Ideal Time to Conduct a Pharmacokinetic Investigation After Delivery to Fully Capture the Effect of Pregnancy on Drug Exposure.

IF 3.8 4区 医学 Q2 IMMUNOLOGY
Open Forum Infectious Diseases Pub Date : 2024-10-15 eCollection Date: 2024-10-01 DOI:10.1093/ofid/ofae585
Mattia Berton, Felix Stader, Sara Bettonte, Manuel Battegay, Catia Marzolini
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引用次数: 0

Abstract

Background: The World Health Organization is pushing to accelerate the study of new human immunodeficiency virus drugs in pregnant women. However, regulatory guidelines do not specify when to conduct pharmacokinetic studies in postpartum women. This knowledge gap carries the potential to jeopardize the outcomes and conclusions of clinical trials aiming to study the effect of pregnancy on drug exposure. We used physiologically based pharmacokinetic (PBPK) modeling along with clinical data to determine the time needed after delivery for drug exposure to return to prepregnancy levels.

Methods: A literature review was conducted to collect physiological parameters of pregnant and postpartum women. Regression analyses were performed to derive equations describing the parameters trajectory throughout pregnancy and post partum to inform our PBPK model. Published pharmacokinetic data in pregnant and postpartum women were used for the model verification. The PBPK model was subsequently applied to investigate pharmacokinetic changes throughout pregnancy and post partum.

Results: In agreement with the clinical data the PBPK model was able to describe the different effects of pregnancy on drug exposure, with bictegravir showing the largest reduction in exposure (approximately 50%) during the third trimester while ritonavir and raltegravir showing the lowest (approximately 30%). The successfully verified PBPK model predicted that all evaluated antiretrovirals mostly return to prepregnancy exposure 4 weeks after delivery.

Conclusions: Pharmacokinetic investigations on hepatically cleared drugs should not be conducted before the fifth week after delivery to fully characterize the effect of pregnancy on drug exposure. Because physiological changes remain after delivery, early measurements can underestimate the pregnancy effect on pharmacokinetics, leading to suboptimal dosing recommendations during pregnancy.

产后进行药代动力学调查的理想时间,以充分捕捉妊娠对药物暴露的影响。
背景:世界卫生组织正在推动加快在孕妇中研究新的人类免疫缺陷病毒药物。然而,监管指南并未明确规定何时对产后妇女进行药代动力学研究。这一知识空白有可能危及旨在研究妊娠对药物暴露影响的临床试验的结果和结论。我们利用基于生理学的药代动力学(PBPK)模型和临床数据来确定产后药物暴露恢复到孕前水平所需的时间:方法:通过文献回顾收集孕妇和产后妇女的生理参数。进行回归分析,得出描述整个孕期和产后参数轨迹的方程,为我们的 PBPK 模型提供依据。已发表的孕妇和产后妇女药代动力学数据被用于模型验证。PBPK 模型随后被用于研究整个孕期和产后的药代动力学变化:结果:与临床数据一致,PBPK 模型能够描述妊娠对药物暴露量的不同影响,其中比特拉韦在妊娠三个月期间的暴露量减少最多(约 50%),而利托那韦和拉替拉韦的暴露量减少最少(约 30%)。经成功验证的 PBPK 模型预测,所有评估的抗逆转录病毒药物在分娩 4 周后大多会恢复到孕前的暴露量:结论:为全面了解妊娠对药物暴露的影响,不应在产后第五周之前对肝脏清除药物进行药代动力学研究。由于分娩后生理变化依然存在,早期测量可能会低估妊娠对药物代谢动力学的影响,从而导致在妊娠期间提出次优用药建议。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Open Forum Infectious Diseases
Open Forum Infectious Diseases Medicine-Neurology (clinical)
CiteScore
6.70
自引率
4.80%
发文量
630
审稿时长
9 weeks
期刊介绍: Open Forum Infectious Diseases provides a global forum for the publication of clinical, translational, and basic research findings in a fully open access, online journal environment. The journal reflects the broad diversity of the field of infectious diseases, and focuses on the intersection of biomedical science and clinical practice, with a particular emphasis on knowledge that holds the potential to improve patient care in populations around the world. Fully peer-reviewed, OFID supports the international community of infectious diseases experts by providing a venue for articles that further the understanding of all aspects of infectious diseases.
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