含利匹韦林加地瑞那韦/利托那韦的核苷类药物节省双重治疗方案在初治HIV-1感染个体中的药代动力学和药效学

Pharmacokinetics and pharmacodynamics of the nucleoside sparing dual regimen containing rilpivirine plus darunavir/ritonavir in treatment-naïve HIV-1-infected individuals.

作者信息

Jackson Akil, Else Laura, Higgs Christopher, Karolia Zeenat, Khoo Saye, Back David, Devitt Emma, Pozniak Anton, Boffito Marta

机构信息

a St Stephen's Centre, Chelsea and Westminster Hospital , London , UK.

b Department of Clinical and Molecular Pharmacology , University of Liverpool , Liverpool , UK.

出版信息

HIV Clin Trials. 2018 Feb;19(1):31-37. doi: 10.1080/15284336.2017.1408928. Epub 2017 Nov 30.

DOI:10.1080/15284336.2017.1408928

PMID:29189101

Abstract

BACKGROUND

We aimed at investigating the antiviral activity and the pharmacokinetics of the dual antiretroviral (ARV) combination of rilpivirine plus darunavir/ritonavir 25/800/100 mg once-daily in naïve HIV-1-infected individuals (NHII) with different baseline viral loads.

SETTINGS

Pharmacokinetic/pharmacodynamics study in ARV-naïve HIV-infected individuals.

METHODS

The primary endpoint was the number of NHII with HIV-RNA < 40 copies/mL at week 48. Secondary endpoints included rilpivirine/darunavir/ritonavir pharmacokinetics, HIV-RNA decay, and changes in ECG QT interval.

RESULTS

Thirty-six individuals were enrolled, 18 with a baseline viral load < 100,000 copies/mL (group A) and 18 with a baseline viral load > 100,000 copies/mL (group B). All but 1 (HIV-RNA = 63 copies/mL) subjects achieved viral load < 50 copies/mL by week 36, and all at week 48. Median (range) HIV-RNA reduction (Log10 copies/mL) was 1.3 (0.6-1.9) over the first week, with no differences between groups A and B. Geometric mean and 95%CI rilpivirine C, C, AUC were 183 (165-239), 114 (104-109) ng/mL, 2966 (2704-3820) ng h/mL. No QTcF interval changes were recorded.

CONCLUSIONS

rilpivirine/darunavir/ritonavir could be efficacious, with limited short-term toxicity in ARV-naïve patients. Although rilpivirine was co-administered with ritonavir, its exposure was within ranges measured during phase III trials.

摘要

背景

我们旨在研究利匹韦林联合达芦那韦/利托那韦（25/800/100毫克，每日一次）的双重抗逆转录病毒（ARV）组合在不同基线病毒载量的初治HIV-1感染个体（NHII）中的抗病毒活性和药代动力学。

设置

在初治HIV感染个体中进行药代动力学/药效学研究。

方法

主要终点是第48周时HIV-RNA<40拷贝/毫升的NHII数量。次要终点包括利匹韦林/达芦那韦/利托那韦的药代动力学、HIV-RNA衰减以及心电图QT间期的变化。

结果

招募了36名个体，18名基线病毒载量<100,000拷贝/毫升（A组），18名基线病毒载量>100,000拷贝/毫升（B组）。除1名受试者（HIV-RNA = 63拷贝/毫升）外，所有受试者在第36周时病毒载量均<50拷贝/毫升，第48周时全部达到。第一周内HIV-RNA降低的中位数（范围）为1.3（0.6 - 1.9）log10拷贝/毫升，A组和B组之间无差异。利匹韦林的几何均值和95%CI的Cmax、Cmin、AUC分别为183（165 - 239）、114（104 - 109）纳克/毫升、2966（2704 - 3820）纳克·小时/毫升。未记录到QTcF间期变化。