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糖皮质激素化合物可改变平滑蛋白的定位和刺猬信号通路活性。

Glucocorticoid compounds modify smoothened localization and hedgehog pathway activity.

作者信息

Wang Yu, Davidow Lance, Arvanites Anthony C, Blanchard Joel, Lam Kelvin, Xu Ke, Oza Vatsal, Yoo Jin Woo, Ng Jessica M Y, Curran Tom, Rubin Lee L, McMahon Andrew P

机构信息

Department of Stem Cell and Regenerative Biology, Harvard University, Cambridge, MA 02138, USA.

出版信息

Chem Biol. 2012 Aug 24;19(8):972-82. doi: 10.1016/j.chembiol.2012.06.012.

Abstract

The Hedgehog signaling pathway is linked to a variety of diseases, notably a range of cancers. The first generation of drug screens identified Smoothened (Smo), a membrane protein essential for signaling, as an attractive drug target. Smo localizes to the primary cilium upon pathway activation, and this transition is critical for the response to Hedgehog ligands. In a high content screen directly monitoring Smo distribution in Hedgehog-responsive cells, we identified different glucocorticoids as specific modulators of Smo ciliary accumulation. One class promoted Smo accumulation, conferring cellular hypersensitivity to Hedgehog stimulation. In contrast, a second class inhibited Smo ciliary localization and signaling activity by both wild-type Smo, and mutant forms of Smo, SmoM2, and SmoD473H, that are refractory to previously identified Smo antagonists. These findings point to the potential for developing glucocorticoid-based pharmacological modulation of Smo signaling to treat mutated drug-resistant forms of Smo, an emerging problem in long-term cancer therapy. They also raise a concern about potential crosstalk of glucocorticoid drugs in the Hedgehog pathway, if therapeutic administration exceeds levels associated with on-target transcriptional mechanisms of glucocorticoid action.

摘要

刺猬信号通路与多种疾病相关,尤其是一系列癌症。第一代药物筛选将平滑肌瘤(Smo)确定为一种对信号传导至关重要的膜蛋白,是一个有吸引力的药物靶点。通路激活后,Smo定位于初级纤毛,这种转变对于对刺猬配体的反应至关重要。在一项直接监测刺猬反应性细胞中Smo分布的高内涵筛选中,我们确定了不同的糖皮质激素是Smo纤毛积累的特异性调节剂。一类促进Smo积累,使细胞对刺猬刺激产生超敏反应。相比之下,另一类通过野生型Smo以及Smo的突变形式SmoM2和SmoD473H抑制Smo的纤毛定位和信号活性,而这些突变形式对先前确定的Smo拮抗剂具有抗性。这些发现表明,有可能开发基于糖皮质激素的Smo信号药理调节方法来治疗Smo的突变耐药形式,这是长期癌症治疗中出现的一个新问题。它们还引发了一个担忧,即如果治疗给药超过与糖皮质激素作用的靶向转录机制相关的水平,糖皮质激素药物在刺猬通路中可能存在潜在的串扰。

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