Abstract

The goal of the proposed research is to developed methods for the design of biologically active compounds based on a knowledge of the structure and conformation of oligopeptide ligands and protein binding sites. Five distinct systems will be explored through the synthesis, evaluation, and refinement of a series of peptide mimics. The compounds to be synthesized include: Inhibitors of alpha-Amylase: Tricyclic molecules incorporating tyrosine, arginine, and tryptophan sidechains of the key triad of amino acids of the amylase inhibitor tendamistat. Serine Protease Inhibitors: Macrocyclic mimics of the active loop of bovine pancreatic trypsin inhibitor, incorporating elements of residues 13-17, the lysine-15 side chain, and a reactive ketone in place of the scissile amide. This series of inhibitor mimics can be readily extended to other serine proteases. Alpha-Helix Mimics: A pair of bicyclic molecules containing three hydrogen bonding groups fixed in the orientation found within a peptide alpha-helix. These molecules will be appended to oligopeptides as their N- or C-terminal residues and evaluated for their ability to induce or stabilize the alpha-helical conformation. Thermolysin Inhibitors: Macrocyclic derivatives of high affinity phosphonate inhibitors which adopt a specific loop conformation in the active site of thermolysin. These compounds will be used to explore in a structurally verifiable manner the effect of conformational restriction on protein-ligand binding. Haloalkene Isosteres of the Peptide Bond: Dipeptide analogs in which the amide linkage is replaced with a fluorine- or chlorine- substituted double bond. Such analogs will be prepared for enkephalin, thyrotropin releasing hormone, aspartame, and as ground-state substrate analogs for peptidases. The synthetic methodology will also be adapted for the stereospecific synthesis of ketomethylene dipeptide isoteres. In addition to direct evaluation of the ability of the above compounds to exert their intended biochemcial or biophysical effect, collaborative studies will be undertaken to determine their solution structure through 2-D NMR or their bound conformation through X-ray crystallography, where appropriate.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Method to Extend Research in Time (MERIT) Award (R37)
Project #
5R37GM030759-16
Application #
3484688
Study Section
Bio-Organic and Natural Products Chemistry Study Section (BNP)
Project Start
1977-09-01
Project End
1993-03-31
Budget Start
1991-04-01
Budget End
1992-03-31
Support Year
16
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
University of California Berkeley
Department
Type
Schools of Arts and Sciences
DUNS #
094878337
City
Berkeley
State
CA
Country
United States
Zip Code
94704

  Publications

Phillips, Scott T; Blasdel, Landy K; Bartlett, Paul A (2005) @-tides as reporters for molecular associations. J Am Chem Soc 127:4193-8
Hansen, Kristina K; Grosch, Benjamin; Greiveldinger-Poenaru, Sorana et al. (2003) Synthesis and evaluation of macrocyclic transition state analogue inhibitors for alpha-chymotrypsin. J Org Chem 68:8465-70
Hansen, Kristina K; Hansen, Henrik C; Clark, Ryan C et al. (2003) Identification of novel macrocyclic peptidase substrates via on-bead enzymatic cyclization. J Org Chem 68:8459-64
Lewis, Jason G; Bartlett, Paul A (2003) Amino acid-derived heterocycles as combinatorial library targets: bicyclic aminal lactones. J Comb Chem 5:278-84
Trump, Ryan P; Bartlett, Paul A (2003) Amino acid-derived heterocycles as combinatorial library targets: spirocyclic ketal lactones. J Comb Chem 5:285-91
Todd, Matthew H; Ndubaku, Chudi; Bartlett, Paul A (2002) Amino acid derived heterocycles: lewis acid catalyzed and radical cyclizations from peptide acetals. J Org Chem 67:3985-8
Spaller, Mark R; Thielemann, Wolfgang T; Brennan, Paul E et al. (2002) Combinatorial synthetic design. Solution and polymer-supported synthesis of heterocycles via intramolecular aza Diels-Alder and imino alcohol cyclizations. J Comb Chem 4:516-22
Bartlett, Paul A; Yusuff, Naeem; Rico, Alice C et al. (2002) Antihydrophobic solvent effects: an experimental probe for the hydrophobic contribution to enzyme-inhibitor binding. J Am Chem Soc 124:3853-7
An, M; Toochinda, T; Bartlett, P A (2001) Five-membered ring analogues of shikimic acid. J Org Chem 66:1326-33
Fraser, M E; Meyer, J H; Bartlett, P A et al. (1998) Overcoming the unfavourable entropic contribution of ligand binding with a macrocyclic inhibitor bound to penicillopepsin. Adv Exp Med Biol 436:355-9

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