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首页> 外文期刊>International Journal of Cardiology >Distinctive sodium and calcium regulation associated with sex differences in atrial electrophysiology of rabbits
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Distinctive sodium and calcium regulation associated with sex differences in atrial electrophysiology of rabbits

机译:钠和钙的不同调节与家兔心房电生理的性别差异有关

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Background Sex and sodium/calcium regulation play critical roles in cardiac electrophysiology and atrial arrhythmogenesis. We investigated whether sodium and calcium contributed to sex differences in atrial electrophysiology. Methods Whole-cell patch clamp techniques and the indo-1 fluorometric ratio technique were used to investigate the ionic current and intracellular calcium in single isolated male and female rabbit myocytes from the left atrium posterior wall (LAPW) and right atrium (RA). Results Female LAPW (n = 95) and RA (n = 49) myocytes had larger cell widths (15.1 ± 0.4 vs. 13.8 ± 0.4 μm, p 0.05; 14.9 ± 0.6 vs. 13.5 ± 0.4 μm, p 0.05) than male LAPW (n = 142) and RA (n = 57) myocytes. Male LAPW myocytes (n = 26) had a higher incidence (57 vs. 16%, p 0.05) of delayed afterdepolarizations (DADs) than female LAPW myocytes (n = 24) but there were similar incidences (20 vs. 20%, p 0.05) of DADs in male and female RA myocytes. The late sodium current, calcium transients, and sarcoplasmic reticulum calcium contents were larger in male than female LAPW myocytes but were similar in male and female RA myocytes. However, the ICa-L and nickel-sensitive sodium/calcium exchanger currents were similar between two groups. Different from those in female myocytes, ouabain (10 μM) only induced repeated atrial beats (0 to 45%, p 0.05) in male myocytes (n = 11). Moreover, ranolazine (3 μM) perfusion (4.5 ± 0.6 vs. 1 min, p 0.05) was required to decrease the amplitude of DADs in male but not female LAPW myocytes. Conclusions Increased late sodium currents and calcium contents may contribute to higher arrhythmogenesis in male LAPW myocytes.
机译:背景性别和钠/钙调节在心脏电生理和心律失常的发生中起关键作用。我们调查了钠和钙是否有助于心房电生理的性别差异。方法采用全细胞膜片钳技术和indo-1荧光比率技术研究左心房后壁(LAPW)和右心房(RA)单个分离的雄性和雌性兔心肌细胞的离子电流和细胞内钙。结果女性LAPW(n = 95)和RA(n = 49)心肌细胞具有更大的细胞宽度(15.1±0.4 vs. 13.8±0.4μm,p <0.05; 14.9±0.6 vs. 13.5±0.4μm,p <0.05)男性LAPW(n = 142)和RA(n = 57)心肌细胞。男性LAPW心肌细胞(n = 26)的延迟除极后极化(DAD)发生率较高(57 = 16%,p <0.05),而女性LAPW心肌细胞(n = 24)发生率较高(20 = 20%, p> 0.05)男性和女性RA心肌细胞中的DAD。男性的晚期钠电流,钙瞬变和肌浆网钙含量大于女性的LAPW心肌细胞,但在男性和女性的RA心肌细胞中相似。但是,两组之间的ICa-L和对镍敏感的钠/钙交换器电流相似。与雌性心肌细胞不同,哇巴因(10μM)仅诱导雄性心肌细胞(n = 11)重复心房搏动(0至45%,p <0.05)。此外,需要雷诺嗪(3μM)灌注(4.5±0.6 vs. 1分钟,p <0.05),以降低雄性而非雌性LAPW心肌细胞中DAD的幅度。结论晚期钠电流和钙含量增加可能有助于男性LAPW心肌细胞的心律失常发生。

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