MerTK regulates thymic selection of autoreactive T cells

  1. Mark A. Walleta,
  2. Rafael R. Floresa,
  3. Yaming Wanga,
  4. Zuoan Yia,
  5. Charles J. Krogera,
  6. Clayton E. Mathewsb,
  7. H. Shelton Earpc,d,
  8. Glenn Matsushimaa,c,e,
  9. Bo Wanga and
  10. Roland Tischa,c,1
  1. aDepartment of Microbiology and Immunology,
  2. cUNC Lineberger Comprehensive Cancer Center,
  3. dDepartment of Medicine and Pharmacology,
  4. eUNC Neuroscience Center, University of North Carolina, Chapel Hill, NC 27599-7020; and
  5. bDepartment of Pathology, Immunology, and Laboratory Medicine, University of Florida, Gainesville, FL 32610

  1. Communicated by Hugh O. McDevitt, Stanford University, Stanford, CA, January 23, 2009 (received for review September 30, 2008)

Abstract

T cell-mediated autoimmune diseases such as type 1 diabetes (T1D) are believed to be the result in part of inefficient negative selection of self-specific thymocytes. However, the events regulating thymic negative selection are not fully understood. In the current study, we demonstrate that nonobese diabetic (NOD) mice lacking expression of the Mer tyrosine kinase (MerTK) have reduced inflammation of the pancreatic islets and fail to develop diabetes. Furthermore, NOD mice deficient in MerTK expression (Mer−/−) exhibit a reduced frequency of β cell-specific T cells independent of immunoregulatory effectors. The establishment of bone marrow chimeric mice demonstrated that the block in β cell autoimmunity required hematopoietic-derived cells lacking MerTK expression. Notably, fetal thymic organ cultures and self-peptide administration showed increased thymic negative selection in Mer−/− mice. Finally, thymic dendritic cells (DC) prepared from Mer−/− mice exhibited an increased capacity to induce thymocyte apoptosis in a peptide-specific manner in vitro. These findings provide evidence for a unique mechanism involving MerTK-mediated regulation of thymocyte negative selection and thymic DC, and suggest a role for MerTK in contributing to β cell autoimmunity.

Keywords:

Footnotes

  • 1To whom correspondence should be addressed. E-mail: rmtisch{at}med.unc.edu

  • Author contributions: M.A.W. and R.T. designed research; M.A.W., R.R.F., Y.W., Z.Y., C.J.K., and C.E.M. performed research; H.S.E. and G.M. contributed new reagents/analytic tools; M.A.W., C.E.M., H.S.E., G.M., B.W., and R.T. analyzed data; and M.A.W., B.W., and R.T. wrote the paper.

  • The authors declare no conflict of interest.

  • This article contains supporting information online at www.pnas.org/cgi/content/full/0900683106/DCSupplemental.

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  1. Published online before print February 27, 2009, doi: 10.1073/pnas.0900683106 PNAS March 24, 2009 vol. 106 no. 12 4810-4815
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