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Dendritic cells: are they clinically relevant?

机译:树突状细胞:它们在临床上相关吗?

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Cancer vaccines have undergone a renaissance because of recent clinical trials showing promising immunologic data and some clinical benefit to patients. Current trials exploiting dendritic cells (DCs) as vaccines have shown durable tumor regressions in a fraction of patients. Clinical efficacy of current vaccines is hampered by myeloid-derived suppressor cells, inflammatory type 2 T cells, and regulatory T cells, all of which prevent the generation of effector cells. To improve the clinical efficacy of DC vaccines, we need to design novel and improved strategies that can boost adaptive immunity to cancer, help overcome regulatory T cells and allow the breakdown of the immunosuppressive tumor microenvironment. This can be achieved by exploiting the fast increasing knowledge about the DC system, including the existence of distinct DC subsets. Critical to the design of better vaccines is the concept of distinct DC subsets and distinct DC activation pathways, all contributing to the generation of unique adaptive immune responses. Such novel DC vaccines will be used as monotherapy in patients with resected disease and in combination with antibodies and/or drugs targeting suppressor pathways and modulation of the tumor environment in patients with metastatic disease.
机译:由于最近的临床试验显示出有希望的免疫学数据以及对患者有一定的临床益处,因此癌症疫苗已经复兴。利用树突状细胞(DC)作为疫苗的最新试验表明,一部分患者会出现持久的肿瘤消退。当前疫苗的临床功效受到髓样来源的抑制细胞,2型炎症性T细胞和调节性T细胞的阻碍,所有这些都阻止了效应细胞的产生。为了提高DC疫苗的临床疗效,我们需要设计新颖且经过改进的策略,以增强针对癌症的适应性免疫力,帮助克服调节性T细胞并破坏免疫抑制性肿瘤微环境。这可以通过利用有关DC系统的快速增长的知识来实现​​,包括不同DC子集的存在。设计更好的疫苗的关键是不同DC子集和不同DC激活途径的概念,所有这些都有助于产生独特的适应性免疫应答。这样的新型DC疫苗将被用作在切除的疾病患者中的单一疗法,并与靶向抑制因子途径和转移性疾病患者的肿瘤环境调节的抗体和/或药物联合使用。

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