Cynthia A. Gates
Aventis Pharma
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Publication
Featured researches published by Cynthia A. Gates.
Bioorganic & Medicinal Chemistry | 1996
Joseph P. Burkhart; Cynthia A. Gates; Marie E. Laughlin; Robert J Resvick; Norton P. Peet
Steroids bearing a heteroaromatic substituent at C-17 were designed as inhibitors of C17(20) lyase. The thiazoles, furans, and thiophenes appended to the steroid nucleus were positioned on the alpha-face and the beta-face of the steroid, and conjugated with a 16,17-olefin, to test their ability to coordinate the heme iron of the P450 enzyme complex. The position of the heterocycle with respect to the steroid skeleton was determined to be important for optimum affinity and, in general, compounds with the heterocycle attached to a trigonal center at C-17, had the best affinity for C17(20) lyase. Simple molecular models were used to compare the three types of heterocyclic-substituted steroids.
Bioorganic & Medicinal Chemistry | 2002
Joseph P. Burkhart; Philip M. Weintraub; Cynthia A. Gates; Robert J Resvick; Roy J. Vaz; Dirk Friedrich; Michael Angelastro; Philippe Bey; Norton P. Peet
20-fluoro-17(20)-pregnenolone derivatives were designed as enol mimics of pregnenolone. All of the targeted, novel fluoroolefins were potent inhibitors of C17(20) lyase.
Journal of Medicinal Chemistry | 1967
James Pribish; Cynthia A. Gates; Philip M. Weintraub
Archive | 1994
Norton P. Peet; Joseph P. Burkhart; Cynthia A. Gates
Archive | 1994
Philip M. Weintraub; Cynthia A. Gates; Michael R. Angelastro; Timothy T. Curran; J. O'Neal Johnston
Archive | 1997
James Pribish; Cynthia A. Gates; Philipp M Weintraub
Archive | 1991
Philip M. Weintraub; Cynthia A. Gates; Thomas R. Blohm
Archive | 2001
Norton P. Peet; Philip M. Weintraub; Joseph P. Burkhart; Cynthia A. Gates
Archive | 2001
Norton P. Peet; Philip M. Weintraub; Joseph P. Burkhart; Cynthia A. Gates
Archive | 1995
Philip M. Weintraub; Cynthia A. Gates; Michael R. Angelastro; Timothy T. Curran; Gary A. Flynn; Chi-Hsin R King