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再生过程中细胞骨架蛋白的组织和轴突运输变化。

Changes in organization and axonal transport of cytoskeletal proteins during regeneration.

作者信息

Tashiro T, Komiya Y

机构信息

Department of Molecular and Cellular Neurobiology, Gunma University School of Medicine, Japan.

出版信息

J Neurochem. 1991 May;56(5):1557-63. doi: 10.1111/j.1471-4159.1991.tb02051.x.

Abstract

Changes in solubility and transport rate of cytoskeletal proteins during regeneration were studied in the motor fibers of the rat sciatic nerve. Nerves were injured by freezing at the midthigh level either 1-2 weeks before (experiment I) or 1 week after radioactive labeling of the spinal cord with L-[35S]methionine (experiment II). Labeled proteins in 6-mm consecutive segments of the nerve 2 weeks after labeling were analyzed following fractionation into soluble and insoluble populations with 1% Triton at 4 degrees C. When axonal transport of newly synthesized cytoskeleton was examined in the regenerating nerve in experiment I, a new faster component enriched in soluble tubulin and actin was observed that was not present in the control nerve. The rate of the slower main component containing most of the insoluble tubulin and actin together with neurofilament proteins was not affected. A smaller but significant peak of radioactivity enriched in soluble tubulin and actin was also detected ahead of the main peak when the response of the preexisting cytoskeleton was examined in experiment II. It is thus concluded that during regeneration changes in the organization take place in both the newly synthesized and the preexisting axonal cytoskeleton, resulting in a selective acceleration in rate of transport of soluble tubulin and actin.

摘要

在大鼠坐骨神经的运动纤维中研究了再生过程中细胞骨架蛋白的溶解度和运输速率的变化。在脊髓用L-[35S]甲硫氨酸进行放射性标记前1 - 2周(实验I)或后1周(实验II),在大腿中部水平通过冷冻损伤神经。标记后2周,将神经切成6毫米连续节段,用1% Triton在4℃下分级分离为可溶性和不溶性部分后,分析其中的标记蛋白。在实验I中,当在再生神经中检测新合成细胞骨架的轴突运输时,观察到一种新的更快的成分,其富含可溶性微管蛋白和肌动蛋白,而对照神经中不存在。包含大部分不溶性微管蛋白、肌动蛋白以及神经丝蛋白的较慢的主要成分的运输速率未受影响。在实验II中,当检测预先存在的细胞骨架的反应时,在主要峰之前还检测到一个较小但显著的富含可溶性微管蛋白和肌动蛋白的放射性峰。因此得出结论,在再生过程中,新合成的和预先存在的轴突细胞骨架的组织都发生了变化,导致可溶性微管蛋白和肌动蛋白的运输速率选择性加快。

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