Wakefield Lalage M, Stuelten Christina
Lab of Cancer Biology and Genetics, Center for Cancer Research, National Cancer Institute, Bethesda, MD 20892, USA.
Cancer Cell. 2007 Oct;12(4):293-5. doi: 10.1016/j.ccr.2007.10.002.
TGFbetas are thought to have tumor suppressor activity in many organ systems, but receptor inactivation in mouse models has not previously resulted in increased spontaneous tumorigenesis. A study in this issue of Cancer Cell shows that mice with a targeted knockout of the type II TGFbeta receptor in stratified epithelia specifically develop spontaneous squamous cell carcinomas in the anogenital region, but not in the skin. Loss of TGFbeta signaling appears to destabilize the epithelium such that homeostasis fails in the face of persistent proliferative challenge, a normal feature of the anogenital site, and latent invasive and migratory phenotypes are unmasked.
转化生长因子β(TGFβ)在许多器官系统中被认为具有肿瘤抑制活性,但在小鼠模型中,受体失活以前并未导致自发肿瘤发生增加。本期《癌细胞》杂志上的一项研究表明,在分层上皮中靶向敲除II型TGFβ受体的小鼠,会在肛门生殖器区域特异性地发生自发鳞状细胞癌,但在皮肤中不会。TGFβ信号的缺失似乎会破坏上皮的稳定性,以至于在面对持续的增殖挑战(这是肛门生殖器部位的正常特征)时,内环境稳态遭到破坏,潜在的侵袭和迁移表型被暴露出来。
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