A Novel Macrophage Subpopulation Conveys Increased Genetic Risk of Coronary Artery Disease

Jiahao Jiang; Thomas K Hiron; Thomas Agbaedeng; Yashaswat Malhotra; Edward Drydale; James Bancroft; Esther Ng; Michael E Reschen; Lucy J Davison; Chris A O'Callaghan

doi:10.1161/CIRCRESAHA.123.324172

A Novel Macrophage Subpopulation Conveys Increased Genetic Risk of Coronary Artery Disease

Circ Res. 2024 May 15. doi: 10.1161/CIRCRESAHA.123.324172. Online ahead of print.

Authors

Affiliations

¹ Nuffield Department of Medicine, Wellcome Centre for Human Genetics, University of Oxford, United Kingdom. (J.J., T.K.H., T.A., Y.M., E.D., J.B., L.J.D., C.A.O.).
² Nuffield Department of Orthopaedics, Kennedy Institute of Rheumatology, Rheumatology and Musculoskeletal Sciences, University of Oxford, United Kingdom. (E.N.).
³ Oxford University Hospitals NHS Foundation Trust, John Radcliffe Hospital, United Kingdom (M.E.R.).
⁴ Department of Clinical Science and Services, Royal Veterinary College, Hatfield, United Kingdom (L.J.D.).

^# Contributed equally.

PMID: 38747151
DOI: 10.1161/CIRCRESAHA.123.324172

Abstract

Background: Coronary artery disease (CAD), the leading cause of death worldwide, is influenced by both environmental and genetic factors. Although over 250 genetic risk loci have been identified through genome-wide association studies, the specific causal variants and their regulatory mechanisms are still largely unknown, particularly in disease-relevant cell types like macrophages.

Methods: We utilized single-cell RNA-seq and single-cell multiomics approaches in primary human monocyte-derived macrophages to explore the transcriptional regulatory network involved in a critical pathogenic event of coronary atherosclerosis-the formation of lipid-laden foam cells. The relative genetic contribution to CAD was assessed by partitioning disease heritability across different macrophage subpopulations. Meta-analysis of single-cell RNA-seq data sets from 38 human atherosclerotic samples was conducted to provide high-resolution cross-referencing to macrophage subpopulations in vivo.

Results: We identified 18 782 cis-regulatory elements by jointly profiling the gene expression and chromatin accessibility of >5000 macrophages. Integration with CAD genome-wide association study data prioritized 121 CAD-related genetic variants and 56 candidate causal genes. We showed that CAD heritability was not uniformly distributed and was particularly enriched in the gene programs of a novel CD52-hi lipid-handling macrophage subpopulation. These CD52-hi macrophages displayed significantly less lipoprotein accumulation and were also found in human atherosclerotic plaques. We investigated the cis-regulatory effect of a risk variant rs10488763 on FDX1, implicating the recruitment of AP-1 and C/EBP-β in the causal mechanisms at this locus.

Conclusions: Our results provide genetic evidence of the divergent roles of macrophage subsets in atherogenesis and highlight lipid-handling macrophages as a key subpopulation through which genetic variants operate to influence disease. These findings provide an unbiased framework for functional fine-mapping of genome-wide association study results using single-cell multiomics and offer new insights into the genotype-environment interactions underlying atherosclerotic disease.

Keywords: apoptosis; cell proliferation; fibrosis; hypoxia; macrophages.