3-[2-(N-Phenylacetamide)]-1,5-benzodiazepines : Orally active, binding selective CCK-A agonists

Timothy M. Willson,Brad R. Henke,Tanya Momtahen,Peter L. Myers,Elizabeth E. Sugg,Rayomand J. Unwalla,Dallas K. Croom,Robert W. Dougherty,Mary K. Grizzle,Michael F. Johnson,Kennedy L. Queen,Thomas J. Rimele,Jeffrey D. Yingling,Michael K. James

3-[2-(N-Phenylacetamide)]-1,5-benzodiazepines : Orally active, binding selective CCK-A agonists

1996

Timothy M. Willson
Brad R. Henke
Tanya Momtahen
Peter L. Myers
Elizabeth E. Sugg
Rayomand J. Unwalla
Dallas K. Croom
Robert W. Dougherty
Mary K. Grizzle
Michael F. Johnson
Kennedy L. Queen
Thomas J. Rimele
Jeffrey D. Yingling
Michael K. James

A series of modifications were made to the C-3 substituent of the 1,5-benzodiazepine CCK-A agonist 1. Replacement of the inner urea NH and addition of a methyl group to generate a C-3 quaternary carbon resulted in acetamide 6, which showed CCK-A receptor binding selectivity and sub-micromolar agonist activity in vitro. Benzodiazepine 6 was active in an in vivo mouse gallbladder emptying assay and represents a novel orally active, binding selective CCK-A agonist.

Keywords:

Ligand (biochemistry)
Biochemistry
Oral administration
Agonist
Carboxamide
Pharmacology
Cholecystokinin
In vivo
Acetamide
Benzodiazepine
Chemistry

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