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纽蛋白和肌营养不良蛋白的互补分布定义了平滑肌中两个不同的肌膜结构域。

Complementary distributions of vinculin and dystrophin define two distinct sarcolemma domains in smooth muscle.

作者信息

North A J, Galazkiewicz B, Byers T J, Glenney J R, Small J V

机构信息

Institute of Molecular Biology, Austrian Academy of Sciences, Salzburg.

出版信息

J Cell Biol. 1993 Mar;120(5):1159-67. doi: 10.1083/jcb.120.5.1159.

Abstract

The sarcolemma of the smooth muscle cell displays two alternating structural domains in the electron microscope: densely-staining plaques that correspond to the adherens junctions and intervening uncoated regions which are rich in membrane invaginations, or caveolae. The adherens junctions serve as membrane anchorage sites for the actin cytoskeleton and are typically marked by antibodies to vinculin. We show here by immunofluorescence and immunoelectron microscopy that dystrophin is specifically localized in the caveolae-rich domains of the smooth muscle sarcolemma, together with the caveolae-associated molecule caveolin. Additional labeling experiments revealed that beta 1 integrin and fibronectin are confined to the adherens junctions, as indicated by their codistribution with vinculin and tensin. Laminin, on the other hand, is distributed around the entire cell perimeter. The sarcolemma of the smooth muscle cell is thus divided into two distinct domains, featuring different and mutually exclusive components. This simple bipartite domain organization contrasts with the more complex organization of the skeletal muscle sarcolemma: smooth muscle thus offers itself as a useful system for localizing, among other components, potential interacting partners of dystrophin.

摘要

在电子显微镜下,平滑肌细胞的肌膜呈现出两个交替的结构域:对应于黏附连接的深染斑块,以及富含膜内陷(即小窝)的中间无包被区域。黏附连接作为肌动蛋白细胞骨架的膜锚定位点,通常可用抗纽蛋白的抗体标记。我们在此通过免疫荧光和免疫电子显微镜显示,肌营养不良蛋白与小窝相关分子小窝蛋白一起,特异性地定位于平滑肌肌膜富含小窝的区域。额外的标记实验表明,β1整合素和纤连蛋白局限于黏附连接,这可通过它们与纽蛋白和张力蛋白的共分布来表明。另一方面,层粘连蛋白分布在整个细胞周边。因此,平滑肌细胞的肌膜被分为两个不同的结构域,其具有不同且相互排斥的成分。这种简单的二分结构域组织与骨骼肌肌膜更复杂的组织形成对比:因此,平滑肌为定位肌营养不良蛋白的潜在相互作用伙伴等其他成分提供了一个有用的系统。

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