Abstract

This proposal will investigate the expression of human antibody V genes in health and autoimmune disease. Although much has been learned in recent years concerning the molecular mechanisms governing the generation of antibody diversity, the relationship(s) between the factors responsible for diverse V-gene expression and autoimmunity is not clear. Do pathologic self-reactive antibodies arise form enhanced or constitutive V gene hypermutation or do they result from genetic deficiencies in the inherited gene-line genes? This investigation will take advantage of recent technological advances to explore these issues. Using synthetic peptide corresponding to conserved variable region framework or complementary determining regions of human antibodies, we will elicit murine monoclonal antibodies and rabbit antisera for use as molecular probes in the investigation of V gene expression of serum and surfact immunoglobulin. The latter will use multiparameter analyses in flow cytometry performed on blood and marrow lymphoid populations from normal individuals, patients with rheumatoid arthritis and recipients of allogeneic marrow transplants. These studies will investigate for differential expression of selected V gene subgroups, major cross reactive idiotypes associated with autoantibodies, and germ-line encoded variable region framework determinants. In addition, we will use human hybridomas and B lymphoblastoid lines as an in vitro system to study the stability of human isotype and V gene expression, the relationship between isotype switching and V gene somatic mutation, the association of rheumatoid factor activity with major cross reactive idiotypic determinants. Finally, we will investigate for single stranded DNA breaks in specific genes and explore the relationship between such chemical changes and the relative mutation rates in immunoglobulin genes. Through such studies we may gain a greater appreciation of factors controlling human antibody diversity and insight into host factors that may predispose one to autoimmune disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Arthritis and Musculoskeletal and Skin Diseases (NIAMS)
Type
First Independent Research Support & Transition (FIRST) Awards (R29)
Project #
5R29AR038475-02
Application #
3456743
Study Section
(ADDK)
Project Start
1986-08-01
Project End
1991-07-31
Budget Start
1987-08-01
Budget End
1988-07-31
Support Year
2
Fiscal Year
1987
Total Cost
Indirect Cost

  Institution

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

  Publications

Kobayashi, R; Picchio, G; Kirven, M et al. (1992) Transfer of human chronic lymphocytic leukemia to mice with severe combined immune deficiency. Leuk Res 16:1013-23
Martin, T; Duffy, S F; Carson, D A et al. (1992) Evidence for somatic selection of natural autoantibodies. J Exp Med 175:983-91
Pratt, L F; Szubin, R; Carson, D A et al. (1991) Molecular characterization of a supratypic cross-reactive idiotype associated with IgM autoantibodies. J Immunol 147:2041-6
Carson, D A; Chen, P P; Silverman, G J et al. (1991) Immunoglobulin gene expression in systemic rheumatic diseases. Br J Rheumatol 30 Suppl 1:43-6
Kipps, T J; Duffy, S F (1991) Relationship of the CD5 B cell to human tonsillar lymphocytes that express autoantibody-associated cross-reactive idiotypes. J Clin Invest 87:2087-96
Kipps, T J; Robbins, B A; Tefferi, A et al. (1990) CD5-positive B-cell malignancies frequently express cross-reactive idiotypes associated with IgM autoantibodies. Am J Pathol 136:809-16
Roudier, J; Silverman, G J; Chen, P P et al. (1990) Intraclonal diversity in the VH genes expressed by CD5- chronic lymphocytic leukemia-producing pathologic IgM rheumatoid factor. J Immunol 144:1526-30
Kipps, T J; Robbins, B A; Carson, D A (1990) Uniform high frequency expression of autoantibody-associated crossreactive idiotypes in the primary B cell follicles of human fetal spleen. J Exp Med 171:189-96
Kipps, T J (1990) Immunoglobulin idiotypes in human B cell neoplasia. Implications for pathogenesis and therapy. Chem Immunol 48:167-84
Kipps, T J (1989) The CD5 B cell. Adv Immunol 47:117-85

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