接种 BBIBP-CorV 作为基础免疫后加强接种异源 Ad26.COV2.S 对 SARS-CoV-2 感染的效果:一项 1 年随访的 1/2 期开放标签试验。
Heterologous Ad26.COV2.S booster after primary BBIBP-CorV vaccination against SARS-CoV-2 infection: 1-year follow-up of a phase 1/2 open-label trial.
机构信息
Vaccine Trial Centre, Faculty of Tropical Medicine, Mahidol University, Bangkok, Thailand.
Phaholpolpayuhasena Hospital, Kanchanaburi, Thailand.
出版信息
Vaccine. 2024 Jul 25;42(19):3999-4010. doi: 10.1016/j.vaccine.2024.05.010. Epub 2024 May 13.
BACKGROUND
Inactivated whole-virus vaccination elicits immune responses to both SARS-CoV-2 nucleocapsid (N) and spike (S) proteins, like natural infections. A heterologous Ad26.COV2.S booster given at two different intervals after primary BBIBP-CorV vaccination was safe and immunogenic at days 28 and 84, with higher immune responses observed after the longer pre-boost interval. We describe booster-specific and hybrid immune responses over 1 year.
METHODS
This open-label phase 1/2 study was conducted in healthy Thai adults aged ≥ 18 years who had completed primary BBIBP-CorV primary vaccination between 90-240 (Arm A1; n = 361) or 45-75 days (Arm A2; n = 104) before enrolment. All received an Ad26.COV2.S booster. We measured anti-S and anti-N IgG antibodies by Elecsys®, neutralizing antibodies by SARS-CoV-2 pseudovirus neutralization assay, and T-cell responses by quantitative interferon (IFN)-γ release assay. Immune responses were evaluated in the baseline-seronegative population (pre-booster anti-N < 1.4 U/mL; n = 241) that included the booster-effect subgroup (anti-N < 1.4 U/mL at each visit) and the hybrid-immunity subgroup (anti-N ≥ 1.4 U/mL and/or SARS-CoV-2 infection, irrespective of receiving non-study COVID-19 boosters).
RESULTS
In Arm A1 of the booster-effect subgroup, anti-S GMCs were 131-fold higher than baseline at day 336; neutralizing responses against ancestral SARS-CoV-2 were 5-fold higher than baseline at day 168; 4-fold against Omicron BA.2 at day 84. IFN-γ remained approximately 4-fold higher than baseline at days 168 and 336 in 18-59-year-olds. Booster-specific responses trended lower in Arm A2. In the hybrid-immunity subgroup at day 336, anti-S GMCs in A1 were 517-fold higher than baseline; neutralizing responses against ancestral SARS-CoV-2 and Omicron BA.2 were 28- and 31-fold higher, respectively, and IFN-γ was approximately 14-fold higher in 18-59-year-olds at day 336. Durable immune responses trended lower in ≥ 60-year-olds.
CONCLUSION
A heterologous Ad26.COV2.S booster after primary BBIBP-CorV vaccination induced booster-specific immune responses detectable up to 1 year that were higher in participants with hybrid immunity.
CLINICAL TRIALS REGISTRATION
NCT05109559.
背景
灭活全病毒疫苗可诱导针对 SARS-CoV-2 核衣壳 (N) 和刺突 (S) 蛋白的免疫应答,类似于自然感染。在接受 BBIBP-CorV 基础免疫接种后,不同间隔时间给予异源 Ad26.COV2.S 加强针在第 28 天和第 84 天是安全且具有免疫原性的,更长的加强针前间隔时间观察到更高的免疫应答。我们描述了 1 年以上的加强针特异性和混合免疫应答。
方法
这项开放标签的 1/2 期研究在泰国健康成年人中进行,年龄≥18 岁,在接种 BBIBP-CorV 基础免疫接种后 90-240 天(A1 组;n=361)或 45-75 天(A2 组;n=104)入组前完成。所有人都接受了 Ad26.COV2.S 加强针。我们通过 Elecsys®测量抗-S 和抗-N IgG 抗体,通过 SARS-CoV-2 假病毒中和测定测量中和抗体,通过定量干扰素 (IFN)-γ 释放测定测量 T 细胞反应。在基线血清阴性人群(加强针前抗-N<1.4 U/mL;n=241)中评估免疫应答,该人群包括加强针效应亚组(每次访视时抗-N<1.4 U/mL)和混合免疫亚组(抗-N≥1.4 U/mL 和/或 SARS-CoV-2 感染,无论是否接受非研究 COVID-19 加强针)。
结果
在加强针效应亚组的 A1 臂中,第 336 天的抗-S GMC 比基线高 131 倍;第 168 天对原始 SARS-CoV-2 的中和反应比基线高 5 倍;第 84 天对奥密克戎 BA.2 高 4 倍。在 18-59 岁的人群中,IFN-γ在第 168 天和第 336 天仍比基线高约 4 倍。A2 臂的加强针特异性反应呈下降趋势。在第 336 天的混合免疫亚组中,A1 中的抗-S GMC 比基线高 517 倍;对原始 SARS-CoV-2 和奥密克戎 BA.2 的中和反应分别高 28-31 倍,18-59 岁人群的 IFN-γ在第 336 天约高 14 倍。≥60 岁人群的持久免疫应答呈下降趋势。
结论
在 BBIBP-CorV 基础免疫接种后给予异源 Ad26.COV2.S 加强针可诱导可检测到 1 年的加强针特异性免疫应答,在具有混合免疫的参与者中更高。
临床试验注册
NCT05109559。
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