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通过编码嵌合的、捕获应激蛋白的肿瘤相关抗原的DNA疫苗引发保护性CD8 T细胞免疫。

Priming protective CD8 T cell immunity by DNA vaccines encoding chimeric, stress protein-capturing tumor-associated antigen.

作者信息

Schirmbeck Reinhold, Riedl Petra, Kupferschmitt Mark, Wegenka Ursula, Hauser Hansjörg, Rice Jason, Kröger Andrea, Reimann Jörg

机构信息

Department of Internal Medicine I, University of Ulm, Ulm, Germany.

出版信息

J Immunol. 2006 Aug 1;177(3):1534-42. doi: 10.4049/jimmunol.177.3.1534.

Abstract

DNA vaccines encoding heat shock protein (hsp)-capturing, chimeric peptides containing antigenic determinants of the tumor-associated Ag (TAA) gp70 (an envelope protein of endogenous retrovirus) primed stable, specific, and tumor-protective CD8 T cell immunity. Expression of gp70 transcripts was detectable in most normal tissues but was particularly striking in some (but not all) tumor cell lines tested (including the adenocarcinoma cell line CT26). An approximately 200 residue gp70 fragment or its L(d)-binding antigenic AH1 peptide cloned in-frame behind an hsp-capturing (cT(272)) or noncapturing (T(60)) N-terminal large SV40 tumor Ag sequence was expressed as either hsp-binding or -nonbinding chimeric Ags. Only hsp-capturing, chimeric fusion proteins were expressed efficiently in transfected cell lines and primed TAA-specific CD8 T cell immunity. This immunity mediated protection in the CT26 and mKSA models. A vaccination strategy based on delivering antigenic, hsp-associated TAA fragments can thus prime protective CD8 T cell immunity even if these TAA are of low intrinsic immunogenicity.

摘要

编码热休克蛋白(hsp)捕获的DNA疫苗,其包含肿瘤相关抗原(TAA)gp70(内源性逆转录病毒的包膜蛋白)抗原决定簇的嵌合肽,可引发稳定、特异且具有肿瘤保护作用的CD8 T细胞免疫。在大多数正常组织中均可检测到gp70转录本的表达,但在某些(并非全部)测试的肿瘤细胞系(包括腺癌细胞系CT26)中表达尤为显著。一个约200个氨基酸残基的gp70片段或其L(d)结合抗原性AH1肽,在热休克蛋白捕获(cT(272))或非捕获(T(60))的N端大SV40肿瘤抗原序列后框内克隆,表达为热休克蛋白结合或非结合的嵌合抗原。只有热休克蛋白捕获的嵌合融合蛋白在转染细胞系中高效表达,并引发TAA特异性CD8 T细胞免疫。这种免疫在CT26和mKSA模型中介导了保护作用。因此,基于递送抗原性、与热休克蛋白相关的TAA片段的疫苗接种策略,即使这些TAA的内在免疫原性较低,也能引发保护性CD8 T细胞免疫。

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