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通过操纵毒力基因来调整宿主对李斯特菌的免疫反应——先天免疫与获得性免疫之间的界面

Tailoring host immune responses to Listeria by manipulation of virulence genes -- the interface between innate and acquired immunity.

作者信息

Peters Christian, Domann Eugen, Darbouche Abdelhak, Chakraborty Trinad, Mielke Martin E A

机构信息

Aventis Behring, Clinical Research and Development, 1020 First Avenue, King of Prussia, PA 19406, USA.

出版信息

FEMS Immunol Med Microbiol. 2003 Apr 1;35(3):243-53. doi: 10.1016/S0928-8244(02)00469-8.

Abstract

Although attenuated strains of microbial pathogens have triggered vaccine development from its origin, the role of virulence factors in determining host immunity has remained largely unexplored. Using the murine listeriosis model, we investigated whether the induction and expansion of protective and inflammatory T cell responses may be modified by selective manipulation of virulence genes. We intentionally deleted specific genes of Listeria monocytogenes, including those encoding the positive regulatory factor (prfA), hemolysin (hly), the actin nucleator (actA), and phospholipase B (plcB). The resulting strains showed decisive differences in their immunogenic properties. In particular, we identified a double-deletion mutant that retained Listeria's profound ability to induce protective CD8(+) T cells, but that is strongly attenuated and exhibits a significantly reduced ability to induce CD4(+) T cell-mediated inflammation. We conclude that this mutant, L. monocytogenes DeltaactADeltaplcB, is at present the most promising mutant for a bacterial vaccine vector and is able to safely induce potent CD8(+) T cell-mediated immunity.

摘要

尽管减毒的微生物病原体菌株自疫苗研发伊始就引发了疫苗的开发,但毒力因子在决定宿主免疫方面的作用在很大程度上仍未得到探索。利用小鼠李斯特菌病模型,我们研究了通过对毒力基因的选择性操纵是否可以改变保护性和炎症性T细胞反应的诱导和扩增。我们特意删除了单核细胞增生李斯特菌的特定基因,包括那些编码正调控因子(prfA)、溶血素(hly)、肌动蛋白成核因子(actA)和磷脂酶B(plcB)的基因。所得菌株在免疫原性特性上表现出决定性差异。特别是,我们鉴定出一种双缺失突变体,它保留了李斯特菌诱导保护性CD8(+) T细胞的强大能力,但严重减毒,诱导CD4(+) T细胞介导炎症的能力显著降低。我们得出结论,这种突变体,即单核细胞增生李斯特菌ΔactAΔplcB,目前是细菌疫苗载体最有前景的突变体,并且能够安全地诱导强效的CD8(+) T细胞介导的免疫。

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