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泛素样蛋白 Urm1 作为一种非典型赖氨酸定向蛋白修饰物的作用。

Role of the ubiquitin-like protein Urm1 as a noncanonical lysine-directed protein modifier.

机构信息

Whitehead Institute for Biomedical Research, Cambridge, MA 02142, USA.

出版信息

Proc Natl Acad Sci U S A. 2011 Feb 1;108(5):1763-70. doi: 10.1073/pnas.1014402108. Epub 2011 Jan 5.

Abstract

The ubiquitin (Ub)-related modifier Urm1 functions as a sulfur carrier in tRNA thiolation by means of a mechanism that requires the formation of a thiocarboxylate at the C-terminal glycine residue of Urm1. However, whether Urm1 plays an additional role as a Ub-like protein modifier remains unclear. Here, we show that Urm1 is conjugated to lysine residues of target proteins and that oxidative stress enhances protein urmylation in both Saccharomyces cerevisiae and mammalian cells. Similar to ubiquitylation, urmylation involves a thioester intermediate and results in the formation of a covalent peptide bond between Urm1 and its substrates. In contrast to modification by canonical Ub-like modifiers, however, conjugation of Urm1 involves a C-terminal thiocarboxylate of the modifier. We have confirmed that the peroxiredoxin Ahp1 is such a substrate in S. cerevisiae and found that Urm1 targets a specific lysine residue of Ahp1 in vivo. In addition, we have identified several unique substrates in mammalian cells and show that Urm1 targets at least two pathways on oxidant treatment. First, Urm1 is appended to lysine residues of three components that function in its own pathway (i.e., MOCS3, ATPBD3, and CTU2). Second, Urm1 is conjugated to the nucleocytoplasmic shuttling factor cellular apoptosis susceptibility protein. Thus, Urm1 has a conserved dual role by integrating the functions of prokaryotic sulfur carriers with those of eukaryotic protein modifiers of the Ub family.

摘要

泛素(Ub)相关修饰物 Urm1 通过一种需要在 Urm1 的 C 末端甘氨酸残基形成硫代羧酸酯的机制,充当 tRNA 硫代修饰的硫载体。然而,Urm1 是否作为另一种 Ub 样蛋白修饰物发挥作用尚不清楚。在这里,我们表明 Urm1 被连接到靶蛋白的赖氨酸残基上,并且氧化应激增强了酿酒酵母和哺乳动物细胞中蛋白质的 urmylation。与泛素化相似,urmylation 涉及硫酯中间物,并且导致 Urm1 与其底物之间形成共价肽键。然而,与经典 Ub 样修饰物的修饰不同,Urm1 的连接涉及修饰物的 C 末端硫代羧酸酯。我们已经证实,过氧化物酶 Ahp1 是酿酒酵母中的这种底物,并发现 Urm1 在体内靶向 Ahp1 的特定赖氨酸残基。此外,我们在哺乳动物细胞中鉴定了几个独特的底物,并表明 Urm1 至少靶向氧化应激处理的两个途径。首先,Urm1 被连接到其自身途径中的三个组件的赖氨酸残基上(即,MOCS3、ATPBD3 和 CTU2)。其次,Urm1 与核细胞质穿梭因子细胞凋亡易感性蛋白结合。因此,Urm1 通过整合原核硫载体的功能与真核 Ub 家族蛋白修饰物的功能,具有保守的双重作用。

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