Abstract

The long term goal of this research is to develop novel anti-infective disease agents using rational drug design and combinatorial chemistry. The broad objectives of this program are the development of novel antibacterial agents that will address issues of drug resistance. The narrow objectives of the several projects are: discovery of inhibitors of the microbial histidine-aspartate kinase two-component signaling system that is responsible for vancomycin resistance; discovery of inhibitors of a metallopeptidase involved in lipid A biosynthesis; discovery of inhibitors of a 3-arabinosyl transferase involve din the biosynthesis of arabinan segments of mycobacterial cell wall. These molecular targets for antibacterial action come from both gram-negative and gram-positive bacteria. One project will also investigate the total synthesis on sold phase of molecules that exhibit strong anti-infective activity, butt whose molecular targets are not known. Methods to prepare combinatorial libraries of these materials for the discovery of more potent or different antibacterial actions will then be developed. An additional project will involved a """"""""generic"""""""" combinatorial library that can be used to map space in active sites of novel protein targets derived from microbial pathogens, allowed integration of combinatorial techniques and rational design principles. One particularly valuable aspect of this work will be the development of a new combinatorial library tagging methodology that permits rapid identification of molecules by NMR. This project will utilize the methods of organic synthesis on the solid phase, combinatorial chemistry, and antibacterial screening. This research will be significant because of the great difficulty medicine now perceives with pathogens that are resistant to conventional antibacterial drugs. Molecules that can modulate signaling events associated with histidine-aspartate kinases would be of great value in both basic scientific investigation and in potential control of microbial physiology and growth. An ancillary benefit of this project will be the development of novel techniques in solid phase synthesis through the total synthesis of natural products.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Allergy and Infectious Diseases (NIAID)
Type
Research Project (R01)
Project #
1R01AI042151-01
Application #
2448808
Study Section
Bio-Organic and Natural Products Chemistry Study Section (BNP)
Project Start
1998-09-30
Project End
2002-08-31
Budget Start
1998-09-30
Budget End
1999-08-31
Support Year
1
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Duke University
Department
Chemistry
Type
Schools of Arts and Sciences
DUNS #
071723621
City
Durham
State
NC
Country
United States
Zip Code
27705

  Publications

Pirrung, Michael C; Tumey, L Nathan; Raetz, Christian R H et al. (2002) Inhibition of the antibacterial target UDP-(3-O-acyl)-N-acetylglucosamine deacetylase (LpxC): isoxazoline zinc amidase inhibitors bearing diverse metal binding groups. J Med Chem 45:4359-70
Pirrung, Michael C; Park, Kaapjoo; Tumey, L Nathan (2002) (19)F-encoded combinatorial libraries: discovery of selective metal binding and catalytic peptoids. J Comb Chem 4:329-44
Pirrung, M C; Pansare, S V (2001) Trityl isothiocyanate support for solid-phase synthesis. J Comb Chem 3:90-6
Pirrung, M C; James, K D; Rana, V S (2000) Thiophosphorylation of histidine. J Org Chem 65:8448-53
Pirrung, M C; Tumey, L N (2000) Oxazoline synthesis from hydroxyamides by resin capture and ring-forming release. J Comb Chem 2:675-80
Pirrung, M C; Pei, T (2000) Synthesis of (+/-)-homohistidine. J Org Chem 65:2229-30
Pirrung, M C; Drabik, S J; Ahamed, J et al. (2000) Caged chemotactic peptides. Bioconjug Chem 11:679-81