Departments of Internal Medicine and Molecular and Integrative Physiology, Division of Gastroenterology, University of Michigan, United States.
Cancer Treat Rev. 2014 Feb;40(1):12-21. doi: 10.1016/j.ctrv.2013.08.003. Epub 2013 Aug 13.
This review summarizes emerging information regarding the Hedgehog (Hh) signaling pathway during neoplastic transformation in the gastrointestinal tract. Although there is a role for the well-established canonical pathway in which Hedgehog ligands interact with their receptor Patched, there is sufficient evidence that downstream components of the Hh pathway, e.g., Gli1, are hijacked by non-Hh signaling pathways to promote the conversion of the epithelium to dysplasia and carcinoma. We review the canonical pathway and involvement of primary cilia, and then focus on current evidence for Hh signaling in luminal bowel cancers as well as accessory organs, i.e., liver, pancreas and biliary ducts. We conclude that targeting the Hh pathway with small molecules, nutriceuticals and other mechanisms will likely require a combination of inhibitors that target Gli transcription factors in addition to canonical modulators such as Smoothened.
这篇综述总结了 Hedgehog(Hh)信号通路在胃肠道肿瘤形成过程中的最新信息。尽管 Hedgehog 配体与其受体 Patched 相互作用的经典途径发挥了作用,但有充分的证据表明,Hh 信号通路的下游成分,例如 Gli1,被非 Hh 信号通路劫持,以促进上皮向发育不良和癌的转化。我们综述了经典途径和初级纤毛的作用,然后重点关注 Hh 信号在肠道癌症以及附属器官(即肝、胰腺和胆管)中的最新证据。我们得出结论,用小分子、营养药物和其他机制靶向 Hh 途径可能需要组合使用靶向 Gli 转录因子的抑制剂,以及经典调节剂,如 Smoothened。