青少年在儿童时期免疫接种后 11 年,单次 4CMenB 疫苗加强针的免疫原性。
Immunogenicity of a single 4CMenB vaccine booster in adolescents 11 years after childhood immunisation.
机构信息
Oxford Vaccine Group, Department of Paediatrics, University of Oxford and the NIHR Oxford Biomedical Research Centre, Oxford OX37LE, UK.
Oxford Vaccine Group, Department of Paediatrics, University of Oxford and the NIHR Oxford Biomedical Research Centre, Oxford OX37LE, UK.
出版信息
Vaccine. 2022 Jul 30;40(32):4453-4463. doi: 10.1016/j.vaccine.2022.04.085. Epub 2022 Jun 11.
The clinical development of the meningococcal vaccine, 4CMenB, included 2 doses in vaccine-naïve adolescents, which was considered unlikely to be cost-effective for implementation. Theoretically, priming with 4CMenB in early childhood might drive strong immune responses after only a single booster dose in adolescents and reduce programmatic costs. To address this question, children over 11 years old who took part in previous trials involving the administration of 3-5 doses of 4CMenB at infant/preschool age from 2006 were recruited into a post licensure single-centre trial, and were divided into two groups: those who received their last dose at 12 months old (infant group) and those who received their last dose at 3 years old (infant + preschool group). Naïve age-matched controls were randomised to receive one (adolescent 1 group) or two doses at days 0 and 28 (adolescent 2 group) of 4CMenB. Serum bactericidal antibody (SBA) assays using human complement were performed against three reference strains prior to vaccination, and at 1, 6 and 12 months. Previous vaccination was associated with a higher response to a single booster dose at 11 years of age, one-month post-vaccination, when compared with a single dose in naïve age-matched controls. At day 180, the highest responses were observed in participants in the infant + preschool group against strain 5/99 (GMT 316.1 [CI 158.4 to 630.8]), as compared with naïve adolescents who received two doses (GMTs 84.5 [CI 57.7 to 123.6]). When the last dose was received at 12-months of age, responses to a single adolescent dose were not as robust (GMT 61.1 [CI 14.8 to 252.4] to strain 5/99). This descriptive study indicates that the highest SBA responses after a single dose in adolescence were observed in participants who received a preschool dose, suggesting that B cell memory responses are not sufficiently primed at less than 12 months of age. Trial registration EudraCT 2017-004732-11, ISRCTN16774163.
脑膜炎球菌疫苗 4CMenB 的临床开发包括对疫苗初免的青少年接种 2 剂,这在成本效益方面被认为不太可行。从理论上讲,在幼儿期用 4CMenB 进行初免可能会在青少年期仅接种 1 次加强针后产生强烈的免疫反应,并降低项目成本。为了解决这个问题,从 2006 年开始,参与过在婴儿/幼儿期接种 3-5 剂 4CMenB 的临床试验的年龄在 11 岁以上的儿童被招募到一项许可后单中心试验中,并分为两组:在 12 个月龄(婴儿组)接受最后一剂者和在 3 岁(婴儿+幼儿组)接受最后一剂者。年龄匹配的初免对照者被随机分配在第 0 天和第 28 天接受 4CMenB 1 剂(青少年 1 组)或 2 剂(青少年 2 组)。在接种前和接种后 1、6 和 12 个月,用含有人补体的血清杀菌抗体(SBA)测定试剂盒对 3 株参考株进行检测。与初免年龄匹配的对照者相比,既往接种与 11 岁时单次加强针接种后一个月时的更高反应相关。在第 180 天,婴儿+幼儿组参与者对 5/99 株的反应最高(GMT316.1[158.4 至 630.8]),而接受 2 剂的初免青少年的 GMT 为 84.5[57.7 至 123.6]。当最后一剂在 12 月龄时接种时,对青少年单次剂量的反应并不那么强烈(对 5/99 株的 GMT 为 61.1[14.8 至 252.4])。这项描述性研究表明,在接受学前剂量的参与者中,在青春期单次接种后观察到最高的 SBA 反应,这表明在 12 个月龄以下时,B 细胞记忆反应没有充分被激发。试验注册 EudraCT 2017-004732-11,ISRCTN66324447。
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