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人类热休克蛋白70通过形成复合物和细胞内抗原递呈增强肿瘤抗原呈递,而无需固有免疫信号传导。

Human heat shock protein 70 enhances tumor antigen presentation through complex formation and intracellular antigen delivery without innate immune signaling.

作者信息

Bendz Henriette, Ruhland Sibylle C, Pandya Maya J, Hainzl Otmar, Riegelsberger Stefan, Braüchle Christoph, Mayer Matthias P, Buchner Johannes, Issels Rolf D, Noessner Elfriede

机构信息

Institute of Molecular Immunology, GSF-National Research Center for Environment and Health Klinikum Grosshadern, Ludwig-Maximilians-University, Marchioninistrasse 25, 81377 Munich, Germany.

出版信息

J Biol Chem. 2007 Oct 26;282(43):31688-702. doi: 10.1074/jbc.M704129200. Epub 2007 Aug 7.

DOI:10.1074/jbc.M704129200
PMID:17684010
Abstract

Heat shock proteins (HSPs) have shown promise for the optimization of protein-based vaccines because they can transfer exogenous antigens to dendritic cells and at the same time induce their maturation. Great care must be exercised in interpretating HSP-driven studies, as by-products linked to the recombinant generation of these proteins have been shown to mediate immunological effects. We generated highly purified human recombinant Hsp70 and demonstrated that it strongly enhances the cross-presentation of exogenous antigens resulting in better antigen-specific T cell stimulation. Augmentation of T cell stimulation was a direct function of the degree of complex formation between Hsp70 and peptides and correlated with improved antigen delivery to endosomal compartments. The Hsp70 activity was independent of TAP proteins and was not inhibited by exotoxin A or endosomal acidification. Consequently, Hsp70 enhanced cross-presentation of various antigenic sequences, even when they required different post-uptake processing and trafficking, as exemplified by the tumor antigens tyrosinase and Melan-A/MART-1. Furthermore, Hsp70 enhanced cross-presentation by different antigen-presenting cells (APCs), including dendritic cells and B cells. Importantly, enhanced cross-presentation and antigen-specific T cell activation were observed in the absence of innate signals transmitted by Hsp70. As Hsp70 supports the cross-presentation of different antigens and APCs and is inert to APC function, it may show efficacy in various settings of immune modulation, including induction of antigen-specific immunity or tolerance.

摘要

热休克蛋白(HSPs)已显示出优化基于蛋白质的疫苗的潜力,因为它们可以将外源性抗原传递给树突状细胞,同时诱导其成熟。在解释由HSP驱动的研究时必须格外小心,因为与这些蛋白质的重组产生相关的副产物已被证明可介导免疫效应。我们制备了高度纯化的人重组Hsp70,并证明它能强烈增强外源性抗原的交叉呈递,从而更好地刺激抗原特异性T细胞。T细胞刺激的增强是Hsp70与肽之间复合物形成程度的直接函数,并且与改善的抗原递送至内体区室相关。Hsp70的活性不依赖于TAP蛋白,并且不受外毒素A或内体酸化的抑制。因此,Hsp70增强了各种抗原序列的交叉呈递,即使它们需要不同的摄取后加工和运输,如肿瘤抗原酪氨酸酶和黑色素-A/MART-1所示。此外,Hsp70增强了包括树突状细胞和B细胞在内的不同抗原呈递细胞(APC)的交叉呈递。重要的是,在没有Hsp70传递的先天信号的情况下,观察到交叉呈递增强和抗原特异性T细胞活化。由于Hsp70支持不同抗原和APC的交叉呈递,并且对APC功能无活性,因此它可能在各种免疫调节环境中显示出疗效,包括诱导抗原特异性免疫或耐受。

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