its receptor fibroblast growth factorinducible 14 (Fn14) are upregulated after myocardial infarction (MI) in both humans and mice. They modulate inflammation and the extracellular matrix, and could therefore be important for healing and remodeling after MI. However, the function of TWEAK after MI remains poorly defined.
Methods and results: Following ligation of the left coronary artery, mice were injected twice per week with a recombinant human serum albumin conjugated variant of TWEAK (HSA-Flag-TWEAK), mimicking the activity of soluble TWEAK. Treatment with HSA-Flag-TWEAK resulted in significantly increased mortality in comparison to the placebo group due to myocardial rupture. Infarct size, extracellular matrix remodeling, and apoptosis rates were not different after MI. However, HSA-Flag-TWEAK treatment increased infiltration of proinflammatory cells into the myocardium. Accordingly, depletion of neutrophils prevented cardiac ruptures without modulating all-cause mortality.
Conclusion: Treatment of mice with HSA-Flag-TWEAK induces myocardial healing defects after experimental MI. This is mediated by an exaggerated neutrophil infiltration into the myocardium.
Background
Surgical procedures in small animal models of heart disease might evoke alterations in cardiac morphology and function. The aim of this study was to reveal and quantify such potential artificial early or long term effects in vivo, which might account for a significant bias in basic cardiovascular research, and, therefore, could potentially question the meaning of respective studies.
Methods
Female Wistar rats (n = 6 per group) were matched for weight and assorted for sham left coronary artery ligation or control. Cardiac morphology and function was then investigated in vivo by cine magnetic resonance imaging at 7 Tesla 1 and 8 weeks after the surgical procedure. The time course of metabolic and inflammatory blood parameters was determined in addition.
Results
Compared to healthy controls, rats after sham surgery showed a lower body weight both 1 week (267.5±10.6 vs. 317.0±11.3 g, n<0.05) and 8 weeks (317.0±21.1 vs. 358.7±22.4 g, n<0.05) after the intervention. Left and right ventricular morphology and function were not different in absolute measures in both groups 1 week after surgery. However, there was a confined difference in several cardiac parameters normalized to the body weight (bw), such as myocardial mass (2.19±0.30/0.83±0.13 vs. 1.85±0.22/0.70±0.07 mg left/right per g bw, p<0.05), or enddiastolic ventricular volume (1.31±0.36/1.21±0.31 vs. 1.14±0.20/1.07±0.17 µl left/right per g bw, p<0.05). Vice versa, after 8 weeks, cardiac masses, volumes, and output showed a trend for lower values in sham operated rats compared to controls in absolute measures (782.2±57.2/260.2±33.2 vs. 805.9±84.8/310.4±48.5 mg, p<0.05 for left/right ventricular mass), but not normalized to body weight. Matching these findings, blood testing revealed only minor inflammatory but prolonged metabolic changes after surgery not related to cardiac disease.
Conclusion
Cardio-thoracic surgical procedures in experimental myocardial infarction cause distinct alterations upon the global integrity of the organism, which in the long term also induce circumscribed repercussions on cardiac morphology and function. This impact has to be considered when analyzing data from respective animal studies and transferring these findings to conditions in patients.
Atherosclerosis is an active and progressive condition where the vascular cell adhesion molecules as VCAM-1 play a vital role controlling the recruitment of immune cells within the early and advanced plaques. Therefore targeting of VCAM-1 molecules with specific contrast agent bears the possibility to monitor the VCAM-1 expression, visualize the plaque progression starting at the early alterations, and help to establish early prevention of atherosclerosis before the origin of the thrombus formation, of which late recognition leads to myocardial infarction. Furthermore noninvasive magnetic resonance imaging (MRI) offers the benefit of combining the molecular and anatomic data and would thus enable specific detection of VCAM-1 targeted iron oxide contrast agent within inflammatory process of atherosclerosis. This thesis exactly presents the VCAM-1 concept as a suitable molecular approach and the potential of specific ultrasmall superparamagnetic iron oxide (USPIO) conjugated to the VCAM-1 binding peptide over unspecific non-targeted USPIO particles for evaluation of atherosclerosis. This work firstly demonstrated that selection of VCAM-1 molecules offers a good and potential strategy for imaging of atherosclerosis, as these vascular cell adhesion molecules are highly expressed in the early phase of inflammation and also continuously up-regulated within the advanced plaques. Secondly, this thesis showed the proof of principle and capability of the newly designed USPIO contrast agent conjugated to the specific cyclic peptide for VCAM-1 recognition. The experimental studies including ultra-high field MRI enabled further ex vivo and in vivo detection of applied USPIO-VCAM-1 particles within the aortic root region of early and advanced atherosclerotic plaques of 12 and 30 week old apolipoprotein E deficient (ApoE-/-) mice. Using a combination of histology and electron microscopy, this study for the first time pointed to distribution of targeted USPIO-VCAM-1 particles within plaque cells expressing VCAM-1 not only in luminal regions but also in deeper medial smooth muscle cell areas. Hence functionalized USPIO particles targeting VCAM-1 molecules allow specific and sensitive detection of early and advanced plaques at the molecular level, giving the new possibilities for early recognition of atherosclerotic plaques before the appearance of advanced and prone to rupture lesions. In contrast to the functionalized USPIO-VCAM-1, utilized non-targeted USPIO particles did not succeed in early plaque 6 identification limiting visualization of atherosclerosis to advanced forms in atherosclerotic ApoE-/- mice.
Die Simulationstechnologie in der Medizin hat in den letzten Jahren große Fortschritte gemacht. In der Zwischenzeit gibt es auch für Herzkatheteruntersuchungen und -interventionen „Virtual reality“ Simulatoren, die ein realistisches Training von Kathetereingriffen erlauben. Nicht geklärt ist bislang, ob Simulationstraining das Stressniveau des Untersuchers reduzieren kann.
Im Rahmen dieser Studie wurde zur Beantwortung der genannten Fragestellung der Effekt von Virtual-Reality-Training auf das Stressniveau von Anfängern in der interventionellen Kardiologie untersucht. Hierzu wurde eine randomisiert-stratifizierte Studie bei 33 Anfängern in der interventionellen Kardiologie durchgeführt. Die Probanden wurden in eine Kontroll- und Simulationsgruppe aufgeteilt. Die Simulationsgruppe erhielt ein achtstündiges intensives Training an verschiedenen Simulatoren, während die Kontrollgruppe kein Simulationstraining, sondern lediglich eine theoretische Wissensvermittlung erhielt. Alle Teilnehmer mussten unter realitätsnahen Umständen im Herzkatheterlabor der Universitätsklinik Würzburg innerhalb von 30 Minuten eine PCI an einem pulsatilen Herzkreislaufmodell durchführen. Die Probanden dokumentierten vor und nach der Prä- und Postevaluation ihr aktuelles „Befinden“ anhand eines psychologi-schen Fragebogens PANAS. Ebenso wurden die Probanden hinsichtlich ihrer manuellen Fähigkeiten nach einem strukturierten Evaluationsbogen von einem interventionell tätigen Kardiologen bewertet
Die Ergebnisse zeigten initial für die Parameter „aktiv, interessiert, freudig erregt, stark, angeregt, stolz, begeistert, wach, entschlossen und aufmerksam“ des Fragebogens PANAS keinen gruppenspezifischen Unterschied. Nach einem achtstündigen Simulationstraining gab die Simulationsgruppe eine signifikante Reduktion des Stressniveaus im Vergleich zur Kontrollgruppe an.
Die aktuelle Studie zeigte, dass das Training an den Virtual Reality Simulatoren die herkömmliche Ausbildung in effektiver Weise ergänzen kann.
Weitere Studien mit einer größeren und zugleich homogeneren Stichprobengröße sind nötig, um die genannten Hypothesen zu bestätigen.
Objectives
The aim of this study was to explore the left ventricular (LV) deformation changes and the potential impact of deformation on outcome in patients with proven light-chain (AL) amyloidosis and LV hypertrophy.
Background
Cardiac involvement in AL amyloidosis patients is associated with poor outcome. Detecting regional cardiac function by advanced non-invasive techniques might be favorable for predicting outcome.
Methods
LV longitudinal, circumferential and radial peak systolic strains (Ssys) were assessed by speckle tracking imaging (STI) in 44 biopsy-proven systemic AL amyloidosis patients with LV hypertrophy (CA) and in 30 normal controls. Patients were divided into compensated (n = 18) and decompensated (n = 26) group based on clinical assessment and followed-up for a median period of 345 days.
Results
Ejection fraction (EF) was preserved while longitudinal Ssys (LSsys) was significantly reduced in both compensated and decompensated groups. Survival was significantly reduced in decompensated group (35% vs. compensated 78%, P = 0.001). LSsys were similar in apical segments and significantly reduced in basal segments between two patient groups. LSsys at mid-segments were significantly reduced in all LV walls of decompensated group. Patients were further divided into 4 subgroups according to the presence or absence of reduced LSsys in no (normal), only basal (mild), basal and mid (intermediate) and all segments of the septum (severe). This staging revealed continuously worse prognosis in proportion to increasing number of segments with reduced LSsys (mortality: normal 14%, mild 27%, intermediate 67%, and severe 64%). Mid-septum LSsys<11% suggested a 4.8-fold mortality risk than mid-septum LSsys≥11%. Multivariate regression analysis showed NYHA class and mid-septum LSsys were independent predictors for survival.
Conclusions
Reduced deformation at mid-septum is associated with worse prognosis in systemic amyloidosis patients with LV hypertrophy.