Efficacy and safety of Butantan-DV in participants aged 2-59 years through an extended follow-up: results from a double-blind, randomised, placebo-controlled, phase 3, multicentre trial in Brazil.

IF 36.4 1区 医学 Q1 INFECTIOUS DISEASES Lancet Infectious Diseases Pub Date : 2024-11-01 Epub Date: 2024-08-05 DOI:10.1016/S1473-3099(24)00376-1
Mauricio L Nogueira, Monica A T Cintra, José A Moreira, Elizabeth G Patiño, Patricia Emilia Braga, Juliana C V Tenório, Lucas Bassolli de Oliveira Alves, Vanessa Infante, Daniela Haydee Ramos Silveira, Marcus Vínicius Guimarães de Lacerda, Dhelio Batista Pereira, Allex Jardim da Fonseca, Ricardo Queiroz Gurgel, Ivo Castelo-Branco Coelho, Cor Jesus Fernandes Fontes, Ernesto T A Marques, Gustavo Adolfo Sierra Romero, Mauro Martins Teixeira, André M Siqueira, Viviane Sampaio Boaventura, Fabiano Ramos, Erivaldo Elias Júnior, José Cassio de Moraes, Stephen S Whitehead, Alejandra Esteves-Jaramillo, Tulin Shekar, Jung-Jin Lee, Julieta Macey, Sabrina Gozlan Kelner, Beth-Ann G Coller, Fernanda Castro Boulos, Esper G Kallás
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We assessed the safety and efficacy of the live, attenuated, tetravalent Butantan-dengue vaccine (Butantan-DV) in adults, adolescents, and children. We previously reported the primary and secondary efficacy and safety endpoints in the initial 2 years of follow-up. Here we report the results through an extended follow-up period, with an average of 3·7 years of follow-up.</p><p><strong>Methods: </strong>In this double-blind, randomised, placebo-controlled, phase 3, multicentre trial in Brazil, healthy participants (aged 2-59 years) who had not previously received a dengue vaccine were enrolled and randomly assigned 2:1 (stratified by age 18-59 years, 7-17 years, and 2-6 years) using a central electronic randomisation system to receive 0·5 mL of Butantan-DV (containing approximately 10<sup>3</sup> plaque-forming units of each of the four vaccine virus strains) or placebo, administered subcutaneously. Syringes containing vaccine or placebo were prepared by an unmasked trial pharmacist who was not involved in any subsequent participant assessments; other site staff and the participants remained unaware of the group allocations. Vaccine efficacy was calculated with the accrual of virologically confirmed dengue (VCD) cases (by RT-PCR) at least 28 days after vaccination up until the cutoff (at least 2 years of follow-up from the last participant enrolled). The primary endpoint was vaccine efficacy against VCD after day 28 by any dengue virus (DENV) serotype regardless of dengue serostatus at baseline in the per-protocol population. The primary and secondary safety endpoints up until day 21 were previously reported; secondary safety endpoints include the frequency of unsolicited vaccine-related adverse events after day 22. Safety analyses were done on all participants as treated. This trial is registered with ClinicalTrials.gov (NCT02406729) and is ongoing.</p><p><strong>Findings: </strong>Of 16 363 participants assessed for eligibility, 16 235 were randomly assigned between Feb 22, 2016, and July 5, 2019, and received single-dose Butantan-DV (10 259 participants) or placebo (5976 participants). 16 162 participants (Butantan-DV n=10 215; placebo n=5947) were included in the per-protocol population and 16 235 (Butantan-DV n=10 259; placebo n=5976) in the safety population. At the data cutoff (July 13, 2021), participants had 2-5 years of follow-up (mean 3·7 years [SD 1·0], median 4·0 years [IQR 3·2-4·5]). 356 VCD cases were captured through the follow-up (128 in the vaccine group and 228 in the placebo group). Vaccine efficacy against VCD caused by any DENV serotype was 67·3% (95% CI 59·4-73·9); cases caused by DENV-3 or DENV-4 were not observed. The proportions of participants who had serious adverse events were similar between treatment groups (637 [6·2%] in the vaccine group and 395 [6·6%] in the placebo group) up until the cutoff.</p><p><strong>Interpretation: </strong>A single dose of Butantan-DV was generally well tolerated and efficacious against symptomatic VCD (caused by DENV-1 and DENV-2) for a mean of 3·7 years. These findings support the continued development of Butantan-DV to prevent dengue disease in children, adolescents, and adults regardless of dengue serostatus.</p><p><strong>Funding: </strong>Instituto Butantan and Merck Sharp & Dohme LLC, a subsidiary of Merck & Co.</p><p><strong>Translations: </strong>For the Spanish and Portuguese translations of the abstract see Supplementary Materials section.</p>","PeriodicalId":49923,"journal":{"name":"Lancet Infectious Diseases","volume":" ","pages":"1234-1244"},"PeriodicalIF":36.4000,"publicationDate":"2024-11-01","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"Lancet Infectious Diseases","FirstCategoryId":"3","ListUrlMain":"https://doi.org/10.1016/S1473-3099(24)00376-1","RegionNum":1,"RegionCategory":"医学","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"2024/8/5 0:00:00","PubModel":"Epub","JCR":"Q1","JCRName":"INFECTIOUS DISEASES","Score":null,"Total":0}
引用次数: 0

Abstract

Background: A single-dose dengue vaccine that protects individuals across a wide age range and regardless of dengue serostatus is an unmet need. We assessed the safety and efficacy of the live, attenuated, tetravalent Butantan-dengue vaccine (Butantan-DV) in adults, adolescents, and children. We previously reported the primary and secondary efficacy and safety endpoints in the initial 2 years of follow-up. Here we report the results through an extended follow-up period, with an average of 3·7 years of follow-up.

Methods: In this double-blind, randomised, placebo-controlled, phase 3, multicentre trial in Brazil, healthy participants (aged 2-59 years) who had not previously received a dengue vaccine were enrolled and randomly assigned 2:1 (stratified by age 18-59 years, 7-17 years, and 2-6 years) using a central electronic randomisation system to receive 0·5 mL of Butantan-DV (containing approximately 103 plaque-forming units of each of the four vaccine virus strains) or placebo, administered subcutaneously. Syringes containing vaccine or placebo were prepared by an unmasked trial pharmacist who was not involved in any subsequent participant assessments; other site staff and the participants remained unaware of the group allocations. Vaccine efficacy was calculated with the accrual of virologically confirmed dengue (VCD) cases (by RT-PCR) at least 28 days after vaccination up until the cutoff (at least 2 years of follow-up from the last participant enrolled). The primary endpoint was vaccine efficacy against VCD after day 28 by any dengue virus (DENV) serotype regardless of dengue serostatus at baseline in the per-protocol population. The primary and secondary safety endpoints up until day 21 were previously reported; secondary safety endpoints include the frequency of unsolicited vaccine-related adverse events after day 22. Safety analyses were done on all participants as treated. This trial is registered with ClinicalTrials.gov (NCT02406729) and is ongoing.

Findings: Of 16 363 participants assessed for eligibility, 16 235 were randomly assigned between Feb 22, 2016, and July 5, 2019, and received single-dose Butantan-DV (10 259 participants) or placebo (5976 participants). 16 162 participants (Butantan-DV n=10 215; placebo n=5947) were included in the per-protocol population and 16 235 (Butantan-DV n=10 259; placebo n=5976) in the safety population. At the data cutoff (July 13, 2021), participants had 2-5 years of follow-up (mean 3·7 years [SD 1·0], median 4·0 years [IQR 3·2-4·5]). 356 VCD cases were captured through the follow-up (128 in the vaccine group and 228 in the placebo group). Vaccine efficacy against VCD caused by any DENV serotype was 67·3% (95% CI 59·4-73·9); cases caused by DENV-3 or DENV-4 were not observed. The proportions of participants who had serious adverse events were similar between treatment groups (637 [6·2%] in the vaccine group and 395 [6·6%] in the placebo group) up until the cutoff.

Interpretation: A single dose of Butantan-DV was generally well tolerated and efficacious against symptomatic VCD (caused by DENV-1 and DENV-2) for a mean of 3·7 years. These findings support the continued development of Butantan-DV to prevent dengue disease in children, adolescents, and adults regardless of dengue serostatus.

Funding: Instituto Butantan and Merck Sharp & Dohme LLC, a subsidiary of Merck & Co.

Translations: For the Spanish and Portuguese translations of the abstract see Supplementary Materials section.

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在巴西进行的一项双盲、随机、安慰剂对照、第 3 期多中心试验的结果。
背景:目前还没有一种单剂量登革热疫苗能够保护不同年龄段的人,无论其登革热血清状态如何。我们评估了四价布坦坦登革热减毒活疫苗(Butantan-DV)在成人、青少年和儿童中的安全性和有效性。我们之前报告了最初两年随访的主要和次要疗效和安全性终点。在此,我们报告了延长随访期(平均随访 3-7 年)后的结果:在巴西进行的这项双盲、随机、安慰剂对照的第 3 期多中心试验中,既往未接种过登革热疫苗的健康参与者(2-59 岁)被纳入试验,并通过中央电子随机系统以 2:1 的比例随机分配(按 18-59 岁、7-17 岁和 2-6 岁分层)接受 0-5 mL 的 Butantan-DV(含有四种疫苗病毒株中每种约 103 个斑块形成单位)或安慰剂皮下注射。装有疫苗或安慰剂的注射器由一名未蒙面的试验药剂师准备,该药剂师不参与任何后续的参与者评估;其他现场工作人员和参与者对组别分配一无所知。疫苗疗效的计算以接种后至少 28 天出现病毒学确诊登革热 (VCD) 病例(通过 RT-PCR 检测)为依据,直至截止日期(从最后一名参与者开始至少随访 2 年)。主要终点是疫苗对第28天后任何登革热病毒(DENV)血清型登革热病例的疗效,无论按协议人群基线时的登革热血清状态如何。截至第 21 天的主要和次要安全性终点先前已有报告;次要安全性终点包括第 22 天后主动发生的疫苗相关不良事件的频率。安全性分析针对所有接受治疗的参与者。该试验已在 ClinicalTrials.gov (NCT02406729) 注册,目前仍在进行中:在接受资格评估的16 363名参与者中,有16 235人在2016年2月22日至2019年7月5日期间被随机分配,接受单剂量布坦坦-DV(10 259人)或安慰剂(5 976人)治疗。162名参与者(Butantan-DV n=10 215;安慰剂 n=5947)被纳入按协议人群,16 235名参与者(Butantan-DV n=10 259;安慰剂 n=5976)被纳入安全性人群。截至数据截止日(2021 年 7 月 13 日),参与者的随访时间为 2-5 年(平均 3-7 年 [SD 1-0],中位数 4-0 年 [IQR 3-2-4-5])。随访期间共发现 356 例血管性脑损伤病例(疫苗组 128 例,安慰剂组 228 例)。疫苗对任何一种 DENV 血清型引起的 VCD 的有效率为 67-3%(95% CI 59-4-73-9);未观察到 DENV-3 或 DENV-4 引起的病例。各治疗组发生严重不良事件的比例相似(疫苗组为 637 [6-2%],安慰剂组为 395 [6-6%]),直至截止日期:单剂量布坦坦-DV的耐受性普遍良好,对有症状的VCD(由DENV-1和DENV-2引起)平均有效3-7年。这些研究结果支持继续开发布坦坦-DV,以预防儿童、青少年和成年人的登革热疾病,无论其登革热血清状态如何:资金来源:布坦坦研究所和默克公司的子公司默克夏普多美有限责任公司(Merck Sharp & Dohme LLC):摘要的西班牙文和葡萄牙文译文见补充材料部分。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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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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