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Full-length model of the human galectin-4 and insights into dynamics of inter-domain communication

机译:人galectin-4的全长模型和域间通信动力学的见解

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摘要

Galectins are proteins involved in diverse cellular contexts due to their capacity to decipher and respond to the information encoded by β-galactoside sugars. In particular, human galectin-4, normally expressed in the healthy gastrointestinal tract, displays differential expression in cancerous tissues and is considered a potential drug target for liver and lung cancer. Galectin-4 is a tandem-repeat galectin characterized by two carbohydrate recognition domains connected by a linker-peptide. Despite their relevance to cell function and pathogenesis, structural characterization of full-length tandem-repeat galectins has remained elusive. Here, we investigate galectin-4 using X-ray crystallography, small- and wide-angle X-ray scattering, molecular modelling, molecular dynamics simulations, and differential scanning fluorimetry assays and describe for the first time a structural model for human galectin-4. Our results provide insight into the structural role of the linker-peptide and shed light on the dynamic characteristics of the mechanism of carbohydrate recognition among tandem-repeat galectins.
机译:半乳糖凝集素是参与多种细胞环境的蛋白质,因为它们具有解密和响应β-半乳糖苷糖编码信息的能力。特别地,通常在健康胃肠道中表达的人半乳凝素-4在癌组织中显示差异表达,被认为是肝癌和肺癌的潜在药物靶标。 Galectin-4是一种串联重复的半乳糖凝集素,其特征在于两个碳水化合物识别结构域之间通过连接肽连接。尽管它们与细胞功能和发病机制有关,但全长串联重复半乳糖凝集素的结构表征仍然难以捉摸。在这里,我们使用X射线晶体学,小角度和广角X射线散射,分子建模,分子动力学模拟和差示扫描荧光分析法研究galectin-4,并首次描述了人galectin-4的结构模型。我们的结果提供了对连接肽的结构作用的见解,并揭示了串联重复半乳糖凝集素中碳水化合物识别机制的动态特征。

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