Abstract

Bacterial survival strongly depends on the functionality of a unique class of enzymes, the enolpyruvyl transferases. The only representatives of this family are MurA and EPSP synthase. MurA catalyzes the first committed step in the biosynthesis of the bacterial cell wall; EPSP synthase is the sixth enzyme of the shikimate pathway leading to the synthesis of aromatic compounds in numerous microorganisms. Since both pathways are absent from mammals, enolpyruvyl transferases are attractive targets for antibiotic drugs. The reactions catalyzed by enolpyruvyl transferases proceed through the chemically unusual transfer of the enolpyruvyl moiety of phosphoenolpyruvate (PEP) to a second substrate. The uniqueness of these enzymes is also reflected by their distinct 3-dimensional architecture: two globular, inside-out, alpha-beta-barrel domains are connected by a double-stranded hinge. A number of recent structural studies revealed that the two domains approach each other on substrate binding, such that the active site emerges in the interdomain cleft. The central goal of this proposal is to understand how the unusual reaction mechanism, the distinct structural properties, and the dynamics of enolpyruvyl transferases are related to each other.
The specific aims are: 1) to visualize the principle steps of enolpyruvyl transfer by determining the high resolution X-ray structures of binary and ternary enzyme:substrate complexes. Single-site mutant enzymes with altered kinetics and dynamics shall be selected to trap the reaction at different states; 2) to characterize the structural prerequisites and the principles of the induced-fit mechanism by fluorescence studies and X-ray crystallographic analysis of mutant enzymes from MurA and EPSP synthase; 3) to analyze the structure and function of enolpyruvyl transferases from pathogenic bacteria in order to reveal how the requirements for enolpyruvyl transfer are realized in enzymes with low sequence homologies to E. coli and 4) to employ the aptamer technology in order to create novel inhibitors for MurA and EPSP synthase. These studies will contribute directly to the basic knowledge of protein structure families, structural folds, and the relationship between structure and function in enzymatic reactions. Furthermore, the proposed work will provide deep insight in the potential of enolpyruvyl transferases as broad-spectrum antibacterial targets and shall facilitate the design of novel antibiotic drugs.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Center for Research Resources (NCRR)
Type
Exploratory Grants (P20)
Project #
5P20RR016443-02
Application #
6651405
Study Section
Special Emphasis Panel (ZRR1)
Project Start
2002-09-01
Project End
2003-08-31
Budget Start
Budget End
Support Year
2
Fiscal Year
2002
Total Cost
Indirect Cost

  Institution

Name
University of Kansas
Department
Type
DUNS #
016060860
City
Kansas City
State
KS
Country
United States
Zip Code
66160

  Publications

He, Chenchen; Duan, Shaofeng; Dong, Liang et al. (2017) Characterization of a novel p110?-specific inhibitor BL140 that overcomes MDV3100-resistance in castration-resistant prostate cancer cells. Prostate 77:1187-1198
Li, Jiaqin; Wehmeyer, Graham; Lovell, Scott et al. (2016) 1.65?Å resolution structure of the AraC-family transcriptional activator ToxT from Vibrio cholerae. Acta Crystallogr F Struct Biol Commun 72:726-31
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Kumaraswamy, E; Wendt, K L; Augustine, L A et al. (2015) BRCA1 regulation of epidermal growth factor receptor (EGFR) expression in human breast cancer cells involves microRNA-146a and is critical for its tumor suppressor function. Oncogene 34:4333-46
Freitas, Natalia; Abe, Kenji; Cunha, Celso et al. (2014) Support of the infectivity of hepatitis delta virus particles by the envelope proteins of different genotypes of hepatitis B virus. J Virol 88:6255-67
Tang, Yuzhe; Chen, Ruibao; Huang, Yan et al. (2014) Natural compound Alternol induces oxidative stress-dependent apoptotic cell death preferentially in prostate cancer cells. Mol Cancer Ther 13:1526-36
Freitas, Natalia; Cunha, Celso; Menne, Stephan et al. (2014) Envelope proteins derived from naturally integrated hepatitis B virus DNA support assembly and release of infectious hepatitis delta virus particles. J Virol 88:5742-54
Grogan, Patrick T; Sarkaria, Jann N; Timmermann, Barbara N et al. (2014) Oxidative cytotoxic agent withaferin A resensitizes temozolomide-resistant glioblastomas via MGMT depletion and induces apoptosis through Akt/mTOR pathway inhibitory modulation. Invest New Drugs 32:604-17
Luo, Yong; Kleiboeker, Steve; Deng, Xuefeng et al. (2013) Human parvovirus B19 infection causes cell cycle arrest of human erythroid progenitors at late S phase that favors viral DNA replication. J Virol 87:12766-75

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