Cardiovascular Effects of Aspidofractinine-Type Alkaloids from Kopsia

Cardiovascular Effects of Aspidofractinine-Type Alkaloids from Kopsia

Intravenous injection of the aspidofractinine alkaloid, kopsingine (1, 0.2−10.0 mg/kg) from Kopsia teoi, produced dose-related decreases in the mean arterial blood pressure and heart rate in anesthetized spontaneously hypertensive rats, which were similar to those seen in normotensive controls. Mino...

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Veröffentlicht in:Journal of natural products (Washington, D.C.) D.C.), 1998-03, Vol.61 (3), p.328-332
Hauptverfasser: Mok, Shiueh-Lian, Yoganathan, Kanagasundaram, Lim, Tuck-Meng, Kam, Toh-Seok
Format: Artikel
Sprache:eng
Schlagworte:
14,15-DIHYDROKOPSINGINE
ALCALOIDE
ALCALOIDES
ALKALOIDS
Alkaloids - isolation & purification
Alkaloids - pharmacology
Animals
ANTIHYPERTENSIVE AGENTS
Antihypertensive Agents - isolation & purification
Antihypertensive Agents - pharmacology
APOCYNACEAE
ARTERE
ARTERIAS
ARTERIES
Asia, Southeastern
Biological and medical sciences
BLOOD PRESSURE
Blood Pressure - drug effects
CARDIOVASCULAR AGENTS
Cardiovascular system
CHEMICAL COMPOSITION
CHEMICAL STRUCTURE
COMPOSICION QUIMICA
COMPOSITION CHIMIQUE
DRUG PLANTS
ESPECTROMETRIA
ESTRUCTURA QUIMICA
FRECUENCIA CARDIACA
FREQUENCE CARDIAQUE
HEART RATE
Heart Rate - drug effects
HEPTACYCLIC KOPSIDINE A
Injections, Intravenous
KOPSAPORINE
KOPSIA TEOI
KOPSINGINE
Male
Medical sciences
MEDICAMENTOS CARDIOVASCULARES
MODIFICATEUR CARDIOVASCULAIRE
PHARMACEUTICAL PRODUCTS
Pharmacology. Drug treatments
PLANTAS MEDICINALES
PLANTE MEDICINALE
Plants, Medicinal - chemistry
PRESION SANGUINEA
PRESSION SANGUINE
Rats
Rats, Inbred SHR
Rats, Inbred WKY
SPECTRAL ANALYSIS
SPECTROMETRIE
SPECTROMETRY
STRUCTURE CHIMIQUE
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Zusammenfassung:Intravenous injection of the aspidofractinine alkaloid, kopsingine (1, 0.2−10.0 mg/kg) from Kopsia teoi, produced dose-related decreases in the mean arterial blood pressure and heart rate in anesthetized spontaneously hypertensive rats, which were similar to those seen in normotensive controls. Minor modifications in the molecular structure of kopsingine, as in kopsaporine (2, the 12-demethoxy derivative of kopsingine) and 14,15-dihydrokopsingine (4), did not significantly alter the hypotensive responses, whereas a more drastic change in the structure, as in the heptacyclic kopsidine A (3) and the 3-to-17 oxo-bridged compound 5, resulted in an increase in blood pressure. The antihypertensive effects of kopsingine (1) and its congeners (2 and 4) along with the pressor effects produced by the heptacyclic oxo-bridged compounds (5 and 3) could be ascribed to central as well as peripheral actions.
ISSN:0163-3864
1520-6025
DOI:10.1021/np9703712