Abstract

This proposal is for the continuation from the fourteenth through eighteenth years of investigations of aging associated alterations of immune function by investigators in the Immunology Department of The Scripps Research Institute. Over the years, research supported by this grant has played a major role in moving the understanding of the impact of aging on immune responsiveness from purely phenomenological observations at the level of the whole organism, through quantitative and qualitative examinations of alterations in T cell and B cell at the population level, to the initial stages of delineating the underlying alterations in subcellular enzymatic and molecular processes. In its current iteration this program project represents the integrated efforts of three laboratories investigating aging associated alterations in defined B and T cell subpopulations at the cellular, subcellular, and molecular levels. Dr. Linton (Project II) will capitalize on the identification of a distinct """"""""aging phenotype"""""""" in the sequences of phosphorylcholine specific antibodies to compare alterations in defined B cell subsets including her recently defined precursor subset that is responsible for the generation of memory B cells and germinal centers. She will also study the tolerance susceptibility of these cells in mice expressing the influenza hemagglutinin as a transgene. Her studies of the aging associated defect in memory B cell generation will, include a collaboration with Dr. Weigle (Project III) to analyze the competence of TH subsets from young vs aged conventional mice, and (with Dr. Susan Swain) mice expressing a cytochrome c specific TCR as a transgene. Dr. Linton will also provide defined precursor subsets to Dr. Klinman (Project I) who has identified fundamental aging associated change in H chain V region rearrangement that underlie alterations in repertoire expression including those responsible for the """"""""aging phenotype"""""""" of PC responsive B cells. Dr. Klinman will further elucidate the generality and mechanism of this aging associated alteration in gene rearrangement and will evaluate the pace of alterations of precursor cell subsets in various murine strains and possibly humans as well. Dr. Weigle will continue to pursue his seminal studies of the molecular basis of aging associated changes in the function, antigenic stimulation, and tolerance induction of CD4 + T cell subsets. He will assess the pace of these changes in conventional and, autoimmune murine strains as well as diet restricted mice. These sets of mice will also be studied for changes in B cell responses in Projects I and II.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute on Aging (NIA)
Type
Research Program Projects (P01)
Project #
5P01AG001743-17
Application #
2048645
Study Section
Biological and Clinical Aging Review Committee (BCA)
Project Start
1980-02-01
Project End
1996-09-29
Budget Start
1996-03-15
Budget End
1996-09-29
Support Year
17
Fiscal Year
1996
Total Cost
Indirect Cost

  Institution

Name
Scripps Research Institute
Department
Type
DUNS #
City
La Jolla
State
CA
Country
United States
Zip Code
92037

  Publications

Boyman, Onur; Ramsey, Chris; Kim, David M et al. (2008) IL-7/anti-IL-7 mAb complexes restore T cell development and induce homeostatic T Cell expansion without lymphopenia. J Immunol 180:7265-75
Ramsey, Chris; Rubinstein, Mark P; Kim, David M et al. (2008) The lymphopenic environment of CD132 (common gamma-chain)-deficient hosts elicits rapid homeostatic proliferation of naive T cells via IL-15. J Immunol 180:5320-6
Jelley-Gibbs, Dawn M; Strutt, Tara M; McKinstry, K Kai et al. (2008) Influencing the fates of CD4 T cells on the path to memory: lessons from influenza. Immunol Cell Biol 86:343-52
Purton, Jared F; Tan, Joyce T; Rubinstein, Mark P et al. (2007) Antiviral CD4+ memory T cells are IL-15 dependent. J Exp Med 204:951-61
Rubinstein, Mark P; Kovar, Marek; Purton, Jared F et al. (2006) Converting IL-15 to a superagonist by binding to soluble IL-15R{alpha}. Proc Natl Acad Sci U S A 103:9166-71
Ishimaru, Naozumi; Kishimoto, Hidehiro; Hayashi, Yoshio et al. (2006) Regulation of naive T cell function by the NF-kappaB2 pathway. Nat Immunol 7:763-72
Boyman, Onur; Cho, Jae-Ho; Tan, Joyce T et al. (2006) A major histocompatibility complex class I-dependent subset of memory phenotype CD8+ cells. J Exp Med 203:1817-25
Surh, Charles D; Boyman, Onur; Purton, Jared F et al. (2006) Homeostasis of memory T cells. Immunol Rev 211:154-63
Kovar, Marek; Boyman, Onur; Shen, Xuefei et al. (2006) Direct stimulation of T cells by membrane vesicles from antigen-presenting cells. Proc Natl Acad Sci U S A 103:11671-6
Haynes, Laura; Eaton, Sheri M; Burns, Eve M et al. (2005) Newly generated CD4 T cells in aged animals do not exhibit age-related defects in response to antigen. J Exp Med 201:845-51

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