Dihydroxyphenylisoindoline amides as orally bioavailable inhibitors of the heat shock protein 90 (hsp90) molecular chaperone.

Pei-Pei Kung,Buwen Huang,Gang Zhang,Joe Zhongxiang Zhou,Jeff Wang,Jennifer A. Digits,Judith Skaptason,Shinji Yamazaki,David Neul,Michael Zientek,Jeff Elleraas,Pramod P. Mehta,Min-Jean Yin,Michael J. Hickey,Ketan S. Gajiwala,Caroline Rodgers,Jay F. Davies,Michael R. Gehring

Dihydroxyphenylisoindoline amides as orally bioavailable inhibitors of the heat shock protein 90 (hsp90) molecular chaperone.

2010

Pei-Pei Kung
Buwen Huang
Gang Zhang
Joe Zhongxiang Zhou
Jeff Wang
Jennifer A. Digits
Judith Skaptason
Shinji Yamazaki
David Neul
Michael Zientek
Jeff Elleraas
Pramod P. Mehta
Min-Jean Yin
Michael J. Hickey
Ketan S. Gajiwala
Caroline Rodgers
Jay F. Davies
Michael R. Gehring

The discovery and optimization of potency and metabolic stability of a novel class of dihyroxyphenylisoindoline amides as Hsp90 inhibitors are presented. Optimization of a screening hit using structure-based design and modification of log D and chemical structural features led to the identification of a class of orally bioavailable non-quinone-containing Hsp90 inhibitors. This class is exemplified by 14 and 15, which possess improved cell potency and pharmacokinetic profiles compared with the original screening hit.

Keywords:

Hsp90
Heat shock protein
Potency
Chaperone (protein)
Enzyme
Biochemistry
Enzyme inhibitor
Carboxamide
Chemistry
Pharmacokinetics
Chemical synthesis

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