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半胱氨酸乙酰化是一种参与代谢调节的翻译后修饰。

Cysteine -acetylation is a post-translational modification involved in metabolic regulation.

作者信息

Keenan E Keith, Bareja Akshay, Lam Yannie, Grimsrud Paul A, Hirschey Matthew D

机构信息

Duke Molecular Physiology Institute and Sarah W. Stedman Nutrition and Metabolism Center, Duke University Medical Center, Durham NC 27701.

Department of Pharmacology & Cancer Biology, Duke University Medical Center, Durham NC 27710.

出版信息

bioRxiv. 2024 May 21:2024.05.21.595030. doi: 10.1101/2024.05.21.595030.

Abstract

Cysteine is a reactive amino acid central to the catalytic activities of many enzymes. It is also a common target of post-translational modifications (PTMs), such as palmitoylation. This longchain acyl PTM can modify cysteine residues and induce changes in protein subcellular localization. We hypothesized that cysteine could also be modified by short-chain acyl groups, such as cysteine -acetylation. To test this, we developed sample preparation and non-targeted mass spectrometry protocols to analyze the mouse liver proteome for cysteine acetylation. Our findings revealed hundreds of sites of cysteine acetylation across multiple tissue types, revealing a previously uncharacterized cysteine acetylome. Cysteine acetylation shows a marked cytoplasmic subcellular localization signature, with tissue-specific acetylome patterns and specific changes upon metabolic stress. This study uncovers a novel aspect of cysteine biochemistry, highlighting short-chain modifications alongside known long-chain acyl PTMs. These findings enrich our understanding of the landscape of acyl modifications and suggest new research directions in enzyme activity regulation and cellular signaling in metabolism.

摘要

半胱氨酸是一种具有反应活性的氨基酸,对许多酶的催化活性至关重要。它也是翻译后修饰(PTM)的常见靶点,如棕榈酰化。这种长链酰基PTM可以修饰半胱氨酸残基并诱导蛋白质亚细胞定位的变化。我们推测半胱氨酸也可能被短链酰基修饰,如半胱氨酸乙酰化。为了验证这一点,我们开发了样品制备和非靶向质谱分析方法,以分析小鼠肝脏蛋白质组中的半胱氨酸乙酰化情况。我们的研究结果揭示了多种组织类型中数百个半胱氨酸乙酰化位点,揭示了一个以前未被表征的半胱氨酸乙酰化组。半胱氨酸乙酰化显示出明显的细胞质亚细胞定位特征,具有组织特异性的乙酰化组模式以及在代谢应激时的特定变化。这项研究揭示了半胱氨酸生物化学的一个新方面,突出了短链修饰以及已知的长链酰基PTM。这些发现丰富了我们对酰基修饰格局的理解,并为代谢中酶活性调节和细胞信号传导提出了新的研究方向。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d86a/11142221/4d4484efdeac/nihpp-2024.05.21.595030v1-f0001.jpg

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