Abstract

T cell mediated immune responses are the net result of the behavior of individual cells in the T cell compartment. The use of TCR transgenic mice have enabled the identification of antigen-specific cells within a lymphocyte population, for determination of cell cycle status, activation phenotype, and viability. These studies have made important advances, but have been limited by the inability to examine effector functions such as proliferation and cytokine expression on a single cell basis. Recently, we have adapted and refined methods to track the proliferative history of individual cells within a population flow cytometry. Our studies indicate that TCR and CD28-mediated costimulation serve to cooperatively increase the frequency of cells which enter the proliferative pool, and the number of mitoses they undergo. Surprisingly, even with maximal levels of TCR plus co-stimulatory signals sufficient to activate 95% of the population, roughly 40% if T cells never divide yet remain viable. When isolated by flow cytometry and restimulated, these cells exhibit anergic behavior (refractory to restimulation but rescuable with IL-2). These studies raise a series of interesting questions which we will address. To do so we have adapted our system for use with flow cytometric detection of intracellular cytokines and cell surface detection of a transgenic TCR.
Aim #1 will use in vitro studies to define the parameters which determine the frequency of cells which enter the proliferative pool, focusing on precursor percentage, T cell:APC ratio, APC type, and the availability of co-stimulatory and off signals.
This aim will analyze the cell cycle status and checkpoint of non-proliferative cells.
Aim #2 will determine if cytokine secretion (either qualitative or quantitative) is linked to proliferative history. Studies will be performed in vitro and using in vivo adoptive transfer techniques.
Aim #3 will ask how TCR and CD28 signals influence cell survival in vitro and in vivo. These studies will also use mice transgenic (on the T cell lineage) for the CD28- inducible cell survival gene bcl-x to permit us to separately study the role(s) of the inductive effects of CD28 stimulation on cytokine and bcl-x expression. These studies should provide important insights into the control of T cell responses and assist in the development of strategies to modulate the immune system and induce tolerance. We will work with Dr. Monroe, whose project examines similar parameters during B cell responses. Dr. Greene's project will characterize biochemical events during anergy, and we will apply his findings to our system to examine the basis of primary non-responsiveness.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Program Projects (P01)
Project #
5P01AI043620-02
Application #
6201426
Study Section
Project Start
1999-09-01
Project End
2000-08-31
Budget Start
1997-10-01
Budget End
1998-09-30
Support Year
2
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
University of Pennsylvania
Department
Type
DUNS #
042250712
City
Philadelphia
State
PA
Country
United States
Zip Code
19104

  Publications

Han, Daehee; Walsh, Matthew C; Cejas, Pedro J et al. (2013) Dendritic cell expression of the signaling molecule TRAF6 is critical for gut microbiota-dependent immune tolerance. Immunity 38:1211-22
Hunter, Christopher A; Kastelein, Rob (2012) Interleukin-27: balancing protective and pathological immunity. Immunity 37:960-9
Hall, Aisling O'Hara; Beiting, Daniel P; Tato, Cristina et al. (2012) The cytokines interleukin 27 and interferon-? promote distinct Treg cell populations required to limit infection-induced pathology. Immunity 37:511-23
Schrum, Adam G; Gil, Diana; Turka, Laurence A et al. (2011) Physical and functional bivalency observed among TCR/CD3 complexes isolated from primary T cells. J Immunol 187:870-8
Wojno, Elia D Tait; Hosken, Nancy; Stumhofer, Jason S et al. (2011) A role for IL-27 in limiting T regulatory cell populations. J Immunol 187:266-73
Ramon, Hilda E; Cejas, Pedro J; LaRosa, David et al. (2010) EGR-2 is not required for in vivo CD4 T cell mediated immune responses. PLoS One 5:e12904
Liu, Xiaohe; Karnell, Jodi L; Yin, Bu et al. (2010) Distinct roles for PTEN in prevention of T cell lymphoma and autoimmunity in mice. J Clin Invest 120:2497-507
Cejas, Pedro J; Walsh, Matthew C; Pearce, Erika L et al. (2010) TRAF6 inhibits Th17 differentiation and TGF-beta-mediated suppression of IL-2. Blood 115:4750-7
Stumhofer, Jason S; Tait, Elia D; Quinn 3rd, William J et al. (2010) A role for IL-27p28 as an antagonist of gp130-mediated signaling. Nat Immunol 11:1119-26
Passos, Sara T; Silver, Jonathan S; O'Hara, Aisling C et al. (2010) IL-6 promotes NK cell production of IL-17 during toxoplasmosis. J Immunol 184:1776-83

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