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Heat shock protein derived from a non-autologous tumour can be used as an anti-tumour vaccine

机译:来自非自体肿瘤的热休克蛋白可用作抗肿瘤疫苗

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摘要

Antigenic cross-reactivity between certain tumours has allowed the development of more widely applicable, major histocompatibility complex-disparate (allogeneic) whole-cell vaccines. This principle should also allow heat shock proteins (hsp) derived from certain tumours (and carrying cross-reactive antigens) to be used as vaccines to generate anti-tumour immunity in a range of cancer patients. Here, hsp70 derived from gp70-antigen+ B16 melanoma generated cytotoxic-T-lymphocyte-mediated immune protection in BALB/c mice against challenge with gp70-antigen+ CT26 colorectal tumour cells. Using ovalbumin as a model tumour antigen, it is shown that hsp70 enhances peptide re-presentation by dendritic cells via class I over equimolar whole ovalbumin antigen. However, while transfection of tumour cells with inducible hsp70 increases hsp yield from tumours, it does not enhance antigen recognition via purified hsp70 nor via whole cells or their lysate.
机译:某些肿瘤之间的抗原交叉反应性已允许开发更广泛适用的主要组织相容性完全不同的(同种异体)全细胞疫苗。该原理还应允许将源自某些肿瘤(并带有交叉反应性抗原)的热激蛋白(hsp)用作疫苗,以在一系列癌症患者中产生抗肿瘤免疫力。在这里,源自gp70-抗原 + B16黑色素瘤的hsp70在BALB / c小鼠中产生了细胞毒性T淋巴细胞介导的免疫保护,以抵抗gp70-抗原 + CT26结肠直肠肿瘤的攻击细胞。使用卵清蛋白作为模型肿瘤抗原,表明hsp70通过树突状细胞通过I类增强了等摩尔的完整卵清蛋白抗原的肽重新呈递。然而,尽管用可诱导的hsp70转染肿瘤细胞增加了肿瘤的hsp产量,但它不能通过纯化的hsp70或通过全细胞或其裂解物来增强抗原识别。

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