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多沙普仑在患者和志愿者中的药代动力学研究。

A pharmacokinetic study of doxapram in patients and volunteers.

作者信息

Robson R H, Prescott L F

出版信息

Br J Clin Pharmacol. 1979 Jan;7(1):81-7. doi: 10.1111/j.1365-2125.1979.tb00901.x.

Abstract
  1. Following intravenous bolus injections or brief infusions in healthy volunteers, plasma concentrations of doxapram declined in a multi-exponential fashion. The mean half-life from 4-12 h was 3.4 h (range 2.4-4.1h), the mean apparent volume of distribution was 1.5 1 kg-1 and the whole body clearance was 370 ml min-1. 2. Enteric-coated capsules of doxapram base were absorbed rapidly after an initial delay, and the systemic availability was about 60%. 3. Doxapram is extensively metabolized and less than 5% of an i.v. dose was excreted unchanged in the urine in 24 h. A metabolite (AHR 5955) was present in plasma in amounts comparable to the parent compound and had a similar half-life. 4. The disposition of doxapram appears to be similar in healthy volunteers and patients with respiratory failure. 5. The previously held belief that plasma concentrations fall rapidly when an infusion is stopped is only true following short duration infusions. The pharmacokinetic properties of doxapram are such that steady-state plasma concentrations will not be achieved for many hours with the recommended constant rate infusion régime.
摘要
  1. 在健康志愿者中静脉推注或短暂输注多沙普仑后,其血浆浓度呈多指数方式下降。4至12小时的平均半衰期为3.4小时(范围为2.4至4.1小时),平均表观分布容积为1.5升/千克,全身清除率为370毫升/分钟。2. 多沙普仑碱肠溶胶囊在初始延迟后迅速吸收,全身可用性约为60%。3. 多沙普仑广泛代谢,静脉注射剂量的不到5%在24小时内以原形经尿液排泄。一种代谢物(AHR 5955)在血浆中的含量与母体化合物相当,且半衰期相似。4. 多沙普仑在健康志愿者和呼吸衰竭患者中的处置情况似乎相似。5. 先前认为停止输注后血浆浓度会迅速下降的观点仅在短时间输注后才成立。多沙普仑的药代动力学特性使得按照推荐的恒速输注方案,需要数小时才能达到稳态血浆浓度。

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