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A paradigm shift: Cancer therapy with peptide-based B-cell epitopes and peptide immunotherapeutics targeting multiple solid tumor types: Emerging concepts and validation of combination immunotherapy

机译:范式转变:针对多种实体瘤类型的基于肽的B细胞表位和肽免疫疗法的癌症治疗:新兴概念和联合免疫疗法的验证

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摘要

There is a recognizable and urgent need to speed the development and application of novel, more efficacious anti-cancer vaccine therapies that inhibit tumor progression and prevent acquisition of tumor resistance. We have created and established a portfolio of validated peptide epitopes against multiple receptor tyrosine kinases and we have identified the most biologically effective combinations of EGFR (HER-1), HER-2, HER-3, VEGF and IGF-1R peptide vaccines/mimics to selectively inhibit multiple receptors and signaling pathways. The strategy is based on the use of chimeric conformational B-cell epitope peptides incorporating promiscuous T-cell epitopes that afford the possibility of generating an enduring immune response, eliciting protein-reactive high-affinity anti-peptide antibodies as potential vaccines and peptide mimics that act as antagonists to receptor signaling that drive cancer metastasis. In this review we will summarize our ongoing studies based on the development of combinatorial immunotherapeutic strategies that act synergistically to enhance immune-mediated tumor killing aimed at addressing mechanisms of tumor resistance for several tumor types.
机译:迫在眉睫的是,迫切需要加快新型和更有效的抗癌疫苗疗法的开发和应用,这些疗法可以抑制肿瘤的进展并防止获得肿瘤的耐药性。我们创建并建立了针对多种受体酪氨酸激酶的经过验证的肽表位组合,并确定了EGFR(HER-1),HER-2,HER-3,VEGF和IGF-1R肽疫苗/模拟物的最生物有效组合选择性抑制多种受体和信号通路。该策略基于结合有混杂T细胞表位的嵌合构象B细胞表位肽的使用,这些肽提供了产生持久免疫应答的可能性,引发了蛋白反应性高亲和力抗肽抗体作为潜在的疫苗和类似肽充当驱动癌症转移的受体信号转导的拮抗剂。在这篇综述中,我们将基于组合免疫治疗策略的发展来总结我们正在进行的研究,该策略协同作用以增强免疫介导的肿瘤杀伤作用,旨在解决几种肿瘤类型的肿瘤抗性机制。

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