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人类Fas(CD95)与泛素结合酶(UBC-FAP)的关联。

Association of human fas (CD95) with a ubiquitin-conjugating enzyme (UBC-FAP).

作者信息

Wright D A, Futcher B, Ghosh P, Geha R S

机构信息

Department of Medicine, Division of Immunology, Children's Hospital, and Department of Pediatrics, Harvard Medical School, Boston, Massachusetts 02115, USA.

出版信息

J Biol Chem. 1996 Dec 6;271(49):31037-43. doi: 10.1074/jbc.271.49.31037.

Abstract

A novel human ubiquitin conjugating enzyme (UBC) was found to associate with Fas (CD95). The mRNA for this UBC Fas-associated protein (FAP) was widely expressed in human tissues, and the protein was identified in several mammalian cell lines. UBC-FAP shows strong homology to two recently identified UBCs, Hus5 and Ubc9, which control yeast cell cycle progression. UBC-FAP, but not an active site mutant, complemented ubc9-1(ts) mutants. This suggests that UBC-FAP is a human homologue of Ubc9, possesses ubiquitin conjugating activity, and may play an important role in mammalian cell cycle regulation. A single amino acid substitution in the death domain of Fas that abolishes Fas-mediated apoptosis also abolished Fas association with UBC-FAP, suggesting that UBC-FAP may play a role in Fas signal transduction. The sequence of UBC-FAP is identical to that of HsUbc9, a UBC recently shown to interact with Rad51.

摘要

一种新型人类泛素结合酶(UBC)被发现与Fas(CD95)相关联。这种UBC Fas相关蛋白(FAP)的mRNA在人体组织中广泛表达,并且在几种哺乳动物细胞系中鉴定出了该蛋白。UBC-FAP与最近鉴定出的两种控制酵母细胞周期进程的UBC,即Hus5和Ubc9,具有很强的同源性。UBC-FAP而非活性位点突变体能够互补ubc9-1(ts)突变体。这表明UBC-FAP是Ubc9的人类同源物,具有泛素结合活性,并且可能在哺乳动物细胞周期调控中发挥重要作用。Fas死亡结构域中的单个氨基酸取代消除了Fas介导的凋亡,同时也消除了Fas与UBC-FAP的关联,这表明UBC-FAP可能在Fas信号转导中发挥作用。UBC-FAP的序列与HsUbc9相同,HsUbc9是一种最近被证明与Rad51相互作用的UBC。

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