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Engineering α-fetoprotein-based gene vaccines to prevent and treat hepatocellular carcinoma: Review and future prospects

机译:工程化基于甲胎蛋白的基因疫苗预防和治疗肝细胞癌的回顾与未来展望

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Activation of a patient's immune system offers an attractive approach to prevent and treat hepatocellular carcinoma (HCC). However, the antitumor efficacy of current HCC vaccines was weak owing to insufficient immune activation of targeting self/tumor antigens. We recently found that epitope-optimized α-fetoprotein effectively activated CD8 T cells and generated potent antitumor effects in the carcinogen-induced autochthonous HCC mouse model. We predict that the same antigen engineering approach of epitope-optimization will enable us to develop effective human vaccines to prevent HCC recurrence after liver resection. The engineered human HCC vaccines may also allow us to identify high-affinity T-cell receptors and antibodies that can be used to reprogram T cells to treat HCC tumors via adoptive transfer.
机译:激活患者免疫系统提供了一种有吸引力的方法来预防和治疗肝细胞癌(HCC)。然而,由于靶向自身/肿瘤抗原的免疫活化不足,当前的HCC疫苗的抗肿瘤功效较弱。我们最近发现,抗原表位优化的α-甲胎蛋白可以有效激活CD8 T细胞,并在致癌物诱导的本地HCC小鼠模型中产生有效的抗肿瘤作用。我们预测,抗原表位优化的相同抗原工程方法将使我们能够开发有效的人类疫苗来预防肝切除术后HCC复发。工程化的人类HCC疫苗也可能使我们能够鉴定出高亲和力的T细胞受体和抗体,这些受体和抗体可用于重新编程设计T细胞,以通过过继转移来治疗HCC肿瘤。

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