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YCA1 半胱天冬酶的活性在……中通过过硫化作用由反应性硫烷硫调节。

The Activity of YCA1 Metacaspase Is Regulated by Reactive Sulfane Sulfur via Persulfidation in .

作者信息

Wang Qingda, Zhang Xiaokun, Du Zhuang, Liu Honglei, Xia Yongzhen, Xun Luying, Liu Huaiwei

机构信息

State Key Laboratory of Microbial Technology, Shandong University, Qingdao 266237, China.

Department of Chemistry, School of Molecular Biosciences, Washington State University, Pullman, WA 99164-4630, USA.

出版信息

Antioxidants (Basel). 2024 May 10;13(5):589. doi: 10.3390/antiox13050589.

Abstract

YCA1, the only metacaspase in , plays important roles in the regulation of chronological lifespan, apoptosis, and cytokinesis. YCA1 has protein hydrolase activity and functions by cleaving itself and target proteins. However, there are few reports about the regulation of YCA1 activity. In this study, we observed that reactive sulfane sulfur (RSS) can inhibit the activity of YCA1. In vitro experiments demonstrated that RSS reacted with the Cys of YCA1, the residue central to its protein hydrolase activity, to form a persulfidation modification (protein-SSH). This modification inhibited both its self-cleavage and the cleavage of its substrate protein, BIR1. To investigate further, we constructed a low-endogenous-RSS mutant of , BY4742 Δ, in which the RSS-producing enzyme cystathionine-γ-lyase (CYS3) was knocked out. The activity of YCA1 was significantly increased by the deletion of CYS3. Moreover, increased YCA1 activity led to reduced chronological lifespan (CLS) and CLS-driven apoptosis. This study unveils the first endogenous factor that regulates YCA1 activity, introduces a novel mechanism of how yeast cells regulate chronological lifespan, and broadens our understanding of the multifaceted roles played by RSS.

摘要

YCA1是[具体物种]中唯一的 metacaspase,在调控时序寿命、细胞凋亡和胞质分裂中发挥重要作用。YCA1具有蛋白水解酶活性,通过自我切割和切割靶蛋白发挥功能。然而,关于YCA1活性调控的报道较少。在本研究中,我们观察到活性次磺酸硫(RSS)可抑制YCA1的活性。体外实验表明,RSS与YCA1的半胱氨酸(其蛋白水解酶活性的关键残基)反应,形成过硫化修饰(蛋白质-SSH)。这种修饰抑制了其自我切割及其底物蛋白BIR1的切割。为进一步研究,我们构建了[具体物种]的低内源性RSS突变体BY4742Δ,其中产生RSS的酶胱硫醚-γ-裂解酶(CYS3)被敲除。CYS3的缺失显著提高了YCA1的活性。此外,YCA1活性的增加导致时序寿命(CLS)缩短和CLS驱动的细胞凋亡。本研究揭示了第一个调控YCA1活性的内源性因子,引入了酵母细胞调控时序寿命的新机制,并拓宽了我们对RSS所起多方面作用的理解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bb28/11118234/3d51313243ce/antioxidants-13-00589-g001.jpg

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