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在实验性鸟分枝杆菌感染的免疫治疗和疫苗设计中对白细胞介素-12的评估。

Evaluation of IL-12 in immunotherapy and vaccine design in experimental Mycobacterium avium infections.

作者信息

Silva R A, Pais T F, Appelberg R

机构信息

Laboratory of Microbiology and Immunology of Infection, Institute for Molecular and Cell Biology, University of Porto, Portugal.

出版信息

J Immunol. 1998 Nov 15;161(10):5578-85.

PMID:9820535
Abstract

IL-12 is a pivotal cytokine in the induction of IFN-gamma-mediated protective immune responses. We tested the effects of rIL-12 administration to Mycobacterium avium-infected mice and found a limited ability to induce protection against the infection; this ability varied according to the mycobacterial strain studied. IL-12 accelerated the expression and production of IFN-gamma in both immunocompetent and immunodeficient SCID or CD4-depleted mice. Evidence of NK cell activation was found as well as an enhancement of the ability to adoptively transfer resistance with T cell-enriched spleen cell populations and an increase in inflammatory cell recruitment in the liver. The protective ability of IL-12 was dependent upon the endogenous production of IFN-gamma as evaluated by the use of specific neutralizing Abs or IFN-gamma gene-disrupted mice. IL-12 potentiated the protective immunity conferred by a subunit vaccine containing M. avium culture filtrate proteins and dimethyl dioctadecyl ammonium chloride as an adjuvant. Thus, we show limited immunotherapeutic benefits from IL-12 administration in M. avium infections and promising results in its use as a coadjuvant in vaccine design.

摘要

白细胞介素-12是诱导干扰素-γ介导的保护性免疫反应中的一种关键细胞因子。我们测试了给感染鸟分枝杆菌的小鼠施用重组白细胞介素-12的效果,发现其诱导抗感染保护的能力有限;这种能力因所研究的分枝杆菌菌株而异。白细胞介素-12在免疫功能正常以及免疫缺陷的重症联合免疫缺陷(SCID)或CD4缺失小鼠中均加速了干扰素-γ的表达和产生。发现了自然杀伤细胞激活的证据,以及用富含T细胞的脾细胞群体过继转移抗性的能力增强,并且肝脏中炎症细胞募集增加。通过使用特异性中和抗体或干扰素-γ基因敲除小鼠评估发现,白细胞介素-12的保护能力依赖于内源性干扰素-γ的产生。白细胞介素-12增强了由含有鸟分枝杆菌培养滤液蛋白和二甲基二十八烷基氯化铵作为佐剂的亚单位疫苗所赋予的保护性免疫。因此,我们表明在鸟分枝杆菌感染中施用白细胞介素-12的免疫治疗益处有限,而其作为疫苗设计中的辅助佐剂则有令人期待的结果。

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