首页> 外文期刊>European journal of heart failure: journal of the Working Group on Heart Failure of the European Society of Cardiology >Heterogeneous Connexin43 distribution in heart failure is associated with dispersed conduction and enhanced susceptibility to ventricular arrhythmias.
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Heterogeneous Connexin43 distribution in heart failure is associated with dispersed conduction and enhanced susceptibility to ventricular arrhythmias.

机译:心力衰竭中的异质连接蛋白43分布与传导分散和对室性心律不齐的敏感性增加有关。

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摘要

AIMS: Sudden arrhythmogenic cardiac death is a major cause of mortality in patients with congestive heart failure (CHF). To investigate determinants of the increased arrhythmogenic susceptibility, we studied cardiac remodelling and arrhythmogenicity in CHF patients and in a mouse model of chronic pressure overload. METHODS AND RESULTS: Clinical and (immuno)histological data of myocardial biopsies from CHF patients with (VT+) and without (VT-) documented ventricular arrhythmia were compared with controls. In CHF patients, ejection fraction was decreased and QRS duration was increased. Cell size and interstitial fibrosis were increased, but Connexin43 (Cx43) levels, the most abundant gap junction in ventricular myocardium, were unchanged. No differences were found between VT+ and VT- patients, except for the distribution pattern of Cx43, which was significantly more heterogeneous in VT+. Mice were subjected to transverse aortic constriction (TAC) or sham operated. At 16 weeks, cardiac function was determined by echocardiography and epicardial ventricular activation mapping was performed. Transverse aortic constriction mice had decreased fractional shortening and prolonged QRS duration. Right ventricular conduction velocity was reduced, and polymorphic VTs were induced in 44% TAC and 0% sham mice. Interstitial fibrosis was increased and Cx43 quantity was unchanged in TAC mice with and without arrhythmias. Similar to CHF patients, heterogeneous Cx43 distribution was significantly associated with arrhythmias in TAC mice and with spatial heterogeneity of impulse conduction. CONCLUSION: Heterogeneous Cx43 expression during CHF is associated with dispersed impulse conduction and may underlie enhanced susceptibility to ventricular tachyarrhythmias.
机译:目的:心律失常性心源性猝死是充血性心力衰竭(CHF)患者死亡的主要原因。为了调查导致心律失常敏感性增加的决定因素,我们研究了CHF患者和慢性压力超负荷小鼠模型的心脏重塑和心律失常。方法和结果:将有(VT +)和无(VT-)记录的室性心律失常的CHF患者的心肌活检的临床和(免疫)组织学数据与对照组进行比较。在CHF患者中,射血分数降低,QRS持续时间增加。细胞大小和间质纤维化增加,但连接蛋白43(Cx43)水平,心室心肌中最丰富的间隙连接,没有改变。 VT +和VT-患者之间没有发现差异,除了Cx43的分布模式外,Cx43在VT +中的异质性更大。小鼠经受主动脉横缩(TAC)或假手术。在第16周,通过超声心动图确定心脏功能,并进行心外膜心室激活作图。横向主动脉缩窄小鼠缩短了分数缩短并延长了QRS持续时间。右心室传导速度降低,并在44%TAC和0%假手术小鼠中诱发了多形性室速。在有和没有心律不齐的TAC小鼠中,间质纤维化增加,Cx43量不变。与CHF患者相似,异种Cx43分布与TAC小鼠心律不齐以及脉冲传导的空间异质性显着相关。结论:CHF期间异质性Cx43表达与分散的冲动传导有关,可能是对室性快速性心律失常的敏感性增强。

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