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首页> 外文期刊>Differentiation: The Journal of the International Society of Differentiation >The tumor microenvironment: a potential arbitrator of the tumor suppressive and promoting actions of TGFbeta.
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The tumor microenvironment: a potential arbitrator of the tumor suppressive and promoting actions of TGFbeta.

机译:肿瘤微环境:TGFbeta抑制和促进肿瘤作用的潜在仲裁者。

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摘要

Transforming growth factor beta (TGFbeta) members are secreted in biologically inactive complexes that must be activated in order to enable binding to their cell surface receptors. Interestingly, many of the proteins that can activate TGFbeta have been implicated in either suppressing or promoting tumorigenesis. Included among these are matrix proteins (thrombospondin-1), receptors (integrins alphanubeta6 and alphanubeta8) and proteases (matrix metalloproteases and plasmin). These proteins cannot only activate TGFbeta, but can also modulate cell responsiveness to TGFbeta. In this section, we review data highlighting the complexity and bidirectionality of TGFbeta matrix interactions within the tumor microenvironment, and propose that these dynamic interactions are a critical spatial and temporal determinant of the effects of TGFbeta on tumorigenesis.
机译:转化生长因子β(TGFbeta)成员被分泌在必须激活才能使其细胞表面受体结合的生物惰性复合物中。有趣的是,许多可以激活TGFβ的蛋白质都与抑制或促进肿瘤发生有关。其中包括基质蛋白(血小板反应蛋白1),受体(整联蛋白alphanubeta6和alphanubeta8)和蛋白酶(基质金属蛋白酶和纤溶酶)。这些蛋白质不仅可以激活TGFbeta,而且可以调节细胞对TGFbeta的反应性。在本节中,我们回顾了突出肿瘤微环境中TGFbeta基质相互作用的复杂性和双向性的数据,并提出这些动态相互作用是TGFbeta对肿瘤发生作用的关键时空决定因素。

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