National Institute for Health and Care Research Mucosal Pathogens Research Unit, Research Department of Infection, Division of Infection and Immunity, University College London, London, UK; Malawi-Liverpool-Wellcome Research Programme, Blantyre, Malawi.
Malawi-Liverpool-Wellcome Research Programme, Blantyre, Malawi; Department of Clinical Sciences, Liverpool School of Tropical Medicine, Liverpool, UK.
Lancet Infect Dis. 2022 Dec;22(12):1737-1747. doi: 10.1016/S1473-3099(22)00438-8. Epub 2022 Aug 24.
Pneumococcal conjugate vaccines (PCVs) induce serotype-specific IgG antibodies, effectively reducing vaccine-serotype carriage and invasive pneumococcal disease (IPD). IgG production wanes approximately 1 month after vaccination in absence of serotype-specific exposure. With uncertainty surrrounding correlate of protection (CoP) estimates and with persistent vaccine-serotype carriage and vaccine-serotype IPD after PCV13 introduction, we aimed to profile population-level immunogenicity among children younger than 5 years in Blantyre, Malawi.
For this serosurveillance study, we used a random subset of samples from a prospective population-based serosurvey in Blantyre, Malawi, done between Dec 16, 2016, and June 27, 2018. Sample selection was based on age category optimisation among children younger than 5 years, adequate sample volume, and available budget. We measured serotype-specific IgGs against the 13 vaccine serotypes (1, 3, 4, 5, 6A, 6B, 7F, 9V, 14, 18C, 19A, 19F, and 23F) and two non-vaccine serotypes (12F and 33F), as well as IgGs against three pneumococcal proteins (PsaA, NanA, and Ply), using ELISA and a direct-binding electrochemiluminescence-based multiplex assay. We estimated population-level, serotype-specific immunogenicity profiles using a linear spline regression model. Analyses included samples stratified to 20 3-month age strata (eg, age <3 months to 57-59 months).
We evaluated 638 plasma samples: 556 primary samples and 82 unique secondary samples (each linked to one primary sample). Immunogenicity profiles revealed a consistent pattern among vaccine serotypes except serotype 3: a vaccine-induced IgG peak followed by waning to a nadir and subsequent increase in titre. For serotype 3, we observed no apparent vaccine-induced increase. Heterogeneity in parameters included age range at post-vaccination nadir (from 11·2 months [19A] to 27·3 months [7F]). The age at peak IgG titre ranged from 2·69 months (5) to 6·64 months (14). Titres dropped below CoPs against IPD among nine vaccine serotypes (1, 3, 4, 5, 6B, 7F, 9V, 18C, and 23F) and below CoPs against carriage for ten vaccine serotypes (1, 4, 5, 6B, 7F, 9V, 14, 18C, 19F, and 23F). Increasing antibody concentrations among older children and seroincident events were consistent with ongoing vaccine-serotype exposure.
A 3 + 0 PCV13 schedule with high uptake has not led to sustained population-level antibody immunity beyond the first year of life. Indeed, post-vaccine antibody concentrations dropped below putative CoPs for several vaccine serotypes, potentially contributing to persistent vaccine-serotype carriage and residual vaccine-serotype IPD in Malawi and other similar settings. Policy decisions should consider alternative vaccine strategies, including a booster dose, to achieve sustained vaccine-induced antibody titres, and thus control.
Bill & Melinda Gates Foundation, Wellcome UK, and National Institute for Health and Care Research.
肺炎球菌结合疫苗(PCV)可诱导血清型特异性 IgG 抗体,有效降低疫苗血清型的携带率和侵袭性肺炎球菌病(IPD)。在缺乏血清型特异性暴露的情况下,接种疫苗后大约 1 个月 IgG 产量会下降。由于保护相关因素(CoP)的估计存在不确定性,以及在引入 PCV13 后仍存在疫苗血清型携带和疫苗血清型 IPD,我们旨在研究马拉维布兰太尔 5 岁以下儿童的人群免疫原性特征。
在这项血清学监测研究中,我们使用了马拉维布兰太尔前瞻性基于人群的血清学监测的随机样本子集,该研究于 2016 年 12 月 16 日至 2018 年 6 月 27 日进行。样本选择基于 5 岁以下儿童的年龄类别优化、足够的样本量和可用预算。我们使用 ELISA 和直接结合电化学发光的多重分析方法,测量针对 13 种疫苗血清型(1、3、4、5、6A、6B、7F、9V、14、18C、19A、19F 和 23F)和两种非疫苗血清型(12F 和 33F)的血清型特异性 IgG,以及针对三种肺炎球菌蛋白(PsaA、NanA 和 Ply)的 IgG。我们使用线性样条回归模型来估计人群水平、血清型特异性免疫原性特征。分析包括按 20 个 3 个月龄组分层的样本(例如,<3 个月至 57-59 个月)。
我们评估了 638 份血浆样本:556 份原始样本和 82 份独特的二次样本(每个样本与一份原始样本相关联)。免疫原性特征显示除血清型 3 外,疫苗血清型之间存在一致的模式:疫苗诱导的 IgG 峰值,随后下降至最低点,随后增加。对于血清型 3,我们没有观察到明显的疫苗诱导增加。包括疫苗诱导最低点的年龄范围(从 11.2 个月[19A]到 27.3 个月[7F])在内的参数存在异质性。达到 IgG 峰值的年龄范围从 2.69 个月(5 岁)到 6.64 个月(14 岁)。针对 IPD 的九个疫苗血清型(1、3、4、5、6B、7F、9V、18C 和 23F)和针对携带的十个疫苗血清型(1、4、5、6B、7F、9V、14、18C、19F 和 23F)的抗体滴度均低于 CoP。在年龄较大的儿童中抗体浓度的增加和血清型的偶然事件与持续的疫苗血清型暴露一致。
高接种率的 3 剂 PCV13 方案并未导致人群水平的抗体免疫持续到生命的第一年之后。事实上,接种疫苗后的抗体浓度下降到了几种疫苗血清型的假定 CoP 以下,这可能导致马拉维和其他类似环境中持续的疫苗血清型携带和残留疫苗血清型 IPD。政策决策应考虑替代疫苗策略,包括加强剂量,以实现持续的疫苗诱导抗体滴度,从而控制疾病。
比尔及梅琳达·盖茨基金会、英国惠康基金会和英国国家卫生与保健研究所。
