Myocardial infarction triggers cardioprotective antigen-specific T helper cell responses
Max Rieckmann, … , Ulrich Hofmann, Gustavo Campos Ramos
Max Rieckmann, … , Ulrich Hofmann, Gustavo Campos Ramos
Published August 13, 2019
Citation Information: J Clin Invest. 2019;129(11):4922-4936. https://doi.org/10.1172/JCI123859.
View: Text | PDF
Research Article Cardiology Immunology

Myocardial infarction triggers cardioprotective antigen-specific T helper cell responses

Abstract

T cell autoreactivity is a hallmark of autoimmune diseases but can also benefit self-maintenance and foster tissue repair. Here, we investigated whether heart-specific T cells exert salutary or detrimental effects in the context of myocardial infarction (MI), the leading cause of death worldwide. After screening more than 150 class II–restricted epitopes, we found that myosin heavy chain α (MYHCA) was a dominant cardiac antigen triggering post-MI CD4+ T cell activation in Balb/c mice. Transferred MYHCA614–629-specific CD4+ T cells (TCR-M cells) selectively accumulated in the myocardium and mediastinal lymph nodes (med-LNs) of infarcted mice, acquired a Treg phenotype with a distinct prohealing gene expression profile, and mediated cardioprotection. Myocardial Tregs were also detected in autopsy samples from patients who had had a MI. Noninvasive PET/CT imaging using a CXCR4 radioligand revealed enlarged med-LNs with increased cellularity in patients with MI. Notably, the med-LN alterations observed in MI patients correlated with the infarct size and cardiac function. Taken together, the results obtained in our study provide evidence that MI context induces prohealing T cell autoimmunity in mice and confirm the existence of an analogous heart/med-LN/T cell axis in patients with MI.

Authors

Max Rieckmann, Murilo Delgobo, Chiara Gaal, Lotte Büchner, Philipp Steinau, Dan Reshef, Cristina Gil-Cruz, Ellis N. ter Horst, Malte Kircher, Theresa Reiter, Katrin G. Heinze, Hans W.M. Niessen, Paul A.J. Krijnen, Anja M. van der Laan, Jan J. Piek, Charlotte Koch, Hans-Jürgen Wester, Constantin Lapa, Wolfgang R. Bauer, Burkhard Ludewig, Nir Friedman, Stefan Frantz, Ulrich Hofmann, Gustavo Campos Ramos

×

Figure 1

Cardiac epitope mapping.

Options: View larger image (or click on image) Download as PowerPoint
Cardiac epitope mapping. (A) Heatmaps depicting the number of specific T...
(A) Heatmaps depicting the number of specific T cell responses to defined antigens of interest. Splenocytes purified from MI or sham-operated mice (day 7) were cultured in the presence of peptide pools (15 mers, MHC-II–restricted) covering the most important heart-enriched proteins, and the production of IL-2 and IFN-γ was monitored by ELISPOT as a readout for antigen-specific stimulation. The single peptides MYHCA614–628 (included in the MYHCA pool) and OVA323–339 (irrelevant antigen, not expressed in the heart) were also tested. (B and C) Quantification of IL-2–producing cells per well in response to (B) the MYHCA peptide pool and (C) MYHCA614–628. (D and E) Representative ELISPOT images of these antigens. The number of responder cells found in each well is shown directly next to the representative images. The bar graphs display the group mean values, the SEM, and the distribution of each individual value. Statistical analysis was determined with a 2-tailed, unpaired t test (B and C). *P < 0.05. The data were acquired from 3 independent experiments.