SWORD-1/-2 期 3 项研究中多替拉韦/利匹韦林二药方案的药代动力学和药代动力学/药效学特征。
Pharmacokinetic and pharmacokinetic/pharmacodynamic characterization of the dolutegravir/rilpivirine two-drug regimen in SWORD-1/-2 phase 3 studies.
机构信息
GSK, Durham, North Carolina, USA.
GSK, Upper Providence, Pennsylvania, USA.
出版信息
Br J Clin Pharmacol. 2023 Jul;89(7):2190-2200. doi: 10.1111/bcp.15683. Epub 2023 Mar 1.
AIM
SWORD-1 and SWORD-2 phase 3 studies concluded that switching virologically suppressed participants with HIV-1 from their current three- or four-drug antiretroviral regimen (CAR) to the two-drug regimen of once-daily dolutegravir (DTG, 50 mg) and rilpivirine (RPV, 25 mg) was safe, well tolerated and noninferior for maintaining HIV-1 suppression at week 48 and highly efficacious to week 148. A secondary objective was to characterize drug exposure and exposure-efficacy/safety relationships.
METHODS
Adults with plasma HIV-1 RNA <50 copies/mL were randomized to switch to once-daily DTG + RPV on day 1 or to continue CAR for 52 weeks before switching. Trough plasma concentrations (C0) of DTG and RPV, the proportion of participants with HIV-1 RNA <50 copies/mL and adverse events to week 100 were summarized and subjected to exposure-response analyses in the overall population, in the subset of participants who switched from CAR containing enzyme-inducing drugs and by age category (≥50 and <50 years). The relationship between C0avg (individual average C0 across visits) and efficacy/safety was investigated.
RESULTS
Although week 2 DTG and RPV C0 were lower in participants switching from enzyme-inducing antiretroviral drugs, C0 and C0avg stayed above in vitro antiviral protein binding-adjusted IC90 and to week 100 with viral suppression >89%. DTG or RPV C0avg showed no relationship with virologic failures or safety. Participants ≥50 years had similar C0avg and safety response to younger participants.
CONCLUSION
No clinically relevant relationship between DTG or RPV exposures and virologic or safety response was observed, confirming the DTG + RPV switch for participants as a safe and effective treatment.
目的
SWORD-1 和 SWORD-2 三期研究得出结论,将病毒学抑制的 HIV-1 患者从目前的三或四药物抗逆转录病毒治疗方案(CAR)转换为每日一次的多替拉韦(DTG,50mg)和利匹韦林(RPV,25mg)的两药方案是安全的,耐受性良好,在第 48 周维持 HIV-1 抑制的非劣效性,并且在第 148 周具有高度疗效。次要目标是描述药物暴露和暴露-疗效/安全性关系。
方法
血浆 HIV-1 RNA<50 拷贝/mL 的成年人随机分为第 1 天转换为每日一次 DTG+RPV 或在转换前继续 CAR 治疗 52 周。总结了 DTG 和 RPV 的谷血浆浓度(C0)、第 100 周时 HIV-1 RNA<50 拷贝/mL 的参与者比例和不良事件,并在总体人群、从包含酶诱导药物的 CAR 转换的参与者亚组以及年龄类别(≥50 岁和<50 岁)中进行了暴露-反应分析。研究了 C0avg(个体在访问中的平均 C0)与疗效/安全性的关系。
结果
尽管从酶诱导抗逆转录病毒药物转换的参与者在第 2 周 DTG 和 RPV 的 C0 较低,但 C0 和 C0avg 在体外抗病毒蛋白结合调整的 IC90 以上保持,并且在第 100 周时病毒抑制率>89%。DTG 或 RPV C0avg 与病毒学失败或安全性无关。≥50 岁的参与者与年轻参与者具有相似的 C0avg 和安全性反应。
结论
未观察到 DTG 或 RPV 暴露与病毒学或安全性反应之间存在临床相关关系,证实了 DTG+RPV 转换为参与者提供了一种安全有效的治疗方法。
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