GSK, Avenue Fleming 20, Wavre 1300, Belgium.
The University of Texas Medical Branch (UTMB), 301 University Boulevard, Galveston, TX 77555, United States.
Vaccine. 2024 Apr 11;42(10):2560-2571. doi: 10.1016/j.vaccine.2024.02.001. Epub 2024 Feb 14.
Pneumococcal conjugate vaccines (PCVs) significantly reduced pneumococcal disease burden. Nevertheless, alternative approaches for controlling more serotypes are needed. Here, the safety, tolerability, and immunogenicity of a 24-valent (1/2/3/4/5/6A/6B/7F/8/9N/9V/10A/11A/12F/14/15B/17F/18C/19A/19F/20B/22F/23F/33F) pneumococcal vaccine based on Multiple Antigen-Presenting System (MAPS) technology (Pn-MAPS24v) was assessed in toddlers.
In this phase 1, blinded, dose-escalation, active-controlled multicenter study conducted in the United States (September/2020-April/2022), 12-15-month-old toddlers primed with three doses of 13-valent PCV (PCV13) were randomized 3:2 to receive a single dose of one of three Pn-MAPS24v dose levels (1 μg/2 μg/5 μg per polysaccharide) or PCV13 intramuscularly. Reactogenicity (within 7 days), treatment-emergent adverse events (TEAEs, within 180 days), serious/medically attended adverse events (SAEs/MAAEs, within 180 days), and immunogenicity (serotype-specific anti-capsular polysaccharide immunoglobulin G [IgG] and opsonophagocytic activity [OPA] responses at 30 days post-vaccination) were assessed.
Of 75 toddlers enrolled, 74 completed the study (Pn-MAPS24v 1 μg/2 μg/5 μg: 15/14/16, PCV13: 29). Frequencies of local (60 %/67 %/31 %) and systemic events (67 %/67 %/75 %) in the Pn-MAPS24v 1 μg/2 μg/5 μg and the PCV13 (55 %, 79 %) groups were in similar ranges. TEAEs were reported by 47 %/40 %/63 % of Pn-MAPS24v 1 μg/2 μg/5 μg recipients and 52 % of PCV13 recipients. No vaccine-related SAE was reported. At 30 days post-vaccination, for each of the 13 common serotypes, ≥93 % of participants in each group had IgG concentrations ≥0.35 μg/mL; >92 % had OPA titers ≥lower limit of quantitation (LLOQ), except for serotype 1 (79 %). For 7/11 unique serotypes (2/8/9N/11A/17F/22F/33F), at all dose levels, ≥78 % of Pn-MAPS24v recipients in each group had IgG concentrations ≥0.35 μg/mL and 80 %-100 % had OPA titers ≥LLOQ.
In 12-15-month-old toddlers, a single dose of Pn-MAPS24v showed an acceptable safety profile, regardless of dose level; AEs were reported at similar frequencies by Pn-MAPS24v and PCV13 recipients. Pn-MAPS24v elicited IgG and OPA responses to all common and most unique serotypes. These results support further clinical evaluation in infants.
肺炎球菌结合疫苗(PCV)显著降低了肺炎球菌疾病负担。然而,仍需要其他方法来控制更多血清型。在此,我们评估了一种基于多抗原呈递系统(MAPS)技术的 24 价肺炎球菌疫苗(Pn-MAPS24v)的安全性、耐受性和免疫原性,该疫苗适用于幼儿。
这是一项在美国进行的、1/2/3/4/5/6A/6B/7F/8/9N/9V/10A/11A/12F/14/15B/17F/18C/19A/19F/20B/22F/23F/33F 多价肺炎球菌疫苗的 1 期、双盲、剂量递增、活性对照的多中心研究。研究对象为 12-15 月龄、已接种三剂 13 价 PCV(PCV13)的幼儿,随机分为三组,每组 30 人,接受三种 Pn-MAPS24v 剂量水平(1μg/2μg/5μg 每多糖)之一或 PCV13 肌内注射。在接种后 7 天内评估不良反应(在接种后 180 天内评估治疗后出现的不良事件、严重/需要医疗关注的不良事件和免疫原性(30 天内血清型特异性荚膜多糖免疫球蛋白 G [IgG]和调理吞噬活性 [OPA]应答)。
75 名幼儿中,74 名完成了研究(Pn-MAPS24v 1μg/2μg/5μg:15/14/16,PCV13:29)。Pn-MAPS24v 1μg/2μg/5μg 组和 PCV13 组的局部(60%/67%/31%)和全身(67%/67%/75%)事件的发生率相似。47%/40%/63%的 Pn-MAPS24v 1μg/2μg/5μg 组和 52%的 PCV13 组报告了治疗后出现的不良事件。没有疫苗相关的严重不良事件报告。在接种后 30 天,每组的 13 种常见血清型中,≥93%的参与者的 IgG 浓度≥0.35μg/mL;除血清型 1(79%)外,≥92%的参与者的 OPA 滴度≥定量下限(LLOQ)。对于 7/11 种独特血清型(2/8/9N/11A/17F/22F/33F),在所有剂量水平下,每组≥78%的 Pn-MAPS24v 组参与者的 IgG 浓度≥0.35μg/mL,80%-100%的参与者的 OPA 滴度≥LLOQ。
在 12-15 月龄幼儿中,无论剂量水平如何,单剂 Pn-MAPS24v 均具有可接受的安全性特征;Pn-MAPS24v 组和 PCV13 组报告的不良反应频率相似。Pn-MAPS24v 诱导了针对所有常见和大多数独特血清型的 IgG 和 OPA 应答。这些结果支持在婴儿中进行进一步的临床评估。
