Mosaic HIV-1 vaccine regimen in southern African women (Imbokodo/HVTN 705/HPX2008): a randomised, double-blind, placebo-controlled, phase 2b trial.

IF 36.4 1区 医学 Q1 INFECTIOUS DISEASES Lancet Infectious Diseases Pub Date : 2024-11-01 Epub Date: 2024-07-19 DOI:10.1016/S1473-3099(24)00358-X
Glenda E Gray, Kathryn Mngadi, Ludo Lavreys, Steven Nijs, Peter B Gilbert, John Hural, Ollivier Hyrien, Michal Juraska, Alex Luedtke, Philipp Mann, M Juliana McElrath, Jackline A Odhiambo, Daniel J Stieh, Janine van Duijn, Azwidihwi N Takalani, Wouter Willems, Asa Tapley, Georgia D Tomaras, Johan Van Hoof, Hanneke Schuitemaker, Edith Swann, Dan H Barouch, James G Kublin, Lawrence Corey, Maria G Pau, Susan Buchbinder, Frank Tomaka
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引用次数: 0

Abstract

Background: HIV type 1 (HIV-1) remains a global health concern, with the greatest burden in sub-Saharan Africa. Despite 40 years of research, no vaccine candidate has shown durable and protective efficacy against HIV-1 acquisition. Although pre-exposure prophylaxis in groups with high vulnerability can be very effective, barriers to its use, such as perceived low acquisition risk, fear of stigma, and concerns about side-effects, remain. Thus, a population-based approach, such as an HIV-1 vaccine, is needed. The current study aimed to evaluate the efficacy and safety of a heterologous HIV-1 vaccine regimen, consisting of a tetravalent mosaic adenovirus 26-based vaccine (Ad26.Mos4.HIV) and aluminium phosphate-adjuvanted clade C glycoprotein (gp) 140, in young women at risk of acquiring HIV-1 in southern Africa.

Methods: This randomised, double-blind, phase 2b study enrolled sexually active women without HIV-1 or HIV-2 aged 18-35 years at 23 clinical research sites in Malawi, Mozambique, South Africa, Zambia, and Zimbabwe. Participants were centrally randomly assigned (1:1) to receive intramuscular injections of vaccine or saline placebo in stratified permuted blocks via an interactive web response system. Study participants, study site personnel (except those with primary responsibility for study vaccine preparation and dispensing), and investigators were masked to treatment group allocation. The vaccine regimen consisted of Ad26.Mos4.HIV administered at months 0 and 3 followed by Ad26.Mos4.HIV administered concurrently with aluminium phosphate-adjuvanted clade C gp140 at months 6 and 12. The primary efficacy outcome was vaccine efficacy in preventing laboratory-confirmed HIV-1 acquisition diagnosed between visits at month 7 and month 24 after the first vaccination (VE[7-24]) in the per-protocol population, which included participants who had not acquired HIV-1 4 weeks after the third vaccination, received all planned vaccinations at the first three vaccination visits within the protocol-specified windows, and had no major protocol deviations that could affect vaccine efficacy. Primary safety outcomes were assessed in randomly assigned participants who received one study injection or more based on the actual injection received. The primary safety endpoints were the incidences of unsolicited adverse events (AEs), solicited local and systemic AEs, serious AEs, AEs of special interest, and AEs leading to discontinuation of vaccination. This trial is registered with ClinicalTrials.gov, NCT03060629, and is complete.

Findings: Between Nov 3, 2017, and June 30, 2019, 2654 women were randomly assigned, of whom 2636 women (median age of 23 years [IQR 20-25]) were enrolled and received at least one study injection (1313 assigned vaccine, 1323 placebo; 1317 received vaccine, 1319 placebo). Analysis of the primary efficacy outcome in the per-protocol cohort included 1080 women in the vaccine group and 1108 women in the placebo group; the incidence of HIV-1 acquisition per 100 person-years over months 7-24 after the first vaccination was 3·38 (95% CI 2·54-4·41) in the vaccine group and 3·94 (3·04-5·03) in the placebo group, with an estimated VE(7-24) of 14·10% (95% CI -22·00 to 39·51; p=0·40). There were no serious unsolicited AEs, AEs of special interest, or deaths related to the study vaccine. In the vaccine group, 663 (50·3%) of 1317 participants had grade 1 or 2 solicited local AEs and ten (0·8%) of 1317 participants had grade 3 or 4 solicited local AEs. In the placebo group, 305 (23·1%) of 1319 participants had grade 1 or 2 solicited local AEs and three (0·2%) of 1319 participants had grade 3 or 4 solicited local AEs. 863 (65·5%) of 1317 participants in the vaccine group had grade 1 or 2 solicited systemic AEs and 34 (2·6%) of 1317 participants had grade 3 or 4 solicited systemic AEs. 763 (57·8%) of 1319 participants in the placebo group had grade 1 or 2 solicited systemic AEs and 20 (1·5%) of 1319 participants had grade 3 or 4 solicited systemic AEs. Overall, three (0·2%) of 1317 participants in the vaccine group and three (0·2%) of 1319 participants in the placebo group discontinued vaccination due to an unsolicited AE, and three (0·2%) of 1317 participants in the vaccine group and one (0·1%) of 1319 participants in the placebo group discontinued vaccination due to a solicited AE.

Interpretation: The heterologous Ad26.Mos4.HIV and clade C gp140 vaccine regimen was safe and well tolerated but did not show efficacy in preventing HIV-1 acquisition in a population of young women in southern Africa at risk of HIV-1.

Funding: Division of AIDS at the National Institute of Allergy and Infectious Diseases through the HIV Vaccine Trials Network, Bill & Melinda Gates Foundation, Janssen Vaccines & Prevention, US Army Medical Materiel Development Activity, and Ragon Institute.

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针对南部非洲妇女的 Mosaic HIV-1 疫苗疗法(Imbokodo/HVTN 705/HPX2008):一项随机、双盲、安慰剂对照的 2b 期试验。
背景:1 型艾滋病毒(HIV-1)仍然是全球关注的健康问题,撒哈拉以南非洲地区的负担最重。尽管进行了 40 年的研究,但还没有候选疫苗显示出对 HIV-1 感染具有持久的保护效力。虽然在易感人群中进行暴露前预防非常有效,但仍存在使用障碍,如认为感染风险低、害怕耻辱和担心副作用。因此,需要一种基于人群的方法,如 HIV-1 疫苗。本研究旨在评估一种异源 HIV-1 疫苗方案的有效性和安全性,该方案由基于四价镶嵌腺病毒 26 的疫苗(Ad26.Mos4.HIV)和磷酸铝佐剂的 C 支系糖蛋白(gp)140 组成,适用于南部非洲有感染 HIV-1 风险的年轻女性:这项随机、双盲、2b 期研究在马拉维、莫桑比克、南非、赞比亚和津巴布韦的 23 个临床研究机构招募了 18-35 岁未感染 HIV-1 或 HIV-2 的性活跃女性。通过交互式网络响应系统,参与者被集中随机分配(1:1)到分层排列的区块中接受肌肉注射疫苗或生理盐水安慰剂。研究参与者、研究机构人员(主要负责研究疫苗制备和分发的人员除外)和研究人员均被蒙蔽,不知道治疗组的分配情况。疫苗方案包括在第 0 个月和第 3 个月接种 Ad26.Mos4.HIV,然后在第 6 个月和第 12 个月接种 Ad26.Mos4.HIV,同时接种磷酸铝佐剂的 C 支系 gp140。主要疗效结局是疫苗在预防首次接种后第 7 个月至第 24 个月期间实验室确诊的 HIV-1 感染方面的疗效(VE[7-24]),按方案人群包括在第三次接种后 4 周未感染 HIV-1、在方案规定的窗口期内接受了前三次接种的所有计划接种、没有可能影响疫苗疗效的重大方案偏差的参与者。根据实际注射情况,对随机分配的接受一次或多次研究注射的参与者进行主要安全性结果评估。主要安全性终点是非主动性不良事件 (AE)、主动性局部和全身不良事件、严重不良事件、特别关注的不良事件以及导致停止接种的不良事件的发生率。该试验已在 ClinicalTrials.gov 注册,编号为 NCT03060629,目前已完成:2017年11月3日至2019年6月30日期间,2654名女性被随机分配,其中2636名女性(中位年龄23岁[IQR 20-25])入组并接受了至少一次研究注射(1313名分配疫苗,1323名安慰剂;1317名接受疫苗,1319名安慰剂)。按协议队列的主要疗效结果分析包括疫苗组 1080 名妇女和安慰剂组 1108 名妇女;首次接种疫苗后第 7-24 个月每百人年的 HIV-1 感染率为:疫苗组 3-38 (95% CI 2-54-4-41) ,安慰剂组 3-94 (3-04-5-03),估计 VE(7-24) 为 14-10% (95% CI -22-00 至 39-51;P=0-40)。没有发生与研究疫苗相关的严重非主动AE、特别关注AE或死亡病例。在疫苗组中,1317 名参与者中有 663 人(50-3%)出现了 1 级或 2 级主动引起的局部不良反应,1317 名参与者中有 10 人(0-8%)出现了 3 级或 4 级主动引起的局部不良反应。在安慰剂组中,1319 名参与者中有 305 名(23-1%)出现了 1 或 2 级征集到的局部 AE,1319 名参与者中有 3 名(0-2%)出现了 3 或 4 级征集到的局部 AE。在疫苗组的 1317 名参与者中,有 863 人(65-5%)出现了 1 或 2 级招致的全身性 AE,1317 名参与者中有 34 人(2-6%)出现了 3 或 4 级招致的全身性 AE。在安慰剂组的 1319 名参与者中,有 763 人(57-8%)出现了 1 级或 2 级招致的全身性 AE,有 20 人(1-5%)出现了 3 级或 4 级招致的全身性 AE。总体而言,疫苗组1317名参与者中有3名(0-2%)和安慰剂组1319名参与者中有3名(0-2%)因主动引起的AE而中止接种,疫苗组1317名参与者中有3名(0-2%)和安慰剂组1319名参与者中有1名(0-1%)因主动引起的AE而中止接种:异源Ad26.Mos4.HIV和C族gp140疫苗方案安全且耐受性良好,但在南部非洲高危年轻女性人群中预防HIV-1感染的效果并不明显:美国国立过敏与传染病研究所艾滋病处通过艾滋病疫苗试验网络、比尔及梅琳达-盖茨基金会、杨森疫苗与预防公司、美国陆军医疗材料开发活动和拉贡研究所提供。
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来源期刊
Lancet Infectious Diseases
Lancet Infectious Diseases 医学-传染病学
CiteScore
60.90
自引率
0.70%
发文量
1064
审稿时长
6-12 weeks
期刊介绍: The Lancet Infectious Diseases was launched in August, 2001, and is a lively monthly journal of original research, review, opinion, and news covering international issues relevant to clinical infectious diseases specialists worldwide.The infectious diseases journal aims to be a world-leading publication, featuring original research that advocates change or sheds light on clinical practices related to infectious diseases. The journal prioritizes articles with the potential to impact clinical practice or influence perspectives. Content covers a wide range of topics, including anti-infective therapy and immunization, bacterial, viral, fungal, and parasitic infections, emerging infectious diseases, HIV/AIDS, malaria, tuberculosis, mycobacterial infections, infection control, infectious diseases epidemiology, neglected tropical diseases, and travel medicine. Informative reviews on any subject linked to infectious diseases and human health are also welcomed.
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