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非人灵长类动物中的ErbB2基因癌症疫苗:单核苷酸多态性的相关性

ErbB2 genetic cancer vaccine in nonhuman primates: relevance of single nucleotide polymorphisms.

作者信息

Fattori Elena, Aurisicchio Luigi, Zampaglione Immacolata, Arcuri Mirko, Cappelletti Manuela, Cipriani Barbara, Mennuni Carmela, Calvaruso Francesco, Nuzzo Maurizio, Ciliberto Gennaro, Monaci Paolo, La Monica Nicola

机构信息

Istituto di Ricerca di Biologia Molecolare, Via Pontina, Pomezia, Italy.

出版信息

Hum Gene Ther. 2009 Mar;20(3):253-65. doi: 10.1089/hum.2008.153.

Abstract

Aberrant Her2/neu expression is associated with the development of epithelial-derived human carcinomas and for this reason it is considered a good target for immunologic intervention. To define methods to circumvent immunologic tolerance and to elicit immunity against the Her2/neu tumor-associated antigen in a suitable animal model, we have isolated the cDNA encoding the rhesus monkey homolog of human Her2/neu (RhErbB2) to construct DNA plasmids and adenoviral vectors for the development of a cancer vaccine against this protein. To further increase the immunogenic potency of these vectors, a synthetic codon-optimized RhErbB2 cDNA (RhErbB2OPT) was constructed and characterized. Genetic vaccination of rhesus monkeys was effective in inducing a response against RhErbB2 in immunized animals; importantly, the elicited immunity was associated with natural RhErbB2 polymorphisms, thus distinguishing responses against "self " and "nonself " epitopes. In particular, the postpriming response recognized mainly nonself epitopes whereas the boosted response cross-reacted with self epitopes. Our findings are particularly relevant in the investigation of the impact of TAA polymorphisms on the efficacy of a cancer vaccine strategy.

摘要

异常的Her2/neu表达与上皮来源的人类癌症的发生发展相关,因此它被认为是免疫干预的一个良好靶点。为了确定在合适的动物模型中规避免疫耐受并引发针对Her2/neu肿瘤相关抗原的免疫的方法,我们分离了编码人类Her2/neu恒河猴同源物(RhErbB2)的cDNA,以构建DNA质粒和腺病毒载体,用于开发针对该蛋白的癌症疫苗。为了进一步提高这些载体的免疫原性效力,构建并表征了一个合成的密码子优化的RhErbB2 cDNA(RhErbB2OPT)。恒河猴的基因疫苗接种有效地诱导了免疫动物对RhErbB2的反应;重要的是,引发的免疫与天然RhErbB2多态性相关,从而区分了对“自身”和“非自身”表位的反应。特别是,初次免疫后的反应主要识别非自身表位,而加强免疫后的反应与自身表位发生交叉反应。我们的发现对于研究肿瘤相关抗原多态性对癌症疫苗策略疗效的影响尤为重要。

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