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In vitro reconstitution of heat shock protein-peptide complexes for generating peptide-specific vaccines against cancers and infectious diseases.

机译:热休克蛋白-肽复合物的体外重建,以产生针对癌症和传染病的肽特异性疫苗。

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摘要

Known commonly as molecular chaperones for proteins, heat shock proteins (HSPs) have also been found to chaperone small molecular weight cellular peptides. HSP-peptide complexes can prime T cell immunity specific against the peptides bound to HSPs, but not against HSPs per se. This immunomodulatory functions of HSPs are based on two intrinsic properties. One, HSPs are excellent adjuvants due to their ability to activate dendritic cells (DCs). Two, HSPs can bind directly to their receptors on DCs to then channel HSP-associated peptides to associate with MHC molecules. When a specific antigenic peptide is defined, this peptide can also be complexed with either tissue derived or recombinant HSPs in vitro to generate HSP-peptide complexes as peptide-specific vaccines. This article focuses on the methods commonly used to reconstitute HSP-peptide complexes, and discusses assays to verify the efficiency of complexing for immunotherapy against cancers and infectious diseases.
机译:通常被称为蛋白质的分子伴侣,热激蛋白(HSP)也被发现可以伴侣小分子细胞肽。 HSP-肽复合物可以引发针对结合于HSP的肽特异的T细胞免疫性,而不是针对本身的HSP。 HSP的这种免疫调节功能基于两个固有特性。第一,HSP由于其激活树突状细胞(DC)的能力而成为极好的佐剂。第二,HSP可以直接与其DC上的受体结合,然后引导HSP相关肽与MHC分子缔合。当定义了特定的抗原肽时,该肽也可以在体外与组织衍生的HSP或重组HSP进行复合,以生成HSP肽复合物作为肽特异性疫苗。本文着重介绍通常用于重组HSP肽复合物的方法,并讨论了用于验证复合物对癌症和传染病进行免疫治疗的效率的测定方法。

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