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发育中小鼠骨骼肌中T小管/肌浆网连接的顺序对接、分子分化及定位

Sequential docking, molecular differentiation, and positioning of T-Tubule/SR junctions in developing mouse skeletal muscle.

作者信息

Takekura H, Flucher B E, Franzini-Armstrong C

机构信息

Department of Physiological Sciences, National Institute of Fitness and Sports, Kanoya, Kagoshima, 891-2393, Japan.

出版信息

Dev Biol. 2001 Nov 15;239(2):204-14. doi: 10.1006/dbio.2001.0437.

Abstract

Skeletal muscle Ca(2+) release units (CRUs) are junctions of the surface membrane/T-tubule system and the sarcoplasmic reticulum (SR) that function in excitation-contraction coupling. They contain high concentrations of dihydropyridine receptors (DHPRs) in the T-tubules and of ryanodine receptors (RyR) in the SR and they are positioned at specific locations in the sarcomere. In order to characterize the sequence of developmental steps leading to the specific molecular and structural organization of CRUs, we applied a range of imaging techniques that allowed us to follow the differentiation of the membrane compartments and the expression of junctional proteins in developing mouse diaphragm muscle. We find that docking of the two membrane systems precedes the incorporation of the RyRs into the junctions, and that T-tubule/SR junctions are formed and positioned at the I-A interface at a stage when the orientation of T-tubule is predominantly longitudinal. Thus, the sequence of developmental events is first the docking of T-tubules and SR, secondly the incorporation of RyR in the junctions, thirdly the positioning of the junctions in the sarcomere, and only much later the transverse orientation of the T-tubules. These sequential stages suggests an order of inductive processes for the molecular differentiation and structural organization of the CRUs in skeletal muscle development.

摘要

骨骼肌钙释放单位(CRUs)是表面膜/T小管系统与肌浆网(SR)的连接点,在兴奋-收缩偶联中发挥作用。它们在T小管中含有高浓度的二氢吡啶受体(DHPRs),在肌浆网中含有高浓度的兰尼碱受体(RyR),并且位于肌节的特定位置。为了描述导致CRUs特定分子和结构组织的发育步骤顺序,我们应用了一系列成像技术,使我们能够追踪发育中小鼠膈肌膜隔室的分化和连接蛋白的表达。我们发现,两个膜系统的对接先于RyRs并入连接点,并且在T小管的方向主要为纵向的阶段,T小管/肌浆网连接点在I-A界面形成并定位。因此,发育事件的顺序首先是T小管和肌浆网的对接,其次是RyR并入连接点,第三是连接点在肌节中的定位,只有在很久以后才是T小管的横向取向。这些连续阶段表明了骨骼肌发育中CRUs分子分化和结构组织的诱导过程顺序。

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