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Laa1p,一种对酵母中AP-1定位很重要的保守AP-1辅助蛋白。

Laa1p, a conserved AP-1 accessory protein important for AP-1 localization in yeast.

作者信息

Fernández G Esteban, Payne Gregory S

机构信息

Department of Biological Chemistry, David Geffen School of Medicine at University of California, Los Angeles, Los Angeles, CA 90095, USA.

出版信息

Mol Biol Cell. 2006 Jul;17(7):3304-17. doi: 10.1091/mbc.e06-02-0096. Epub 2006 May 10.

Abstract

AP-1 and Gga adaptors participate in clathrin-mediated protein transport between the trans-Golgi network and endosomes. Both adaptors contain homologous domains that act to recruit accessory proteins involved in clathrin-coated vesicle formation, but the spectrum of known adaptor-binding partners is limited. This study describes an evolutionarily conserved protein of Saccharomyces cerevisiae, Laa1p (Yjl207cp), that interacts and functions specifically with AP-1. Deletion of LAA1, when combined with a conditional mutation in clathrin heavy chain or deletion of GGA genes, accentuated growth defects and increased disruption of clathrin-dependent alpha-factor maturation and transport of carboxypeptidase Y to the vacuole. In contrast, such genetic interactions were not observed between deletions of LAA1 and AP-1 subunit genes. Laa1p preferentially interacted with AP-1 compared with Gga proteins by glutathione S-transferase-fusion affinity binding and coimmunoprecipitations. Localization of AP-1 and Laa1p, but not Gga proteins, was highly sensitive to brefeldin A, an inhibitor of ADP-ribosylation factor (Arf) activation. Importantly, deletion of LAA1 caused mislocalization of AP-1, especially in cells at high density (postdiauxic shift), but it did not affect Gga protein distribution. Our results identify Laa1p as a new determinant of AP-1 localization, suggesting a model in which Laa1p and Arf cooperate to direct stable association of AP-1 with appropriate intracellular membranes.

摘要

AP-1和Gga衔接蛋白参与网格蛋白介导的蛋白在反式高尔基体网络和内体之间的运输。这两种衔接蛋白都含有同源结构域,其作用是招募参与网格蛋白包被囊泡形成的辅助蛋白,但已知的衔接蛋白结合伴侣的范围有限。本研究描述了酿酒酵母中一种进化保守的蛋白Laa1p(Yjl207cp),它与AP-1特异性相互作用并发挥功能。LAA1缺失与网格蛋白重链的条件性突变或GGA基因缺失相结合时,会加剧生长缺陷,并增加网格蛋白依赖性α因子成熟以及羧肽酶Y向液泡运输的破坏。相比之下,LAA1缺失与AP-1亚基基因缺失之间未观察到这种遗传相互作用。通过谷胱甘肽S-转移酶融合亲和结合和共免疫沉淀实验,与Gga蛋白相比,Laa1p优先与AP-1相互作用。AP-1和Laa1p(而非Gga蛋白)的定位对布雷菲德菌素A高度敏感,布雷菲德菌素A是一种ADP-核糖基化因子(Arf)激活抑制剂。重要的是,LAA1缺失导致AP-1定位错误,尤其是在高密度细胞(二次生长转换后)中,但不影响Gga蛋白分布。我们的结果确定Laa1p是AP-1定位的一个新决定因素,提示了一个模型,其中Laa1p和Arf协同作用以指导AP-1与合适的细胞内膜稳定结合。

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