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定量过硫化物位点鉴定(qPerS-SID)揭示了在哺乳动物细胞中 H2S 释放供体的蛋白质靶标。

Quantitative Persulfide Site Identification (qPerS-SID) Reveals Protein Targets of H2S Releasing Donors in Mammalian Cells.

机构信息

Pharmazentrum Frankfurt/ZAFES, Universitätsklinikum Frankfurt, Frankfurt am Main, Germany.

Functional Proteomics, SFB 815 Core Unit, Goethe University Frankfurt, Frankfurt, Germany.

出版信息

Sci Rep. 2016 Jul 14;6:29808. doi: 10.1038/srep29808.

Abstract

H2S is an important signalling molecule involved in diverse biological processes. It mediates the formation of cysteine persulfides (R-S-SH), which affect the activity of target proteins. Like thiols, persulfides show reactivity towards electrophiles and behave similarly to other cysteine modifications in a biotin switch assay. In this manuscript, we report on qPerS-SID a mass spectrometry-based method allowing the isolation of persulfide containing peptides in the mammalian proteome. With this method, we demonstrated that H2S donors differ in their efficacy to induce persulfides in HEK293 cells. Furthermore, data analysis revealed that persulfide formation affects all subcellular compartments and various cellular processes. Negatively charged amino acids appeared more frequently adjacent to cysteines forming persulfides. We confirmed our proteomic data using pyruvate kinase M2 as a model protein and showed that several cysteine residues are prone to persulfide formation finally leading to its inactivation. Taken together, the site-specific identification of persulfides on a proteome scale can help to identify target proteins involved in H2S signalling and enlightens the biology of H2S and its releasing agents.

摘要

H2S 是一种参与多种生物过程的重要信号分子。它介导半胱氨酸过硫化物(R-S-SH)的形成,从而影响靶蛋白的活性。与硫醇类似,过硫化物对亲电试剂表现出反应性,并在生物素开关测定中类似于其他半胱氨酸修饰物的行为。在本手稿中,我们报告了基于质谱的 qPerS-SID 方法,该方法允许在哺乳动物蛋白质组中分离含有过硫化物的肽。使用该方法,我们证明了 H2S 供体在诱导 HEK293 细胞中过硫化物的效力上有所不同。此外,数据分析表明过硫化物的形成影响所有亚细胞区室和各种细胞过程。带负电荷的氨基酸更频繁地出现在形成过硫化物的半胱氨酸附近。我们使用丙酮酸激酶 M2 作为模型蛋白验证了我们的蛋白质组学数据,并表明几个半胱氨酸残基容易形成过硫化物,最终导致其失活。总之,在蛋白质组范围内对过硫化物进行特异性鉴定有助于识别参与 H2S 信号的靶蛋白,并阐明 H2S 及其释放剂的生物学。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/560a/4944133/f121d5cacc85/srep29808-f1.jpg

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