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基于质粒的候选炭疽疫苗抗原接种可诱导持久的1型和2型辅助性T细胞免疫反应。

Plasmid-based vaccination with candidate anthrax vaccine antigens induces durable type 1 and type 2 T-helper immune responses.

作者信息

Zhang Yongxin, Qiu Jianxia, Zhou Yu, Farhangfar Farhang, Hester Jenny, Lin Augustine Y, Decker William K

机构信息

MithraGen, Inc., 8030 El Rio, Houston, TX 77054, USA.

出版信息

Vaccine. 2008 Jan 30;26(5):614-22. doi: 10.1016/j.vaccine.2007.11.072. Epub 2007 Dec 18.

Abstract

The current anthrax vaccine imparts protective immunity by generating a humoral immune response against a single antigen, the PA exotoxin subunit. While this response neutralizes the two anthrax exotoxins and protects the recipient from toxin-related mortality, the recipient is not protected from spore germination, infection, and/or bacteremia. Moreover, protective immunity against PA must be generated via a lengthy injection schedule and maintained by a yearly booster. In an effort to improve upon the current vaccine formulation, we screened six of seven known virulence factors encoded by Bacillus anthracis epigenetic elements pXO1 and pXO2 as well as the major surface proteins EA1 and SAP. Screening was carried out in conjunction with a plasmid-based technology known for its ability to generate type 1 and type 2 T-helper responses. Long-term high level antibody titers were generated against the products of eag (EA1), sap (SAP), and the capA capsule synthesis subunit in vivo. Further analysis of PA- and EA1-vaccinated mice demonstrated antigen-specific type 1 helper responses including IFN-gamma secretion and lysis of EA1- or PA-loaded macrophages; further, an EA1 T-cell epitope was identified. The results demonstrate that anthrax antigens other than PA might be suitable for the generation of durable immune responses against anthrax.

摘要

目前的炭疽疫苗通过产生针对单一抗原——保护性抗原(PA)外毒素亚基的体液免疫反应来赋予保护性免疫。虽然这种反应可中和两种炭疽外毒素并保护接种者免受毒素相关的死亡,但接种者无法免受孢子萌发、感染和/或菌血症的影响。此外,针对PA的保护性免疫必须通过冗长的注射程序来产生,并通过每年一次的加强注射来维持。为了改进当前的疫苗配方,我们筛选了炭疽芽孢杆菌表观遗传元件pXO1和pXO2编码的七个已知毒力因子中的六个,以及主要表面蛋白EA1和SAP。筛选是结合一种基于质粒的技术进行的,该技术以能够产生1型和2型辅助性T细胞反应而闻名。在体内针对eag(EA1)、sap(SAP)和capA荚膜合成亚基的产物产生了长期的高抗体滴度。对接种PA和EA1的小鼠的进一步分析表明存在抗原特异性1型辅助性T细胞反应,包括干扰素-γ分泌以及对负载EA1或PA的巨噬细胞的裂解;此外,还鉴定出了一个EA1 T细胞表位。结果表明,除PA之外的炭疽抗原可能适合产生针对炭疽的持久免疫反应。

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