Dravid Ameet, Morkar Dnyanesh, Prasad Dwijendra, Ramapuram John T, Patel Kartik Vikrambhai, Naik K Sunil, Bhrusundi Milind, Kulkarni Milind, Hegde Sanjeev, Anuradha S, Nageswaramma Siddabathuni, Madan Surabhi, Jayaprakash Thammisetty, Kulkarni Vinay
Department of Infectious Diseases and Clinical Research, Poona Hospital and Research Centre, Pune, Maharashtra, India.
Department of Medicine, KLE's Dr Prabhakar Kore Hospital and MRC, Belagavi, Karnataka, India.
Pragmat Obs Res. 2022 Aug 10;13:75-84. doi: 10.2147/POR.S361907. eCollection 2022.
WHO recommends dolutegravir (DTG) based regimens as first-line treatment for HIV-1 infection. However, few studies have been conducted in Indian population. Hence, our study evaluated the safety, tolerability, and efficacy of DTG 50 mg with Tenofovir and Lamivudine (300/300mg) fixed dose combination in treatment naïve adult Indian patients.
This was an open label, multicenter, prospective, interventional, phase IV study conducted across 14 sites between February 2019 and July 2020. 24 weeks was the treatment duration for each subject. The primary end point was to assess the incidence of adverse events (AEs) and secondary end points were to assess the proportion of patients achieving plasma HIV-1 RNA levels <50 copies/mL at week 24 and change in CD4+ cell count from the baseline. Safety analysis was conducted using Safety Analysis Set and efficacy analysis was carried out using Full Analysis Set and Per protocol set.
A total of 288 patients were screened; 250 were enrolled; and 229 completed the study. 389 AEs were reported from 58% of patients. Of these, 61 were related to study treatment. One event of decreased creatinine clearance led to study discontinuation. One serious event of pyrexia was reported, which was unrelated to the study drug. The most common AEs were headache (18%), pyrexia (14%), vomiting (6.4%) and upper respiratory tract infections (6%). No deaths were reported. At week 24, 86.8% of the patients achieved plasma HIV-1 RNA levels <50 copies/mL and the mean CD4 cell count increased from 350.2 (SD, 239.73) at baseline to 494.6 (SD, 261.40) with an average increase of 143.2 (SD, 226.14) cells.
This study demonstrated the safety and efficacy of DTG based regimen in treatment naïve HIV-1 patients in Indian population and support use of DTG as first-line treatment regimen.
世界卫生组织推荐以多替拉韦(DTG)为基础的治疗方案作为HIV-1感染的一线治疗方案。然而,针对印度人群开展的研究较少。因此,我们的研究评估了DTG 50毫克与替诺福韦和拉米夫定(300/300毫克)固定剂量组合在初治成年印度患者中的安全性、耐受性和疗效。
这是一项开放标签、多中心、前瞻性、干预性的IV期研究,于2019年2月至2020年7月在14个地点进行。每位受试者的治疗时长为24周。主要终点是评估不良事件(AE)的发生率,次要终点是评估在第24周时血浆HIV-1 RNA水平<50拷贝/毫升的患者比例以及CD4+细胞计数相对于基线的变化。使用安全性分析集进行安全性分析,使用全分析集和符合方案集进行疗效分析。
共筛查了288名患者;250名患者入组;229名患者完成了研究。58%的患者报告了389起不良事件。其中,61起与研究治疗相关。1例肌酐清除率下降事件导致研究中断。报告了1例严重发热事件,与研究药物无关。最常见的不良事件是头痛(18%)、发热(14%)、呕吐(6.4%)和上呼吸道感染(6 %)。未报告死亡病例。在第24周时,86.8%的患者血浆HIV-1 RNA水平<50拷贝/毫升,CD4细胞计数的平均值从基线时的350.2(标准差,239.73)增至494.6(标准差,261.40),平均增加了143.2(标准差,226.14)个细胞。
本研究证明了以DTG为基础的治疗方案在印度初治HIV-1患者中的安全性和疗效,并支持将DTG用作一线治疗方案。
