Synthesis and SAR of a novel, potent and structurally simple LTD4 antagonist of the quinoline class.

Andreas von Sprecher,Marc Gerspacher,Andreas Beck,Sabine Kimmel,Hansruedi Wiestner,Gary P. Anderson,Ulrich Niederhauser,Natarajan Subramanian,Michael A. Bray

Synthesis and SAR of a novel, potent and structurally simple LTD4 antagonist of the quinoline class.

1998

Andreas von Sprecher
Marc Gerspacher
Andreas Beck
Sabine Kimmel
Hansruedi Wiestner
Gary P. Anderson
Ulrich Niederhauser
Natarajan Subramanian
Michael A. Bray

Abstract The two geminal ethyl groups in the succinic acid moiety of CGP57698 (4-[3-(7-fluoro-2-quinolinyl-methoxy)phenyl-amino]-2,2-diethyl-4-oxo-butanoic acid) are responsible for the high in vitro and in vivo potency of this peptidoleukotriene antagonist of the quinoline type. The synthesis and structure activity relationships of CGP57698 and its analogs are described.

Keywords:

Dicarboxylic acid
Moiety
Potency
Geminal
Stereochemistry
Biochemistry
Structure–activity relationship
Succinic acid
Quinoline
Chemistry
Carboxamide
Antagonist
Chemical synthesis

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