在布基纳法索儿童中,与疟疾候选疫苗 BK-SE36 接种同时发生的感染会干扰免疫反应。
infection coinciding with the malaria vaccine candidate BK-SE36 administration interferes with the immune responses in Burkinabe children.
机构信息
Groupe de Recherche Action en Santé, Ouagadougou (GRAS), Ouagadougou, Burkina Faso.
Centre National de Recherche et de Formation sur le Paludisme (CNRFP), Ouagadougou, Burkina Faso.
出版信息
Front Immunol. 2023 Mar 10;14:1119820. doi: 10.3389/fimmu.2023.1119820. eCollection 2023.
BACKGROUND
A vaccine targeting the erythrocyte stages of could play a role in preventing clinical disease. BK-SE36 is a promising malaria vaccine candidate that has shown a good safety profile and immunological responses during field evaluations. It was observed that repeated natural infections could result in immune tolerance against SE36 molecule.
METHODS
The primary trial was conducted to assess the safety and immunogenicity of the BK-SE36 in two cohorts of children aged 25-60 months (Cohort 1) and 12-24 months (Cohort 2). Immunization was at full dose (1.0 mL) administered at 0, 1, and 6 months. Blood samples were collected before each vaccination for immunological assessments and detection of infection by microscopy. Blood samples were further collected one month post each vaccination to evaluate immunogenicity.
RESULTS
Of seventy-two (72) subjects that have received BK-SE36 vaccination, 71 had available blood smears during vaccination days. One month post Dose 2, the geometric mean of SE36 antibodies was 263.2 (95% CI: 178.9-387.1) in uninfected individuals compared to 77.1 (95% CI: 47.3-125.7) in infected participants. The same trend was observed one-month post booster dose. Participants uninfected at the time of booster vaccination had significantly higher GMTs compared to those who were infected (424.1 (95% CI: 301.9-595.8) . 92.8 (95% CI: 34.9-246.6), = 0.002. There was a 14.3 (95% CI: 9.7-21.1) and 2.4 (95% CI: 1.3-4.4) fold-change, respectively, in uninfected and infected participants between one-month post Dose 2 and booster. The difference was statistically significant ( < 0.001).
CONCLUSION
Concomitant infection by during BK-SE36 vaccine candidate administration is associated with reduced humoral responses. However, it is to be noted that the BK-SE36 primary trial was not designed to investigate the influence of concomitant infection on vaccine-induced immune response and should be interpreted cautiously.
TRIAL REGISTRATION
WHO ICTRP, PACTR201411000934120.
背景
针对红细胞期疟原虫的疫苗可能在预防临床疾病方面发挥作用。BK-SE36 是一种有前途的疟疾疫苗候选物,在现场评估中表现出良好的安全性和免疫反应。观察到重复的自然感染可能导致对 SE36 分子的免疫耐受。
方法
该主要试验旨在评估 25-60 个月龄儿童(队列 1)和 12-24 个月龄儿童(队列 2)两组儿童中 BK-SE36 的安全性和免疫原性。免疫接种采用全剂量(1.0 毫升),在 0、1 和 6 个月时进行。在每次接种前采集血样进行免疫学评估和显微镜检测疟原虫感染。在每次接种后一个月进一步采集血样,以评估免疫原性。
结果
在接受 BK-SE36 疫苗接种的 72 名受试者中,有 71 名在接种日期间有可用的血涂片。在第 2 剂后一个月,未感染者 SE36 抗体的几何平均滴度为 263.2(95%CI:178.9-387.1),而感染者为 77.1(95%CI:47.3-125.7)。在加强剂量后一个月也观察到相同的趋势。与感染时接受加强疫苗接种的参与者相比,加强疫苗接种时未感染的参与者的 GMT 显著更高(424.1(95%CI:301.9-595.8).92.8(95%CI:34.9-246.6), = 0.002。未感染者和感染者之间分别有 14.3(95%CI:9.7-21.1)和 2.4(95%CI:1.3-4.4)的倍数变化,在第 2 剂后一个月和加强剂量后一个月之间。差异具有统计学意义(<0.001)。
结论
在 BK-SE36 候选疫苗接种期间同时感染疟原虫与体液反应降低有关。然而,应当指出,BK-SE36 主要试验并非旨在研究同时感染对疫苗诱导免疫反应的影响,因此应谨慎解释。
试验注册
世界卫生组织 ICTRP,PACTR201411000934120。
Zotero 插件