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哺乳动物非经典 Hedgehog 信号通路中的 Smoothened 依赖性和非依赖性途径。

Smoothened-dependent and -independent pathways in mammalian noncanonical Hedgehog signaling.

机构信息

From the Department of Gastroenterology and Hepatology, Erasmus MC, University Medical Center Rotterdam, PO Box 2040, NL-3000 CA Rotterdam, The Netherlands.

the Department of Biochemistry and Tissue Biology, Biology Institute, University of Campinas, Campinas, São Paulo 13083-862, Brazil.

出版信息

J Biol Chem. 2019 Jun 21;294(25):9787-9798. doi: 10.1074/jbc.RA119.007956. Epub 2019 Apr 16.

Abstract

Hedgehog proteins are pivotal morphogens acting through a canonical pathway involving first activation of ligand binding to Patched followed by alleviation of Smoothened receptor inhibition, leading to activation of Gli transcription factors. Noncanonical Hedgehog signaling remains poorly characterized but is thought to be mainly dependent on Smoothened. However, Smoothened inhibitors have yielded only partial success in combating Hedgehog signal transduction-dependent cancer, suggesting that noncanonical Smoothened-independent pathways also are clinically relevant. Moreover, several Smoothened-dependent effects ( neurite projection) do not require transcriptional activation, further suggesting biological importance of noncanonical Smoothened-dependent pathways. We comprehensively characterized the cellular kinome in Hedgehog-challenged murine WT and Smoothened fibroblasts as well as Smoothened agonist-stimulated cells. A peptide assay-based kinome analysis (in which cell lysates are used to phosphorylate specific kinase substrates), along with endocytosis, Lucifer Yellow-based, and immunoblotting assays, identified an elaborate signaling network of both Smoothened-dependent and -independent pathways that mediates actin reorganization through Src-like kinases, activates various proinflammatory signaling cascades, and concomitantly stimulates Wnt and Notch signaling while suppressing bone morphogenetic protein (BMP) signaling. The contribution of noncanonical Smoothened-independent signaling to the overall effects of Hedgehog on cellular physiology appears to be much larger than previously envisioned and may explain the transcriptionally independent effects of Hedgehog signaling on cytoskeleton. The observation that Patched-dependent, Smoothened-independent, noncanonical Hedgehog signaling increases Wnt/Notch signaling provides a possible explanation for the failure of Smoothened antagonists in combating Hedgehog-dependent but Smoothened inhibitor-resistant cancer. Our findings suggest that inhibiting Hedgehog-Patched interaction could result in more effective therapies as compared with conventional Smoothened-directed therapies.

摘要

刺猬蛋白是重要的形态发生素,通过涉及配体与 patched 首先结合的经典途径发挥作用,随后减轻 smoothened 受体抑制,导致 Gli 转录因子激活。非经典 Hedgehog 信号通路仍未得到充分描述,但被认为主要依赖于 smoothened。然而,smoothened 抑制剂在对抗 Hedgehog 信号转导依赖性癌症方面仅取得部分成功,表明非经典 smoothened 非依赖性途径在临床上也具有相关性。此外,几种 smoothened 依赖性效应(神经突投射)不需要转录激活,进一步表明非经典 smoothened 依赖性途径的生物学重要性。我们全面描述了 Hedgehog 挑战的野生型和 smoothened 成纤维细胞以及 smoothened 激动剂刺激细胞中的细胞激酶组。基于肽测定的激酶组分析(其中细胞裂解物用于磷酸化特定的激酶底物),以及内吞作用、Lucifer Yellow 基于和免疫印迹分析,鉴定了一个复杂的信号网络,包括 smoothened 依赖性和非依赖性途径,通过 Src 样激酶介导肌动蛋白重组,激活各种促炎信号级联,同时刺激 Wnt 和 Notch 信号通路,同时抑制骨形态发生蛋白(BMP)信号通路。非经典 smoothened 非依赖性信号对 Hedgehog 对细胞生理学的整体影响的贡献似乎比以前想象的要大得多,并且可能解释了 Hedgehog 信号对细胞骨架的转录独立效应。观察到 patched 依赖性、smoothened 非依赖性、非经典 Hedgehog 信号增加 Wnt/Notch 信号,为 Smoothened 拮抗剂在对抗 Hedgehog 依赖性但 smoothened 抑制剂抗性癌症方面的失败提供了可能的解释。我们的研究结果表明,与传统的 smoothened 定向治疗相比,抑制 Hedgehog-Patched 相互作用可能导致更有效的治疗方法。

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