锂对口服氯丙嗪胃排空及吸收的影响。

Psychopharmacology communications Pub Date : 1976-01-01
L Rivera-Calimlim
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引用次数: 0

摘要

最近的一项研究表明,同时服用锂的患者血浆氯丙嗪(CPZ)水平较低(58-70 ng/ml),尽管摄入CPZ剂量(400-1000 MG)通常会产生100-300 ng/ml或更高的血浆水平。我们在大鼠身上研究了锂-氯丙嗪的相互作用。大鼠口服剂量(5 muCi)后,血浆和脑内氯丙嗪(CPZ)的[14C]含量显著降低(p < 0.005),而胃内残留剂量百分比(24-30%)显著高于对照组(p < 0.001)。胃排空用[14C]聚乙二醇测定,口服和口服锂可显著抑制胃排空。锂对胃排空的抑制可能是血浆CPZ水平较低的主要原因,因为在动物和人类中,左旋多巴、氯丙嗪、磺胺类药物和苯丁酮与抗胆碱能药物同时治疗会降低血浆药物水平,这也会降低胃的运动。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Effect of lithium on gastric emptying and absorption of oral chlorpromazine.

A recent study suggested that low plasma levels (58-70 ng/ml) of chlorpromazine (CPZ) were achieved by patients concurrently taking lithium, despite ingestion of doses of CPZ (400-1000 MG) which ordinarily produce plasma levels of 100-300 ng/ml or more. We have studied this lithium-chlorpromazine interaction in rats. The plasma and brain levels of [14C]chlorpromazine (CPZ) after an oral dose (5 muCi) were significantly lower (p less than 0.005) in rats treated with lithium, whereas the percent of dose remaining in the stomach (24-30%) was significantly higher (p less than 0.001), than in matched controls. Gastric emptying was measured by [14C]polyethylene glycol and was shown to be inhibited significantly by oral and i.p. lithium. This inhibition of gastric emptying by lithium may be the major cause of the lower plasma levels of CPZ since diminution of plasma drug levels has been shown for L-dopa, chlorpromazine, sulfa drugs, and phenylbutazone in animals and man treated concomitantly with anticholinergics, which also diminish gastric motility.

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