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Breaking Tolerance to Tumors with Dendritic Cell-Based Immunotherapy

机译:用基于树突细胞的免疫疗法打破对肿瘤的耐受性

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Dendritic cells (DC) are the most potent antigen-presenting cells known, capable of priming both naive CD4 and CD8 T lymphocytes. In their immature state DC are especially efficient at ingesting dying cells and processing their antigens while in their mature state DC express high levels of both MHC class I and II antigens as well as a variety of costimulatory molecules needed to induce a primary T cell response. In addition to stimulating adaptive T cell responses, DC can stimulate NK cells and B cells. Their dual role in innate and adaptive immunity led us to explore their potential utility in tumor immunotherapy. The results of clinical trials in which autologous DC loaded with tumor antigen are administered to tumor-bearing patients have been promising, but overall immunologic potency and clinical efficacy have been un-satisfactory. It has become clear that more potent and more efficient DC based immunotherapies are needed, preferably based on in vivo targeting of DC rather than in vitro manipulation followed by systemic administration of the cells. Recent studies in animal models suggest that DC can be loaded with antigen and activated in vivo in a manner that results in potent antitumor immunity. Two approaches to DC targeting are described in this review, both of which have been shown to overcome immune tolerance to tumors and induce dramatic tumor regression.
机译:树突状细胞(DC)是已知最有效的抗原呈递细胞,能够灌注幼稚CD4和CD8 T淋巴细胞。在其未成熟状态下,DC在摄取染色细胞和加工其抗原时特别有效,同时在其成熟状态下表达高水平的MHC I类和II抗原以及诱导初级T细胞应答所需的各种共刺激分子。除了刺激适应性T细胞应答之外,DC可以刺激NK细胞和B细胞。他们在先天和适应症免疫中的双重作用导致我们探讨了肿瘤免疫疗法的潜在效用。临床试验结果,其中施用肿瘤抗原的自体DC的患者对肿瘤患者一直很有前途,但总体免疫效力和临床疗效是不令人满意的。已经清楚地,需要更有效,更高效的直流免疫治疗,优选基于DC的体内靶向而不是体外操纵,然后进行全身施用细胞。最近的动物模型的研究表明DC可以用抗原加载并以导致有效的抗肿瘤免疫力的方式在体内激活。在本综述中描述了两种DC靶向方法,两者都已显示出克服对肿瘤的免疫耐受性并诱导戏剧性肿瘤回归。

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