Ruo Wang scite author profile

For the past decade the immune system has been exploited as a rich source of de novo catalysts. Catalytic antibodies have been shown to have chemoselectivity, enantioselectivity, large rate accelerations, and even an ability to reroute chemical reactions. In many instances catalysts have been made for reactions for which there are no known natural or man-made enzymes. Yet, the full power of this combinatorial system can only be exploited if there was a system that allows for the direct selection of a particular function. A method that allows for the direct chemical selection for catalysis from antibody libraries was so devised, whereby the positive aspects of hybridoma technology were preserved and re-formatted in the filamentous phage system to allow direct selection of catalysis. This methodology is based on a purely chemical selection process, making it more general than biologically based selection systems because it is not limited to reaction products that perturb cellular machinery.

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A search for pyrophosphate mimics for the development of substrates and inhibitors of glycosyltransferases

Wang

Steensma

Takaoka

et al. 1997

Bioorganic & Medicinal Chemistry

111

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Ferrocene-containing hybrids as potential anticancer agents: Current developments, mechanisms of action and structure-activity relationships

Wang

Chen

Yan

et al. 2020

European Journal of Medicinal Chemistry

148

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Synthesis and Evaluation of Homoaza Sugars as Glycosidase Inhibitors

Wong¹,

Provencher²,

Porco³

et al. 1995

J. Org. Chem.

155

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Ruo Wang

Mucosal-associated Invariant T-Cell Function Is Modulated by Programmed Death-1 Signaling in Patients with Active Tuberculosis

Chemical Selection for Catalysis in Combinatorial Antibody Libraries

A search for pyrophosphate mimics for the development of substrates and inhibitors of glycosyltransferases

Ferrocene-containing hybrids as potential anticancer agents: Current developments, mechanisms of action and structure-activity relationships

Synthesis and Evaluation of Homoaza Sugars as Glycosidase Inhibitors

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