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Rab2a和Rab27a通过双效应分子Noc2协同调节从颗粒成熟到胞吐作用的转变。

Rab2a and Rab27a cooperatively regulate the transition from granule maturation to exocytosis through the dual effector Noc2.

作者信息

Matsunaga Kohichi, Taoka Masato, Isobe Toshiaki, Izumi Tetsuro

机构信息

Laboratory of Molecular Endocrinology and Metabolism, Department of Molecular Medicine, Institute for Molecular and Cellular Regulation, Gunma University, Maebashi 371-8512, Japan.

Department of Chemistry, Graduate School of Science, Tokyo Metropolitan University, Hachioji, Tokyo 192-0397, Japan.

出版信息

J Cell Sci. 2017 Feb 1;130(3):541-550. doi: 10.1242/jcs.195479. Epub 2016 Dec 7.

DOI:10.1242/jcs.195479
PMID:27927751
Abstract

Exocytosis of secretory granules entails budding from the trans-Golgi network, sorting and maturation of cargo proteins, and trafficking and fusion to the plasma membrane. Rab27a regulates the late steps in this process, such as granule recruitment to the fusion site, whereas Rab2a functions in the early steps, such as granule biogenesis and maturation. Here, we demonstrate that these two small GTPases simultaneously bind to Noc2 (also known as RPH3AL) in a GTP-dependent manner, although Rab2a binds only after Rab27a has bound. In pancreatic β-cells, the ternary Rab2a-Noc2-Rab27a complex specifically localizes on perinuclear immature granules, whereas the binary Noc2-Rab27a complex localizes on peripheral mature granules. In contrast to the wild type, Noc2 mutants defective in binding to Rab2a or Rab27a fail to promote glucose-stimulated insulin secretion. Although knockdown of any component of the ternary complex markedly inhibits insulin secretion, only knockdown of Rab2a or Noc2, and not that of Rab27a, impairs cargo processing from proinsulin to insulin. These results suggest that the dual effector, Noc2, regulates the transition from Rab2a-mediated granule biogenesis to Rab27a-mediated granule exocytosis.

摘要

分泌颗粒的胞吐作用需要从反式高尔基体网络出芽、货物蛋白的分选和成熟,以及向质膜的运输和融合。Rab27a调节这一过程的后期步骤,如颗粒募集到融合位点,而Rab2a在早期步骤中起作用,如颗粒生物发生和成熟。在这里,我们证明这两种小GTP酶以GTP依赖的方式同时结合到Noc2(也称为RPH3AL),尽管Rab2a仅在Rab27a结合后才结合。在胰腺β细胞中,三元Rab2a-Noc2-Rab27a复合物特异性定位于核周未成熟颗粒上,而二元Noc2-Rab27a复合物定位于外周成熟颗粒上。与野生型相比,在与Rab2a或Rab27a结合方面存在缺陷的Noc2突变体不能促进葡萄糖刺激的胰岛素分泌。尽管三元复合物的任何组分的敲低均显著抑制胰岛素分泌,但只有Rab2a或Noc2的敲低,而不是Rab27a的敲低,会损害从胰岛素原到胰岛素的货物加工。这些结果表明,双重效应分子Noc2调节从Rab2a介导的颗粒生物发生到Rab27a介导的颗粒胞吐作用的转变。

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