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The Metastasis-Associated Extracellular Matrix Protein Osteopontin Forms Transient Structure in Ligand Interaction Sites

骨桥蛋白 外域 整合素 化学 细胞外基质 细胞粘附 生物物理学 无规线圈 CD44细胞 蛋白质结构 圆二色性 细胞 细胞生物学 生物化学 生物 受体 免疫学
作者
Gerald Platzer,Andreas Schedlbauer,Angela Chemelli,Przemysław Ozdowy,Nicolas Coudevylle,Renate Auer,Georg Kontaxis,Markus Hartl,Andrew Miles,B.A. Wallace,Otto Glatter,Klaus Bister,Robert Konrat
出处
期刊:Biochemistry [American Chemical Society]
卷期号:50 (27): 6113-6124 被引量:68
标识
DOI:10.1021/bi200291e
摘要

Osteopontin (OPN) is an acidic hydrophilic glycophosphoprotein that was first identified as a major sialoprotein in bones. It functions as a cell attachment protein displaying a RGD cell adhesion sequence and as a cytokine that signals through integrin and CD44 cell adhesion molecules. OPN is also implicated in human tumor progression and cell invasion. OPN has intrinsic transforming activity, and elevated OPN levels promote metastasis. OPN gene expression is also strongly activated in avian fibroblasts simultaneously transformed by the v-myc and v-mil(raf) oncogenes. Here we have investigated the solution structure of a 220-amino acid recombinant OPN protein by an integrated structural biology approach employing bioinformatic sequence analysis, multidimensional nuclear magnetic resonance spectroscopy, synchrotron radiation circular dichroism spectroscopy, and small-angle X-ray scattering. These studies suggest that OPN is an intrinsically unstructured protein in solution. Although OPN does not fold into a single defined structure, its conformational flexibility significantly deviates from random coil-like behavior. OPN comprises distinct local secondary structure elements with reduced conformational flexibility and substantially populates a compact subspace displaying distinct tertiary contacts. These compacted regions of OPN encompass the binding sites for α(V)β(III) integrin and heparin. The conformational flexibility combined with the modular architecture of OPN may represent an important structural prerequisite for its functional diversity.

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