Pathogenic Autoimmunity in Atherosclerosis Evolves From Initially Protective Apolipoprotein B<sub>100</sub>-Reactive CD4<sup>+</sup> T-Regulatory Cells.

Wolf, Dennis; Gerhardt, Teresa; Winkels, Holger; Michel, Nathaly Anto; Pramod, Akula Bala; Ghosheh, Yanal; Brunel, Simon; Buscher, Konrad; Miller, Jacqueline; McArdle, Sara; Baas, Livia; Kobiyama, Kouji; Vassallo, Melanie; Ehinger, Erik; Dileepan, Thamotharampillai; Ali, Amal; Schell, Maximilian; Mikulski, Zbigniew; Sidler, Daniel; Kimura, Takayuki; Sheng, Xia; Horstmann, Hauke; Hansen, Sophie; Mitre, Lucia Sol; Stachon, Peter; Hilgendorf, Ingo; Gaddis, Dalia E; Hedrick, Catherine; Benedict, Chris A; Peters, Bjoern; Zirlik, Andreas; Sette, Alessandro; Ley, Klaus

Pathogenic Autoimmunity in Atherosclerosis Evolves From Initially Protective Apolipoprotein B₁₀₀-Reactive CD4⁺ T-Regulatory Cells.

Wolf, Dennis; Gerhardt, Teresa; Winkels, Holger; Michel, Nathaly Anto; Pramod, Akula Bala; Ghosheh, Yanal; Brunel, Simon; Buscher, Konrad; Miller, Jacqueline; McArdle, Sara; Baas, Livia; Kobiyama, Kouji; Vassallo, Melanie; Ehinger, Erik; Dileepan, Thamotharampillai; Ali, Amal; Schell, Maximilian; Mikulski, Zbigniew; Sidler, Daniel; Kimura, Takayuki; Sheng, Xia; Horstmann, Hauke; Hansen, Sophie; Mitre, Lucia Sol; Stachon, Peter; Hilgendorf, Ingo; Gaddis, Dalia E; Hedrick, Catherine; Benedict, Chris A; Peters, Bjoern; Zirlik, Andreas; Sette, Alessandro; Ley, Klaus.

Afiliação

Wolf D; 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.
Gerhardt T; 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.).
Winkels H; Medical Faculty, University of Freiburg, Germany (D.W., N.A.M., X.S., H.H., S.H., L.S.M., P.S., I.H.).
Michel NA; 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.
Pramod AB; 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.).
Ghosheh Y; Department of Cardiology, Charité - University Medicine Berlin (Campus Benjamin Franklin), Germany (T.G.).
Brunel S; 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.
Buscher K; 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.).
Miller J; Medical Faculty, University of Freiburg, Germany (D.W., N.A.M., X.S., H.H., S.H., L.S.M., P.S., I.H.).
McArdle S; Department of Cardiology, Medical University Graz, Austria (N.A.M., A.Z.).
Baas L; 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.
Kobiyama K; Department of Psychiatry, University of California San Diego, La Jolla (A.B.P.).
Vassallo M; 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.
Ehinger E; Division of Immune Regulation (S.B., D.S., C.A.B.), La Jolla Institute for Immunology, CA.
Dileepan T; 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.
Ali A; 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.
Schell M; Microscopy Core Facility (S.M.), La Jolla Institute for Immunology, CA.
Mikulski Z; 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.
Sidler D; 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.
Kimura T; 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.
Sheng X; 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.
Horstmann H; Department of Microbiology, University of Minnesota Medical School, Minneapolis (T.D.).
Hansen S; 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.
Mitre LS; 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.
Stachon P; 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.
Hilgendorf I; 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.
Gaddis DE; 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.
Hedrick C; 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.).
Benedict CA; Medical Faculty, University of Freiburg, Germany (D.W., N.A.M., X.S., H.H., S.H., L.S.M., P.S., I.H.).
Peters B; 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.).
Zirlik A; Medical Faculty, University of Freiburg, Germany (D.W., N.A.M., X.S., H.H., S.H., L.S.M., P.S., I.H.).
Sette A; 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.).
Ley K; Medical Faculty, University of Freiburg, Germany (D.W., N.A.M., X.S., H.H., S.H., L.S.M., P.S., I.H.).

Circulation ; 142(13): 1279-1293, 2020 09 29.

Article em En | MEDLINE | ID: mdl-32703007

RESUMO

BACKGROUND: Throughout the inflammatory response that accompanies atherosclerosis, autoreactive CD4+ T-helper cells accumulate in the atherosclerotic plaque. Apolipoprotein B100 (apoB), the core protein of low-density lipoprotein, is an autoantigen that drives the generation of pathogenic T-helper type 1 (TH1) cells with proinflammatory cytokine secretion. Clinical data suggest the existence of apoB-specific CD4+ T cells with an atheroprotective, regulatory T cell (Treg) phenotype in healthy individuals. Yet, the function of apoB-reactive Tregs and their relationship with pathogenic TH1 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 B978-993 (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 Treg-like transcriptome, although only 21% of all apoB+ T cells expressed the Treg 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 TH signatures that suggested overlapping multilineage phenotypes with pro- and anti-inflammatory transcripts of TH1, T helper cell type 2 (TH2), and T helper cell type 17 (TH17), and of follicular-helper T cells. ApoB+ T cells were increased in mice and humans with atherosclerosis and progressively converted into pathogenic TH1/TH17-like cells with proinflammatory properties and only a residual Treg transcriptome. Plaque T cells that expanded during progression of atherosclerosis consistently showed a mixed TH1/TH17 phenotype in single-cell RNA sequencing. In addition, we observed a loss of FoxP3 in a fraction of apoB+ Tregs in lineage tracing of hyperlipidemic Apoe-/- mice. In adoptive transfer experiments, converting apoB+ Tregs 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 Tregs as a novel cellular target in atherosclerosis.

Assuntos

Apolipoproteína B-100/imunologia; Aterosclerose/imunologia; Autoimunidade; Linfócitos T Reguladores/imunologia; Animais; Apolipoproteína B-100/genética; Aterosclerose/genética; Camundongos; Camundongos Knockout para ApoE; Linfócitos T Reguladores/patologia

Palavras-chave

T-lymphocytes; T-lymphocytes, regulatory; apolipoprotein B-100; atherosclerosis; autoimmunity

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Texto completo: 1 Base de dados: MEDLINE Assunto principal: Autoimunidade / Linfócitos T Reguladores / Aterosclerose / Apolipoproteína B-100 Idioma: En Ano de publicação: 2020 Tipo de documento: Article

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