Abstract

T-cell homeostasis is an essential process for maintaining peripheral lymphocyte pool size. T cells must provide a diverse repertoire of antigen recognition to effectively recognize and destroy pathogens that they encounter. Antigen-specific T-cell pools are expanded during viral infection and are contracted after the initial viral clearance to make space for the entire T-cell repertoire. This is a tightly regulated process since the space available for lymphocytes is limited. Transforming Growth Factor (3 signaling is required to prevent autoimmune disease and dysregulation of T-cell homeostasis. Normally, T cells must interact with self-MHC molecules for their survival, maintenance and homeostatic expansion, but under some pathological conditions such interactions cause inappropriate activation of T cells leading to autoimmune disease. Characterization of TGF01-deficient mice has revealed that their autoimmune disease results from spontaneous activation of their T cells in response to self-antigen recognition by having an inappropriately low threshold level of activation through a Calcium-Calcineurin signaling cascade. Elimination of T cells or their self-antigen recognition is sufficient to prevent autoimmune disease in these mice, and reducing calcineurin signaling drastically attenuates their autoimmune disease. In addition, it is known that without TGF(3 signaling there are less T-regulatory cells, the cells that mediate immune tolerance. Here we propose to investigate mechanisms and processes underlying the role of TGFp in the regulation of T-cell homeostasis and self-tolerance. Firstly, we will address how TGF01 regulates T-cell pool size using an Ovalbumin-specific T-cell receptor transgenic TGF(31-deficientmouse strain. Adoptive transfer and Ovalbumin activation studies will be used. Secondly, we will study the role of TGF(31 and its signaling pathways in peripheral T-cell regulation. T-regulatory cell transfer to effect tolerizing activity will beperformed and the passive or infectious nature of that activity will be determined. Relevance: Dysregulation of homeostatic process has been implicated in many human diseases such as AIDS, leukemia, inflammatory bowl disease, and autoimmune diseases such as type 1 diabetes, multiple sclerosis and arthritis. Processes involved in T-cell homeostasis such as lymphocyte activation, survival and death are presently under intensive study because of their relevance to these diseases. The information gained from these studies will be useful for developing therapies for the induction of tolerance during transplantation, for enhancing tumor vaccine potential, and for the prevention of autoimmune disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI067903-04
Application #
7759458
Study Section
Transplantation, Tolerance, and Tumor Immunology (TTT)
Program Officer
Ferguson, Stacy E
Project Start
2006-03-15
Project End
2011-02-28
Budget Start
2009-03-01
Budget End
2010-02-28
Support Year
4
Fiscal Year
2009
Total Cost
$365,528
Indirect Cost

  Institution

Name
University of Arizona
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
806345617
City
Tucson
State
AZ
Country
United States
Zip Code
85721

  Publications

Daniel, Scott G; Ball, Corbie L; Besselsen, David G et al. (2017) Functional Changes in the Gut Microbiome Contribute to Transforming Growth Factor ?-Deficient Colon Cancer. mSystems 2:
Doetschman, Thomas; Georgieva, Teodora; Li, Hongqi et al. (2012) Generation of mice with a conditional allele for the transforming growth factor beta3 gene. Genesis 50:59-66
Doetschman, Thomas (2011) GI GEMs: genetically engineered mouse models of gastrointestinal disease. Gastroenterology 140:380-385.e2
Doetschman, Thomas; Sholl, Allyson; Chen, Hwu dau rw et al. (2011) Divergent effects of calcineurin A? on regulatory and conventional T-cell homeostasis. Clin Immunol 138:321-30
Azhar, Mohamad; Yin, Moying; Bommireddy, Ramireddy et al. (2009) Generation of mice with a conditional allele for transforming growth factor beta 1 gene. Genesis 47:423-31
Bommireddy, R; Bueno, O F; Martin, J et al. (2009) Calcineurin deficiency decreases inflammatory lesions in transforming growth factor beta1-deficient mice. Clin Exp Immunol 158:317-24
Doetschman, Thomas (2009) Influence of genetic background on genetically engineered mouse phenotypes. Methods Mol Biol 530:423-33
Saxena, Vijay; Lienesch, Douglas W; Zhou, Min et al. (2008) Dual roles of immunoregulatory cytokine TGF-beta in the pathogenesis of autoimmunity-mediated organ damage. J Immunol 180:1903-12
Bommireddy, Ramireddy; Babcock, George F; Singh, Ram R et al. (2008) TGFbeta1 deficiency does not affect the generation and maintenance of CD4+CD25+FOXP3+ putative Treg cells, but causes their numerical inadequacy and loss of regulatory function. Clin Immunol 127:206-13
Bommireddy, Ramireddy; Doetschman, Thomas (2007) TGFbeta1 and Treg cells: alliance for tolerance. Trends Mol Med 13:492-501