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酿酒酵母的RAD6基因产物在某些蛋白质的泛素化过程中需要一种假定的泛素蛋白连接酶(E3)。

RAD6 gene product of Saccharomyces cerevisiae requires a putative ubiquitin protein ligase (E3) for the ubiquitination of certain proteins.

作者信息

Sharon G, Raboy B, Parag H A, Dimitrovsky D, Kulka R G

机构信息

Department of Biological Chemistry, Alexander Silberman Institute of Life Sciences, Hebrew University of Jerusalem, Israel.

出版信息

J Biol Chem. 1991 Aug 25;266(24):15890-4.

PMID:1651925
Abstract

The RAD6 (UBC2) gene of Saccharomyces cerevisiae which is involved in DNA repair, induced mutagenesis, and sporulation, encodes a ubiquitin-conjugating enzyme (E2). Since the RAD6 gene product can transfer ubiquitin directly to histones in vitro without the participation of a ubiquitin protein ligase (E3), it has been suggested that in vivo it also acts by the unassisted conjugation of ubiquitin to histones or to other target proteins. Here we show that the RAD6 protein can ligate ubiquitin in vitro to a hitherto unknown set of exogenous target proteins (alpha-, beta-, and kappa-casein and beta-lactoglobulin) when supplemented by a putative ubiquitin protein ligase (E3-R) from S. cerevisiae. RAD6 supplemented with E3-R ligates 1 or, sometimes, 2 ubiquitin molecules to the target protein molecule. UBC3 (CDC34) protein in the presence of E3-R has barely detectable activity on the non-histone substrates. Other ubiquitin-conjugating enzymes tested (products of the UBC1 and UBC4 genes) do not cooperate with E3-R in conjugating ubiquitin to the same substrates. Thus, E3-R apparently interacts selectively with RAD6 protein. These findings suggest that some of the in vivo activities of the RAD6 gene may involve E3-R.

摘要

酿酒酵母的RAD6(UBC2)基因参与DNA修复、诱变和孢子形成,编码一种泛素结合酶(E2)。由于RAD6基因产物在体外可在无泛素蛋白连接酶(E3)参与的情况下直接将泛素转移至组蛋白,因此有人提出,在体内它也是通过将泛素直接结合至组蛋白或其他靶蛋白来发挥作用。我们在此表明,当补充来自酿酒酵母的一种假定泛素蛋白连接酶(E3-R)时,RAD6蛋白在体外可将泛素连接至一组此前未知的外源靶蛋白(α-、β-和κ-酪蛋白以及β-乳球蛋白)。补充有E3-R的RAD6将1个或有时2个泛素分子连接至靶蛋白分子。在E3-R存在的情况下,UBC3(CDC34)蛋白对非组蛋白底物几乎没有可检测到的活性。所测试的其他泛素结合酶(UBC1和UBC4基因的产物)在将泛素结合至相同底物方面不与E3-R协同作用。因此,E3-R显然与RAD6蛋白选择性相互作用。这些发现表明,RAD6基因的一些体内活性可能涉及E3-R。

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