与皮内途径相比,非人灵长类动物静脉注射卡介苗可诱导更高的血清抗体滴度,并具有更强的抗体亲和力和蛋白吸附能力。

Vaccine Pub Date : 2024-12-02 Epub Date: 2024-11-10 DOI:10.1016/j.vaccine.2024.126444
Marco Polo Peralta Alvarez, Keya Downward, Andrew White, Stephanie A Harris, Iman Satti, Shuailin Li, Alexandra Morrison, Laura Sibley, Charlotte Sarfas, Mike Dennis, Hugo Redondo Azema, Sally Sharpe, Helen McShane, Rachel Tanner
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引用次数: 0

摘要

目前迫切需要一种新的、更有效的结核病(TB)疫苗,但由于缺乏有效的免疫保护相关因素,疫苗的开发受到了阻碍。通过气溶胶(AE)和静脉注射(IV)途径接种卡介苗(BCG)已证明,与标准皮内注射(ID)相比,在非人灵长类动物(NHP)中接种卡介苗可在结核分枝杆菌(M.tb)挑战下提供更高水平的保护。这一发现为研究免疫力的哪些方面与更好地控制结核分枝杆菌有关并可能代表保护的生物标志物或相关因素提供了宝贵的机会。由于迄今为止的结核病疫苗研究主要集中在细胞免疫方面,我们的目标是更好地描述人们对卡介苗在NHP中不同接种途径下的血清抗体反应知之甚少。与ID或AE途径相比,我们证明静脉注射卡介苗后血清中的M.tb特异性IgG、IgA和IgM滴度更高。我们还观察到静脉注射卡介苗诱导的 IgG 对分枝杆菌表面的蛋白溶解能力有所提高,并首次报告了静脉注射卡介苗动物的 M.tb 特异性 IgG 与 ID 或 AE 卡介苗动物的 IgG 相比具有更高的亲和力。值得注意的是,我们确定了 IgG 阳性度与气溶胶 M.tb 挑战保护措施之间的显著相关性。我们的研究结果突显了抗体作为IV型卡介苗诱导的针对结核病的卓越保护作用的标记物和/或介质的潜在作用,并建议在开发和评估结核病候选疫苗时应考虑抗体的质量和数量。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Intravenous BCG vaccination in non-human primates induces superior serum antibody titers with enhanced avidity and opsonizing capacity compared to the intradermal route.

A new and more effective tuberculosis (TB) vaccine is urgently needed, but development is hampered by the lack of validated immune correlates of protection. Bacillus Calmette Guérin (BCG) vaccination by the aerosol (AE) and intravenous (IV) routes has been shown to confer superior levels of protection from challenge with Mycobacterium tuberculosis (M.tb) in non-human primates (NHP) compared with standard intradermal (ID) administration. This finding offers a valuable opportunity to investigate which aspects of immunity are associated with improved control of M.tb and may represent biomarkers or correlates of protection. As TB vaccine research to date has focused largely on cellular immunity, we aimed to better characterize the poorly-understood serum antibody response to BCG administered by different routes of vaccination in NHP. We demonstrate superior M.tb-specific IgG, IgA, and IgM titers in serum following IV BCG vaccination compared to the ID or AE routes. We also observe improved capacity of IgG induced by IV BCG to opsonize the surface of mycobacteria, and report for the first time that M.tb-specific IgG from IV BCG vaccinated animals is of higher avidity compared with IgG from ID or AE BCG vaccinated animals. Notably, we identified a significant correlation between IgG avidity and measures of protection from aerosol M.tb challenge. Our findings highlight a potential role for antibodies as markers and/or mediators of the superior vaccine-induced protection IV BCG confers against TB and suggest that quality, as well as quantity, of antibodies should be considered when developing and evaluating TB vaccine candidates.

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