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Dendritic cells transduced with wild-type p53 gene elicit potent anti-tumour immune responses

机译:野生型p53基因转导的树突状细胞引发有效的抗肿瘤免疫反应

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摘要

In this study we have tested the concept of using wild-type p53 gene for immunotherapy of cancer. Dendritic cells (DC) were transduced with a human wild-type p53 containing recombinant adenovirus (Ad-p53). About a half of DC transduced with this virus expressed p53 protein by FACS analysis 48 h after infection. Mice immunized twice with Ad-p53 DC developed substantial cytotoxic T lymphocyte (CTL) responses against tumour cells expressing wild-type and different mutant human and murine p53 genes. Very low CTL responses were observed against target cells infected with control adenovirus (Ad-c). Immunization with Ad-p53 provided complete tumour protection in 85% of mice challenged with tumour cells expressing human mutant p53 and in 72.7% of mice challenged with tumour cells with murine mutant p53. Treatment with Ad-p53-transduced DC significantly slowed the growth of established tumours. Thus, DC transduced with wild-type p53 may be a promising new tool for the immunotherapy of cancer.
机译:在这项研究中,我们测试了使用野生型p53基因进行癌症免疫治疗的概念。树突细胞(DC)用含有重组腺病毒(Ad-p53)的人类野生型p53进行转导。感染后48小时,通过FACS分析,用该病毒转导的DC约表达p53蛋白。用Ad-p53 DC免疫两次的小鼠对表达野生型和不同突变型人和鼠p53基因的肿瘤细胞产生了实质性的细胞毒性T淋巴细胞(CTL)反应。对于感染了对照腺病毒(Ad-c)的靶细胞,观察到非常低的CTL反应。用Ad-p53免疫可在表达人突变型p53的肿瘤细胞攻击的小鼠中的85%和用鼠突变型p53的肿瘤细胞攻击的72.7%的小鼠中提供完全的肿瘤保护。用Ad-p53转导的DC治疗可显着减慢已建立的肿瘤的生长。因此,用野生型p53转导的DC可能是用于癌症免疫治疗的有前途的新工具。

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