| Literature DB >> 34715018 |
Junnan Wu1, Ziyuan Ma2, Archana Raman2, Pazit Beckerman2, Poonam Dhillon2, Dhanunjay Mukhi2, Matthew Palmer3, Hua Chang Chen4, Cassiane Robinson Cohen5, Thomas Dunn6, John Reilly6, Nuala Meyer6, Michael Shashaty7, Zoltan Arany8, György Haskó9, Krzysztof Laudanski10, Adriana Hung5, Katalin Susztak11.
Abstract
The incidence and severity of sepsis is higher among individuals of African versus European ancestry. We found that genetic risk variants (RVs) in the trypanolytic factor apolipoprotein L1 (APOL1), present only in individuals of African ancestry, were associated with increased sepsis incidence and severity. Serum APOL1 levels correlated with sepsis and COVID-19 severity, and single-cell sequencing in human kidneys revealed high expression of APOL1 in endothelial cells. Analysis of mice with endothelial-specific expression of RV APOL1 and in vitro studies demonstrated that RV APOL1 interfered with mitophagy, leading to cytosolic release of mitochondrial DNA and activation of the inflammasome (NLRP3) and the cytosolic nucleotide sensing pathways (STING). Genetic deletion or pharmacological inhibition of NLRP3 and STING protected mice from RV APOL1-induced permeability defects and proinflammatory endothelial changes in sepsis. Our studies identify the inflammasome and STING pathways as potential targets to reduce APOL1-associated health disparities in sepsis and COVID-19.Entities:
Keywords: APOL1; COVID-19; endothelial cell; mitophagy; sepsis
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Year: 2021 PMID: 34715018 PMCID: PMC9338439 DOI: 10.1016/j.immuni.2021.10.004
Source DB: PubMed Journal: Immunity ISSN: 1074-7613 Impact factor: 43.474