Trottier Benoît, Lake Jordan E, Logue Ken, Brinson Cynthia, Santiago Lizette, Brennan Clare, Koteff Justin A, Wynne Brian, Hopking Judy, Granier Catherine, Aboud Michael
Clinique medicale l'Actuel, Montreal, QC, Canada.
UCLA Clinical AIDS Research and Education Center, University of California, Los Angeles, CA, USA.
Antivir Ther. 2017;22(4):295-305. doi: 10.3851/IMP3166. Epub 2017 Apr 12.
Simplified dosing regimens are important for patients who face challenges in adhering to HIV-1 therapy. We investigated the safety and virological efficacy of switching to once-daily abacavir/dolutegravir/lamivudine (ABC/DTG/3TC).
The STRIIVING study was a randomized, open-label, Phase IIIb study in adults with HIV-1 RNA <50 copies/ml on antiretroviral therapy (ART) at enrolment (ClinicalTrials.gov identifier, NCT02105987). Subjects were randomly assigned to switch to ABC/DTG/3TC once daily for 48 weeks (early-switch group) or continue current ART for 24 weeks and then switch to ABC/DTG/3TC (late-switch group). The primary end point was the proportion of subjects with HIV-1 RNA <50 copies/ml at week 24.
Of 553 subjects enrolled, 275 were randomly assigned to switch immediately to ABC/DTG/3TC and 278 continued on current ART. At week 24, 85% and 88% of subjects who switched to ABC/DTG/3TC or remained on current ART, respectively, were virologically suppressed, indicating that ABC/DTG/3TC was non-inferior (difference in proportion, -3.4%; 95% CI -9.1, 2.4). At week 48, 83% and 92% were virologically suppressed in the early- and late-switch groups, respectively. Adverse events were reported more frequently with ABC/DTG/3TC (66%) than with current ART (47%) by week 24, and in the late-switch group, 60% of subjects reported adverse events post-switch. Pharmacokinetic data supported immediate switch. HIV Treatment Satisfaction Questionnaire scores improved in participants switching to ABC/DTG/3TC versus current ART.
Data demonstrating non-inferiority of switching to ABC/DTG/3TC versus continuing current ART support ABC/DTG/3TC as an option when considering switch regimens in HIV-1-infected adults with stable viral suppression.
简化给药方案对于坚持接受HIV-1治疗面临挑战的患者很重要。我们调查了换用每日一次阿巴卡韦/多替拉韦/拉米夫定(ABC/DTG/3TC)的安全性和病毒学疗效。
STRIIVING研究是一项随机、开放标签的IIIb期研究,纳入了入组时接受抗逆转录病毒治疗(ART)且HIV-1 RNA<50拷贝/ml的成人(ClinicalTrials.gov标识符,NCT02105987)。受试者被随机分配为每日一次换用ABC/DTG/3TC,持续48周(早期换药组),或继续当前ART治疗24周,然后换用ABC/DTG/3TC(晚期换药组)。主要终点是第24周时HIV-1 RNA<50拷贝/ml的受试者比例。
在纳入的553名受试者中,275名被随机分配立即换用ABC/DTG/3TC,278名继续接受当前ART治疗。在第24周时,换用ABC/DTG/3TC或继续接受当前ART治疗的受试者中,分别有85%和88%实现了病毒学抑制,这表明ABC/DTG/3TC不差于当前治疗(比例差异为-3.4%;95%CI -9.1,2.4)。在第48周时,早期换药组和晚期换药组分别有83%和92%实现了病毒学抑制。到第24周时,报告ABC/DTG/3TC组不良事件的频率(66%)高于当前ART治疗组(),在晚期换药组中,60%的受试者在换药后报告了不良事件。药代动力学数据支持立即换药。与当前ART治疗相比,换用ABC/DTG/3TC的参与者的HIV治疗满意度问卷得分有所提高。
数据表明,与继续当前ART治疗相比,换用ABC/DTG/3TC不差,这支持在考虑为病毒抑制稳定的HIV-1感染成人更换治疗方案时,ABC/DTG/3TC可作为一种选择。
