Design, synthesis, and characterization of novel, nonquaternary reactivators of GF-inhibited human acetylcholinesterase.

Stanton F. McHardy,Jonathan A. Bohmann,Michael R. Corbett,Bismarck Campos,Michael W. Tidwell,Paul M. Thompson,Chris J. Bemben,Tony A. Menchaca,Tony E. Reeves,William R. Cantrell,William E. Bauta,Ambrosio Lopez,Donald M. Maxwell,Karen M. Brecht,Richard E. Sweeney,John McDonough

Design, synthesis, and characterization of novel, nonquaternary reactivators of GF-inhibited human acetylcholinesterase.

2014

Stanton F. McHardy
Jonathan A. Bohmann
Michael R. Corbett
Bismarck Campos
Michael W. Tidwell
Paul M. Thompson
Chris J. Bemben
Tony A. Menchaca
Tony E. Reeves
William R. Cantrell
William E. Bauta
Ambrosio Lopez
Donald M. Maxwell
Karen M. Brecht
Richard E. Sweeney
John McDonough

The goal of this research was to identify structurally novel, non-quaternarypyridinium reactivators of GF (cyclosarin)-inhibited hAChE that possess the capacity to mediate in vitro reactivation of GF-inhibited human acetylcholinesterase (hAChE). New compounds were designed, synthesized and assessed in GF-inhibited hAChE assays. Structure activity relationships for AChE binding and reactivation of GF-inhibited hAChE were developed. Lead compounds from two different chemical series, represented by compounds 17 and 38, displayed proficient in vitro reactivation of GF-inhibited hAChE, while also possessing low inhibition of native enzyme.

Keywords:

Enzyme
Cyclosarin
Aché
Cholinesterase
Stereochemistry
Structure–activity relationship
In vitro
Chemistry
Biochemistry
Acetylcholinesterase
design synthesis

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