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中期分析:提高药代动力学研究效率的工具:哺乳期母婴血药浓度分析。

Interim analysis, a tool to enhance efficiency of pharmacokinetic studies: Pharmacokinetics of rifampicin in lactating mother-infant pairs.

机构信息

Infectious Diseases Institute, Makerere University College of Health Sciences, Kampala, Uganda.

Department of Pharmacology and Therapeutics, Gulu University, Gulu, Uganda.

出版信息

CPT Pharmacometrics Syst Pharmacol. 2024 Nov;13(11):1915-1923. doi: 10.1002/psp4.13247. Epub 2024 Oct 2.

Abstract

Pharmacokinetic studies are important for understanding drug disposition in the human body. However, pregnant and lactating women are often excluded from primary pharmacokinetic studies and as such there is often limited dosing information regarding drug use in pregnant and/or lactating women. The objectives of this interim analysis were to define the transfer of rifampicin to a breastfed infant and to determine the area under the concentration-time curve of rifampicin in maternal plasma, breastmilk and infant plasma. Performing this interim analysis enabled us to substantiate whether prior assumptions we made on several study design issues including patient sample size and pharmacokinetic sampling times held and whether we needed to amend our protocol or not. We enrolled lactating mothers on treatment for tuberculosis with their breastfeeding infants (below 12 months of age), performed intensive pharmacokinetic sampling (0-24 h post-dose) on plasma samples from both the mother, infant(s) and breastmilk samples from the mother on two separate occasions (once during the initiation phase and another during the continuation phase of tuberculosis treatment). The initial study design, including sampling times, was informed by a stochastic simulation and estimation exercise, with very limited prior breastmilk data. An interim analysis after recruiting 6 mother-infant pairs ascertained that our initial assumptions were ideal for achieving our study objectives and no amendments to the sampling times were necessary. Initial data from 6 mother-infant pairs show that rifampicin penetrates breastmilk with an approximate milk-to-plasma ratio of 0.169 and 0.189 on two separate visits. However, it was undetectable in most infants.

摘要

药代动力学研究对于了解药物在人体中的处置非常重要。然而,孕妇和哺乳期妇女通常被排除在主要药代动力学研究之外,因此关于孕妇和/或哺乳期妇女用药的剂量信息通常有限。本中期分析的目的是确定利福平向母乳喂养婴儿的转移,并确定母体血浆、母乳和婴儿血浆中利福平的浓度-时间曲线下面积。进行这项中期分析使我们能够证实我们之前对几个研究设计问题的假设是否成立,包括患者样本量和药代动力学采样时间,以及我们是否需要修改方案。我们招募了正在接受结核病治疗的哺乳期母亲及其母乳喂养的婴儿(年龄在 12 个月以下),在两次不同的时间点(一次在结核病治疗的起始阶段,另一次在持续阶段)对母亲和婴儿的血浆样本以及母亲的母乳样本进行了密集的药代动力学采样(给药后 0-24 小时)。最初的研究设计,包括采样时间,是根据随机模拟和估计练习确定的,仅有非常有限的先前母乳数据。在招募了 6 对母婴后进行了中期分析,结果表明我们最初的假设非常适合实现我们的研究目标,不需要对采样时间进行修改。来自 6 对母婴的初步数据表明,利福平通过母乳渗透,两次单独访问的乳汁与血浆的比例约为 0.169 和 0.189。然而,它在大多数婴儿中无法检测到。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cf78/11578122/67e5c85c3f6c/PSP4-13-1915-g002.jpg

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