Interferon regulatory factor-5-dependent CD11c+ macrophages contribute to the formation of rupture–prone atherosclerotic plaques-Reference-Cited by-同舟云学术

Interferon regulatory factor-5-dependent CD11c+ macrophages contribute to the formation of rupture–prone atherosclerotic plaques

Published:2022-02-09 Issue:19 Volume:43 Page:1864-1877
ISSN:0195-668X
Container-title:European Heart Journal
language:en
Short-container-title:

Author:

Edsfeldt Andreas¹²³⁴^ORCID,Swart Maarten³,Singh Pratibha¹,Dib Lea³^ORCID,Sun Jiangming¹,Cole Jennifer E³^ORCID,Park Inhye³,Al-Sharify Dania¹^ORCID,Persson Ana¹,Nitulescu Mihaela¹,Borges Patricia Das Neves³^ORCID,Kassiteridi Christina³^ORCID,Goddard Michael E³,Lee Regent⁵⁶^ORCID,Volkov Petr¹,Orho-Melander Marju¹^ORCID,Maegdefessel Lars⁷⁸^ORCID,Nilsson Jan¹^ORCID,Udalova Irina³,Goncalves Isabel¹²^ORCID,Monaco Claudia³^ORCID

Affiliation:

1. Department of Clinical Sciences, Clinical Research Center, Lund University , Malmö , Sweden

2. Department of Cardiology, Skåne University Hospital , Lund/Malmö , Sweden

3. Kennedy Institute of Rheumatology, Nuffield Department of Orthopaedics, Rheumatology and Musculoskeletal Sciences, University of Oxford , Roosevelt Drive, Headington, Oxford , UK

4. Wallenberg Center for Molecular Medicine, Lund University , Malmö , Sweden

5. Nuffield Department of Surgical Sciences , Oxford,

6. University of Oxford , Oxford,

7. Department of Medicine, Karolinska Institute , Stockholm , Sweden

8. Department of Vascular and Endovascular Surgery, Technical University Munich and DZHK Partner Site Munich , Munich , Germany

Abstract

Abstract Aims Inflammation is a key factor in atherosclerosis. The transcription factor interferon regulatory factor-5 (IRF5) drives macrophages towards a pro-inflammatory state. We investigated the role of IRF5 in human atherosclerosis and plaque stability. Methods and results Bulk RNA sequencing from the Carotid Plaque Imaging Project biobank were used to mine associations between major macrophage associated genes and transcription factors and human symptomatic carotid disease. Immunohistochemistry, proximity extension assays, and Helios cytometry by time of flight (CyTOF) were used for validation. The effect of IRF5 deficiency on carotid plaque phenotype and rupture in ApoE−/− mice was studied in an inducible model of plaque rupture. Interferon regulatory factor-5 and ITGAX/CD11c were identified as the macrophage associated genes with the strongest associations with symptomatic carotid disease. Expression of IRF5 and ITGAX/CD11c correlated with the vulnerability index, pro-inflammatory plaque cytokine levels, necrotic core area, and with each other. Macrophages were the predominant CD11c-expressing immune cells in the plaque by CyTOF and immunohistochemistry. Interferon regulatory factor-5 immunopositive areas were predominantly found within CD11c+ areas with a predilection for the shoulder region, the area of the human plaque most prone to rupture. Accordingly, an inducible plaque rupture model of ApoE−/−Irf5−/− mice had significantly lower frequencies of carotid plaque ruptures, smaller necrotic cores, and less CD11c+ macrophages than their IRF5-competent counterparts. Conclusion Using complementary evidence from data from human carotid endarterectomies and a murine model of inducible rupture of carotid artery plaque in IRF5-deficient mice, we demonstrate a mechanistic link between the pro-inflammatory transcription factor IRF5, macrophage phenotype, plaque inflammation, and its vulnerability to rupture.

Funder

British Heart Foundation

Swedish Society for Medical Research, Emil and Wera Cornell foundation

Swedish Research Council

Crafoord foundation

Swedish Society of Medicine

Diabetes foundation

Swedish Heart and Lung Foundation

Diabetes Research and Wellness foundation

Southern Sweden Regional Research Funding

SUS foundations and funds

Lund University Diabetes Center