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Systemic but not mucosal immunity induced by AVA prevents inhalational anthrax

机译:AVA诱导的全身性而非粘膜免疫性可预防吸入性炭疽

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摘要

Improved vaccines and adjuvants are being developed to reduce the threat posed by a terrorist attack involving aerosolized anthrax spores. Nevertheless, uncertainty persists concerning the relative benefits of inducing mucosal vs systemic immunity to host survival following inhalational exposure to anthrax spores. This work examines the effect of delivering the licensed human vaccine (Anthrax Vaccine Adsorbed, AVA) combined with a CpG oligodeoxynucleotide (ODN) adjuvant intraperitoneally or intranasally to A/J mice. Results indicate that protection from inhalational anthrax correlates with the induction of a strong systemic rather than mucosal immune response, and demonstrate that protection is significantly improved and accelerated by the addition of CpG ODN.
机译:正在开发改进的疫苗和佐剂,以减少涉及气雾化炭疽孢子的恐怖袭击所造成的威胁。然而,在吸入炭疽孢子后,诱导粘膜与全身免疫对宿主存活的相对益处仍存在不确定性。这项工作检查了腹膜内或鼻内向C / G寡脱氧核苷酸(ODN)佐剂与许可的人源疫苗(炭疽吸附疫苗,AVA)的结合。结果表明,针对吸入性炭疽的保护作用与诱导强烈的全身性免疫反应而非粘膜免疫反应有关,并表明通过添加CpG ODN可以显着改善和加速保护作用。

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