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Development of an intravaginal ring delivering simultaneously anastrozole and levonorgestrel: a pharmacokinetic perspective

机译:同时递送阿那曲唑和左炔诺孕酮的阴道内环的开发:药代动力学的观点

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Intravaginal rings (IVRs) are an option for continuous administration of drugs in women. As an attractive approach for the treatment of endometriosis-associated pelvic pain, IVRs delivering a combination of the aromatase inhibitor anastrozole (ATZ) and the progestin levonorgestrel (LNG) have been developed. This article describes the developmental pharmacokinetic (PK) aspects covering the characterization of in vitro release, preclinical IVR PK investigations in monkeys, and clinical PK considerations. An IVR for ATZ has been developed and investigated in healthy menstruating female cynomolgus monkeys showing effective in vivo release. PK data from the size-adapted IVR used in these animals can be translated into a human context as confirmed in human studies where predefined exposure levels of ATZ were reached. As ATZ may cause harm to the fetus, use of effective contraception has to be assured in women of childbearing potential. Therefore, the IVR delivers a low dose of LNG as a contraceptive. Although the daily dose differed strongly between both drugs (20?μg LNG/d to 1?mg ATZ/d), simultaneous delivery of ATZ and LNG in vitro and in vivo was observed with a high correlation between the in vitro release and PK profiles. The PK characteristics successfully guided the design of clinical studies investigating the drug-drug interaction (DDI) potential. No relevant DDI between both the investigated or other vaginally administered drugs were identified.
机译:阴道环(IVR)是女性连续给药的一种选择。作为治疗子宫内膜异位症相关盆腔痛的一种有吸引力的方法,已开发出结合芳香酶抑制剂阿那曲唑(ATZ)和孕激素左炔诺孕酮(LNG)的IVR。本文介绍了发展药代动力学(PK)方面,包括体外释放的特征,猴子的临床前IVR PK研究以及临床PK注意事项。已经开发了用于ATZ的IVR,并在月经期健康的雌性食蟹猕猴中进行了研究,并显示了有效的体内释放。这些动物中使用的适应大小IVR的PK数据可以转化为人类环境,这在人体研究中得到了证实,其中达到了预定的ATZ暴露水平。由于ATZ可能会对胎儿造成伤害,因此必须确保有生育能力的妇女使用有效的避孕措施。因此,IVR提供低剂量的LNG作为避孕药。尽管两种药物之间的日剂量差异很大(20?μgLNG / d至> 1?mg ATZ / d),但观察到ATZ和LNG在体内和体外同时递送,在体外释放与PK之间具有高度相关性个人资料。 PK特性成功地指导了研究药物-药物相互作用(DDI)潜力的临床研究的设计。在研究或其他经阴道给药的药物之间均未发现相关的DDI。

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