Exploring T Cell Receptor Repertoires in Myocardial Diseases

Author:

Ashour DiyaaElDin12ORCID,Le Gouge Kenz3ORCID,Rainer Peter P.456ORCID,Mariotti-Ferrandiz Encarnita37ORCID,Campos Ramos Gustavo12ORCID

Affiliation:

1. Department of Internal Medicine I (D.A., G.C.R.), University Hospital Würzburg, Germany.

2. Comprehensive Heart Failure Center (D.A., G.C.R.), University Hospital Würzburg, Germany.

3. Immunology-Immunopathology-Immunotherapy Laboratory, Sorbonne Université, France (K.L.G., E.M.-F.).

4. Division of Cardiology, Medical University of Graz, Austria (P.P.R.).

5. BioTechMed Graz, Austria (P.P.R.).

6. St. Johann in Tirol General Hospital, Austria (P.P.R.).

7. Institut national de la santé et de la recherche médicale (INSERM) (E.M.-F.).

Abstract

Mounting experimental and clinical evidence has revealed that adaptive immune mechanisms targeting myocardial antigens are triggered by different forms of cardiac injury and impact disease progression. B and T lymphocytes recognize specific antigens via unique adaptive immune receptors generated through a somatic rearrangement process that generates a potential repertoire of 10 19 unique receptors. While the adaptive immune receptor repertoire diversity provides the basis for immunologic specificity, making sense of it can be a challenging task. In the present review, we discuss key aspects underlying the generation of TCRs (T cell receptors) and emerging tools for their study in the context of myocardial diseases. Moreover, we outline how exploring TCR repertoires could lead to a deeper understanding of myocardial pathophysiological principles and potentially serve as diagnostic tools.

Publisher

Ovid Technologies (Wolters Kluwer Health)

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