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人血清淀粉样蛋白P成分在亲和毛细管电泳中对Ca2+、Mg2+和肝素的结合

Binding of Ca2+, Mg2+, and heparin by human serum amyloid P component in affinity capillary electrophoresis.

作者信息

Heegaard Niels H H, He Xinya, Blomberg Lars G

机构信息

Department of Autoimmunology, Statens Serum Institut, Copenhagen S, Denmark.

出版信息

Electrophoresis. 2006 Jul;27(13):2609-15. doi: 10.1002/elps.200600005.

Abstract

Human serum amyloid P component (SAP) is a glycoprotein circulating in the blood and found in association with all types of amyloid (malfolded potein aggregates) examined so far. Despite uncertainties regarding the precise function of SAP in vivo, the lectin-like properties of this Ca(2+)-activated protein with affinity for anionic saccharides and malfolded proteins are well known. The propensity to form homomeric penta- or decamers in solution and the selfaggregation in the presence of Ca(2+) as well as the tendency of SAP to attach to uncoated fused silica have precluded the analysis of SAP by microelectrophoretic methods. We now work out conditions to characterize the binding of Ca(2+) and Mg(2+) and the binding of heparin to SAP in the presence of divalent metal ions by ACE. The results show a strong binding of heparin (sub-muM apparent dissociation constants) even in the abscence of Ca(2+) at low ionic strength, pH 8.2. Also, a selective interaction with Ca(2+) compared with Mg(2+) is demonstrated. The approach will further the use of microelectrophoretic methods to examine the interactions of SAP with ligands of putative pathophysiological relevance such as lipopolysaccharides and misfolded proteins.

摘要

人血清淀粉样蛋白P成分(SAP)是一种在血液中循环的糖蛋白,在迄今为止检测的所有类型的淀粉样蛋白(错误折叠的蛋白质聚集体)中均有发现。尽管SAP在体内的确切功能尚不确定,但这种对阴离子糖类和错误折叠蛋白质具有亲和力的Ca(2+)激活蛋白的凝集素样特性是众所周知的。SAP在溶液中形成同型五聚体或十聚体的倾向、在Ca(2+)存在下的自我聚集以及SAP附着于未涂层熔融石英的趋势,使得通过微电泳方法对SAP进行分析变得困难。我们现在制定了一些条件,通过ACE来表征Ca(2+)和Mg(2+)的结合以及在二价金属离子存在下肝素与SAP的结合。结果表明,即使在低离子强度、pH 8.2且不存在Ca(2+)的情况下,肝素也有很强的结合(表观解离常数为亚微摩尔)。此外,还证明了与Mg(2+)相比,SAP与Ca(2+)存在选择性相互作用。该方法将进一步推动使用微电泳方法来研究SAP与潜在病理生理相关配体(如脂多糖和错误折叠蛋白质)的相互作用。

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