简短报告：在DRIVE - AHEAD和DRIVE - FORWARD试验的开放标签扩展研究中，转换为基于多拉韦林的治疗方案后神经精神不良事件的缓解情况

Brief Report: Resolution of Neuropsychiatric Adverse Events After Switching to a Doravirine-Based Regimen in the Open-Label Extensions of the DRIVE-AHEAD and DRIVE-FORWARD Trials.

作者信息

Moyle Graeme, Meng Fanxia, Wan Hong, Sklar Peter, Plank Rebeca M, Lahoulou Rima

机构信息

Chelsea & Westminster Hospital, London, United Kingdom.

Merck & Co., Inc., Rahway, NJ; and.

出版信息

J Acquir Immune Defic Syndr. 2025 May 1;99(1):81-86. doi: 10.1097/QAI.0000000000003599.

DOI:10.1097/QAI.0000000000003599

PMID:39748155

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11970612/

Abstract

BACKGROUND

Neuropsychiatric adverse events (NPAEs) are associated with several antiretrovirals. Doravirine (DOR), a non-nucleoside reverse transcriptase inhibitor indicated for HIV-1 treatment, does not interact significantly with known neurotransmitter receptors in vitro. First-line therapy with DOR-based regimens resulted in significantly fewer NPAEs than efavirenz/emtricitabine/tenofovir disoproxil fumarate (EFV/FTC/TDF) and similar rates to those of ritonavir-boosted darunavir (DRV/r) with 2 nucleos(t)ide reverse transcriptase inhibitors (NRTIs) through week 96 of the phase 3 DRIVE-AHEAD and DRIVE-FORWARD studies, respectively.

METHODS

In the DRIVE-AHEAD (NCT02403674) and DRIVE-FORWARD studies (NCT02275780), treatment-naive adults randomly received DOR/lamivudine/TDF or EFV/FTC/TDF and DOR + 2 NRTIs or DRV/r + 2 NRTIs, respectively, for a 96-week double-blind phase; afterward, participants could continue or switch to a DOR-based regimen for a 96-week open-label extension.

RESULTS

Overall, 269 and 233 participants in the DRIVE-AHEAD and DRIVE-FORWARD studies, respectively, switched to a DOR-based regimen. At week 96, 26 and 15 participants randomized to EFV/FTC/TDF and DRV/r + 2 NRTIs, respectively, had ongoing NPAEs, resolving by week 192 in 73% (19/26) and 40% (6/15) of participants switching to a DOR-based regimen. New-onset NPAEs were reported by 9% (25/269) and 8% (18/233) of participants; by week 192, new-onset NPAEs were resolved and/or resolving in 60% (15/25) and 61% (11/18) of participants.

CONCLUSIONS

In both trial extensions, NPAEs persisted in 3%-4% of participants 96 weeks after switching to a DOR-based regimen, possibly representing the background rate for these events. This suggests that DOR-based therapy may be a good option for adults with baseline neuropsychiatric symptoms or those experiencing NPAEs with other antiretrovirals.

摘要

背景

神经精神不良事件（NPAEs）与多种抗逆转录病毒药物相关。多拉韦林（DOR）是一种用于治疗HIV-1的非核苷类逆转录酶抑制剂，在体外与已知神经递质受体无明显相互作用。在3期DRIVE-AHEAD和DRIVE-FORWARD研究的第96周，基于DOR的一线治疗方案导致的NPAEs明显少于依非韦伦/恩曲他滨/替诺福韦酯（EFV/FTC/TDF），且与含两种核苷类逆转录酶抑制剂（NRTIs）的利托那韦增强达芦那韦（DRV/r）的发生率相似。

方法

在DRIVE-AHEAD（NCT02403674）和DRIVE-FORWARD研究（NCT02275780）中，初治成人分别随机接受DOR/拉米夫定/TDF或EFV/FTC/TDF以及DOR + 2种NRTIs或DRV/r + 2种NRTIs，进行为期96周的双盲阶段治疗；之后，参与者可继续或改用基于DOR的方案进行为期96周的开放标签扩展治疗。

结果

总体而言，DRIVE-AHEAD和DRIVE-FORWARD研究中分别有269名和233名参与者改用基于DOR的方案。在第96周时，分别随机接受EFV/FTC/TDF和DRV/r + 2种NRTIs治疗的26名和15名参与者仍有持续性NPAEs，在改用基于DOR的方案的参与者中，分别有73%（19/26）和40%（6/15）的人在第192周时症状缓解。改用基于DOR的方案的参与者中分别有9%（25/269）和8%（18/233）报告了新发NPAEs；到第192周时，新发NPAEs在60%（15/25）和61%（11/18）的参与者中得到缓解和/或正在缓解。