| Literature DB >> 35290573 |
Yuntao Liu1,2, Lan Song3, Nairen Zheng3, Jinwen Shi3, Hongxing Wu4, Xing Yang4, Nianci Xue1,3, Xing Chen5, Yimin Li6,7, Changqing Sun8, Cha Chen1, Lijuan Tang1, Xiaotian Ni4, Yi Wang3, Yaling Shi9, Jianwen Guo10,11, Guangshun Wang12, Zhongde Zhang13,14, Jun Qin15.
Abstract
Signaling pathway alterations in COVID-19 of living humans as well as therapeutic targets of the host proteins are not clear. We analyzed 317 urine proteomes, including 86 COVID-19, 55 pneumonia and 176 healthy controls, and identified specific RNA virus detector protein DDX58/RIG-I only in COVID-19 samples. Comparison of the COVID-19 urinary proteomes with controls revealed major pathway alterations in immunity, metabolism and protein localization. Biomarkers that may stratify severe symptoms from moderate ones suggested that macrophage induced inflammation and thrombolysis may play a critical role in worsening the disease. Hyper activation of the TCA cycle is evident and a macrophage enriched enzyme CLYBL is up regulated in COVID-19 patients. As CLYBL converts the immune modulatory TCA cycle metabolite itaconate through the citramalyl-CoA intermediate to acetyl-CoA, an increase in CLYBL may lead to the depletion of itaconate, limiting its anti-inflammatory function. These observations suggest that supplementation of itaconate and inhibition of CLYBL are possible therapeutic options for treating COVID-19, opening an avenue of modulating host defense as a means of combating SARS-CoV-2 viruses.Entities:
Keywords: CLYBL; COVID-19; itaconate; proteome; urine
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Year: 2022 PMID: 35290573 PMCID: PMC8922985 DOI: 10.1007/s11427-021-2070-y
Source DB: PubMed Journal: Sci China Life Sci ISSN: 1674-7305 Impact factor: 10.372