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Fully reduced granulin-B is intrinsically disordered and displays concentration-dependent dynamics

机译:完全还原的颗粒蛋白B本质上是无序的,并且表现出浓度依赖性的动力学

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摘要

Granulins (Grns) are a family of small, cysteine-rich proteins that are generated upon proteolytic cleavage of their precursor, progranulin (Pgrn). All seven Grns (A-G) contain 12 conserved cysteines that form 6 intramolecular disulfide bonds, rendering this family of proteins unique. Grns are known to play multi-functional roles, including wound healing, embryonic growth, and inflammation and are implicated in neurodegenerative diseases. Despite their manifold functions, there exists a dearth of information regarding their structure-function relationship. Here, we sought to establish the role of disulfide bonds in promoting structure by investigating the fully reduced GrnB (rGrnB). We report that monomeric rGrnB is an intrinsically disordered protein (IDP) at low concentrations. rGrnB undergoes dimerization at higher concentrations to form a fuzzy complex without a net gain in the structure-a behavior increasingly identified as a hallmark of some IDPs. Interestingly, we show that rGrnB is also able to activate NF-kappa B in human neuroblastoma cells in a concentration-dependent manner. This activation correlates with the observed monomer-dimer dynamics. Collectively, the presented data establish that the intrinsic disorder of rGrnB governs conformational dynamics within the reduced form of the protein, and suggest that the overall structure of Grns could be entirely dictated by disulfide bonds.
机译:颗粒蛋白(Grns)是一类富含半胱氨酸的小蛋白家族,这些蛋白是通过对其前体颗粒蛋白原(Pgrn)进行蛋白水解而产生的。所有七个Grns(A-G)都包含12个保守的半胱氨酸,这些半胱氨酸形成6个分子内二硫键,这使得该蛋白家族具有独特性。已知Grns发挥着多种功能,包括伤口愈合,胚胎生长和炎症,并且与神经退行性疾病有关。尽管它们具有多种功能,但是关于它们的结构-功能关系的信息却很少。在这里,我们试图通过研究完全还原的GrnB(rGrnB)来确立二硫键在促进结构中的作用。我们报告说单体rGrnB是一种低浓度的内在无序蛋白(IDP)。 rGrnB在较高浓度下进行二聚化,形成模糊复合物,但结构中没有净收益-越来越多的行为被视为某些IDP的标志。有趣的是,我们表明rGrnB还能够以浓度依赖的方式激活人神经母细胞瘤细胞中的NF-κB。该活化与观察到的单体-二聚体动力学相关。总体而言,目前的数据表明,rGrnB的内在障碍控制着蛋白质还原形式内的构象动力学,并暗示了Grns的整体结构可能完全由二硫键决定。

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