Abstract

In this application we propose to examine the role of the novel protein Chat-H in signaling pathways that regulate T lymphocyte migration. In preliminary studies, we used lentivirus-mediated RNA interference (RNAi) to silence expression of Chat-H in mouse primary T cells and study the effect of Chat-H deletion on T cell function. We found that whereas Chat-H downregulation had no effect on T cell receptor (TCR)-mediated signaling, in vitro and in vivo chemokine-induced migration of Chat-H deficient T cells was dramatically impaired. Defects in migration and adhesion correlated with impaired activation of the Rap-1 GTPase, which is a key regulator of integrin-mediated cellular adhesion and migration. Chat-H constitutively associated with the signaling protein CasL and formation of this complex was necessary for migration. These observations suggest that Chat-H is an important regulator of chemokine receptor signaling and T lymphocyte migration and it that it acts together with CasL to regulate these processes. To study the in vivo requirement for Chat-H we recently generated Chat-H knockout mice and consistent with previous results, preliminary studies show that T cells from these mice exhibit impaired in vitro migration. In the experiments described here, we propose to examine the mechanisms through which Chat-H regulates chemokine-induced T lymphocyte migration and the effect of Chat-H deficiency in this process. We will test the following hypothesis: Chat-H regulates chemokine-induced T lymphocyte migration by activating Rap1 and Rap1-mediated integrin activation, cell adhesion and migration. Deficiency in Chat-H expression results in defective integrin-mediated adhesion and as a result impaired homeostatic homing of T cells to secondary lymphoid organs, and compromised T-cell-mediated immune responses. To test this hypothesis we will use first use T cells in which Chat-H has been dowregulated by RNAi to define the biochemical mechanisms of how Chat-H regulates Rap1 activation and integrin-mediated adhesion. To study the in vivo requirement for Chat-H we will use Chat-H knockout mice to determine whether Chat-H deficiency affects in vivo migration and homeostatic trafficking of mature T cells to peripheral lymphoid organs, and T-cell-mediated immune responses. We anticipate that these experiments will lead to novel insight into the mechanisms that regulate lymphocyte chemotaxis and reveal important roles for both Chat-H and CasL in this process downstream of chemokine receptors. Through these studies we also aim towards gaining insight into the role of Chat-H in chronic inflammation and conditions associated with leukocyte adhesion deficiencies and identify therapeutic targets for treating human diseases. ? ? ?

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
7R01AI068963-03
Application #
7727164
Study Section
Cellular and Molecular Immunology - A Study Section (CMIA)
Program Officer
Miller, Lara R
Project Start
2007-06-15
Project End
2012-05-31
Budget Start
2008-10-02
Budget End
2009-05-31
Support Year
3
Fiscal Year
2008
Total Cost
$291,412
Indirect Cost

  Institution

Name
Icahn School of Medicine at Mount Sinai
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
078861598
City
New York
State
NY
Country
United States
Zip Code
10029

  Publications

Santos, Luís C; Blair, David A; Kumari, Sudha et al. (2016) Actin polymerization-dependent activation of Cas-L promotes immunological synapse stability. Immunol Cell Biol 94:981-993
Herbin, Olivier; Bonito, Anthony J; Jeong, Seihwan et al. (2016) Medullary thymic epithelial cells and CD8?+ dendritic cells coordinately regulate central tolerance but CD8?+ cells are dispensable for thymic regulatory T cell production. J Autoimmun 75:141-149
Herbin, Olivier; Regelmann, Adam G; Ramkhelawon, Bhama et al. (2016) Monocyte Adhesion and Plaque Recruitment During Atherosclerosis Development Is Regulated by the Adapter Protein Chat-H/SHEP1. Arterioscler Thromb Vasc Biol 36:1791-801
Haines, Jeffery D; Herbin, Olivier; de la Hera, Belén et al. (2015) Nuclear export inhibitors avert progression in preclinical models of inflammatory demyelination. Nat Neurosci 18:511-20
Alexandropoulos, Konstantina; Bonito, Anthony J; Weinstein, Erica G et al. (2015) Medullary thymic epithelial cells and central tolerance in autoimmune hepatitis development: novel perspective from a new mouse model. Int J Mol Sci 16:1980-2000
Danzl, Nichole M; Jeong, Seihwan; Choi, Yongwon et al. (2014) Identification of novel thymic epithelial cell subsets whose differentiation is regulated by RANKL and Traf6. PLoS One 9:e86129
Bonito, Anthony J; Aloman, Costica; Fiel, M Isabel et al. (2013) Medullary thymic epithelial cell depletion leads to autoimmune hepatitis. J Clin Invest 123:3510-24
Alexandropoulos, Konstantina; Danzl, Nichole M (2012) Thymic epithelial cells: antigen presenting cells that regulate T cell repertoire and tolerance development. Immunol Res 54:177-90
Danzl, Nichole M; Donlin, Laura T; Alexandropoulos, Konstantina (2010) Regulation of medullary thymic epithelial cell differentiation and function by the signaling protein Sin. J Exp Med 207:999-1013
Alexandropoulos, Konstantina; Regelmann, Adam G (2009) Regulation of T-lymphocyte physiology by the Chat-H/CasL adapter complex. Immunol Rev 232:160-74