一种独立的通用流感疫苗 FLU-v 在健康成年人中的免疫原性、安全性和有效性:一项随机临床试验。
Immunogenicity, Safety, and Efficacy of a Standalone Universal Influenza Vaccine, FLU-v, in Healthy Adults: A Randomized Clinical Trial.
机构信息
SEEK, London, United Kingdom (O.P., A.F.P., E.J., G.S.).
Isala Hospital, Zwolle, the Netherlands (J.D., S.D., P.G.).
出版信息
Ann Intern Med. 2020 Apr 7;172(7):453-462. doi: 10.7326/M19-0735. Epub 2020 Mar 10.
BACKGROUND
FLU-v is a broad-spectrum influenza vaccine that induces antibodies and cell-mediated immunity.
OBJECTIVE
To compare the safety, immunogenicity, and exploratory efficacy of different formulations and dosing regimens of FLU-v versus placebo.
DESIGN
Randomized, double-blind, placebo-controlled, single-center phase 2b clinical trial. (ClinicalTrials.gov: NCT02962908; EudraCT: 2015-001932-38).
SETTING
The Netherlands.
PARTICIPANTS
175 healthy adults aged 18 to 60 years.
INTERVENTION
0.5-mL subcutaneous injection of 500 µg of adjuvanted (1 dose) or nonadjuvanted (2 doses) FLU-v (A-FLU-v or NA-FLU-v) or adjuvanted or nonadjuvanted placebo (A-placebo or NA-placebo) (2:2:1:1 ratio).
MEASUREMENTS
Vaccine-specific cellular responses at days 0, 42, and 180 were assessed via flow cytometry and enzyme-linked immunosorbent assay. Solicited information on adverse events (AEs) was collected for 21 days after vaccination. Unsolicited information on AEs was collected throughout the study.
RESULTS
The AEs with the highest incidence were mild to moderate injection site reactions. The difference between A-FLU-v and A-placebo in the median fold increase in secreted interferon-γ (IFN-γ) was 38.2-fold (95% CI, 4.7- to 69.7-fold; P = 0.001) at day 42 and 25.0-fold (CI, 5.7- to 50.9-fold; P < 0.001) at day 180. The differences between A-FLU-v and A-placebo in median fold increase at day 42 were 4.5-fold (CI, 2.3- to 9.8-fold; P < 0.001) for IFN-γ-producing CD4+ T cells, 4.9-fold (CI, 1.3- to 40.0-fold; P < 0.001) for tumor necrosis factor-α (TNF-α), 7.0-fold (CI, 3.5- to 18.0-fold; P < 0.001) for interleukin-2 (IL-2), and 1.7-fold (CI, 0.1- to 4.0-fold; P = 0.004) for CD107a. At day 180, differences were 2.1-fold (CI, 0.0- to 6.0-fold; P = 0.030) for IFN-γ and 5.7-fold (CI, 2.0- to 15.0-fold; P < 0.001) for IL-2, with no difference for TNF-α or CD107a. No differences were seen between NA-FLU-v and NA-placebo.
LIMITATION
The study was not powered to evaluate vaccine efficacy against influenza infection.
CONCLUSION
Adjuvanted FLU-v is immunogenic and merits phase 3 development to explore efficacy.
PRIMARY FUNDING SOURCE
SEEK and the European Commission Directorate-General for Research and Innovation, European Member States within the UNISEC (Universal Influenza Vaccines Secured) project.
背景
FLU-v 是一种广谱流感疫苗,可诱导抗体和细胞介导的免疫。
目的
比较不同配方和剂量方案的 FLU-v 与安慰剂在安全性、免疫原性和探索性疗效方面的差异。
设计
随机、双盲、安慰剂对照、单中心 2b 期临床试验。(ClinicalTrials.gov:NCT02962908;EudraCT:2015-001932-38)。
地点
荷兰。
参与者
175 名年龄在 18 至 60 岁之间的健康成年人。
干预措施
皮下注射 0.5 毫升 500µg 佐剂(1 剂)或非佐剂(2 剂)FLU-v(A-FLU-v 或 NA-FLU-v)或佐剂或非佐剂安慰剂(A-placebo 或 NA-placebo)(2:2:1:1 比例)。
测量
通过流式细胞术和酶联免疫吸附试验评估接种疫苗后第 0、42 和 180 天的疫苗特异性细胞反应。接种疫苗后 21 天内收集与不良事件(AE)相关的信息。整个研究期间收集与 AE 相关的不相关信息。
结果
最高发生率的 AE 为轻度至中度注射部位反应。在第 42 天,A-FLU-v 与 A-placebo 之间分泌干扰素-γ(IFN-γ)的中位数倍数增加分别为 38.2 倍(95%CI,4.7 至 69.7 倍;P=0.001),第 180 天为 25.0 倍(CI,5.7 至 50.9 倍;P<0.001)。第 42 天,A-FLU-v 与 A-placebo 之间 IFN-γ产生的 CD4+T 细胞中位数倍数增加分别为 4.5 倍(CI,2.3 至 9.8 倍;P<0.001)、肿瘤坏死因子-α(TNF-α)4.9 倍(CI,1.3 至 40.0 倍;P<0.001)、白细胞介素-2(IL-2)7.0 倍(CI,3.5 至 18.0 倍;P<0.001)和 CD107a 1.7 倍(CI,0.1 至 4.0 倍;P=0.004)。第 180 天,IFN-γ差异为 2.1 倍(CI,0.0 至 6.0 倍;P=0.030),IL-2 差异为 5.7 倍(CI,2.0 至 15.0 倍;P<0.001),TNF-α和 CD107a 无差异。NA-FLU-v 与 NA-placebo 之间无差异。
局限性
该研究没有足够的效力来评估流感感染的疫苗疗效。
结论
佐剂 FLU-v 具有免疫原性,值得进行 3 期开发以探索疗效。
主要资金来源
SEEK 和欧盟委员会研究与创新总局、欧盟成员国在 UNISEC(通用流感疫苗保障)项目内。
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