Characterization of complement C3 as a marker of alpha-amanitin toxicity by comparative secretome profiling.

IF 1.6 4区 医学 Q4 TOXICOLOGY
Toxicological Research Pub Date : 2022-12-22 eCollection Date: 2023-04-01 DOI:10.1007/s43188-022-00163-z
Doeun Kim, Min Seo Lee, Hyunchae Sim, Sangkyu Lee, Hye Suk Lee
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Abstract

In the human body, proteins secreted into peripheral blood vessels are known as the secretome, and they represent the physiological or pathological status of cells. The unique response of cells to toxin exposure can be confirmed via secretome analysis, which can be used to discover toxic mechanisms or exposure markers. Alpha-amanitin (α-AMA) is the most widely studied amatoxin and inhibits transcription and protein synthesis by directly interacting with RNA polymerase II. However, secretory proteins released during hepatic failure caused by α-AMA have not been fully characterized. In this study, we analyzed the secretome of α-AMA-treated Huh-7 cells and mice using a comparative proteomics technique. Overall, 1440 and 208 proteins were quantified in cell media and mouse serum, respectively. Based on the bioinformatics results for the commonly downregulated proteins in cell media and mouse serum, we identified complement component 3 (C3) as a marker for α-AMA-induced hepatotoxicity. Through western blot in cell secretome and C3 ELISA assays in mouse serum, we validated α-AMA-induced downregulation of C3. In conclusion, using comparative proteomics and molecular biology techniques, we found that α-AMA-induced hepatotoxicity reduced C3 levels in the secretome. We expect that this study will aid in identifying new toxic mechanisms, therapeutic targets, and exposure markers of α-AMA-induced hepatotoxicity.

Supplementary information: The online version contains supplementary material available at 10.1007/s43188-022-00163-z.

通过比较分泌组特征分析作为α-amanitin毒性标志的补体C3。
在人体中,分泌到外周血管中的蛋白质被称为分泌组,它们代表了细胞的生理或病理状态。通过分泌组分析可以确认细胞对毒素暴露的独特反应,从而发现毒性机制或暴露标记。α-amanitin(α-AMA)是研究最广泛的一种氨毒素,它通过与RNA聚合酶II直接作用来抑制转录和蛋白质合成。然而,α-AMA 引起肝功能衰竭时释放的分泌蛋白尚未完全定性。在本研究中,我们采用比较蛋白质组学技术分析了经α-AMA处理的Huh-7细胞和小鼠的分泌组。在细胞培养基和小鼠血清中分别量化了 1440 和 208 种蛋白质。根据生物信息学对细胞介质和小鼠血清中常见下调蛋白的研究结果,我们确定补体成分3(C3)是α-AMA诱导肝毒性的标志物。通过细胞分泌物中的 Western 印迹和小鼠血清中的 C3 酶联免疫吸附试验,我们验证了 α-AMA 诱导的 C3 下调。总之,利用比较蛋白质组学和分子生物学技术,我们发现α-AMA诱导的肝毒性降低了分泌组中的C3水平。我们希望这项研究有助于确定α-AMA诱导的肝毒性的新毒性机制、治疗靶点和暴露标志物:在线版本包含补充材料,可查阅 10.1007/s43188-022-00163-z。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
4.20
自引率
4.30%
发文量
39
期刊介绍: Toxicological Research is the official journal of the Korean Society of Toxicology. The journal covers all areas of Toxicological Research of chemicals, drugs and environmental agents affecting human and animals, which in turn impact public health. The journal’s mission is to disseminate scientific and technical information on diverse areas of toxicological research. Contributions by toxicologists, molecular biologists, geneticists, biochemists, pharmacologists, clinical researchers and epidemiologists with a global view on public health through toxicological research are welcome. Emphasis will be given to articles providing an understanding of the toxicological mechanisms affecting animal, human and public health. In the case of research articles using natural extracts, detailed information with respect to the origin, extraction method, chemical profiles, and characterization of standard compounds to ensure the reproducible pharmacological activity should be provided.
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