Literature DB >> 33393624

Novel insights into plasma biomarker candidates in patients with chronic mountain sickness based on proteomics.

Peili Zhang1,2,3, Zhanquan Li1,2,4, Faman Yang4, Linhua Ji1,2,5, Yingzhong Yang1,2, Chuanchuan Liu1,2, Huihui Liu1,2, Jie Ma4, Jie Liu1,2, Zhancui Dang1,2, Shengyan Wang1,2, Rili Ge1,2, Sen Cui4.   

Abstract

Chronic mountain sickness (CMS) is a progressive incapacitating syndrome induced by lifelong exposure to hypoxia. In the present study, proteomic analysis was used to identify the differentially expressed proteins (DEPs) and then evaluate the potential plasma biomarkers between CMS and non-CMS groups. A total of 145 DEPs were detected in CMS Han Chinese people who live in the plateau (CMS-HPu), among which 89 were significantly up-regulated and 56 were significantly down-regulated. GO enrichment analysis showed that various biological processes were enriched, including the hydrogen peroxide metabolic/catabolic process, reactive oxygen species (ROS) metabolic, and acute inflammatory response. Protein-protein interaction analysis showed that antioxidant activity, the hydrogen peroxide catabolic process and peroxidase activity were primarily mapped in interaction proteins. Nine modules showed significantly clustering based on WGCNA analysis, with two being the most significant, and GO analysis showed that proteins of both modules were primarily enriched in oxidative stress-related biological processes. Four DEPs increased in CMS patients were evaluated as the candidate biomarkers, and three showed significant AUC: hemoglobin β chain (HB-β), thioredoxin-1 (TRX1), and phosphoglycerate kinase 1 (PGK1). The present study provides insights into the pathogenesis of CMS and further evaluates the potentially biomarkers for its prevention and treatment of it.
© 2021 The Author(s).

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Keywords:  biomarkers; chronic mountain sickness; hemoglobin beta chain; phosphoglycerate kinase 1; proteomics; thioredoxin-1

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Year:  2021        PMID: 33393624      PMCID: PMC7816071          DOI: 10.1042/BSR20202219

Source DB:  PubMed          Journal:  Biosci Rep        ISSN: 0144-8463            Impact factor:   3.840


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  2 in total

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