Pathogenic Autoimmunity in Atherosclerosis Evolves From Initially Protective Apolipoprotein B 100 –Reactive CD4 + T-Regulatory Cells-Reference-Cited by-同舟云学术

Pathogenic Autoimmunity in Atherosclerosis Evolves From Initially Protective Apolipoprotein B 100 –Reactive CD4 + T-Regulatory Cells

Published:2020-09-29 Issue:13 Volume:142 Page:1279-1293
ISSN:0009-7322
Container-title:Circulation
language:en
Short-container-title:Circulation

Author:

Wolf Dennis¹²³,Gerhardt Teresa¹²⁴,Winkels Holger¹,Michel Nathaly Anto²³⁵,Pramod Akula Bala¹⁶,Ghosheh Yanal¹,Brunel Simon⁷,Buscher Konrad¹,Miller Jacqueline¹,McArdle Sara⁸^ORCID,Baas Livia¹,Kobiyama Kouji¹,Vassallo Melanie¹^ORCID,Ehinger Erik¹,Dileepan Thamotharampillai⁹,Ali Amal¹,Schell Maximilian¹,Mikulski Zbigniew¹,Sidler Daniel¹,Kimura Takayuki¹,Sheng Xia²³,Horstmann Hauke²³,Hansen Sophie²³,Mitre Lucia Sol²³,Stachon Peter²³^ORCID,Hilgendorf Ingo²³,Gaddis Dalia E.¹⁰,Hedrick Catherine¹⁰,Benedict Chris A.⁷,Peters Bjoern¹¹,Zirlik Andreas⁵,Sette Alessandro¹¹,Ley Klaus¹¹⁰^ORCID

Affiliation:

1. Laboratory of Inflammation Biology(D.W., T.G., H.W., A.B.P., Y.G., K.B., J.M., L.B., K.K., M.V., E.E., A.A., M.S., T.K., K.L.), La Jolla Institute for Immunology, CA.

2. Department of Cardiology/Angiology I, University Heart Center Freiburg-Bad Krozingen, Germany (D.W., T.G., N.A.M., X.S., H.H., S.H., L.S.M., P.S., I.H.).

3. Medical Faculty, University of Freiburg, Germany (D.W., N.A.M., X.S., H.H., S.H., L.S.M., P.S., I.H.).

4. Department of Cardiology, Charité - University Medicine Berlin (Campus Benjamin Franklin), Germany (T.G.).

5. Department of Cardiology, Medical University Graz, Austria (N.A.M., A.Z.).

6. Department of Psychiatry, University of California San Diego, La Jolla (A.B.P.).

7. Division of Immune Regulation (S.B., D.S., C.A.B.), La Jolla Institute for Immunology, CA.

8. Microscopy Core Facility (S.M.), La Jolla Institute for Immunology, CA.

9. Department of Microbiology, University of Minnesota Medical School, Minneapolis (T.D.).

10. Center for Autoimmunity and Inflammation (D.E.G., C.H., K.L.), La Jolla Institute for Immunology, CA.

11. Division of Vaccine Discovery (B.P., A.S.), La Jolla Institute for Immunology, CA.

Abstract

Background: Throughout the inflammatory response that accompanies atherosclerosis, autoreactive CD4 + T-helper cells accumulate in the atherosclerotic plaque. Apolipoprotein B 100 (apoB), the core protein of low-density lipoprotein, is an autoantigen that drives the generation of pathogenic T-helper type 1 (T H 1) cells with proinflammatory cytokine secretion. Clinical data suggest the existence of apoB-specific CD4 + T cells with an atheroprotective, regulatory T cell (T reg ) phenotype in healthy individuals. Yet, the function of apoB-reactive T regs and their relationship with pathogenic T H 1 cells remain unknown. Methods: To interrogate the function of autoreactive CD4 + T cells in atherosclerosis, we used a novel tetramer of major histocompatibility complex II to track T cells reactive to the mouse self-peptide apo B 978-993 (apoB + ) at the single-cell level. Results: We found that apoB + T cells build an oligoclonal population in lymph nodes of healthy mice that exhibit a T reg -like transcriptome, although only 21% of all apoB + T cells expressed the T reg transcription factor FoxP3 (Forkhead Box P3) protein as detected by flow cytometry. In single-cell RNA sequencing, apoB + T cells formed several clusters with mixed T H signatures that suggested overlapping multilineage phenotypes with pro- and anti-inflammatory transcripts of T H 1, T helper cell type 2 (T H 2), and T helper cell type 17 (T H 17), and of follicular-helper T cells. ApoB + T cells were increased in mice and humans with atherosclerosis and progressively converted into pathogenic T H 1/T H 17-like cells with proinflammatory properties and only a residual T reg transcriptome. Plaque T cells that expanded during progression of atherosclerosis consistently showed a mixed T H 1/T H 17 phenotype in single-cell RNA sequencing. In addition, we observed a loss of FoxP3 in a fraction of apoB + T regs in lineage tracing of hyperlipidemic Apoe –/– mice. In adoptive transfer experiments, converting apoB + T regs failed to protect from atherosclerosis. Conclusions: Our results demonstrate an unexpected mixed phenotype of apoB-reactive autoimmune T cells in atherosclerosis and suggest an initially protective autoimmune response against apoB with a progressive derangement in clinical disease. These findings identify apoB autoreactive T regs as a novel cellular target in atherosclerosis.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Physiology (medical),Cardiology and Cardiovascular Medicine

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