Abstract

The same properties that allow T cells to mount an effective immune response can be turned against host tissue, provoking an autoimmune response. Intriguingly, T cell auto-reactivity is often the result of deregulated signaling pathways within T cells. Thus, understanding the etiology of different autoimmune diseases will require a thorough and integrated understanding of the mechanisms that control T cell activation. The long-term objective of my research is to understand the regulation of T cell activation. Currently, my laboratory is studying how two related proteins, Sts-1 and Sts-2, act in concert to negatively regulate T cell signaling pathways. The Sts proteins have a unique modular structure, with an N- terminal ubiquitin-interacting domain (UBA), a central protein-protein interaction domain (SH3), and a C- terminal region with homology to the enzyme phosphoglycerate mutase (PGM). The realization that the Sts proteins have a role in regulating TCR signaling pathways emerged from an analysis of mice lacking Sts-1 and -2. T cells from Sts-1/2-/- mice dramatically hyper-proliferate in response to TCR stimulation. This hyper- proliferative phenotype is accompanied by increased activation of signaling pathways downstream of the TCR, elevated levels of cytokine production, and increased susceptibility of Sts-1/2-/- mice to autoimmunity in a mouse model of multiple sclerosis. In our ongoing effort to characterize the functions of the Sts proteins, we recently discovered a novel protein tyrosine phosphatase activity associated with the Sts PGM domain. Intriguingly, the Sts phosphatase domain shows no similarity to classical PTPs in primary amino acid sequence and important catalytic features. Coupled with the fact that no known PTP contains a UBA or SH3 domain, our results suggest that the Sts proteins operate in an intracellular signaling niche within T cells that is separate and distinct from classical PTPs. The experiments outlined in this proposal are designed to address the underlying function(s) and mechanism(s) of action of the Sts-1 and Sts-2.
Our Specific Aims are: 1. Determine how the Sts proteins regulate T cell activation thresholds via regulation of Zap-70. 2. Determine how the three Sts modular domains (UBA, SH3, PGM) cooperate to negatively regulate TCR signaling pathways. We will use a combination of biochemical, biophysical, and cell biological approaches to accomplish our goals. Completion of the studies described herein will help us build a model of how the Sts proteins cooperate to negatively regulate TCR signaling pathways.

Public Health Relevance

Autoimmune diseases arise when normal regulatory mechanisms within the immune system fail. Developing therapies that will prevent or cure autoimmune diseases will require a thorough and integrated understanding of the mechanisms that control the immune response. This project focuses on understanding the function(s) and mechanism(s) of action of a closely related pair of negative regulators of T cell receptor signaling, Sts-1 and Sts-2.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI080892-02
Application #
7997173
Study Section
Cellular and Molecular Immunology - B Study Section (CMIB)
Program Officer
Mallia, Conrad M
Project Start
2009-12-10
Project End
2014-11-30
Budget Start
2010-12-01
Budget End
2011-11-30
Support Year
2
Fiscal Year
2011
Total Cost
$384,128
Indirect Cost

  Institution

Name
State University New York Stony Brook
Department
Genetics
Type
Schools of Medicine
DUNS #
804878247
City
Stony Brook
State
NY
Country
United States
Zip Code
11794

  Publications

Parashar, Kaustubh; Kopping, Erik; Frank, David et al. (2017) Increased Resistance to Intradermal Francisella tularensis LVS Infection by Inactivation of the Sts Phosphatases. Infect Immun 85:
Ivanova, Elitza; Carpino, Nick (2016) Negative regulation of TCR signaling by ubiquitination of Zap-70 Lys-217. Mol Immunol 73:19-28
Naseem, Shamoon; Frank, David; Konopka, James B et al. (2015) Protection from systemic Candida albicans infection by inactivation of the Sts phosphatases. Infect Immun 83:637-45
Luis, Boris S; Carpino, Nick (2014) Insights into the suppressor of T-cell receptor (TCR) signaling-1 (Sts-1)-mediated regulation of TCR signaling through the use of novel substrate-trapping Sts-1 phosphatase variants. FEBS J 281:696-707
Cieniewicz, Brandon; Carpino, Nicholas; Krug, Laurie T (2014) Enhanced response of T cells from murine gammaherpesvirus 68-infected mice lacking the suppressor of T cell receptor signaling molecules Sts-1 and Sts-2. PLoS One 9:e90196
San Luis, Boris; Nassar, Nicolas; Carpino, Nick (2013) New insights into the catalytic mechanism of histidine phosphatases revealed by a functionally essential arginine residue within the active site of the Sts phosphatases. Biochem J 453:27-35
Back, Steven H; Adapala, Naga Suresh; Barbe, Mary F et al. (2013) TULA-2, a novel histidine phosphatase, regulates bone remodeling by modulating osteoclast function. Cell Mol Life Sci 70:1269-84
San Luis, Boris; Sondgeroth, Ben; Nassar, Nicolas et al. (2011) Sts-2 is a phosphatase that negatively regulates zeta-associated protein (ZAP)-70 and T cell receptor signaling pathways. J Biol Chem 286:15943-54
Thomas, Dafydd H; Getz, Todd M; Newman, Tiffanny N et al. (2010) A novel histidine tyrosine phosphatase, TULA-2, associates with Syk and negatively regulates GPVI signaling in platelets. Blood 116:2570-8