Functional Characterization of a Small-Molecule Inhibitor of the DKK1-LRP6 Interaction.

ISRN molecular biology Pub Date : 2012-01-23 eCollection Date: 2012-01-01 DOI:10.5402/2012/823875

Sara Iozzi, Rosaria Remelli, Barbara Lelli, Daniela Diamanti, Silvia Pileri, Luisa Bracci, Renza Roncarati, Andrea Caricasole, Simonetta Bernocco

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引用次数: 28

Abstract

Background. DKK1 antagonizes canonical Wnt signalling through high-affinity binding to LRP5/6, an essential component of the Wnt receptor complex responsible for mediating downstream canonical Wnt signalling. DKK1 overexpression is known for its pathological implications in osteoporosis, cancer, and neurodegeneration, suggesting the interaction with LRP5/6 as a potential therapeutic target. Results. We show that the small-molecule NCI8642 can efficiently displace DKK1 from LRP6 and block DKK1 inhibitory activity on canonical Wnt signalling, as shown in binding and cellular assays, respectively. We further characterize NCI8642 binding activity on LRP6 by Surface Plasmon Resonance (SPR) technology. Conclusions. This study demonstrates that the DKK1-LRP6 interaction can be the target of small molecules and unlocks the possibility of new therapeutic tools for diseases associated with DKK1 dysregulation.

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DKK1-LRP6相互作用小分子抑制剂的功能表征

背景。DKK1通过高亲和力结合LRP5/6来拮抗典型Wnt信号，LRP5/6是Wnt受体复合物的重要组成部分，负责介导下游典型Wnt信号传导。众所周知，DKK1过表达在骨质疏松症、癌症和神经退行性疾病中具有病理意义，这表明与LRP5/6的相互作用是一个潜在的治疗靶点。结果。我们发现，小分子NCI8642可以有效地从LRP6中取代DKK1，并阻断DKK1对典型Wnt信号的抑制活性，分别在结合和细胞实验中得到证实。利用表面等离子体共振(SPR)技术进一步表征了NCI8642与LRP6的结合活性。结论。这项研究表明，DKK1- lrp6相互作用可以成为小分子的靶标，并为DKK1失调相关疾病的新治疗工具提供了可能。

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ISRN molecular biology

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