首页> 外文期刊>The Journal of Physiology >Checking your SOCCs and feet: the molecular mechanisms of Ca2+ entry in skeletal muscle.
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Checking your SOCCs and feet: the molecular mechanisms of Ca2+ entry in skeletal muscle.

机译:检查您的SOCC和脚:骨骼肌中Ca2 +进入的分子机制。

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摘要

It has long been known that skeletal muscle contraction persists in the absence of extracellular Ca(2+). Nevertheless, recent evidence indicates that multiple distinct Ca(2+) entry pathways exist in skeletal muscle: one active at negative potentials that requires store depletion (store-operated calcium entry or SOCE) and a second that is independent of store depletion and is activated by depolarization (excitation-coupled calcium entry or ECCE). This review highlights recent findings regarding the molecular identity, subcellular localization, and inter-relationship between SOCE and ECCE in skeletal muscle. The respective roles of ryanodine receptors (RyRs), dihydropyridine receptors (DHPRs), inositol-1,4,5-trisphosphate receptors (IP(3)Rs), canonical transient receptor potential channels (TRPCs), STIM1 Ca(2+) sensor proteins, and Orai1 Ca(2+) permeable channels in mediating SOCE and ECCE in skeletal muscle are discussed. Differences between SOCE and ECCE in skeletal muscle with Ca(2+) entry mechanisms in non-excitable cells are also reviewed. Finally, potential physiological roles for SOCE and ECCE in skeletal muscle development and function, as well as other currently unanswered questions and controversies in the field are also considered.
机译:早就知道,骨骼肌收缩在没有细胞外Ca(2+)的情况下持续存在。然而,最近的证据表明骨骼肌中存在多个独特的Ca(2+)进入途径:一种在负电位下活跃,需要商店耗竭(商店操作的钙进入或SOCE),而另一条与商店耗竭无关并被激活通过去极化(激励耦合钙进入或ECCE)。这篇综述突出了关于骨骼肌中SOCE和ECCE之间的分子同一性,亚细胞定位以及相互关系的最新发现。 ryanodine受体(RyRs),二氢吡啶受体(DHPRs),肌醇-1,4,5-三磷酸受体(IP(3)Rs),规范瞬时受体电位通道(TRPC),STIM1 Ca(2+)传感器的各自作用蛋白质和Orai1 Ca(2+)渗透通道介导骨骼肌中的SOCE和ECCE进行了讨论。还审查了在非兴奋性细胞中Ca(2+)进入机制的骨骼肌中SOCE和ECCE之间的差异。最后,还考虑了SOCE和ECCE在骨骼肌发育和功能中的潜在生理作用,以及该领域中其他目前尚未解决的问题和争议。

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