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在转移经P815AB脉冲处理的树突状细胞后,白细胞介素-12对于启动T细胞对I类限制性肿瘤肽(P815AB)的反应性而言既是必需的也是充分的。

IL-12 is both required and sufficient for initiating T cell reactivity to a class I-restricted tumor peptide (P815AB) following transfer of P815AB-pulsed dendritic cells.

作者信息

Bianchi R, Grohmann U, Belladonna M L, Silla S, Fallarino F, Ayroldi E, Fioretti M C, Puccetti P

机构信息

Department of Experimental Medicine, University of Perugia, Italy.

出版信息

J Immunol. 1996 Aug 15;157(4):1589-97.

PMID:8759743
Abstract

Delayed-type hypersensitivity responses, mediated by CD8+ cells and detected by skin test assay, occur in sensitized mice in response to challenge with a class I-restricted synthetic peptide related to a poorly immunogenic tumor rejection Ag, P815AB, of murine mastocytoma cells. Efficient priming for this response, which requires functional CD4+ cells and production of IFN-gamma in the host, is achieved by transfer of dendritic cells (DC) pulsed in vitro with a physical mixture of P815AB and T helper peptides, such as a class II-restricted synthetic peptide of tetanus toxin. We now show that the adjuvant effect of the T helper peptide was associated with the appearance of early and late IL-12 transcripts in the spleens of DC recipient mice, correlated with a late IFN-gamma response, and was negated by serologic ablation of endogenous IL-12 at the time of cell transfer. rIL-12, administered in vivo to the DC recipient mice, could substitute for the T helper peptide in initiating skin test reactivity following transfer of DC pulsed with P815AB alone, leading to Ag-specific production of IFN-gamma by CD4+ and CD8+ T cells. In vitro and in vivo cell depletion experiments suggested the following: 1) the exogenous IL-12 required both CD4+ and CD8+ cells for activity; 2) the immune response initiated by IL-12 relied on later production of IL-12 by the host; and 3) the early adjuvanticity of the exogenous IL-12 involved improved recognition of class II-restricted epitopes of this otherwise poorly immunogenic tumor peptide.

摘要

迟发型超敏反应由CD8 +细胞介导,通过皮肤试验检测,在致敏小鼠中,针对与小鼠肥大细胞瘤细胞免疫原性较差的肿瘤排斥抗原P815AB相关的I类限制性合成肽进行攻击时会出现。这种反应的有效启动需要功能性CD4 +细胞和宿主中IFN-γ的产生,通过用P815AB和T辅助肽的物理混合物(如破伤风毒素的II类限制性合成肽)在体外脉冲处理的树突状细胞(DC)转移来实现。我们现在表明,T辅助肽的佐剂作用与DC受体小鼠脾脏中早期和晚期IL-12转录本的出现相关,与晚期IFN-γ反应相关,并且在细胞转移时通过血清学消除内源性IL-12而被消除。在体内给予DC受体小鼠的rIL-12可以替代T辅助肽,在单独用P815AB脉冲处理的DC转移后启动皮肤试验反应性,导致CD4 +和CD8 + T细胞产生Ag特异性IFN-γ。体外和体内细胞耗竭实验表明如下:1)外源性IL-12的活性需要CD4 +和CD8 +细胞;2)由IL-12引发的免疫反应依赖于宿主后来产生的IL-12;3)外源性IL-12的早期佐剂作用涉及改善对这种免疫原性较差的肿瘤肽的II类限制性表位的识别。

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IL-12 is both required and sufficient for initiating T cell reactivity to a class I-restricted tumor peptide (P815AB) following transfer of P815AB-pulsed dendritic cells.在转移经P815AB脉冲处理的树突状细胞后,白细胞介素-12对于启动T细胞对I类限制性肿瘤肽(P815AB)的反应性而言既是必需的也是充分的。
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Clin Exp Immunol. 2000 Aug;121(2):216-25. doi: 10.1046/j.1365-2249.2000.01293.x.
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A long-lasting interferon-gamma response is induced to a single inoculation of antigen-pulsed dendritic cells.单次接种抗原脉冲树突状细胞可诱导产生持久的γ干扰素反应。
Immunology. 1998 Sep;95(1):132-40. doi: 10.1046/j.1365-2567.1998.00546.x.