Abstract

The extreme conformational flexibility of small peptide hormones has hindered the elucidation of their biologically active structures by either spectroscopic or crystallographic methods. Since their membrane-bound receptors are, in most cases, inaccessible and not possible to crystallize, it has been difficult. to experimentally address the question of how these unstructured peptides are recognized with extremely high affinities by their receptors. In fact, at the present time there is no structural information about binding of hormone peptides to any protein. One way to obtain information about the high-affinity binding of flexible peptides by proteins is to study the peptides bound with receptor-like affinities to monoclonal antibodies. By studying a number of antibody-peptide complexes, one might not only make use of the specific information for each particular complex, but also begin to delineate some general rules which govern the interactions of small peptide hormones with proteins. We have a panel of monoclonal antibodies which bind with extremely high affinities to Angiotensin II (AII), the major effector of the renin/angiotensin system. We have, in addition, several monoclonals that bind GnRH, the gonadotropin releasing hormone. Crystals have been grown of the uncomplexed and complexed forms of one of these Fabs, Fab-131, and its structure determined and refined by crystallographic methods. In this project we propose to study the three-dimensional structure of several peptide-hormone/Fab complexes The proposed work includes: 1) Completion of the refinement of the structure of the anti-angiotensin(AII) Fab-131 and of the Fab-131/AII cocrystals; 2)Determination of the structures of bound AII analogs by difference Fourier methods and crystallographic refinement of the structure of the complexes; 3) Analysis of the interactions of the binding site of Fab-131 with AH and AH analogs; 4) Design, synthesis and characterization of new AH analogs with potential high affinity for Fab-131; 5) Determination of the structures of the complexes of AII and AII analogs with Fab-133, Fab-110 and Fab-A25; 6)Crystallization of other Fab fragments complexes to AH and GnRH. The structural information obtained in this project will be used to gain insight about receptor/hormone interactions.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM044692-02
Application #
3303942
Study Section
Biophysical Chemistry Study Section (BBCB)
Project Start
1992-02-01
Project End
1996-01-31
Budget Start
1993-02-01
Budget End
1994-01-31
Support Year
2
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Type
Schools of Medicine
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

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Prigge, S T; Kolhekar, A S; Eipper, B A et al. (1997) Amidation of bioactive peptides: the structure of peptidylglycine alpha-hydroxylating monooxygenase. Science 278:1300-5
D'Aquino, J A; Gomez, J; Hilser, V J et al. (1996) The magnitude of the backbone conformational entropy change in protein folding. Proteins 25:143-56
Prigge, S T; Boyington, J C; Gaffney, B J et al. (1996) Structure conservation in lipoxygenases: structural analysis of soybean lipoxygenase-1 and modeling of human lipoxygenases. Proteins 24:275-91
Pan, Y; Yuhasz, S C; Amzel, L M (1995) Anti-idiotypic antibodies: biological function and structural studies. FASEB J 9:43-9
Amzel, L M; Gaffney, B J (1995) Structural immunology: problems in molecular recognition. FASEB J 9:7-8
Lee, K H; Xie, D; Freire, E et al. (1994) Estimation of changes in side chain configurational entropy in binding and folding: general methods and application to helix formation. Proteins 20:68-84
Garcia, K C; Ronco, P M; Verroust, P J et al. (1992) Three-dimensional structure of an angiotensin II-Fab complex at 3 A: hormone recognition by an anti-idiotypic antibody. Science 257:502-7