Abstract

Immune maturation is viewed as a Darwinian process that involves selection of the structures with best fit. The long term objective of this project is to study the molecular basis of antigen recognition and its contribution as a selective force in shaping the antibody response to phosphocholine-protein PC-KLH conjugates. The evolution of antibodies to PC-KLH will be analyzed in three families of clonally related hybridomas isolated during the memory antibody response. These families are representative of group II antibodies which have a strong requirement for the phenyl structure that links PC to the carrier protein. Each of these families uses a distinct V gene pair to form the active site. The interaction of members of these families with antigen will be studied at the molecular and atomic levels to determine the structural evolution of their antibody combining sites during maturation of the response. We shall also evaluate the concept of B cell """"""""wastage"""""""" during the antibody somatic diversification process by studying the ability of random mutations in the VH CDR2 to lead to antigen binding loss mutations in hybridomas producing anti-PC-KLH antibodies. We have observed that mutations in the VH CDR2 of certain antibodies leads to loss of antibody secretion. We shall study the molecular basis for this effect by studying the intracellular assembly and trafficking of immunoglobulin molecules bearing particular mutations. The proposed studies make use of biochemical and immunochemical methods to study the function of antibodies modified through the use of site directed and saturation mutagenesis. The mutant molecules will be examined by computer assisted molecular modeling and the interactions of antibody fragments with antigen will be examined using nuclear magnetic resonance (NMR). These studies will provide important information on the structure of antibody combining sites that will be important in redesigning antibodies to improve their function and may lead to new understanding of diseases where antibody secretion may be impaired.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
5R01AI026827-08
Application #
2063571
Study Section
Immunobiology Study Section (IMB)
Project Start
1988-07-01
Project End
1998-06-30
Budget Start
1995-07-01
Budget End
1996-06-30
Support Year
8
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Oregon Health and Science University
Department
Microbiology/Immun/Virology
Type
Schools of Medicine
DUNS #
009584210
City
Portland
State
OR
Country
United States
Zip Code
97239

  Publications

Whitcomb, Elizabeth A; Martin, Tammy M; Rittenberg, Marvin B (2003) Restoration of Ig secretion: mutation of germline-encoded residues in T15L chains leads to secretion of free light chains and assembled antibody complexes bearing secretion-impaired heavy chains. J Immunol 170:1903-9
Wiens, Gregory D; Brown, McKay; Rittenberg, Marvin B (2003) Repertoire shift in the humoral response to phosphocholine-keyhole limpet hemocyanin: VH somatic mutation in germinal center B cells impairs T15 Ig function. J Immunol 170:5095-102
Wiens, G D; O'Hare, T; Rittenberg, M B (2001) Recovering antibody secretion using a hapten ligand as a chemical chaperone. J Biol Chem 276:40933-9
Wiens, G D; Lekkerkerker, A; Veltman, I et al. (2001) Mutation of a single conserved residue in VH complementarity-determining region 2 results in a severe Ig secretion defect. J Immunol 167:2179-86
Brown, M; Schumacher, M A; Wiens, G D et al. (2000) The structural basis of repertoire shift in an immune response to phosphocholine. J Exp Med 191:2101-12
Brown, M; Wiens, G D; O'Hare, T et al. (1999) Replacements in the exposed loop of the T15 antibody VH CDR2 affect carrier recognition of PC-containing pathogens. Mol Immunol 36:205-11
O'Hare, T; Wiens, G D; Whitcomb, E A et al. (1999) Cutting edge: proteasome involvement in the degradation of unassembled Ig light chains. J Immunol 163:11-4
Wiens, G D; Roberts, V A; Whitcomb, E A et al. (1998) Harmful somatic mutations: lessons from the dark side. Immunol Rev 162:197-209
Martin, T M; Wiens, G D; Rittenberg, M B (1998) Inefficient assembly and intracellular accumulation of antibodies with mutations in V(H) CDR2. J Immunol 160:5963-70
Heldwein, K A; Duncan, J E; Stenzel, P et al. (1997) Endotoxin regulates corticotropin-releasing hormone receptor 2 in heart and skeletal muscle. Mol Cell Endocrinol 131:167-72

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