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Myocardial calcium signaling in physiology and disease

机译:心肌钙信号在生理和疾病中的作用

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Abstract: It is now well-established that calcium (Ca2+) is a critical regulator of myocardial function and that abnormalities in cardiomyocyte intracellular Ca2+ dynamics contribute to pathophysiologic changes observed in several cardiac diseases, including cardiac hypertrophy, chronic heart failure, and ventricular tachyarrhythmias. Although Ca2+ plays a key role in maintaining cardiac excitation–contraction coupling, it is increasingly apparent that changes in myocardial Ca2+ also contribute to the regulation of normal and pathological signal transduction that controls myocyte growth, hypertrophic signaling, mitochondrial energetics, and transcriptional gene expression. Interestingly, experimental evidence suggests that these multifarious Ca2+-dependent responses are spatially and temporally mediated by distinct cellular Ca2+ pools (ie, microdomains), which are generated by diverse channels and molecular signals with widely differing timescales of activation. These concepts are discussed in this review, as well as the emerging role of microRNAs in cardiac remodeling and myocardial Ca2+ dynamics.
机译:摘要:众所周知,钙(Ca2 +)是心肌功能的关键调节剂,心肌细胞内Ca2 +动态异常会导致多种心脏疾病的病理生理变化,包括心脏肥大,慢性心力衰竭和室性心律失常。尽管Ca2 +在维持心脏兴奋-收缩偶联中起着关键作用,但越来越明显的是,心肌Ca2 +的变化也有助于调节正常和病理信号转导,从而控制心肌细胞的生长,肥大信号,线粒体能量和转录基因表达。有趣的是,实验证据表明,这些多种多样的Ca2 +依赖性反应是由不同的细胞Ca2 +池(即微区)在空间和时间上介导的,而细胞Ca2 +池是由具有不同激活时间尺度的各种通道和分子信号产生的。本文对这些概念进行了讨论,同时还讨论了microRNA在心脏重构和心肌Ca2 +动态中的新兴作用。

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