Abstract

The requirements for growing and propagating antigen-specific and idiotype-specific suppressor T cells will be studied, with the aim of developing a reproducible cloning strategy. In order to accomplish this, the response will be initiated with Ts-inducing determinants and appropriate specific accessory inducer cells, as well as driving the response (a) by using conjugates of mitogens and specific ligands, or (b) performing cyclic enrichment (specific selection and nonspecific stimulation) and by using combinations of special growth factors. Recent evidence points to the reactivity of regulatory cells with the recognition structures on MHC-restricted T cells. This T-T network and especially, the specificity of its idiotypic interaction, will be the focus of these studies. The development of such regulatory cells in fetal thymic lobe cultures will be studied and intercellular restrictions between closely related strains (B6 and its Ia mutant strain, bm12) will be examined. The study of tolerance induced by immunogenic or suppressogenic determinants will be completed and the contributions of clonal inactivation vs. suppressive cell involvement in tolerance induction will be detailed. Further, the induction of tolerance in various regulatory subpopulations of T cells will be investigated among antigen-specific and idiotype- specific sets. In the lysozyme and beta-galactosidase systems, small peptide are known to induce suppression. These """"""""suppressor determinants"""""""" (SD) will be studied in detail to determine each essential residue and whether it is required for T suppressor cell binding (or is related to MHC function); also, it can be asked whether certain """"""""Th"""""""" cells have a suppressive phenotype. To investigate the mechanism of Ts action, """"""""grafts"""""""" of an SD onto an immunogenic peptide will be made and the requirements for this antigen-bridging suppression studied. A model peptide containing a Ts-inducing determinant, a Th-inducing determinant and a B cell determinant will be utilized to study the positional and specificity requirements associated with cell interaction. The interrelations of the different predominant idiotypes of the primary and secondary antibody responses to lysozyme will be studied.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI011183-20
Application #
3124912
Study Section
Immunobiology Study Section (IMB)
Project Start
1978-04-01
Project End
1994-01-14
Budget Start
1992-04-01
Budget End
1994-01-14
Support Year
20
Fiscal Year
1992
Total Cost
Indirect Cost

  Institution

Name
University of California Los Angeles
Department
Type
Schools of Arts and Sciences
DUNS #
119132785
City
Los Angeles
State
CA
Country
United States
Zip Code
90095

  Publications

Melo, Marco E F; Gabaglia, Claudia Raja; Moudgil, Kamal D et al. (2002) Strain-dependent effect of nasal instillation of antigen on the immune response in mice. Isr Med Assoc J 4:902-7
Moudgil, K D; Kim, E; Yun, O J et al. (2001) Environmental modulation of autoimmune arthritis involves the spontaneous microbial induction of T cell responses to regulatory determinants within heat shock protein 65. J Immunol 166:4237-43
Kang, H K; Mikszta, J A; Deng, H et al. (2000) Processing and reactivity of T cell epitopes containing two cysteine residues from hen egg-white lysozyme (HEL74-90). J Immunol 164:1775-82
Moudgil, K D; Sercarz, E E (2000) The self-directed T cell repertoire: its creation and activation. Rev Immunogenet 2:26-37
Schneider, S C; Ohmen, J; Fosdick, L et al. (2000) Cutting edge: introduction of an endopeptidase cleavage motif into a determinant flanking region of hen egg lysozyme results in enhanced T cell determinant display. J Immunol 165:20-3
Moudgil, K D; Southwood, S; Ametani, A et al. (1999) The self-directed T cell repertoire against mouse lysozyme reflects the influence of the hierarchy of its own determinants and can be engaged by a foreign lysozyme. J Immunol 163:4232-7
Gabaglia, C R; Pedersen, B; Hitt, M et al. (1999) A single intramuscular injection with an adenovirus-expressing IL-12 protects BALB/c mice against Leishmania major infection, while treatment with an IL-4-expressing vector increases disease susceptibility in B10.D2 mice. J Immunol 162:753-60
Moudgil, K D (1998) Diversification of response to hsp65 during the course of autoimmune arthritis is regulatory rather than pathogenic. Immunol Rev 164:175-84
Borghans, J A; De Boer, R J; Sercarz, E et al. (1998) T cell vaccination in experimental autoimmune encephalomyelitis: a mathematical model. J Immunol 161:1087-93
Moudgil, K D; Wang, J; Yeung, V P et al. (1998) Heterogeneity of the T cell response to immunodominant determinants within hen eggwhite lysozyme of individual syngeneic hybrid F1 mice: implications for autoimmunity and infection. J Immunol 161:6046-53

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