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The dual adverse effects of TGF-beta secretion on tumor progression.

机译:TGF-β分泌对肿瘤进展的双重不良影响。

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摘要

When a cancer escapes the growth-inhibitory effects of TGF-beta secreted by cancer cells themselves or by cells in the local stroma, a further adverse outcome for the host is the associated TGF-beta-induced suppression of anticancer T cell immunity. In addition to the previously described dampening of T cell activation and proliferation, TGF-beta markedly and directly suppresses the transcription of genes encoding multiple key proteins of the "cytotoxic program" of CD8+ CTL, such as perforin and granzymes, cytotoxins that act through the granule exocytosis pathway. The findings described below suggest that TGF-beta and its signaling pathways will be major targets for novel cancer therapeutics.
机译:当癌症摆脱了癌细胞本身或局部基质细胞分泌的TGF-β的生长抑制作用时,宿主的另一不利后果是相关的TGF-β诱导的抗癌T细胞免疫抑制作用。除了先前描述的抑制T细胞活化和增殖的功能外,TGF-β还可以显着并直接抑制编码CD8 + CTL的“细胞毒性程序”的多个关键蛋白的基因的转录,这些蛋白例如穿孔素和颗粒酶,通过该蛋白起作用的细胞毒素。颗粒胞吐途径。下述发现表明,TGF-β及其信号传导途径将成为新型癌症治疗的主要靶标。

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