利用 PBPK 模型补充临床数据,支持在孕妇和哺乳期妇女中安全有效地使用多鲁曲韦。

IF 3.1 3区 医学 Q2 PHARMACOLOGY & PHARMACY
Jia Ning, Amita Pansari, Karen Rowland Yeo, Aki T. Heikkinen, Catriona Waitt, Lisa M. Almond
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引用次数: 0

摘要

孕妇和哺乳期妇女的最佳用药剂量需要了解母亲、胎儿和母乳喂养婴儿的药代动力学。基于生理学的药代动力学(PBPK)模型可用于模拟未经测试的情况,从而补充临床数据,为用药决策提供支持。利用报告的非怀孕健康志愿者、孕妇、脐带、哺乳母亲和母乳喂养新生儿的暴露量,验证了抗逆转录病毒药物多鲁曲韦(主要通过 UGT1A1 代谢)的 PBPK 模型。然后应用该模型预测 UGT1A1 表型对广泛代谢者(EM)、不良代谢者(PM)和超快速代谢者(UM)的影响。UGT1A1 PM 预测的多罗替拉韦母体血浆和脐带 AUC 是 EM 的 1.6 倍。UGT1A1 UMs 母亲的多罗替拉韦母体血浆和脐带 AUC 预测值比 EMs 母亲低 1.3 倍。无论 UGT1A1 表型如何,预测的全身和脐静脉平均浓度在 17、28 和 40 孕周都超过了多罗拉韦 IC90,这表明在妊娠晚期,无论 UGT1A1 表型如何,多罗拉韦的标准剂量(50 毫克 q.d.,喂养状态)一般都是合适的。在母乳喂养的婴儿中应用该模型,与同龄的 EM 相比,2 天大的新生儿、10 天大的新生儿和 UGT1A1 PMs 婴儿的暴露量分别高出 1.5 倍、1.7 倍和 2.2 倍。然而,需要注意的是,母乳喂养的 UGT1A1 PMs 婴儿的暴露量仍比母体暴露量低一个数量级,婴儿的相对日剂量为
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Using PBPK modeling to supplement clinical data and support the safe and effective use of dolutegravir in pregnant and lactating women

Using PBPK modeling to supplement clinical data and support the safe and effective use of dolutegravir in pregnant and lactating women

Optimal dosing in pregnant and lactating women requires an understanding of the pharmacokinetics in the mother, fetus, and breastfed infant. Physiologically-based pharmacokinetic (PBPK) modeling can be used to simulate untested scenarios and hence supplement clinical data to support dosing decisions. A PBPK model for the antiretroviral dolutegravir (mainly metabolized by UGT1A1) was verified using reported exposures in non-pregnant healthy volunteers, pregnant women, and the umbilical cord, lactating mothers, and breastfed neonates. The model was then applied to predict the impact of UGT1A1 phenotypes in extensive (EM), poor (PM), and ultra-rapid metabolizers (UM). The predicted dolutegravir maternal plasma and umbilical cord AUC in UGT1A1 PMs was 1.6-fold higher than in EMs. The predicted dolutegravir maternal plasma and umbilical cord AUC in UGT1A1 UMs mothers was 1.3-fold lower than in EMs. The predicted mean systemic and umbilical vein concentrations were in excess of the dolutegravir IC90 at 17, 28, and 40 gestational weeks, regardless of UGT1A1 phenotype, indicating that the standard dose of dolutegravir (50 mg q.d., fed state) is generally appropriate in late pregnancy, across UGT1A1 phenotypes. Applying the model in breastfed infants, a 1.5-, 1.7-, and 2.2-fold higher exposure in 2-day-old neonates, 10-day-old neonates, and infants who were UGT1A1 PMs, respectively, compared with EMs of the same age. However, it should be noted that the exposure in breastfed infants who were UGT1A1 PMs was still an order of magnitude lower than maternal exposure with a relative infant daily dose of <2%, suggesting safe use of dolutegravir in breastfeeding women.

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来源期刊
CiteScore
5.00
自引率
11.40%
发文量
146
审稿时长
8 weeks
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