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首页> 外文期刊>Analytical chemistry >Interactions of Intact Unfractionated Heparin with Its Client Proteins Can Be Probed Directly Using Native Electrospray Ionization Mass Spectrometry
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Interactions of Intact Unfractionated Heparin with Its Client Proteins Can Be Probed Directly Using Native Electrospray Ionization Mass Spectrometry

机译:完整的普通肝素与其客户蛋白的相互作用可以使用天然电喷雾电离质谱法直接探测

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摘要

Heparin and related members of the glycosaminoglycan (GAG) family are highly polyanionic linear saccharides that play important roles in a variety of physiological processes ranging from blood coagulation to embryo- and oncogenesis, tissue regeneration, and immune response regulation. These diverse functions are executed via a variety of mechanisms, including protein sequestration, activation, and facilitation of their interactions with cell-surface receptors, but deciphering the specific molecular mechanisms is frequently impossible due to the extremely high degree of GAG heterogeneity. As a result, the vast majority of studies of heparin (or related GAGs) interactions with its client proteins use synthetically produced heparin mimetics with defined structure or short heparin fragments. In this work we use native electrospray ionization mass spectrometry (ESI MS) in combination with limited charge reduction in the gas phase to obtain meaningful information on noncovalent complexes formed by intact unfractionated heparin and antithrombin-III, interaction which is central to preventing blood clotting. Complexes of different stoichiometries are observed ranging from 1:1 to 1:3 (heparin/protein ratio). In addition to binding stoichiometry, the measurements allow the range of heparin chain lengths to be obtained for each complex and the contribution of each complex to the total ionic signal to be calculated. Incorporation of ion mobility measurements in the experimental workflow allows the total analysis time to be shortened very significantly and the charge state assignment for the charge-reduced species to be verified. The possibility to study interactions of intact unfractionated heparin with a client protein carried out directly by native ESI MS without the need to use relatively homogeneous surrogates demonstrated in this work opens up a host of new exciting opportunities and goes a long way toward ameliorating the persistent but outdated view of the intractability of such interactions.
机译:肝素和糖胺聚糖(GAG)家族的相关成员是高度聚阴离子的线性糖类,在从血液凝固到胚胎和肿瘤发生,组织再生以及免疫应答调节等各种生理过程中起着重要作用。这些多样化的功能通过多种机制执行,包括蛋白质螯合,激活以及促进它们与细胞表面受体的相互作用,但是由于极高的GAG异质性,经常无法破解特定的分子机制。结果,绝大多数肝素(或相关GAG)与其客户蛋白相互作用的研究均使用合成生产的具有确定结构或短肝素片段的肝素模拟物。在这项工作中,我们将天然电喷雾电离质谱(ESI MS)与气相中有限的电荷减少结合使用,以获得有关由完整的普通肝素和抗凝血酶III形成的非共价复合物的有意义的信息,这种相互作用对于防止血液凝结至关重要。观察到不同化学计量的复合物的范围为1:1至1:3(肝素/蛋白质比)。除了结合化学计量之外,测量还允许获得每种复合物的肝素链长范围,并计算每种复合物对总离子信号的贡献。将离子迁移率测量结果纳入实验工作流程可以大大缩短总分析时间,并可以验证减少电荷的物质的电荷状态分配。研究完整的普通肝素与由天然ESI MS直接进行的客户蛋白相互作用的可能性,而无需使用这项工作中证明的相对均一的替代物,为我们带来了许多新的令人兴奋的机会,并且可以大大改善持久性但这种互动难以处理的观点已经过时。

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