Impaired thymic tolerance to α-myosin directs autoimmunity to the heart in mice and humans
HuiJuan Lv, … , Bruno Kyewski, Myra A. Lipes
HuiJuan Lv, … , Bruno Kyewski, Myra A. Lipes
Published March 23, 2011
Citation Information: J Clin Invest. 2011;121(4):1561-1573. https://doi.org/10.1172/JCI44583.
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Research Article

Impaired thymic tolerance to α-myosin directs autoimmunity to the heart in mice and humans

Abstract

Autoimmunity has long been linked to myocarditis and its sequela, dilated cardiomyopathy, the leading causes of heart failure in young patients. However, the underlying mechanisms are poorly defined, with most clinical investigations focused on humoral autoimmunity as the target for intervention. Here, we show that the α-isoform of myosin heavy chain (α-MyHC, which is encoded by the gene Myh6) is the pathogenic autoantigen for CD4+ T cells in a spontaneous mouse model of myocarditis. Further, we found that Myh6 transcripts were absent in mouse medullary thymic epithelial cells (mTECs) and peripheral lymphoid stromal cells, which have been implicated in mediating central and peripheral T cell tolerance, respectively. Transgenic expression of α-MyHC in thymic epithelium conferred tolerance to cardiac myosin and prevented myocarditis, demonstrating that α-MyHC is a primary autoantigen in this disease process. Remarkably, we found that humans also lacked α-MyHC in mTECs and had high frequencies of α-MyHC–specific T cells in peripheral blood, with markedly augmented T cell responses to α-MyHC in patients with myocarditis. Since α-MyHC constitutes a small fraction of MyHC in human heart, these findings challenge the longstanding notion that autoimmune targeting of MyHC is due to its cardiac abundance and instead suggest that it is targeted as a result of impaired T cell tolerance mechanisms. These results thus support a role for T cell–specific therapies for myocarditis.

Authors

HuiJuan Lv, Evis Havari, Sheena Pinto, Raju V.S.R.K. Gottumukkala, Lizbeth Cornivelli, Khadir Raddassi, Takashi Matsui, Anthony Rosenzweig, Roderick T. Bronson, Ross Smith, Anne L. Fletcher, Shannon J. Turley, Kai Wucherpfennig, Bruno Kyewski, Myra A. Lipes

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Figure 6

Expression of α-MyHC in thymus prevents the development of myocarditis.

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Expression of α-MyHC in thymus prevents the development of myocarditis. ...
(A) Schema of the transgenic strategy to target expression of α-MyHC into thymic epithelium. (B) Western blot analysis of expression of α-MyHC protein in thymic, splenic, and lymph node lysates from NOD WT and the indicated samples probed with a monoclonal antibody to MyHC. (C) TaqMan RT-PCR analysis of expression of transgenic α-MyHC transcripts in thymus (Thy), spleen (Sp), lymph node, heart (He), kidney (Kid), liver (Liv), and lung (Lu). Shown are the representative results of 3 TOM+TA+ mice; values are expressed relative to TOM+TA+ thymus. n.d., not detected. (D) Prevalence of cardiac myosin autoantibodies in the indicated mice at 10 weeks of age (***P < 0.0001). (E) Comparison of IFN-γ responses of splenic T cells to stimulation with cardiac myosin in 22- and 12-week-old TOM+TA+DQ8+ mice and a 12-week-old female littermate. Shown is the mean ± SD of triplicate wells for each analysis. (F) H&E staining of heart sections from a 19-week-old female TOM+TA+DQ8+ and a littermate. Original magnification, ×10 and ×40 (insets). Scale bars: 400 μm and 100 μm (insets).