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利用酶/人工底物系统增强细胞过硫化物并减轻神经炎症。

Leveraging an enzyme/artificial substrate system to enhance cellular persulfides and mitigate neuroinflammation.

作者信息

Bora Prerona, Manna Suman, Nair Mrutyunjay A, Sathe Rupali R M, Singh Shubham, Sreyas Adury Venkata Sai, Gupta Kavya, Mukherjee Arnab, Saini Deepak K, Kamat Siddhesh S, Hazra Amrita B, Chakrapani Harinath

机构信息

Department of Chemistry, Indian Institute of Science Education and Research Pune Dr. Homi Bhabha Road, Pashan Pune 411 008 Maharashtra India

Department of Biology, Indian Institute of Science Education and Research Pune Dr. Homi Bhabha Road, Pashan Pune 411 008 Maharashtra India.

出版信息

Chem Sci. 2021 Aug 24;12(39):12939-12949. doi: 10.1039/d1sc03828a. eCollection 2021 Oct 13.

DOI:10.1039/d1sc03828a
PMID:34745524
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC8513928/
Abstract

Persulfides and polysulfides, collectively known as the sulfane sulfur pool along with hydrogen sulfide (HS), play a central role in cellular physiology and disease. Exogenously enhancing these species in cells is an emerging therapeutic paradigm for mitigating oxidative stress and inflammation that are associated with several diseases. In this study, we present a unique approach of using the cell's own enzyme machinery coupled with an array of artificial substrates to enhance the cellular sulfane sulfur pool. We report the synthesis and validation of artificial/unnatural substrates specific for 3-mercaptopyruvate sulfurtransferase (3-MST), an important enzyme that contributes to sulfur trafficking in cells. We demonstrate that these artificial substrates generate persulfides as well as mediate sulfur transfer to low molecular weight thiols and to cysteine-containing proteins. A nearly 100-fold difference in the rates of HS production for the various substrates is observed supporting the tunability of persulfide generation by the 3-MST enzyme/artificial substrate system. Next, we show that the substrate permeates cells and is selectively turned over by 3-MST to generate 3-MST-persulfide, which protects against reactive oxygen species-induced lethality. Lastly, in a mouse model, is found to significantly mitigate neuroinflammation in the brain tissue. Together, the approach that we have developed allows for the on-demand generation of persulfides and using a range of shelf-stable, artificial substrates of 3-MST, while opening up possibilities of harnessing these molecules for therapeutic applications.

摘要

过硫化物和多硫化物与硫化氢(HS)一起统称为硫烷硫池,在细胞生理学和疾病中起着核心作用。在细胞中外源性增强这些物质是一种新兴的治疗模式,用于减轻与多种疾病相关的氧化应激和炎症。在本研究中,我们提出了一种独特的方法,即利用细胞自身的酶机制与一系列人工底物相结合,以增强细胞硫烷硫池。我们报告了对3-巯基丙酮酸硫转移酶(3-MST)具有特异性的人工/非天然底物的合成与验证,3-MST是一种在细胞硫转运中起重要作用的酶。我们证明这些人工底物能生成过硫化物,并介导硫向低分子量硫醇和含半胱氨酸的蛋白质转移。观察到各种底物生成HS的速率存在近100倍的差异,这支持了3-MST酶/人工底物系统生成过硫化物的可调性。接下来,我们表明该底物可渗透细胞,并被3-MST选择性转化以生成3-MST-过硫化物,从而保护细胞免受活性氧诱导的杀伤。最后,在小鼠模型中,发现该底物能显著减轻脑组织中的神经炎症。总之,我们开发的方法能够利用一系列稳定的3-MST人工底物按需生成过硫化物和多硫化物,同时为将这些分子用于治疗应用开辟了可能性。

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