Substituted pyrazolopyridopyridazines as orally bioavailable potent and selective PDE5 inhibitors: potential agents for treatment of erectile dysfunction.

Guixue Yu,Helen J. Mason,Ximao Wu,Jian Wang,Saeho Chong,Bruce Beyer,Andrew Henwood,Ronald Pongrac,Laurie Seliger,Bin He,Diane E. Normandin,Pam Ferrer,Rongan Zhang,Leonard P. Adam,William G. Humphrey,John Krupinski,John E. Macor

Substituted pyrazolopyridopyridazines as orally bioavailable potent and selective PDE5 inhibitors: potential agents for treatment of erectile dysfunction.

2003

Guixue Yu
Helen J. Mason
Ximao Wu
Jian Wang
Saeho Chong
Bruce Beyer
Andrew Henwood
Ronald Pongrac
Laurie Seliger
Bin He
Diane E. Normandin
Pam Ferrer
Rongan Zhang
Leonard P. Adam
William G. Humphrey
John Krupinski
John E. Macor

Novel pyrazolopyridopyridazine derivatives have been prepared as potent and selective PDE5 inhibitors. Compound 6 has been identified as a more potent and selective PDE5 inhibitor than sildenafil (1). It is as efficacious as sildenafil in in vitro and in vivo PDE5 inhibition models, and it is orally bioavailable in rats and dogs. The superior isozyme selectivity of 6 is expected to exert less adverse effects in humans when used for erectile dysfunction treatment.

Keywords:

Sildenafil
In vivo
Oral administration
Biochemistry
Erectile dysfunction
Chemistry
Pharmacokinetics
Adverse effect
Endocrinology
Internal medicine
In vitro
Enzyme inhibitor

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