OX40 配体融合蛋白与卡介苗疫苗同时给药可提供针对小鼠结核分枝杆菌感染的优异保护。
OX40 ligand fusion protein delivered simultaneously with the BCG vaccine provides superior protection against murine Mycobacterium tuberculosis infection.
机构信息
Imperial College, London, UK.
出版信息
J Infect Dis. 2012 Mar 15;205(6):975-83. doi: 10.1093/infdis/jir868. Epub 2012 Feb 7.
Abstract
Mycobacterium tuberculosis infection claims approximately 2 million lives per year, and improved efficacy of the BCG vaccine remains a World Health Organization priority. Successful vaccination against M. tuberculosis requires the induction and maintenance of T cells. Targeting molecules that promote T-cell survival may therefore provide an alternative strategy to classic adjuvants. We show that the interaction between T-cell-expressed OX40 and OX40L on antigen-presenting cells is critical for effective immunity to BCG. However, because OX40L is lost rapidly from antigen-presenting cells following BCG vaccination, maintenance of OX40-expressing vaccine-activated T cells may not be optimal. Delivering an OX40L:Ig fusion protein simultaneously with BCG provided superior immunity to intravenous and aerosol M. tuberculosis challenge even 6 months after vaccination, an effect that depends on natural killer 1.1(+) cells. Attenuated vaccines may therefore lack sufficient innate stimulation to maintain vaccine-specific T cells, which can be replaced by reagents binding inducible T-cell costimulators.
摘要
结核分枝杆菌感染每年导致约 200 万人死亡,提高卡介苗疫苗的效力仍然是世界卫生组织的优先事项。成功预防结核分枝杆菌感染需要诱导和维持 T 细胞。因此,针对促进 T 细胞存活的分子可能为经典佐剂提供替代策略。我们表明,T 细胞表达的 OX40 与抗原呈递细胞上的 OX40L 之间的相互作用对于对卡介苗的有效免疫至关重要。然而,由于在卡介苗接种后抗原呈递细胞中的 OX40L 迅速丢失,因此维持 OX40 表达的疫苗激活的 T 细胞可能不是最佳的。同时给予 OX40L:Ig 融合蛋白与卡介苗一起提供了对静脉内和雾化结核分枝杆菌挑战的优越免疫力,甚至在接种后 6 个月仍然有效,这一效果依赖于自然杀伤 1.1(+)细胞。因此,减毒疫苗可能缺乏足够的先天刺激来维持疫苗特异性 T 细胞,这些细胞可以被结合诱导性 T 细胞共刺激物的试剂所取代。
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