Abstract

The two-signal model in which an antigen-presenting cell-derived costimulatory signal, epitomized by CD28, is needed for T cells to respond maximally to T cell receptor (TCR) stimulation is now part of the immunology canon and fueled exciting immunotherapies for transplant rejection, autoimmunity, and cancer. Most of the advances in the costimulation field, however, applied to conventional Foxp3neg CD4+ T cells. Although CD28 enhances the development of Foxp3+ regulatory (Treg) cells as they are selected by high affinity TCR recognition of self peptides in the thymus, and is required for their autoimmunity-suppressing functions, much less is known about the costimulatory requirements of Treg cells as they participate in immune responses to foreign peptides. During the last funding period, we found that the pre-immune repertoires of CD4+ T cells specific for foreign peptides from microbes contain both conventional AND Treg cells. Both populations underwent clonal expansion in the secondary lymphoid organs after infection with a microbe expressing the relevant peptide but the two populations formed different types of effector cells and generated memory cells with different efficiencies. Our results lead to the remarkable conclusion that two parallel CD4+ T cell repertoires exist for each foreign peptide ? one composed of conventional nave cells and a smaller one composed of Treg cells. Almost nothing is known about the signals that govern the activation of foreign peptide-specific Treg cells during immune responses to infection or their interactions with conventional T cells responding to the same peptide. The goal of this project is to determine whether foreign peptide-specific Treg cells require CD28 costimulation during immune responses to infection and if so understand the signal transduction process. We will also test the intriguing possibility that foreign peptide-specific Treg cells play special roles in regulating the expansion and differentiation of the conventional T cells specific for the same peptide as both populations respond during infection. This research could shed light on the understudied role that Treg cells play during infection and provide new uses for modulation of T cell costimulation.

Public Health Relevance

Regulatory T cells are critical for immune self tolerance and suppression of autoimmunity. We will use new technologies to explore how these T cells become activated and what role they play in immune responses to infection.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI027998-31
Application #
9897522
Study Section
Cellular and Molecular Immunology - B Study Section (CMIB)
Program Officer
Jiang, Chao
Project Start
1989-04-01
Project End
2023-03-31
Budget Start
2020-04-01
Budget End
2021-03-31
Support Year
31
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
University of Minnesota Twin Cities
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
555917996
City
Minneapolis
State
MN
Country
United States
Zip Code
55455

  Publications

Pape, Kathryn A; Maul, Robert W; Dileepan, Thamotharampillai et al. (2018) Naive B Cells with High-Avidity Germline-Encoded Antigen Receptors Produce Persistent IgM+ and Transient IgG+ Memory B Cells. Immunity 48:1135-1143.e4
Taylor, Justin J; Pape, Kathryn A; Steach, Holly R et al. (2015) Humoral immunity. Apoptosis and antigen affinity limit effector cell differentiation of a single naïve B cell. Science 347:784-7
Yang, Jessica A; Tubo, Noah J; Gearhart, Micah D et al. (2015) Cutting edge: Bcl6-interacting corepressor contributes to germinal center T follicular helper cell formation and B cell helper function. J Immunol 194:5604-8
Tubo, Noah J; Jenkins, Marc K (2014) TCR signal quantity and quality in CD4(+) T cell differentiation. Trends Immunol 35:591-596
Jenkins, Marc K; Moon, James J (2012) The role of naive T cell precursor frequency and recruitment in dictating immune response magnitude. J Immunol 188:4135-40
Pepper, Marion; Linehan, Jonathan L; Pagán, Antonio J et al. (2010) Different routes of bacterial infection induce long-lived TH1 memory cells and short-lived TH17 cells. Nat Immunol 11:83-9
McLachlan, James B; Catron, Drew M; Moon, James J et al. (2009) Dendritic cell antigen presentation drives simultaneous cytokine production by effector and regulatory T cells in inflamed skin. Immunity 30:277-88
Costalonga, Massimo; Zell, Traci (2007) Lipopolysaccharide enhances in vivo interleukin-2 production and proliferation by naive antigen-specific CD4 T cells via a Toll-like receptor 4-dependent mechanism. Immunology 122:124-30
McLachlan, James B; Jenkins, Marc K (2007) Migration and accumulation of effector CD4+ T cells in nonlymphoid tissues. Proc Am Thorac Soc 4:439-42
Huddleston, S J; Hays, W S; Filatenkov, A et al. (2006) CD154+ graft antigen-specific CD4+ T cells are sufficient for chronic rejection of minor antigen incompatible heart grafts. Am J Transplant 6:1312-9

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