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使用葡萄糖酸锑钠或葡甲胺锑酸盐治疗内脏利什曼病期间锑的药代动力学。

Pharmacokinetics of antimony during treatment of visceral leishmaniasis with sodium stibogluconate or meglumine antimoniate.

作者信息

Chulay J D, Fleckenstein L, Smith D H

机构信息

Department of Immunology, Walter Reed Army Institute of Research, Washington, DC.

出版信息

Trans R Soc Trop Med Hyg. 1988;82(1):69-72.

PMID:2845611
Abstract

5 patients with visceral leishmaniasis were treated with sodium stibogluconate (2 patients) or meglumine antimoniate (3 patients) given intramuscularly at a dose of 10 mg antimony (Sb) per kg body weight daily for 30 d. Blood samples were obtained at intervals during treatment and blood Sb concentrations measured by anodic stripping voltametry. The pharmacokinetics of both drugs were remarkably similar, with peak concentrations of approximately 10 mg/litre occurring 2 h after the initial dose. Most of the Sb was eliminated rapidly, but nadir Sb concentrations increased gradually during treatment from 0.04-0.08 mg/litre 24 h after the first dose to 0.19-0.33 mg/litre 24 h after the 30th dose. For both drugs, the data were best described by a two compartment, three term pharmacokinetic model representing an initial absorption phase with a mean half-life of 0.85 h, a rapid elimination phase with a mean half-life of 2.02 h, and a slow elimination phase with a mean half-life of 76 h. The slow terminal elimination phase may be related to in vivo conversion of pentavalent Sb to trivalent Sb, which could contribute to the toxicity associated with long-term high dose therapy.

摘要

5例内脏利什曼病患者接受了葡萄糖酸锑钠(2例)或葡甲胺锑酸盐(3例)治疗,每日按每千克体重10毫克锑(Sb)的剂量肌肉注射,持续30天。在治疗期间定期采集血样,并通过阳极溶出伏安法测量血锑浓度。两种药物的药代动力学非常相似,初始剂量后2小时出现的峰值浓度约为10毫克/升。大部分锑迅速消除,但治疗期间最低点锑浓度从首次给药后24小时的0.04 - 0.08毫克/升逐渐增加到第30次给药后24小时的0.19 - 0.33毫克/升。对于两种药物,数据最好用二室、三参数药代动力学模型来描述,该模型代表一个初始吸收期,平均半衰期为0.85小时,一个快速消除期,平均半衰期为2.02小时,以及一个缓慢消除期,平均半衰期为76小时。缓慢的终末消除期可能与五价锑在体内转化为三价锑有关,这可能导致与长期高剂量治疗相关的毒性。

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