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Crystal structure of the human vascular adhesion protein-1: Unique structural features with functional implications

机译:人类血管粘附蛋白-1的晶体结构:具有功能含义的独特结构特征

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摘要

The expression of human vascular adhesion protein-1 (hVAP-1) is induced at sites of inflammation where extravasation of lymphocytes from blood to the peripheral tissue occurs. We have solved the X-ray structure of hVAP-1, a human copper amine oxidase (CAO), which is distinguished from other CAOs in being membrane-bound. The dimer structure reveals some intriguing features that may have fundamental roles in the adhesive and enzymatic functions of hVAP-1, especially regarding the role of hVAP-1 in inflammation, lymphocyte attachment, and signaling. Firstly, Leu469 at the substrate channel may play a key role in controlling the substrate entry; depending on its conformation, it either blocks or gives access to the active site. Secondly, sugar units are clearly observed at two of the six predicted N-glycosylation sites. Moreover, mutagenesis analysis showed that all of the predicted sites were glycosylated in the protein used for crystallization. Thirdly, the existence of a solvent-exposed RGD motif at the entrance to each active site in hVAP-1 suggests that it may have a functional role.
机译:人血管粘附蛋白1(hVAP-1)的表达是在炎症部位诱导的,其中淋巴细胞从血液溢出到周围组织。我们已经解决了人类铜胺氧化酶(CAO)hVAP-1的X射线结构,该结构与其他CAO的区别在于被膜结合。二聚体结构揭示了一些有趣的特征,这些特征可能在hVAP-1的粘附和酶促功能中具有基本作用,特别是在hVAP-1在炎症,淋巴细胞附着和信号传导中的作用方面。首先,底物通道处的Leu469可能在控制底物进入方面起关键作用。根据其构形,它会阻止或提供对活动站点的访问。其次,在六个预测的N-糖基化位点中的两个位点清楚地观察到糖单位。此外,诱变分析表明,所有预测的位点在用于结晶的蛋白质中都被糖基化。第三,在hVAP-1中每个活性位点的入口处都存在溶剂暴露的RGD基序,这表明它可能具有功能性作用。

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