Your search keyword '"Schrickel, Jan Wilko"' showing total 6 results

1. Deficiency of cyclase-associated protein 2 promotes arrhythmias associated with connexin43 maldistribution and fibrosis.

Author

Stöckigt, Florian, Peche, Vivek Shahaji, Linhart, Markus, Nickenig, Georg, Noegel, Angelika Anna, and Schrickel, Jan Wilko

Subjects

CYCLASES, CYTOSKELETON, LABORATORY mice, ARRHYTHMIA, CONNEXIN 43, CARDIOMYOPATHIES, ELECTROPHYSIOLOGY

Abstract

Introduction: Cyclase-associated protein 2 (CAP2) plays a major role in regulating the actin cytoskeleton. Since inactivation of CAP2 in a mouse model by a gene trap approach (Cap2 (gt/gt) ) results in cardiomyopathy and increased mortality, we hypothesized that CAP2 has a major impact on arrhythmias and electrophysiological parameters.Material and Methods: We performed long-term-ECG recordings in transgenic CAP2 deficient mice (C57BL/6) to detect spontaneous arrhythmias. In vivo electrophysiological studies by right heart catheterization and ex vivo epicardial mapping were used to analyze electrophysiological parameters, the inducibility of arrhythmias, and conduction velocities. Expression and distribution of cardiac connexins and the amount of cardiac fibrosis were evaluated.Results: Spontaneous ventricular arrhythmias could be detected in Cap2 (gt/gt) during the long-term-ECG recording. Cap2 (gt/gt) showed marked conduction delays at atrial and ventricular levels, including a reduced heart rate (421.0 ±40.6 bpm vs. 450.8 ±27.9 bpm; p < 0.01), and prolongations of PQ (46.3 ±4.1 ms vs. 38.6 ±6.5 ms; p < 0.01), QRS (16.2 ±2.6 ms vs. 12.6 ±1.4 ms; p < 0.01), and QTc interval (55.8 ±6.0 ms vs. 45.2 ±3.3 ms; p = 0.02) in comparison to wild type mice. The PQ prolongation was due to an infra-Hisian conduction delay (HV: 9.7 ±2.1 ms vs. 6.5 ±3.1 ms; p = 0.02). The inducibility of ventricular tachycardias during the electrophysiological studies was significantly elevated in the mutant mice (inducible animals: 88% vs. 33%; p = 0.04). Cap2 (gt/gt) showed more abnormal distribution of connexin43 compared to WT (23.0 ±4.7% vs. 2.9 ±0.8%; p < 0.01). Myocardial fibrosis was elevated in Cap2 (gt/gt) hearts (9.1 ±6.7% vs. 5.5 ±3.3%; p < 0.01).Conclusions: Loss of CAP2 results in marked electrophysiological disturbances including impaired sinus node function, conduction delays, and susceptibility to malignant arrhythmias. Structural changes in Cap2 (gt/gt) are associated with alterations in myocardial connexins and fibrosis. [ABSTRACT FROM AUTHOR]

Published

2016

2. Association of Heart Rate Turbulence With Arrhythmia Susceptibility and Heart Disease in Mice.

Author

STÖCKIGT, FLORIAN, JÜNGST, PHILIPP, LINHART, MARKUS, NICKENIG, GEORG, ANDRIÉ, RENÉ, BEIERT, THOMAS, and SCHRICKEL, JAN WILKO

Subjects

ARRHYTHMIA, MYOCARDIAL infarction complications, VENTRICULAR tachycardia, HEART disease complications, ANALYSIS of variance, ANIMAL experimentation, BAROREFLEXES, BIOLOGICAL models, CONFIDENCE intervals, DISEASE susceptibility, ELECTROPHYSIOLOGY, FISHER exact test, HEART beat, MICE, REFERENCE values, RESEARCH funding, T-test (Statistics), DATA analysis software, DESCRIPTIVE statistics, ODDS ratio, MANN Whitney U Test, KRUSKAL-Wallis Test, DISEASE risk factors

Abstract

Heart Rate Turbulence in Mice Introduction Recent studies have demonstrated the feasibility of measuring heart rate turbulence (HRT) as a marker of baroreflex function in healthy mice. The aim of this investigation was to measure HRT in a mouse model with induced structural heart defects and to determine if there were threshold values of HRT for inducible ventricular tachycardias (VTs). Methods and Results HRT was measured during electrophysiological investigations 2 weeks after transverse aortic constriction (TAC, n = 13) or myocardial cryoinfarction (MCI, n = 14). Sham-operated mice served as controls (n = 8 for TAC controls and n = 9 for MCI controls). Mice with heart disease lacked an early acceleration (turbulence onset [TO]) in heart rate after extrastimulus pacing (heart disease: 0.39% [0.19%-0.59%] vs. all controls: -0.04% [-0.25-0.19%]; P < 0.01). At a cutoff value of >0.25%, TO could be used to classify mice with induced heart disease with a sensitivity of 64.0% and specificity of 88.2% (P < 0.01) but did not identify mice at higher risk of induced VTs. Animals that were susceptible to VTs (n = 8) had lower values for turbulence slope (TS) compared with noninducible mice (6.2 milliseconds/beat [3.1-9.5 milliseconds/beat] vs. 10.1 milliseconds/beat [7.2-14.2 milliseconds/beat]; P = 0.03). TS <7.8 milliseconds/beat identified mice with inducible VTs with a sensitivity of 75.0% and specificity of 75.8% (P = 0.02). Conclusion Measurement of HRT is feasible in mouse models with induced structural heart disease. More abnormal values for TO were found in the presence of structural heart disease but did not predict susceptibility to VTs. Decreased TS was associated with VTs induced by programmed stimulation. [ABSTRACT FROM AUTHOR]

Published

2015

3. AMP-Activated Protein Kinase α1 Regulates Cardiac Gap Junction Protein Connexin 43 and Electrical Remodeling Following Pressure Overload.

Author

alesutan, Ioana, Voelkl, Jakob, Stöckigt, Florian, Mia, Sobuj, Feger, Martina, Primessnig, Uwe, Sopjani, Mentor, Munoz, Carlos, Borst, Oliver, Gawaz, Meinrad, Pieske, Burkert, Metzler, Bernhard, Heinzel, Frank, Schrickel, Jan Wilko, and Lang, Florian

Subjects

ADENOSINE monophosphate, PROTEIN kinases, CONNEXINS, ELECTROPHYSIOLOGY, UBIQUITINATION, MEMBRANE proteins

Abstract

Background/Aims: Adenosine 5'-monophosphate (AMP)-activated protein kinase (Ampk) modulates a wide array of cellular functions and regulates various ion channels and transporters. In failing human hearts an increased Ampkα1 activity was observed. The present study aimed to uncover the impact of Ampkα1 on cardiac electrical remodeling. Methods: Gene-targeted mice lacking functional Ampkα1 (Ampkα1-/-) and corresponding wild-type mice were exposed to pressure overload by 'transverse aortic constriction' (TAC). In vivo electrophysiology was performed with a single catheter technique, myocardial conduction velocities and conduction characteristics investigated in isolated hearts, transcript levels quantified by RT-PCR and protein abundance determined by Western blotting. Moreover, connexin 43 (Cx43) was expressed in Xenopus oocytes with or without coexpression of wild-type or mutant AMPK and Cx43 protein abundance quantified utilizing confocal microscopy. Results: TAC treatment increased Ampkα1 protein expression in cardiac tissue from wild-type mice. TAC further increased left ventricular conduction inhomogeneity and triggered conduction blocks, effects blunted in the Ampkα1-/- mice. TAC treatment decreased Cx43 protein abundance in cardiac tissue, an effect significantly blunted in the Ampkα1-/- mice. TAC treatment did not modify Cx43 mRNA levels but increased ubiquitination of Cx43 protein, an effect mitigated by Ampkα1 deficiency. As shown in Xenopus oocytes, Cx43 cell membrane protein abundance was significantly downregulated by wild-type AMPKWT and constitutively active AMPKγR70Q, but not by catalytically inactive AMPKαK45R. Conclusion: Ampkα1 stimulates ubiquitination of the gap junction protein Cx43, thereby contributing to gap junction remodeling following pressure overload. © 2015 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2015

4. Role of High Frequency Atrial Pacing for the Termination of Acute Atrial Fibrillation and Atypical Atrial Flutter.

Author

SHLEVKOV, NIKOLAY, YANG, ALEXANDER, SCHRICKEL, JAN WILKO, SCHWAB, JOERG OTTO, BIELIK, HELGA, LICKFETT, LARS, BITZEN, ALEXANDER, NICKENIG, GEORG, LÜDERITZ, BERNDT, and LEWALTER, THORSTEN

Subjects

ATRIAL fibrillation, ATRIAL flutter, ELECTROPHYSIOLOGY, ARRHYTHMIA, HEART failure

Abstract

Background: The aim of this study was to assess the efficacy of high-frequency (HF) pacing from the right atrial appendage (RAA) or coronary sinus ostium (CS-Os) for the termination of acute atrial fibrillation (AF) and atypical atrial flutter (AAFL) during an electrophysiological (EP) study. Methods: 128 episodes of acute fast atrial arrhythmias (FAAs; 93 AF and 35 AAFL) were analyzed in 110 patients. Patients were initially observed for 60s leading to spontaneous termination of 28 FAAs. The remaining 100 FAAs (70 AF) episodes were randomized to the following strategies: (A) pacing at RAA using up to 10 consecutive 20-Hz trains followed by the same stimulation protocol at CS-Os if RAA pacing failed, (B) pacing at CS-Os using the same stimulation protocol followed by HF pacing at RAA, or (C) observation up to 6 minutes (“no pacing”). Results: The 20-Hz pacing at both RAA and CS-Os was associated with higher conversion of AAFL, as compared to strategy C (60% and 77% vs 11%; P < 0.05). Only HF pacing at CS-Os was superior to observation strategy for the conversion of AF (21% vs 4%; P < 0.05). Conclusions: The 20-Hz pacing protocol is superior to observation strategy for interruption of either acute AF or acute AAFL episodes; however, its efficacy is higher in AAFLs. These results can be helpful for the termination of acute atrial tachyarrhythmias during EPstudy and should be further evaluated in patients with implantable devices capable of antitachycardia pacing. [ABSTRACT FROM AUTHOR]

Published

2007

5. Induction of atrial fibrillation in mice by rapid transesophageal atrial pacing.

Author

Schrickel, Jan Wilko, Bielik, Helga, Yang, Alexander, Schimpf, Rainer, Shlevkov, Nikolay, Burkhardt, Dietmar, Meyer, Rainer, Grohé, Christian, Fink, Klaus, Tiemann, Klaus, Lüderitz, Berndt, and Lewalter, Thorsten

Subjects

ATRIAL fibrillation, ATRIAL arrhythmias, HEART beat, LABORATORY mice, HEART diseases, ELECTROCARDIOGRAPHY

Abstract

Objective: Atrial fibrillation (AF) as an “indicator arrhythmia” for enhanced atrial vulnerability in mouse hearts has not yet been systematically examined. We therefore evaluated a transesophageal rapid atrial stimulation protocol for the induction of AF in C57Bl/6 mice. Methods: 40 C57Bl/6 mice (19 female and 21 male; 5.2 ± 2.1 months; 18 – 27 g) were examined by closed chest transesophageal atrial stimulation. Baseline ECG and electrophysiological parameters, AF-inducing stimulation cycle length (CL) and AF duration were analyzed. Results: The surface ECG demonstrated a significantly faster heart rate in female mice (R-R: 138.7 ± 19.9 ms versus 150.5 ± 15.7 ms, P < 0.05). AF was inducible in 90 % of the population and not inducible in 4 mice, all female (21 % in this subgroup). Mean induction CL was 27.4 ± 7.3 ms. Mean AF duration was 26.9 ± 42.6 s before spontaneous termination. In a subgroup of 4 female and 4 male mice (mean age 7.5 months), successive testing of AF induction showed a range of higher susceptibility to AF at stimulus amplitudes of 3.0 – 4.0 mA and stimulation CLs between 15 – 25 ms. AF induction was observed to be constantly reproducible in the individual animals. No correlation to pacing stimulus length and amplitude was found. Conclusions: This study demonstrates that it is possible to reproducibly induce self-terminating AF and supraventricular arrhythmias in mice by transesophageal atrial burst stimulation. The presented method allowing serial testings of the same animal can be a useful tool in further investigations with transgenic mice and might be helpful in the characterization of underlying genetic or molecular mechanisms of AF. [ABSTRACT FROM AUTHOR]

Published

2002

6. The Connexin40A96S mutation from a patient with atrial fibrillation causes decreased atrial conduction velocities and sustained episodes of induced atrial fibrillation in mice.

Author

Lübkemeier, Indra, Andrié, René, Lickfett, Lars, Bosen, Felicitas, Stöckigt, Florian, Dobrowolski, Radoslaw, Draffehn, Astrid M., Fregeac, Julien, Schultze, Joachim L., Bukauskas, Feliksas F., Schrickel, Jan Wilko, and Willecke, Klaus

Subjects

*CONNEXINS, *GENETIC mutation, *ATRIAL fibrillation, *NEURAL conduction, *LABORATORY mice, *ARRHYTHMIA, *ELECTROPHYSIOLOGY, *IMMUNOCHEMISTRY, *PATIENTS

Abstract

Abstract: Atrial fibrillation (AF) is the most common type of cardiac arrhythmia and a major cause of stroke. In the mammalian heart the gap junction proteins connexin40 (Cx40) and connexin43 (Cx43) are strongly expressed in the atrial myocardium mediating effective propagation of electrical impulses. Different heterozygous mutations in the coding region for Cx40 were identified in patients with AF. We have generated transgenic Cx40A96S mice harboring one of these mutations, the loss-of-function Cx40A96S mutation, as a model for atrial fibrillation. Cx40A96S mice were characterized by immunochemical and electrophysiological analyses. Significantly reduced atrial conduction velocities and strongly prolonged episodes of atrial fibrillation were found after induction in Cx40A96S mice. Analyses of the gating properties of Cx40A96S channels in cultured HeLa cells also revealed significantly lower junctional conductance and enhanced sensitivity voltage gating of Cx40A96S in comparison to Cx40 wild-type gap junctions. This is caused by reduced open probabilities of Cx40A96S gap junction channels, while single channel conductance remained the same. Similar to the corresponding patient, heterozygous Cx40A96S mice revealed normal expression levels and localization of the Cx40 protein. We conclude that heterozygous Cx40A96S mice exhibit prolonged episodes of induced atrial fibrillation and severely reduced atrial conduction velocities similar to the corresponding human patient. [Copyright &y& Elsevier]

Published

2013