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Innate immune sensing of cancer: Clues from an identified role for type I IFNs

机译:癌症的先天免疫感知:I型干扰素的确定作用线索

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A subset of patients with a variety of cancers shows evidence of a natural adaptive immune response against their tumor, as evidenced by spontaneous T-cell infiltration, circulating anti-Tumor T cells, or antibody responses. Evidence has indicated that such natural immune responses have positive prognostic import in early stage disease and may be predictive of clinical response to immunotherapeutics in advanced disease. However, these observations raise a new critical fundamental question- what innate immune signals might be generated in the context of non-pathogen-induced cancers that drive productive antigen presentation toward induction of an adaptive immune response? Gene expression profiling in melanoma revealed that tumors having high expression of T-cell markers also show evidence of a type I IFN transcriptional signature. Mechanistic experiments in mice have revealed that a spontaneous CD8+ T-cell response against transplantable tumors depends on host type I IFN signaling, through a mechanism dependent upon CD8a? dendritic cells (DCs). The requirement for type I IFN production by host DCs has suggested a subset of innate immune sensing receptors and signaling pathways that might be involved with initiating this process. Elucidating further these innate immune mechanisms should provide new insights into cancer immunotherapy.
机译:一部分患有多种癌症的患者显示出针对其肿瘤的自然适应性免疫反应的证据,如自发性T细胞浸润,循环性抗肿瘤T细胞或抗体反应所证明。有证据表明,这种天然免疫反应在早期疾病中具有积极的预后意义,并且可以预测晚期疾病对免疫疗法的临床反应。但是,这些发现提出了一个新的关键性基本问题:在非病原体诱导的癌症中,哪些驱动力将生产性抗原呈递给适应性免疫应答,会产生哪些先天免疫信号?黑色素瘤中的基因表达谱分析表明,具有T细胞标记物高表达的肿瘤也显示出I型IFN转录特征的证据。小鼠的机械实验表明,针对可移植肿瘤的自发性CD8 + T细胞应答取决于宿主I型IFN信号传导,其机制依赖于CD8a?树突状细胞(DC)。宿主DC对I型IFN产生的要求表明,可能与启动此过程有关的先天性免疫传感受体和信号传导途径的子集。进一步阐明这些先天免疫机制应为癌症免疫疗法提供新的见解。

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