Abstract

Rapid developments in genomics, proteomics, and combinatorial chemistry have reshaped the field of drug discovery, providing new drug targets for selective screens and new compounds to be tested in those screens. While combinatorial methods have given rise to large libraries of compounds, typically these compounds result in improved lead candidates that must undergo further transformations by conventional medicinal chemistry to yield new drug candidates. Bioengineering, in the context of high-throughput combinatorial methodologies, has not impacted lead optimization nearly as much as it has lead discovery, mainly because of the highly selective, intricate chemistries often required to optimize lead compounds and the lack of a suitably broad high-throughput platform. Combinatorial biocatalysis can help overcome these obstacles by exploiting the exquisite selectivity and unique reactivity of enzymes and microbial biocatalysts; however, to date this technology has been limited to the derivatization of soluble substrates. We propose to expand the scope of combinatorial biocatalysis to include reactions on, and the generation of libraries from, lead molecules attached to solid and soluble polymer supports. In the process, we will develop a high-throughput, biocatalytic technology for drug discovery.
The specific aims are: 1. To expand the breadth of biocatalysis on solid- and polymer-supported compounds in aqueous and nonaqueous media; 2. To develop strategies for attaching lead compounds and removing their derivatives from solid and polymeric supports; 3. To demonstrate high-throughput, combinatorial biocatalytic lead optimization of complex natural and synthetic molecules, screen resulting derivatives for biological activity, and scale up structurally and functionally interesting derivatives using biotransformations. A series of lead molecules will be used in this work, ranging from enzyme substrates that are attached onto solid and soluble polymer supports to complex compounds (the flavonoid bergenin and the current HIV-1 protease inhibitor indinavir). Successful completion of this research program will result in a powerful methodology that can be used by biomedical investigators in the search for new, more potent small molecule therapeutics.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
1R01GM066712-01A1
Application #
6700385
Study Section
Special Emphasis Panel (ZRG1-BECM (01))
Program Officer
Schwab, John M
Project Start
2004-02-03
Project End
2008-01-31
Budget Start
2004-02-03
Budget End
2005-01-31
Support Year
1
Fiscal Year
2004
Total Cost
$713,432
Indirect Cost

  Institution

Name
Rensselaer Polytechnic Institute
Department
Engineering (All Types)
Type
Schools of Engineering
DUNS #
002430742
City
Troy
State
NY
Country
United States
Zip Code
12180

  Publications

Kwon, Seok Joon; Kim, Moon Il; Ku, Bosung et al. (2010) Unnatural polyketide analogues selectively target the HER signaling pathway in human breast cancer cells. Chembiochem 11:573-80
Akbar, Umar; Shin, Dong-Sik; Schneider, Elizabeth et al. (2010) Two-Step Enzymatic Modification of Solid-Supported Bergenin in Aqueous and Organic Media. Tetrahedron Lett 51:1220
Reeder, Philippa J; Huang, Yao-Ming; Dordick, Jonathan S et al. (2010) A rewired green fluorescent protein: folding and function in a nonsequential, noncircular GFP permutant. Biochemistry 49:10773-9
Fernandes, Tiago G; Kwon, Seok-Joon; Bale, Shyam Sundhar et al. (2010) Three-dimensional cell culture microarray for high-throughput studies of stem cell fate. Biotechnol Bioeng 106:106-18
Hudson, Elton P; Eppler, Ross K; Beaudoin, Julianne M et al. (2009) Active-site motions and polarity enhance catalytic turnover of hydrated subtilisin dissolved in organic solvents. J Am Chem Soc 131:4294-300
Kim, Moon Il; Kwon, Seok Joon; Dordick, Jonathan S (2009) In vitro precursor-directed synthesis of polyketide analogues with coenzyme a regeneration for the development of antiangiogenic agents. Org Lett 11:3806-9
Fernandes, Tiago G; Diogo, Maria Margarida; Clark, Douglas S et al. (2009) High-throughput cellular microarray platforms: applications in drug discovery, toxicology and stem cell research. Trends Biotechnol 27:342-9
Jamadagni, Sumanth N; Godawat, Rahul; Garde, Shekhar (2009) How surface wettability affects the binding, folding, and dynamics of hydrophobic polymers at interfaces. Langmuir 25:13092-9
Jamadagni, Sumanth N; Godawat, Rahul; Dordick, Jonathan S et al. (2009) How interfaces affect hydrophobically driven polymer folding. J Phys Chem B 113:4093-101
Antipov, Eugene; Cho, Art E; Klibanov, Alexander M (2009) How a single-point mutation in horseradish peroxidase markedly enhances enantioselectivity. J Am Chem Soc 131:11155-60

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