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首页> 外文期刊>Nature Communications >Myoscape controls cardiac calcium cycling and contractility via regulation of L-type calcium channel surface expression
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Myoscape controls cardiac calcium cycling and contractility via regulation of L-type calcium channel surface expression

机译:Myoscape通过调节L型钙通道表面表达来控制心脏钙循环和收缩力

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摘要

Calcium signalling plays a critical role in the pathogenesis of heart failure. Here we describe a cardiac protein named Myoscape/FAM40B/STRIP2, which directly interacts with the L-type calcium channel. Knockdown of Myoscape in cardiomyocytes decreases calcium transients associated with smaller Ca2+ amplitudes and a lower diastolic Ca2+ content. Likewise, L-type calcium channel currents are significantly diminished on Myoscape ablation, and downregulation of Myoscape significantly reduces contractility of cardiomyocytes. Conversely, overexpression of Myoscape increases global Ca2+ transients and enhances L-type Ca2+ channel currents, and is sufficient to restore decreased currents in failing cardiomyocytes. In vivo , both Myoscape-depleted morphant zebrafish and Myoscape knockout (KO) mice display impairment of cardiac function progressing to advanced heart failure. Mechanistically, Myoscape-deficient mice show reduced L-type Ca2+currents, cell capacity and calcium current densities as a result of diminished LTCC surface expression. Finally, Myoscape expression is reduced in hearts from patients suffering of terminal heart failure, implying a role in human disease.
机译:钙信号传导在心力衰竭的发病机制中起关键作用。在这里,我们描述了一种称为Myoscape / FAM40B / STRIP2的心脏蛋白,它直接与L型钙通道相互作用。敲除心肌细胞中的Myoscape可减少与Ca 2 + 幅度较小和舒张期Ca 2 + 含量相关的钙瞬变。同样,L型钙通道电流在Myoscape消融后显着减少,而Myoscape的下调显着降低了心肌细胞的收缩性。相反,Myoscape的过表达增加了整体Ca 2 + 的瞬变,并增强了L型Ca 2 + 的通道电流,足以恢复心肌细胞衰竭时降低的电流。在体内,Myoscape耗尽型吗啡斑马鱼和Myoscape敲除(KO)小鼠均显示出心脏功能损害,并发展为晚期心力衰竭。从机制上讲,由于LTCC表面表达减少,Myoscape缺陷小鼠的L型Ca 2 + 电流,细胞容量和钙电流密度降低。最后,患有晚期心力衰竭的患者的心脏中Myoscape的表达降低,这暗示着在人类疾病中的作用。

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