心脏糖苷和钙拮抗剂联合作用下犬房室传导的改变。

Journal de pharmacologie Pub Date : 1986-07-01
J Lang, Q Timour Chah, M el Chebly, G Faucon
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引用次数: 0

摘要

从逻辑上讲,地高辛-维拉帕米联用可能导致传导障碍,因为已知这两种药物都会增加房室结的传导时间(CT)和有效不应期(ERP)。在没有迷走神经张力的情况下,维拉帕米(1.27 mg/kg, 90分钟)显著抑制房室传导时,以1微克/kg/min的速率输注地高辛,超过40分钟,引起维拉帕米作用的进行性但不完全消退,高达5.5 mmol/l的高钙血症也是如此。以2.5微克/千克/分的速率输注20min后,其拮抗作用与超过5.5 mmol/l的高钙血症一样越来越不明显,甚至被一定的协同作用所取代。当地高辛(静脉注射40微克/千克)在高迷走神经张力下抑制房室传导时,维拉帕米(两次0.2毫克/千克)不会加重这种抑制,甚至会减弱这种抑制,但这种减弱在ERP上比在房室结的CT上更为明显。因此,通常,相互作用不会导致阻滞,因为一种药物的最大作用与另一种药物作用的减少有关,甚至是协同作用转化为拮抗作用。
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Modification of atrioventricular conduction under the combined influence of a cardiac glycoside and a calcium antagonist in the dog.

Conduction disorders may be logically expected from the digoxin-verapamil association, since each of these drugs is known to increase conduction time (CT) and effective refractory period (ERP) in the atrioventricular (AV) node. When AV conduction is considerably depressed by verapamil (1.27 mg/kg over 90 min) in the absence of vagal tone, digoxin, infused at 1 microgram/kg/min rate over 40 min, elicits a progressive but incomplete regression of the verapamil effects, as does hypercalcaemia up to 5.5 mmol/l. Infused at the 2.5 microgram/kg/min rate over 20 min, its antagonistic effects, like those of hypercalcaemia exceeding 5.5 mmol/l, are less and less marked and even replaced by a certain synergism. When AV conduction is considerably depressed by digoxin (i.v. injection of 40 micrograms/kg) under high vagal tone, verapamil (twice 0.2 mg/kg) does not aggravate this depression and even attenuates it, this attenuation being however more significant on ERP than CT in the AV node. Consequently, as a rule, the interaction does not lead to block, since the maximum action of one drug is associated with the reduction in the action of the other or even the conversion of synergism into antagonism.

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