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COPI 和 COPII 囊泡的分裂独立于 GTP 水解。

Scission of COPI and COPII vesicles is independent of GTP hydrolysis.

机构信息

Heidelberg University Biochemistry Center, University of Heidelberg, Im Neuenheimer Feld 328, D-69120, Heidelberg, Germany.

出版信息

Traffic. 2013 Aug;14(8):922-32. doi: 10.1111/tra.12084. Epub 2013 Jun 10.

Abstract

Intracellular transport and maintenance of the endomembrane system in eukaryotes depends on formation and fusion of vesicular carriers. A seeming discrepancy exists in the literature about the basic mechanism in the scission of transport vesicles that depend on GTP-binding proteins. Some reports describe that the scission of COP-coated vesicles is dependent on GTP hydrolysis, whereas others found that GTP hydrolysis is not required. In order to investigate this pivotal mechanism in vesicle formation, we analyzed formation of COPI- and COPII-coated vesicles utilizing semi-intact cells. The small GTPases Sar1 and Arf1 together with their corresponding coat proteins, the Sec23/24 and Sec13/31 complexes for COPII and coatomer for COPI vesicles were required and sufficient to drive vesicle formation. Both types of vesicles were efficiently generated when GTP hydrolysis was blocked either by utilizing the poorly hydrolyzable GTP analogs GTPγS and GMP-PNP, or with constitutively active mutants of the small GTPases. Thus, GTP hydrolysis is not required for the formation and release of COP vesicles.

摘要

真核生物细胞内的物质运输和内膜系统的维持依赖于囊泡载体的形成和融合。在依赖 GTP 结合蛋白的运输囊泡分裂的基本机制方面,文献中存在一些差异。一些报道描述了 COP 被覆囊泡的分裂依赖于 GTP 水解,而另一些报道则发现 GTP 水解不是必需的。为了研究囊泡形成中的这一关键机制,我们利用半质膜细胞分析了 COPI 和 COPII 被覆囊泡的形成。Sar1 和 Arf1 这两种小 GTP 酶以及它们相应的被膜蛋白 Sec23/24 和 Sec13/31 复合物(COPII 囊泡)和衣被蛋白复合物(COPI 囊泡)足以驱动囊泡的形成。当利用水解能力差的 GTP 类似物 GTPγS 和 GMP-PNP 阻断 GTP 水解,或者使用小 GTP 酶的组成性激活突变体时,两种类型的囊泡都能有效地生成。因此,COP 囊泡的形成和释放不需要 GTP 水解。

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