Department of Cell Biology, Harvard Medical School, 240 Longwood Avenue, Boston, MA 02115, USA.
Department of Biological Chemistry and Molecular Pharmacology, Harvard Medical School, 250 Longwood Avenue, Boston, MA 02115, USA.
Cell. 2018 Jul 12;174(2):312-324.e16. doi: 10.1016/j.cell.2018.04.029. Epub 2018 May 24.
The seven-transmembrane-spanning protein Smoothened is the central transducer in Hedgehog signaling, a pathway fundamental in development and in cancer. Smoothened is activated by cholesterol binding to its extracellular cysteine-rich domain (CRD). How this interaction leads to changes in the transmembrane domain and Smoothened activation is unknown. Here, we report crystal structures of sterol-activated Smoothened. The CRD undergoes a dramatic reorientation, allosterically causing the transmembrane domain to adopt a conformation similar to active G-protein-coupled receptors. We show that Smoothened contains a unique inhibitory π-cation lock, which is broken on activation and is disrupted in constitutively active oncogenic mutants. Smoothened activation opens a hydrophobic tunnel, suggesting a pathway for cholesterol movement from the inner membrane leaflet to the CRD. All Smoothened antagonists bind the transmembrane domain and block tunnel opening, but cyclopamine also binds the CRD, inducing the active transmembrane conformation. Together, these results define the mechanisms of Smoothened activation and inhibition.
七跨膜蛋白 Smoothened 是 Hedgehog 信号通路中的核心转导蛋白,该通路在发育和癌症中起着基础性作用。Smoothened 通过胆固醇与其细胞外富含半胱氨酸的结构域(CRD)结合而被激活。这种相互作用如何导致跨膜结构域的变化和 Smoothened 的激活尚不清楚。在这里,我们报告了固醇激活的 Smoothened 的晶体结构。CRD 发生了剧烈的重定向,变构导致跨膜结构域采用与活性 G 蛋白偶联受体相似的构象。我们表明 Smoothened 含有独特的抑制性 π-阳离子锁,该锁在激活时被破坏,并且在组成性激活的致癌突变体中被破坏。Smoothened 的激活打开了一个疏水性隧道,表明胆固醇从内膜小叶到 CRD 的运动途径。所有 Smoothened 拮抗剂都结合跨膜结构域并阻止隧道打开,但环巴胺也结合 CRD,诱导活性跨膜构象。总之,这些结果定义了 Smoothened 激活和抑制的机制。
