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LRP6 外显结构域的结构和功能研究揭示了 Wnt 信号的一个平台。

Structural and functional studies of LRP6 ectodomain reveal a platform for Wnt signaling.

机构信息

Division of Structural Biology, Wellcome Trust Centre for Human Genetics, University of Oxford, Roosevelt Drive, Oxford OX3 7BN, UK.

出版信息

Dev Cell. 2011 Nov 15;21(5):848-61. doi: 10.1016/j.devcel.2011.09.007. Epub 2011 Oct 13.

Abstract

LDL-receptor-related protein 6 (LRP6), alongside Frizzled receptors, transduces Wnt signaling across the plasma membrane. The LRP6 ectodomain comprises four tandem β-propeller-EGF-like domain (PE) pairs that harbor binding sites for Wnt morphogens and their antagonists including Dickkopf 1 (Dkk1). To understand how these multiple interactions are integrated, we combined crystallographic analysis of the third and fourth PE pairs with electron microscopy (EM) to determine the complete ectodomain structure. An extensive inter-pair interface, conserved for the first-to-second and third-to-fourth PE interactions, contributes to a compact platform-like architecture, which is disrupted by mutations implicated in developmental diseases. EM reconstruction of the LRP6 platform bound to chaperone Mesd exemplifies a binding mode spanning PE pairs. Cellular and binding assays identify overlapping Wnt3a- and Dkk1-binding surfaces on the third PE pair, consistent with steric competition, but also suggest a model in which the platform structure supports an interplay of ligands through multiple interaction sites.

摘要

低密度脂蛋白受体相关蛋白 6(LRP6)与卷曲受体一起,在质膜上转导 Wnt 信号。LRP6 的胞外域包含四个串联的β-螺旋桨-表皮生长因子样结构域(PE)对,这些结构域含有 Wnt 形态发生素及其拮抗剂(包括 Dickkopf 1(Dkk1))的结合位点。为了了解这些多种相互作用是如何整合的,我们结合了第三和第四 PE 对的晶体学分析和电子显微镜(EM)来确定完整的胞外域结构。广泛的对-对界面,对于第一到第二和第三到第四 PE 相互作用都是保守的,有助于形成一个紧凑的平台样结构,而这种结构被与发育性疾病相关的突变所破坏。LRP6 平台与 Mesd 伴侣结合的 EM 重建示例了一个跨越 PE 对的结合模式。细胞和结合测定确定了第三个 PE 对上重叠的 Wnt3a 和 Dkk1 结合表面,这与空间位阻竞争一致,但也提出了一个模型,其中平台结构通过多个相互作用位点支持配体的相互作用。

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