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-4位苯丙氨酸是HECT泛素连接酶催化底物泛素化所必需的。

The -4 phenylalanine is required for substrate ubiquitination catalyzed by HECT ubiquitin ligases.

作者信息

Salvat Catherine, Wang Guangli, Dastur Anahita, Lyon Nancy, Huibregtse Jon M

机构信息

Institute for Cellular and Molecular Biology, Section of Molecular Genetics and Microbiology, University of Texas at Austin, Austin, Texas 78712, USA.

出版信息

J Biol Chem. 2004 Apr 30;279(18):18935-43. doi: 10.1074/jbc.M312201200. Epub 2004 Feb 13.

Abstract

The reaction cycle of HECT domain ubiquitin ligases consists of three steps: 1) binding of an E2 protein, 2) transfer of ubiquitin from E2 to the HECT domain, and 3) transfer of ubiquitin to the substrate. We report the identification of a determinant that is specifically required for the last step of this cycle, a phenylalanine residue located four amino acids from the C terminus of most HECT domains, referred to here as the -4F. Alteration of this residue in human E6AP and Saccharomyces cerevisae Rsp5p did not affect ubiquitin-thioester formation, but effectively blocked substrate ubiquitination. Alteration of the -4F to alanine with concomitant substitution of a nearby residue to phenylalanine only partially restored Rsp5p activity, indicating that precise spatial placement of this residue is important. C-terminally extended E6AP and Rsp5p proteins were also defective for substrate ubiquitination, providing a likely biochemical understanding of a previously isolated Angelman syndrome-associated mutation of E6AP that alters the stop codon of an otherwise wild-type gene. We propose that the -4F may play a role in orienting ubiquitin when it is tethered to the HECT active site cysteine. This may be necessary to allow for approach of the incoming lysine epsilon-amino group of the substrate.

摘要

HECT结构域泛素连接酶的反应循环由三个步骤组成:1)E2蛋白的结合;2)泛素从E2转移至HECT结构域;3)泛素转移至底物。我们报告了一个在该循环最后一步特别需要的决定因素的鉴定结果,即大多数HECT结构域C末端四个氨基酸处的一个苯丙氨酸残基,在此称为-4F。人E6AP和酿酒酵母Rsp5p中该残基的改变不影响泛素硫酯的形成,但有效地阻断了底物泛素化。将-4F替换为丙氨酸并同时将附近一个残基替换为苯丙氨酸仅部分恢复了Rsp5p的活性,表明该残基精确的空间位置很重要。C末端延伸的E6AP和Rsp5p蛋白在底物泛素化方面也存在缺陷,这为先前分离出的与天使综合征相关的E6AP突变提供了可能的生化解释,该突变改变了一个原本野生型基因的终止密码子。我们提出,-4F在泛素连接到HECT活性位点半胱氨酸上时,可能在其定向中发挥作用。这对于底物赖氨酸ε-氨基的接近可能是必要的。

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