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雄激素对大鼠心脏的致心律失常作用。

Arrhythmogenic effect of androgens on the rat heart.

作者信息

Argenziano Mariana, Tiscornia Gisela, Moretta Rosalia, Casal Leonardo, Potilinski Constanza, Amorena Carlos, Gras Eduardo Garcia

机构信息

Centro de Estudios en Salud y Medio Ambiente (CESyMA), Escuela de Ciencia y Tecnología (ECyT), Universidad Nacional de General San Martín (UNSAM), Av. Gral. Paz 5445, INTI, Edificio 23, 1650, San Martin, Buenos Aires, Argentina.

The National Scientific and Technical Research Council (CONICET), Buenos Aires, Argentina.

出版信息

J Physiol Sci. 2017 Jan;67(1):217-225. doi: 10.1007/s12576-016-0459-y. Epub 2016 May 30.

Abstract

In most species androgens shorten the cardiac action potential and reduce the risk of afterdepolarizations. Despite the central role of the rat model in physiological studies, the effects of androgens on the rat heart are still inconclusive. We therefore performed electrophysiological studies on the perfused rat right ventricular free wall. We found a correlation between androgenic activity and a propensity to generate ventricular ectopic action potentials. We also found that the testosterone treatment increased action potential duration at 90 % of repolarization (APD90), while androgenic inhibition increased the time to peak and decreased APD90. We observed that the voltage-gated potassium channel Kv4.3 and the bi-directional membrane ion transporter NCX in the rat myocardium were regulated by androgenic hormones. One possible explanation for these findings is that due to the expression of specific ion channels in the rat myocardium, the action potential response to its hormonal background is different from those described in other experimental models. Our results indicate that androgenic control of NCX expression plays a key role in determining arrhythmogenicity in the rat heart.

摘要

在大多数物种中,雄激素会缩短心脏动作电位并降低后去极化的风险。尽管大鼠模型在生理学研究中具有核心作用,但雄激素对大鼠心脏的影响仍尚无定论。因此,我们对灌注的大鼠右心室游离壁进行了电生理研究。我们发现雄激素活性与产生室性异位动作电位的倾向之间存在相关性。我们还发现,睾酮处理增加了复极化90%时的动作电位时程(APD90),而雄激素抑制则增加了达到峰值的时间并缩短了APD90。我们观察到,大鼠心肌中的电压门控钾通道Kv4.3和双向膜离子转运体NCX受雄激素调节。这些发现的一个可能解释是,由于大鼠心肌中特定离子通道的表达,其动作电位对激素背景的反应不同于其他实验模型中所描述的。我们的结果表明,雄激素对NCX表达的控制在决定大鼠心脏的致心律失常性方面起着关键作用。

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