Transgenic Mice Expressing Functional TCRs Specific to Cardiac Myhc-α 334-352 on Both CD4 and CD8 T Cells Are Resistant to the Development of Myocarditis on C57BL/6 Genetic Background

Authors

Meghna Sur, University of Nebraska - Lincoln
Mahima T. Rasquinha, University of Nebraska - Lincoln
Rajkumar Arumugam, University of Nebraska - Lincoln
Chandirasegaran Massilamany, University of Nebraska - Lincoln
Arunkumar Gangaplara, University of Nebraska - Lincoln
Kiruthiga Mone, University of Nebraska - Lincoln
Ninaad Lasrado, University of Nebraska - Lincoln
Bharathi Yalaka, University of Nebraska - Lincoln
Aakash Doiphode, University of Nebraska - Lincoln
Channabasavaiah B. Gurumurthy, University of Nebraska Medical CenterFollow
David Steffen, University of Nebraska - Lincoln
Jay Reddy, University of Nebraska - Lincoln

Document Type

Article

Journal Title

Cells

Publication Date

2023

Volume

12

Abstract

Myocarditis is a predominant cause of congestive heart failure and sudden death in children and young adolescents that can lead to dilated cardiomyopathy. Lymphocytic myocarditis mediated by T cells can result from the recognition of cardiac antigens that may involve CD4 or CD8 T cells or both. In this report, we describe the generation of T cell receptor (TCR) transgenic mice on a C57BL/6 genetic background specific to cardiac myosin heavy chain (Myhc)-α 334-352 and make the following observations: First, we verified that Myhc-α 334-352 was immunogenic in wild-type C57BL/6 mice and induced antigen-specific CD4 T cell responses despite being a poor binder of IA^b; however, the immunized animals developed only mild myocarditis. Second, TCRs specific to Myhc-α 334-352 in transgenic mice were expressed in both CD4 and CD8 T cells, suggesting that the expression of epitope-specific TCR is common to both cell types. Third, although T cells from naïve transgenic mice did not respond to Myhc-α 334-352, both CD4 and CD8 T cells from animals immunized with Myhc-α 334-352 responded to the peptide, indicating that antigen priming is necessary to break tolerance. Fourth, although the transgenic T cells could produce significant amounts of interferon-γ and interleukin-17, the immunized animals developed only mild disease, indicating that other soluble factors might be necessary for developing severe myocarditis. Alternatively, the C57BL/6 genetic background might be a major contributing factor for resistance to the development of myocarditis. Taken together, our model permits the determination of the roles of both CD4 and CD8 T cells to understand the disease-resistance mechanisms of myocarditis in a single transgenic system antigen-specifically.

DOI Link

10.3390/cells12192346

ISSN

2073-4409

Creative Commons License

This work is licensed under a Creative Commons Attribution 4.0 International License.

Recommended Citation

Sur, Meghna; Rasquinha, Mahima T.; Arumugam, Rajkumar; Massilamany, Chandirasegaran; Gangaplara, Arunkumar; Mone, Kiruthiga; Lasrado, Ninaad; Yalaka, Bharathi; Doiphode, Aakash; Gurumurthy, Channabasavaiah B.; Steffen, David; and Reddy, Jay, "Transgenic Mice Expressing Functional TCRs Specific to Cardiac Myhc-α 334-352 on Both CD4 and CD8 T Cells Are Resistant to the Development of Myocarditis on C57BL/6 Genetic Background" (2023). Journal Articles: Genetics, Cell Biology & Anatomy. 53.
https://digitalcommons.unmc.edu/com_gcba_articles/53