Wang Yanxia, Shi Gang, Wang Xue, Xie Zhiqiang, Gou Jinbo, Huang Lili, Huang Haitao, You Wangyang, Wang Ruijie, Yang Yongli, Wang Feiyu, Zhu Tao, Zhao Dongyang
Henan Center for Disease Control and Prevention, Zhengzhou 450016, China.
National Institutes for Food and Drug Control, Beijing 100050, China.
Vaccines (Basel). 2024 Jul 23;12(8):827. doi: 10.3390/vaccines12080827.
: Protein-based pneumococcal vaccines (PBPVs) may offer expanded protection against and tackle the antimicrobial resistance crisis in pneumococcal infections. This study examined the safety and immunogenicity in healthy adults vaccinated with three doses of a protein-based pneumococcal vaccine containing pneumococcal surface protein A (PspA) (PRX1, P3296 and P5668) and in combination with a recombinant detoxified pneumolysin protein (PlyLD). : This phase Ia randomized, double blind, placebo-controlled clinical study enrolled healthy adults aged 18-49 years. The participants were randomized into experimental (low-dose, medium-dose, high-dose) and placebo groups in a ratio of 3:1. Three doses of investigational vaccine were given to the participants with an interval of two months. Safety endpoints included the occurrence of total adverse reactions, solicited local and systemic adverse reactions, unsolicited adverse reactions, serious adverse events (SAEs), and several laboratory parameters. Immunogenicity endpoints included geometric mean titers (GMT) of anti-PspA (PRX1, P3296 and P5668) and anti-PlyLD antibodies level as determined by ELISA, seropositivity rates of PspA and PlyLD antibodies (>4-fold increase) and neutralization activity of anti-Ply antibody in serum. : A total of 118 participants completed the study of three doses. The candidate PBPV was safe and well-tolerated in all experimental groups. No vaccine-related SAEs were observed in this study. Most solicited adverse reactions were mild and transient. The most frequently reported solicited adverse reactions in the medium- and high-dose groups was pain at the injection site, while in the low-dose group it was elevated blood pressure. The immunogenicity data showed a sharp increase in the GMT level of anti-PspA-RX1, anti-PspA-3296, anti-PspA-5668, and anti-PlyLD antibodies in serum. The results also showed that the elicited antibodies were dosage-dependent. The high-dose group showed a higher immune response against PspA-RX1, PspA-3296, PspA-5668, and PlyLD antigens. However, repeat vaccination did not increase the level of anti-PspA antibodies but the level of anti-PlyLD antibody. High seropositivity rates were also observed for anti-PspA-RX1, anti-PspA-3296, anti-PspA-5668, and anti-PlyLD antibodies. In addition, a significant difference in the GMT levels of anti-Ply antibody between the high-, medium-, and low-dose groups post each vaccination were indicated by neutralization activity tests. : The PBPV showed a safe and immunogenic profile in this clinical trial. Taking into consideration both safety and immunogenicity data, we propose a single dose of 50 µg (medium dose) of PBPV as the optimum approach in providing expanded protection against .
基于蛋白质的肺炎球菌疫苗(PBPVs)可能提供更广泛的保护,应对肺炎球菌感染中的抗菌药物耐药性危机。本研究检测了接种三剂含肺炎球菌表面蛋白A(PspA)(PRX1、P3296和P5668)的基于蛋白质的肺炎球菌疫苗并联合重组解毒肺炎溶血素蛋白(PlyLD)的健康成年人的安全性和免疫原性。 : 这项Ia期随机、双盲、安慰剂对照临床研究纳入了18至49岁的健康成年人。参与者按3:1的比例随机分为试验组(低剂量、中剂量、高剂量)和安慰剂组。给参与者接种三剂研究用疫苗,间隔两个月。安全性终点包括总不良反应、预期的局部和全身不良反应、非预期不良反应、严重不良事件(SAEs)以及多项实验室参数的发生情况。免疫原性终点包括通过酶联免疫吸附测定(ELISA)测定的抗PspA(PRX1、P3296和P5668)几何平均滴度(GMT)和抗PlyLD抗体水平、PspA和PlyLD抗体的血清阳性率(>4倍增加)以及血清中抗Ply抗体的中和活性。 : 共有118名参与者完成了三剂疫苗的研究。候选PBPV在所有试验组中均安全且耐受性良好。本研究中未观察到与疫苗相关的SAEs。大多数预期不良反应为轻度且短暂。中剂量和高剂量组最常报告的预期不良反应是注射部位疼痛,而低剂量组是血压升高。免疫原性数据显示血清中抗PspA-RX1、抗PspA-3296、抗PspA-5668和抗PlyLD抗体的GMT水平急剧上升。结果还表明诱导产生的抗体具有剂量依赖性。高剂量组对PspA-RX1、PspA-3296、PspA-5668和PlyLD抗原表现出更高的免疫反应。然而,重复接种并未增加抗PspA抗体水平,但增加了抗PlyLD抗体水平。抗PspA-RX1、抗PspA-3296、抗PspA-5668和抗PlyLD抗体也观察到高血清阳性率。此外,中和活性试验表明每次接种后高剂量、中剂量和低剂量组之间抗Ply抗体的GMT水平存在显著差异。 : PBPV在该临床试验中显示出安全且具有免疫原性的特征。综合考虑安全性和免疫原性数据,我们建议单剂量50μg(中剂量)的PBPV作为提供更广泛保护的最佳方法。
