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胺碘酮在大鼠小肠中的肠道吸收动力学

Intestinal absorption kinetics of amiodarone in rat small intestine.

作者信息

Martín-Algarra R V, Pascual-Costa R M, Merino M, Casabó V G

机构信息

Departamento de Farmacia y Tecnologia Farmacéutica, Facultad de Farmacia, Universidad de Valencia, Spain.

出版信息

Biopharm Drug Dispos. 1997 Aug;18(6):523-32. doi: 10.1002/(sici)1099-081x(199708)18:6<523::aid-bdd39>3.0.co;2-2.

Abstract

Amiodarone is a widely used antiarrhythmic agent with highly variable therapeutic effects. These seem to be related, at least in part, to the pharmacokinetics of the drug and particularly to some features of its gastrointestinal absorption process. The drug exhibits physico-chemical properties highly suitable for diffusion across lipophilic absorbing membranes, but its low aqueous solubility can act as the rate limiting step for absorption, making the process erratic and variable. In order to gain an insight into the intestinal absorption mechanism of the drug and detect possible non-linearities, a series of experiments using a classical rat gut in situ preparation were carried out with three amiodarone hydrochloride solutions (10, 75, and 200 micrograms mL-1). A synthetic non-ionic surfactant, polysorbate 80, at supramicellar concentration (2 mM) was used as the drug solubilizer. Amiodarone was assayed in biological samples by HPLC using a rapid, sensitive technique that was validated. The amiodarone first-order absorption rate constants obtained in these conditions were similar. No significant differences between ka values were found. Amiodarone absorption was clearly identified as a passive diffusion process.

摘要

胺碘酮是一种广泛使用的抗心律失常药物,其治疗效果差异很大。这些差异似乎至少部分与药物的药代动力学有关,特别是与其胃肠道吸收过程的某些特征有关。该药物具有非常适合跨亲脂性吸收膜扩散的物理化学性质,但其低水溶性可能成为吸收的限速步骤,导致吸收过程不稳定且可变。为了深入了解该药物的肠道吸收机制并检测可能的非线性,使用经典的大鼠肠道原位制备方法,对三种盐酸胺碘酮溶液(10、75和200微克/毫升)进行了一系列实验。一种超胶束浓度(2 mM)的合成非离子表面活性剂聚山梨酯80用作药物增溶剂。通过高效液相色谱法(HPLC)使用经过验证的快速、灵敏技术对生物样品中的胺碘酮进行测定。在这些条件下获得的胺碘酮一级吸收速率常数相似。ka值之间未发现显著差异。胺碘酮的吸收被明确确定为被动扩散过程。

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