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p53-based immunotherapy of cancer. Approaches ro reversing unresponsiveness to T lymphocytes and preventing tumor escape.

机译:基于p53的癌症免疫疗法。可逆转对T淋巴细胞的无反应性并防止肿瘤逃逸。

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Genetic alterations in p53 are common to a wide range of human tumors, including squamous cell carcinomas of the head and neck. Given the need for novel adjuvant therapies for this disease and the renewed interest in immunotherapy as an adjuvant therapy, p53 has become an attractive candidate for vaccines to treat patients. Although p53 is frequently mutated, the remainder of the molecule keeps its wild-type sequence (wt). As a consequence, several nonmutated peptides can be processed from the altered p53 molecules and presented by tumor cells for T cell recognition. Thus, the targeting of wt p53 peptides represents an approach to developing broadly applicable cancer vaccines. Like most things, however, targeting p53 seems more difficult than originally thought. Whether these difficulties can be circumvented remains to be determined. The development of p53-based vaccines over the past decade is reviewed together with the promising initial findings of their clinical introduction.
机译:p53的遗传改变是广泛的人类肿瘤所共有的,包括头颈部鳞状细胞癌。鉴于需要针对这种疾病的新型辅助疗法,以及对免疫疗法作为辅助疗法的新兴趣,p53已成为治疗患者疫苗的有吸引力的候选药物。尽管p53经常发生突变,但分子的其余部分保持其野生型序列(wt)。结果,可以从改变的p53分子中加工出几种未突变的肽,并由肿瘤细胞呈递以识别T细胞。因此,wt p53肽的靶向代表了开发广泛适用的癌症疫苗的方法。但是,像大多数事情一样,靶向p53似乎比原先想象的要困难。是否可以规避这些困难还有待确定。回顾了过去十年中基于p53的疫苗的开发以及其临床引入的有希望的初步发现。

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