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用分泌超抗原的胞内细菌病原体免疫后增强CD8 T细胞反应的刺激。

Stimulation of enhanced CD8 T cell responses following immunization with a hyper-antigen secreting intracytosolic bacterial pathogen.

作者信息

Smithey Megan J, Brandt Suzanne, Freitag Nancy E, Higgins Darren E, Bouwer H G Archie

机构信息

Veterans Affairs Medical Center, Portland, OR 97239, USA.

出版信息

J Immunol. 2008 Mar 1;180(5):3406-16. doi: 10.4049/jimmunol.180.5.3406.

Abstract

The intracytosolic niche for replication of Listeria monocytogenes (Lm) facilitates delivery of bacteria-derived Ags into the MHC class I pathway for subsequent stimulation of CD8 effector T cells. Using Lm strains that are equivalent for in vivo virulence yet express marked differences in the level of secretion of a protective target Ag, we have evaluated how these specific differences in secretion levels influences the magnitude and effector function of Ag-specific CD8 T cell responses following Lm injection. Immunization with low doses of a hyperantigen-secreting Lm strain stimulated enhanced target-Ag specific CD8 T cell responses compared with the magnitude stimulated following immunization with the same dose of wild-type Lm. The enhanced determinant-specific response was also evident by in vivo CTL activity, increased numbers of memory cells 4 wk following immunization, and enhanced antilisterial protection following a challenge infection. Initiation of antibiotic treatment 24 h following infection with wild-type Lm markedly reduced the magnitude of the effector CD8 T cell response. In contrast, antibiotic treatment initiated 24 h following immunization with the hyperantigen secreting strain of Lm did not impact the frequency of the target-Ag specific CD8 T cells. Thus, immunization with a low dose of a hyperantigen secreting Lm strain, followed by antibiotic treatment to limit the extent of the infection, may represent a safe strategy for the stimulation of enhanced effector CD8 T cell responses to specific Ag by a rLm vaccine.

摘要

单核细胞增生李斯特菌(Lm)的胞内复制微环境有助于将细菌衍生的抗原递送至MHC I类途径,进而刺激CD8效应T细胞。我们使用了体内毒力相当但保护性靶抗原分泌水平存在显著差异的Lm菌株,评估了这些分泌水平的特定差异如何影响Lm注射后抗原特异性CD8 T细胞反应的强度和效应功能。与相同剂量野生型Lm免疫后刺激的强度相比,低剂量高抗原分泌Lm菌株免疫刺激了增强的靶抗原特异性CD8 T细胞反应。体内CTL活性、免疫后4周记忆细胞数量增加以及攻击感染后抗李斯特菌保护增强也表明了增强的决定簇特异性反应。野生型Lm感染后24小时开始抗生素治疗显著降低了效应CD8 T细胞反应的强度。相比之下,高抗原分泌Lm菌株免疫后24小时开始抗生素治疗并不影响靶抗原特异性CD8 T细胞的频率。因此,低剂量高抗原分泌Lm菌株免疫,随后进行抗生素治疗以限制感染程度,可能是一种通过重组Lm疫苗刺激增强的效应CD8 T细胞对特定抗原反应的安全策略。

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