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Heat Shock Protein–Peptide and HSP-Based Immunotherapies for the Treatment of Cancer

机译:热休克蛋白肽和基于HSP的免疫疗法可治疗癌症

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摘要

Intracellular residing heat shock proteins (HSPs) with a molecular weight of approximately 70 and 90 kDa function as molecular chaperones that assist folding/unfolding and transport of proteins across membranes and prevent protein aggregation after environmental stress. In contrast to normal cells, tumor cells have higher cytosolic heat shock protein 70 and Hsp90 levels, which contribute to tumor cell propagation, metastasis, and protection against apoptosis. In addition to their intracellular chaperoning functions, extracellular localized and membrane-bound HSPs have been found to play key roles in eliciting antitumor immune responses by acting as carriers for tumor-derived immunogenic peptides, as adjuvants for antigen presentation, or as targets for the innate immune system. The interaction of HSP–peptide complexes or peptide-free HSPs with receptors on antigen-presenting cells promotes the maturation of dendritic cells, results in an upregulation of major histocompatibility complex class I and class II molecules, induces secretion of pro- and anti-inflammatory cytokines, chemokines, and immune modulatory nitric oxides, and thus integrates adaptive and innate immune phenomena. Herein, we aim to recapitulate the history and current status of HSP-based immunotherapies and vaccination strategies in the treatment of cancer.
机译:分子量大约为70和90 kDa的细胞内热激蛋白(HSP)充当分子伴侣,可帮助蛋白质折叠/展开和跨膜运输,并防止环境胁迫后蛋白质聚集。与正常细胞相比,肿瘤细胞具有更高的胞质热休克蛋白70和Hsp90水平,这有助于肿瘤细胞的繁殖,转移和防止凋亡。除了其细胞内伴侣功能外,还发现细胞外局部和膜结合的HSP通过充当肿瘤来源的免疫原性肽的载体,抗原呈递的佐剂或先天性靶标,在引发抗肿瘤免疫反应中起关键作用。免疫系统。 HSP肽复合物或无肽HSP与抗原呈递细胞上的受体的相互作用促进树突状细胞的成熟,导致主要的组织相容性复合物I类和II类分子上调,诱导促炎性和抗炎性分泌细胞因子,趋化因子和免疫调节型一氧化氮,因此整合了适应性免疫和先天性免疫现象。在本文中,我们旨在概述基于HSP的免疫疗法和疫苗接种策略在癌症治疗中的历史和现状。

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