OCCUPANCY BY ORAL ADMINISTRATION OF NICARDIPINE OF L-TYPE CALCIUM CHANNELS IN RAT BRAIN

The occupancy of L-type Ca2+ channels by treatment with an oral dose of the dihydropyridine-type Ca2+ antagonist nicardipine (sustained-release formulation) was evaluated in membrane preparations of rat frontal cortex and hippocampus using a radioligand binding assay technique, with [3H]-nicardipine...

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Veröffentlicht in:Clinical and experimental hypertension (1993) 2001-01, Vol.23 (1-2), p.117-125
Hauptverfasser: Amenta, Francesco, Sabbatini, Maurizio, Strocchi, Paola, Tomassoni, Daniele, Tayebati, Seyed K., Vitali, Daniela
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Sprache:eng
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Zusammenfassung:The occupancy of L-type Ca2+ channels by treatment with an oral dose of the dihydropyridine-type Ca2+ antagonist nicardipine (sustained-release formulation) was evaluated in membrane preparations of rat frontal cortex and hippocampus using a radioligand binding assay technique, with [3H]-nicardipine as a ligand. Three hours after nicardipine administration, specific binding was decreased by about 15-20%, both in the frontal cortex and hippocampus. This indicates that oral nicardipine occupied approximately 15-20% of L-type Ca2+ channels. A progressive occupancy of Ca2+ channels was observed between six and 12 h after nicardipine administration. Twelve hours after drug administration, approximately 65-70% of Ca2+ channels were occupied. These findings indicate that oral treatment with 3 mg kg of nicardipine (sustained-release formulation) occupies L-type Ca2+ channels in rat brain by more than 40% from the 6th to the 24th h after drug administration. This suggests that an oral dose of nicardipine (sustained-release formulation) induces a significant occupancy of L-type Ca2+ channels in rat frontal cortex and hippocampus for about one day. The possible clinico-therapeutic relevance of this observation is discussed.
ISSN:1064-1963
1525-6006
DOI:10.1081/CEH-100001203