Discovery of a Peptide-Based Renin Inhibitor with Oral Bioavailability and Efficacy

Discovery of a Peptide-Based Renin Inhibitor with Oral Bioavailability and Efficacy

Peptidic renin inhibitors have been poorly absorbed across the intestine or rapidly eliminated by the liver and have been reported to have oral bioavailabilities of less than 2%. A peptide-based renin inhibitor, A-72517 (molecular mass of 706 daltons), was devised that has oral bioavailabilities of...

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Veröffentlicht in:Science (American Association for the Advancement of Science) 1992-09, Vol.257 (5078), p.1940-1943
Hauptverfasser: Kleinert, Hollis D., Rosenberg, Saul H., Baker, William R., Stein, Herman H., Klinghofer, Vered, Barlow, Jennifer, Spina, Kenneth, Polakowski, James, Kovar, Peter, Cohen, Jerome, Denissen, Jon
Format: Artikel
Sprache:eng
Schlagworte:
administration
Administration, Oral
Animals
Antihypertensive agents
Bioavailability
Biological and medical sciences
Biological Availability
Blood
Blood plasma
Blood pressure
Cardiovascular agents
Cardiovascular system
Dogs
Dosage
efficacy
Ferrets
Health aspects
Hemodynamics - drug effects
inhibitors
Medical sciences
Monkeys
Peptides
Pharmacology. Drug treatments
Physiological aspects
Piperazines - chemistry
Piperazines - pharmacokinetics
Piperazines - pharmacology
Protease Inhibitors - chemistry
Protease Inhibitors - metabolism
Protease Inhibitors - pharmacokinetics
Rats
renin
Renin - antagonists & inhibitors
Renin-angiotensin system
Structure-Activity Relationship
Thiazoles - chemistry
Thiazoles - pharmacokinetics
Thiazoles - pharmacology
Vehicles
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Zusammenfassung:Peptidic renin inhibitors have been poorly absorbed across the intestine or rapidly eliminated by the liver and have been reported to have oral bioavailabilities of less than 2%. A peptide-based renin inhibitor, A-72517 (molecular mass of 706 daltons), was devised that has oral bioavailabilities of 8, 24, 32, and 53% in the monkey, rat, ferret, and dog, respectively. Dose-related reductions in blood pressure, plasma renin activity, and plasma angiotensin II in parallel with increased plasma drug concentrations were observed after oral administration of A-72517 to conscious, salt-depleted dogs. Thus, peptide-based molecules of sizable molecular mass can be absorbed intact into the systemic circulation of animals. These findings support the potential of peptide-based drugs for oral administration.
ISSN:0036-8075
1095-9203
DOI:10.1126/science.1411510