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Sar1促进内质网而非高尔基体区室的囊泡出芽。

Sar1 promotes vesicle budding from the endoplasmic reticulum but not Golgi compartments.

作者信息

Kuge O, Dascher C, Orci L, Rowe T, Amherdt M, Plutner H, Ravazzola M, Tanigawa G, Rothman J E, Balch W E

机构信息

Cellular Biochemistry and Biophysics Program, Memorial Sloan-Kettering Cancer Center, New York 10021.

出版信息

J Cell Biol. 1994 Apr;125(1):51-65. doi: 10.1083/jcb.125.1.51.

Abstract

Two new members (Sar1a and Sar1b) of the SAR1 gene family have been identified in mammalian cells. Using immunoelectron microscopy, Sar1 was found to be restricted to the transitional region where the protein was enriched 20-40-fold in vesicular carriers mediating ER to Golgi traffic. Biochemical analysis revealed that Sar1 was essential for an early step in vesicle budding. A Sar1-specific antibody potently inhibited export of vesicular stomatitis virus glycoprotein (VSV-G) from the ER in vitro. Consistent with the role of guanine nucleotide exchange in Sar1 function, a trans-dominant mutant (Sar1a[T39N]) with a preferential affinity for GDP also strongly inhibited vesicle budding from the ER. In contrast, Sar1 was not found to be required for the transport of VSV-G between sequential Golgi compartments, suggesting that components active in formation of vesicular carriers mediating ER to Golgi traffic may differ, at least in part, from those involved in intra-Golgi transport. The requirement for novel components at different stages of the secretory pathway may reflect the recently recognized differences in protein transport between the Golgi stacks as opposed to the selective sorting and concentration of protein during export from the ER.

摘要

在哺乳动物细胞中已鉴定出SAR1基因家族的两个新成员(Sar1a和Sar1b)。利用免疫电子显微镜技术,发现Sar1局限于过渡区域,在介导内质网到高尔基体运输的囊泡载体中,该区域的蛋白质富集了20至40倍。生化分析表明,Sar1对于囊泡出芽的早期步骤至关重要。一种Sar1特异性抗体在体外能有效抑制水泡性口炎病毒糖蛋白(VSV-G)从内质网的输出。与鸟嘌呤核苷酸交换在Sar1功能中的作用一致,对GDP具有优先亲和力的反式显性突变体(Sar1a[T39N])也强烈抑制内质网的囊泡出芽。相比之下,未发现Sar1是VSV-G在高尔基体连续区室之间运输所必需的,这表明在介导内质网到高尔基体运输的囊泡载体形成中起作用的成分可能至少部分不同于参与高尔基体内运输的成分。分泌途径不同阶段对新成分的需求可能反映了最近认识到的高尔基体堆叠之间蛋白质运输的差异,这与内质网输出过程中蛋白质的选择性分选和浓缩不同。

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