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通过非特异性炎症刺激挽救CD8 T细胞介导的抗微生物免疫。

Rescue of CD8 T cell-mediated antimicrobial immunity with a nonspecific inflammatory stimulus.

作者信息

Tuma Roman A, Giannino Rielle, Guirnalda Patrick, Leiner Ingrid, Pamer Eric G

机构信息

Infectious Disease Service, Department of Medicine and Immunology Program, Memorial Sloan-Kettering Institute, New York, New York 10021, USA.

出版信息

J Clin Invest. 2002 Nov;110(10):1493-501. doi: 10.1172/JCI16356.

Abstract

Reconstitution of protective immunity by adoptive transfer of pathogen-specific T cells has been successful in patients with compromised cellular immunity. The in vivo effectiveness of in vitro-expanded CD8 CTLs is variable, however. For example, adoptively transferred Listeria monocytogenes-specific CD8 CTLs only confer protective immunity if challenge infection occurs within 48 hours of T cell infusion. Herein we show that transferred CTLs persist in lymphoid compartments for many weeks, but that their response to bacterial challenge decreases during the first week following transfer. While T cells transferred less than 48 hours before infection proliferate, those transferred 7 days before infection die. Remarkably, treatment of mice with anti-CD40 at the time of T cell infusion reprograms transferred T cells, allowing them to proliferate and confer protective immunity upon bacterial challenge 7 days later. Our study demonstrates, for the first time to our knowledge that CD40-mediated stimuli can influence CD8 T cell activation independent of concurrent antigen exposure. The ability to modulate long-term responsiveness of CD8 T cells with a transient, nonspecific inflammatory stimulus has importation implications for adoptive immunotherapy.

摘要

通过过继转移病原体特异性T细胞来重建保护性免疫,在细胞免疫受损的患者中已取得成功。然而,体外扩增的CD8细胞毒性T淋巴细胞(CTL)在体内的有效性存在差异。例如,过继转移的单核细胞增生李斯特菌特异性CD8 CTL只有在T细胞输注后48小时内发生激发感染时才会赋予保护性免疫。在此我们表明,转移的CTL在淋巴区室中持续存在数周,但它们对细菌攻击的反应在转移后的第一周内会降低。虽然在感染前不到48小时转移的T细胞会增殖,但在感染前7天转移的T细胞会死亡。值得注意的是,在T细胞输注时用抗CD40治疗小鼠可对转移的T细胞进行重编程,使其增殖并在7天后的细菌攻击时赋予保护性免疫。据我们所知,我们的研究首次证明CD40介导的刺激可独立于同时存在的抗原暴露影响CD8 T细胞活化。用短暂的、非特异性炎症刺激调节CD8 T细胞长期反应性的能力对过继免疫疗法具有重要意义。

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