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泛素赖氨酸63参与酵母质膜蛋白的泛素化过程。

Ubiquitin lys63 is involved in ubiquitination of a yeast plasma membrane protein.

作者信息

Galan J M, Haguenauer-Tsapis R

机构信息

Institut Jacques Monod CNRS-UMRC9922 Université Paris VII, 2 place Jussieu, 75251 Paris, Cedex 05, France.

出版信息

EMBO J. 1997 Oct 1;16(19):5847-54. doi: 10.1093/emboj/16.19.5847.

Abstract

We have recently reported that the yeast plasma membrane uracil permease undergoes cell-surface ubiquitination, which is dependent on the Npi1/Rsp5 ubiquitin-protein ligase. Ubiquitination of this permease, like that of some other transporters and receptors, signals endocytosis of the protein, leading to its subsequent vacuolar degradation. This process does not involve the proteasome, which binds and degrades ubiquitin-protein conjugates carrying Lys48-linked ubiquitin chains. The data presented here show that ubiquitination and endocytosis of uracil permease are impaired in yeast cells lacking the Doa4p ubiquitin-isopeptidase. Both processes were rescued by overexpression of wild-type ubiquitin. Mutant ubiquitins carrying Lys-->Arg mutations at Lys29 and Lys48 restored normal permease ubiquitination. In contrast, a ubiquitin mutated at Lys63 did not restore permease polyubiquitination. Ubiquitin-permease conjugates are therefore extended through the Lys63 of ubiquitin. When polyubiquitination through Lys63 is blocked, the permease still undergoes endocytosis, but at a reduced rate. We have thus identified a natural target of Lys63-linked ubiquitin chains. We have also shown that monoubiquitination is sufficient to induce permease endocytosis, but that Lys63-linked ubiquitin chains appear to stimulate this process.

摘要

我们最近报道,酵母质膜尿嘧啶通透酶会发生细胞表面泛素化,这依赖于Npi1/Rsp5泛素 - 蛋白质连接酶。这种通透酶的泛素化,与其他一些转运蛋白和受体的情况类似,标志着该蛋白质的内吞作用,进而导致其随后在液泡中降解。这个过程不涉及蛋白酶体,蛋白酶体负责结合并降解携带赖氨酸48连接的泛素链的泛素 - 蛋白质偶联物。此处呈现的数据表明,在缺乏Doa4p泛素异肽酶的酵母细胞中,尿嘧啶通透酶的泛素化和内吞作用受损。通过野生型泛素的过表达,这两个过程均得以恢复。在赖氨酸29和赖氨酸48处携带赖氨酸到精氨酸突变的突变泛素恢复了正常的通透酶泛素化。相比之下,在赖氨酸63处突变的泛素未能恢复通透酶的多泛素化。因此,泛素 - 通透酶偶联物是通过泛素的赖氨酸63延伸的。当通过赖氨酸63的多泛素化被阻断时,通透酶仍会发生内吞作用,但速率降低。我们由此确定了赖氨酸63连接的泛素链的一个天然靶点。我们还表明,单泛素化足以诱导通透酶内吞作用,但赖氨酸63连接的泛素链似乎会刺激这一过程。

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