Abstract

Infection of inbred strains of mice with Leishmania major has correlated the outcome of disease with the capacity to stimulate the maturation of disparate subsets of CD4+ T cells, designated Th1 and Th2. Control of the parasite has been established when Th1 cells are generated, whereas progressive infection occurs with expansion of Th2. The inability of susceptible mice to heal is not due to a deletion in the T cell receptor repertoire, since several immunologic manipulations, including administration of antibodies to CD4 or IL-4, enable these mice to establish a Th1 response and heal infection. A comprehensive analysis of the CD4 cell repertoire that develops in healing and nonhealing mice revealed expansion of a common a/b+, CD+ population of cells that over-utilized the Va8, Vb4 heterodimeric T cell antigen receptor (TCR). These studies complement findings in various TCR transgenic mouse systems indicating that Th1 and Th2 cells arise from a common bipotential precursor. The L. major system thus offers an invaluable model for investigating signals that regulate the Th1/Th2 switch that has become increasingly implicated in the immune response to infectious agents. The goals of this proposal are to investigate these switch signals by a combination of in vivo and in vitro studies that focus on evolution of CD4 subset maturation within the context of intact animals infected with infectious organisms.
Three specific aims are proposed: 1. to characterize the monokine profile generated during the interaction of infectious metacyclic promastigotes with host macrophages of various strains; 2. to characterize the cytokine milieu within tissues and lymph nodes at critical early periods following inoculation of infectious organisms; and 3. to use transgenic TCR mice expressing an immunodominant and highly conserved Leishmania-specific Vb4- Va8 TCR heterodimer to characterize the influence of these early signals on subsequent CD4+ subset development and to examine the functional status of cytokine genes unique to the Th1 or Th2 phenotype. Understanding the mechanisms that underlie CD4+ subset differentiation will not only contribute to fundamental insights toward leishmaniasis, but to the numerous infectious and autoimmune diseases in which this response has been documented. The implications for vaccine strategy are also substantial.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI030663-05
Application #
2065836
Study Section
Bacteriology and Mycology Subcommittee 2 (BM)
Project Start
1991-01-01
Project End
1997-12-31
Budget Start
1995-01-01
Budget End
1995-12-31
Support Year
5
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Internal Medicine/Medicine
Type
Schools of Medicine
DUNS #
073133571
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Nusse, Ysbrand M; Savage, Adam K; Marangoni, Pauline et al. (2018) Parasitic helminths induce fetal-like reversion in the intestinal stem cell niche. Nature 559:109-113
Ricardo-Gonzalez, Roberto R; Van Dyken, Steven J; Schneider, Christoph et al. (2018) Tissue signals imprint ILC2 identity with anticipatory function. Nat Immunol 19:1093-1099
Schneider, Christoph; O'Leary, Claire E; von Moltke, Jakob et al. (2018) A Metabolite-Triggered Tuft Cell-ILC2 Circuit Drives Small Intestinal Remodeling. Cell 174:271-284.e14
Van Dyken, Steven J; Liang, Hong-Erh; Naikawadi, Ram P et al. (2017) Spontaneous Chitin Accumulation in Airways and Age-Related Fibrotic Lung Disease. Cell 169:497-509.e13
Savage, Adam K; Liang, Hong-Erh; Locksley, Richard M (2017) The Development of Steady-State Activation Hubs between Adult LTi ILC3s and Primed Macrophages in Small Intestine. J Immunol 199:1912-1922
von Moltke, Jakob; O'Leary, Claire E; Barrett, Nora A et al. (2017) Leukotrienes provide an NFAT-dependent signal that synergizes with IL-33 to activate ILC2s. J Exp Med 214:27-37
Van Dyken, Steven J; Nussbaum, Jesse C; Lee, Jinwoo et al. (2016) A tissue checkpoint regulates type 2 immunity. Nat Immunol 17:1381-1387
von Moltke, Jakob; Ji, Ming; Liang, Hong-Erh et al. (2016) Tuft-cell-derived IL-25 regulates an intestinal ILC2-epithelial response circuit. Nature 529:221-5
Mohapatra, A; Van Dyken, S J; Schneider, C et al. (2016) Group 2 innate lymphoid cells utilize the IRF4-IL-9 module to coordinate epithelial cell maintenance of lung homeostasis. Mucosal Immunol 9:275-86
Lee, Min-Woo; Odegaard, Justin I; Mukundan, Lata et al. (2015) Activated type 2 innate lymphoid cells regulate beige fat biogenesis. Cell 160:74-87

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