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卷曲蛋白 4 识别 Dishevelled 2 的结构基础揭示了 WNT 信号激活的机制。

Structural basis of Frizzled 4 in recognition of Dishevelled 2 unveils mechanism of WNT signaling activation.

机构信息

Laboratory of Receptor Structure and Signaling, HIT Center for Life Sciences, School of Life Science and Technology, Harbin Institute of Technology, Harbin, China.

School of Life Science and Technology, Harbin Institute of Technology, Harbin, China.

出版信息

Nat Commun. 2024 Sep 2;15(1):7644. doi: 10.1038/s41467-024-52174-z.

Abstract

WNT signaling is fundamental in development and homeostasis, but how the Frizzled receptors (FZDs) propagate signaling remains enigmatic. Here, we present the cryo-EM structure of FZD4 engaged with the DEP domain of Dishevelled 2 (DVL2), a key WNT transducer. We uncover a distinct binding mode where the DEP finger-loop inserts into the FZD4 cavity to form a hydrophobic interface. FZD4 intracellular loop 2 (ICL2) additionally anchors the complex through polar contacts. Mutagenesis validates the structural observations. The DEP interface is highly conserved in FZDs, indicating a universal mechanism by which FZDs engage with DVLs. We further reveal that DEP mimics G-protein/β-arrestin/GRK to recognize an active conformation of receptor, expanding current GPCR engagement models. Finally, we identify a distinct FZD4 dimerization interface. Our findings delineate the molecular determinants governing FZD/DVL assembly and propagation of WNT signaling, providing long-sought answers underlying WNT signal transduction.

摘要

WNT 信号在发育和内稳态中起着基础性作用,但 Frizzled 受体 (FZDs) 如何传播信号仍然是个谜。在这里,我们展示了与 WNT 转导关键蛋白 Dishevelled 2 (DVL2) 的 DEP 结构域结合的 FZD4 的冷冻电镜结构。我们揭示了一种独特的结合模式,其中 DEP 指状环插入 FZD4 腔中形成疏水面。FZD4 细胞内环 2 (ICL2) 通过极性接触进一步锚定复合物。突变验证了结构观察。DEP 界面在 FZDs 中高度保守,表明 FZDs 与 DVLs 结合的通用机制。我们进一步揭示了 DEP 模拟 G 蛋白/β-抑制蛋白/GRK 以识别受体的活性构象,扩展了当前的 GPCR 结合模型。最后,我们确定了一个独特的 FZD4 二聚化界面。我们的研究结果描绘了调控 FZD/DVL 组装和 WNT 信号转导的分子决定因素,为 WNT 信号转导提供了长期以来寻求的答案。

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