人群药代动力学模型和与利福平联合使用时的多替拉韦的替代给药方案。
Population Pharmacokinetic Model and Alternative Dosing Regimens for Dolutegravir Coadministered with Rifampicin.
机构信息
Division of Clinical Pharmacology, Department of Medicine, University of Cape Towngrid.7836.a, Cape Town, South Africa.
Division of Clinical Pharmacology, Johns Hopkins University School of Medicinegrid.471401.7, Baltimore, Maryland, USA.
出版信息
Antimicrob Agents Chemother. 2022 Jun 21;66(6):e0021522. doi: 10.1128/aac.00215-22. Epub 2022 May 23.
Dolutegravir-based regimens are recommended as first-line therapy for HIV in low- and middle-income countries where tuberculosis is the most common opportunistic infection. Concurrent HIV/tuberculosis treatment is challenging because of drug-drug interactions. Our analysis aimed to characterize dolutegravir's population pharmacokinetics when coadministered with rifampicin and assess alternative dolutegravir dosing regimens. We developed a population pharmacokinetic model of dolutegravir in NONMEM with data from two healthy-volunteer studies (RADIO and ClinicalTrials.gov identifier NCT01231542) and validated it with data from the INSPIRING study, which consisted of participants living with HIV. The model was developed with 817 dolutegravir plasma concentrations from 41 participants. A 2-compartment model with first-order elimination and lagged absorption best described dolutegravir's pharmacokinetics. For a typical 70-kg individual, we estimated a clearance, absorption rate constant, central volume, and peripheral volume of 1.03 L/h, 1.61 h, 12.7 L, and 3.85 L, respectively. Rifampicin coadministration increased dolutegravir clearance by 144% (95% confidence interval [CI], 126 to 161%). Simulations showed that when 50 or 100 mg once-daily dolutegravir is coadministered with rifampicin in 70-kg individuals, 71.7% and 91.5% attain trough concentrations above 0.064 mg/L, the protein-adjusted 90% inhibitory concentration (PA-IC), respectively. The model developed from healthy-volunteer data describes patient data reasonably well but underpredicts trough concentrations. Although 50 mg of dolutegravir given twice daily achieves target concentrations in more than 99% of individuals cotreated with rifampicin, 100 mg of dolutegravir, once daily, in the same population is predicted to achieve satisfactory pharmacokinetic target attainment. The efficacy of this regimen should be investigated since it presents an opportunity for treatment simplification.
基于多替拉韦的方案被推荐作为中低收入国家中艾滋病毒的一线治疗方法,因为结核病是最常见的机会性感染。由于药物相互作用,同时治疗艾滋病毒/结核病具有挑战性。我们的分析旨在描述多替拉韦与利福平联合使用时的群体药代动力学特征,并评估替代多替拉韦给药方案。我们使用 NONMEM 中的群体药代动力学模型开发了多替拉韦的数据,该模型来自两项健康志愿者研究(RADIO 和 ClinicalTrials.gov 标识符 NCT01231542),并使用来自 INSPIRING 研究的数据进行了验证,该研究包括感染艾滋病毒的参与者。该模型是使用 41 名参与者的 817 个多替拉韦血浆浓度开发的。一个具有一阶消除和滞后吸收的两室模型最好地描述了多替拉韦的药代动力学。对于一个典型的 70 公斤个体,我们估计清除率、吸收速率常数、中央容积和外周容积分别为 1.03 L/h、1.61 h、12.7 L 和 3.85 L。利福平联合使用使多替拉韦清除率增加 144%(95%置信区间[CI],126 至 161%)。模拟表明,当 50 或 100 mg 每日一次的多替拉韦与利福平联合用于 70 公斤个体时,分别有 71.7%和 91.5%的个体达到了谷浓度超过 0.064mg/L,即蛋白校正 90%抑制浓度(PA-IC)。从健康志愿者数据中开发的模型很好地描述了患者数据,但低估了谷浓度。虽然每天两次给予 50mg 的多替拉韦在与利福平联合治疗的个体中超过 99%达到目标浓度,但在同一人群中,每天一次给予 100mg 的多替拉韦预计会达到令人满意的药代动力学目标。应该研究这种方案的疗效,因为它为简化治疗提供了机会。
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