Neutrophils restricted contribution of CCRL2 genetic variants to COVID-19 severity
Article 2024 en
Authors
ML
Mattia Laffranchi
EP
Elvezia Maria Paraboschi
FB
Francisco M. Bianchetto-Aguilera
Abstract
1 min read
The 3p21.31 locus is the most robust genomic region associated with COVID-19 severity. This locus contains a main chemokine receptor (CKR) cluster. We tested expression quantitative trait loci (eQTL) targeting the 3p21.31 CKR cluster linked to COVID-19 hospitalization in Europeans from the COVID-19 HGI meta-analysis. Among these, <i>CCRL2</i>, a key regulator of neutrophil trafficking, was targeted by neutrophil-restricted eQTLs. We confirmed these eQTLs in an Italian COVID-19 cohort. Haplotype analysis revealed a link between an increased <i>CCRL2</i> expression and COVID-19 severity and hospitalization. By the exposure of neutrophils to a TLR8 ligand, reflecting a viral infection, we revealed specific chromatin domains within the 3p21.31 locus exclusive to neutrophils. In addition, the identified variants mapped within these regions altered the binding motif of neutrophils-expressed transcription factors. These results support that <i>CCRL2</i> eQTL variants contribute to the risk of severe COVID-19 by selectively affecting neutrophil functions.
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