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表面激活的铺展血小板中肌球蛋白的重组

Reorganization of myosin in surface-activated spreading platelets.

作者信息

Tanaka K, Shibata N, Okamoto K, Matsusaka T, Fukuda H, Takagi M, Fujii N, Toya N, Onji T

机构信息

Research Institute, Center for Adult Diseases, Osaka, Japan.

出版信息

J Ultrastruct Mol Struct Res. 1986 Oct-Dec;97(1-3):165-86. doi: 10.1016/s0889-1605(86)80016-7.

Abstract

To study the localization of myosin in platelets, we utilized polyclonal antibody to heavy chain of platelet myosin. Both immunofluorescence and indirect immunogold staining techniques were employed. (1) In the unactivated platelets, myosin was distributed homogeneously throughout the cytosol. The cytosolic myosin was removed after platelets were treated with Triton X-100. The association of myosin with actin microfilaments in unactivated platelets was minimal. (2) In the surface-activated platelets, myosin was unextractable by Triton X-100. The myosin antibody heavily decorated the actin cable-networks which characterized the activated platelets. (3) In the Triton-unextractable cytoskeleton of both unactivated and activated platelets, we found fine fibrils (about 1-nm wide) that were often associated with immunogolds. These fibrils were similar to purified myosin molecules observed in rotary-shadowed metal replicas and ultrathin sections. These results indicate that cytosolic myosin becomes associated with actin cable-networks after the activation of platelets.

摘要

为研究肌球蛋白在血小板中的定位,我们使用了针对血小板肌球蛋白重链的多克隆抗体。采用了免疫荧光和间接免疫金染色技术。(1)在未活化的血小板中,肌球蛋白均匀分布于整个细胞质溶胶中。用Triton X - 100处理血小板后,细胞质溶胶中的肌球蛋白被去除。未活化血小板中肌球蛋白与肌动蛋白微丝的结合极少。(2)在表面活化的血小板中,肌球蛋白不能被Triton X - 100提取。肌球蛋白抗体大量标记了活化血小板特有的肌动蛋白索网络。(3)在未活化和活化血小板的Triton不可提取细胞骨架中,我们发现了细纤维(约1纳米宽),它们常与免疫金颗粒相关。这些纤维类似于在旋转阴影金属复制品和超薄切片中观察到的纯化肌球蛋白分子。这些结果表明,血小板活化后,细胞质溶胶中的肌球蛋白与肌动蛋白索网络结合。

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