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首页> 外文期刊>Japanese heart journal >Function and Regulation of Sarcoplasmic Reticulum Ca2+-ATPase --- Advances during the Past Decade and Prospects for the Coming Decade ---
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Function and Regulation of Sarcoplasmic Reticulum Ca2+-ATPase --- Advances during the Past Decade and Prospects for the Coming Decade ---

机译:肌浆网Ca2 + -ATPase的功能和调控---过去十年的进展和未来十年的前景---

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摘要

In cardiac muscle, the contraction-relaxation cycle is tightly controlled by the regulated release and uptake of intracellular Ca2+ between sarcoplasmic reticulum and cytoplasm. A major protein controlling Ca2+ cycling is Ca2+-ATPase (SERCA2a) located in the sarcoplasmic reticulum membrane. The function of SERCA2a protein is regulated by the phosphorylatable protein, phospholamban. Phosphorylation of phospholamban releases its inhibitory effect on SERCA2a through direct molecular interaction. Recently, mice whose SERCA2a function is increased (overexpression of the gene) or lost (knock out) were developed. These mice demonstrated that SERCA2a pump levels are a major determinant of cardiac muscle contractility and relaxation. These studies open the prospect that the overexpression of SERCA2a can correct cardiac dysfunction seen in heart failure. Advances in knowledge concerning the function and gene regulation of SERCA2a are discussed in this review. (Jpn Heart J 2000; 41: 1-13)
机译:在心肌中,放松松弛的周期由肌浆网和细胞质之间的细胞内Ca2 +的释放和摄取来严格控制。控制Ca2 +循环的主要蛋白质是位于肌质网膜中的Ca2 + -ATPase(SERCA2a)。 SERCA2a蛋白的功能由可磷酸化的蛋白phosphorlamban调节。磷酸lamban的磷酸化通过直接的分子相互作用释放对SERCA2a的抑制作用。最近,开发了其SERCA2a功能增强(基因过表达)或缺失(敲除)的小鼠。这些小鼠证明SERCA2a泵水平是心肌收缩和松弛的主要决定因素。这些研究为SERCA2a的过表达可以纠正心力衰竭中出现的心脏功能障碍开辟了前景。本文综述了有关SERCA2a功能和基因调控的知识进展。 (Jpn Heart J 2000; 41:1-13)

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