Ad26.COV2.S 成人安全性和免疫原性:一项随机、双盲、安慰剂对照的 2a 期剂量探索研究。
Safety and immunogenicity of Ad26.COV2.S in adults: A randomised, double-blind, placebo-controlled Phase 2a dose-finding study.
机构信息
Janssen Research & Development LLC, Spring House, PA, United States.
Janssen Vaccines & Prevention, Leiden, the Netherlands.
出版信息
Vaccine. 2024 Jun 11;42(16):3536-3546. doi: 10.1016/j.vaccine.2024.04.059. Epub 2024 May 4.
BACKGROUND
A single dose of Ad26.COV2.S is well-tolerated and effective in preventing moderate-to-severe disease outcomes due to COVID-19. We evaluated the impact of dose level, number of doses, and dose interval on immunogenicity, reactogenicity, and safety of Ad26.COV2.S in adults. Anamnestic responses were also explored.
METHODS
This randomised, double-blind, placebo-controlled, Phase 2a study was conducted in adults aged 18-55 years and ≥ 65 years (NCT04535453). Four dose levels (1.25 × 10, 2.5 × 10, 5 × 10, and 1 × 10 viral particles [vp], single and 2-dose schedules, and dose intervals of 56 and 84 days, were assessed. Four or 6 months post-primary vaccination, Ad26.COV2.S 1.25 × 10 vp was given to evaluate anamnestic responses. Humoral and cell-mediated immune responses were measured. Reactogenicity and safety were assessed in all participants.
RESULTS
All Ad26.COV2.S schedules induced humoral responses with evidence of a dose response relationship. A single dose of Ad26.COV2.S (5 × 10 vp) induced antibody and cellular immune responses that persisted for up to at least 6 months. In the 2-dose regimens, antibody responses were higher than 1-dose regimens at comparable dose levels, and the magnitude of the immune response increased when the interval between doses was increased (84 days vs 56 days). Rapid, marked immune responses were observed in all groups after vaccine antigen exposure indicating immune memory. Durable immune responses were observed in all groups for up to at least 6 months post-antigen exposure. Strong and consistent correlations between neutralising and binding antibodies were observed CD4 + and CD8 + T cell responses were similar after all regimens. Reactogenicity within 7 days post-vaccination tended to be dose-related.
CONCLUSION
The study supports the primary, single dose schedule with Ad26.COV2.S at 5 × 10 vp and homologous booster vaccination after a 6 month interval. Rapid and marked responses to vaccine antigen exposure indicate induction of immune memory by 1- and 2-dose primary vaccination.
背景
单次接种 Ad26.COV2.S 可有效预防因 COVID-19 导致的中重度疾病结局,且安全性良好。我们评估了剂量水平、接种剂次和接种间隔对 Ad26.COV2.S 在成年人中的免疫原性、反应原性和安全性的影响,并探索了记忆应答。
方法
这是一项随机、双盲、安慰剂对照的 2a 期研究,纳入 18-55 岁和≥65 岁成年人(NCT04535453)。评估了 4 个剂量水平(1.25×10、2.5×10、5×10 和 1×10 病毒颗粒[vp],单次和 2 剂方案,以及 56 和 84 天的接种间隔)。在初次接种后 4 或 6 个月,给予 1.25×10 vp 的 Ad26.COV2.S 以评估记忆应答。检测体液和细胞介导的免疫应答。所有参与者均评估反应原性和安全性。
结果
所有 Ad26.COV2.S 方案均诱导了体液免疫应答,并表现出剂量反应关系。单次接种 Ad26.COV2.S(5×10 vp)可诱导抗体和细胞免疫应答,且至少持续 6 个月。在 2 剂方案中,在可比剂量水平下,抗体应答高于 1 剂方案,且当两剂之间的间隔增加时(84 天比 56 天),免疫应答的幅度增加。在所有组中,疫苗抗原暴露后均迅速、显著地产生免疫应答,表明存在免疫记忆。在所有组中,在抗原暴露后至少 6 个月均可观察到持久的免疫应答。在所有方案中,均观察到中和抗体和结合抗体之间具有很强的一致性和相关性,CD4+和 CD8+T 细胞应答相似。接种后 7 天内的反应原性趋于与剂量相关。
结论
该研究支持采用 Ad26.COV2.S 进行单次接种,剂量为 5×10 vp,并在 6 个月间隔后进行同源加强接种。疫苗抗原暴露后迅速而显著的应答表明,1 剂和 2 剂基础免疫可诱导免疫记忆。
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