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Multipeptide vaccination in cancer patients.

机译:癌症患者的多肽疫苗接种。

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Since the identification of tumor associated antigens (TAA) in different tumor histotypes, many vaccination strategies have been investigated, including peptide-based vaccines. Results from the first decade of clinical experimentation, though demonstrating the feasibility and the good toxicity profile of this approach, provided evidence of clinical activity only in a minority of patients, despite inducing immunization in up to 50% of them. In this review, we discuss the different approaches recently developed in order to induce stronger peptide-induced immune-mediated tumor growth control, possibly translating into improved clinical response rates, with specific focus on multipeptide-based anti-cancer vaccines. This strategy offers many advantages, such as the possibility of bypassing tumor heterogeneity and selection of antigen (Ag)-negative clones escaping peptide-specific immune responses, or combining HLA class I- and class II-restricted epitopes, thus eliciting both CD4- and CD8-mediated immune recognition. Notably, advances in Ag discovery technologies permit further optimization of peptide selection, in terms of identification of tumor-specific and unique TAA as well as Ags derived from different tumor microenvironment cell components. With the ultimate goal of combining peptide selection with patient-specific immunogenic profile, peptide based anti-cancer vaccines remain a promising treatment for cancer patients, as attested by of pre-clinical and clinical studies.
机译:由于鉴定了不同肿瘤组织型中的肿瘤相关抗原(TAA),因此已经研究了许多疫苗接种策略,包括基于肽的疫苗。尽管证明了这种方法的可行性和良好的毒性,来自临床实验的前十年的结果提供了仅在少数患者中进行临床活动的证据,尽管其中多达50%进行了免疫接种。在这篇综述中,我们讨论了最近开发的不同方法,以诱导更强的肽诱导的免疫介导的肿瘤生长控制,有可能转化为提高的临床反应率,特别关注基于多肽的抗癌疫苗。该策略具有许多优势,例如绕过肿瘤异质性和选择逃避肽特异性免疫反应的抗原(Ag)阴性克隆,或结合HLA I类和II类限制性抗原决定簇的可能性,从而引发CD4和CD8介导的免疫识别。值得注意的是,在发现肿瘤特异性和独特的TAA以及衍生自不同肿瘤微环境细胞成分的Ags方面,Ag发现技术的进步允许进一步优化肽的选择。临床前和临床研究证明,基于肽选择和患者特异性免疫原性特征的最终目标,基于肽的抗癌疫苗仍然是癌症患者的有前途的治疗方法。

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