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转录因子Gcn4的调控性降解

Regulated degradation of the transcription factor Gcn4.

作者信息

Kornitzer D, Raboy B, Kulka R G, Fink G R

机构信息

Whitehead Institute, Nine Cambridge Center, MA 02142.

出版信息

EMBO J. 1994 Dec 15;13(24):6021-30. doi: 10.1002/j.1460-2075.1994.tb06948.x.

Abstract

We report that Gcn4, a yeast transcriptional activator of the bZIP family involved in the regulation of the biosynthesis of amino acids and purines, is rapidly turned over. This degradation is inhibited under conditions of starvation for amino acids. Degradation is also inhibited by single amino acid alterations in a region adjacent to the Gcn4 activation domain. Furthermore, we show that degradation of Gcn4 proceeds through the ubiquitin pathway, a major proteolytic system for cytoplasmic proteins, and is dependent on two specific ubiquitin conjugating enzymes, Cdc34 (Ubc3) and Rad6 (Ubc2). As a first step towards reconstituting the Gcn4 degradation pathway in vitro, we show that purified Cdc34 and Rad6 proteins are able to direct the specific ubiquitination of Gcn4.

摘要

我们报告称,酵母碱性亮氨酸拉链(bZIP)家族的转录激活因子Gcn4参与氨基酸和嘌呤生物合成的调控,其更新迅速。在氨基酸饥饿条件下,这种降解受到抑制。Gcn4激活域附近区域的单个氨基酸改变也会抑制降解。此外,我们发现Gcn4的降解通过泛素途径进行,泛素途径是细胞质蛋白的主要蛋白水解系统,并且依赖于两种特定的泛素结合酶Cdc34(Ubc3)和Rad6(Ubc2)。作为在体外重建Gcn4降解途径的第一步,我们证明纯化的Cdc34和Rad6蛋白能够指导Gcn4的特异性泛素化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8441/395579/40eb09bbb189/emboj00072-0238-a.jpg

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