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血清淀粉样蛋白P与层粘连蛋白结合的特性研究

Characterization of the binding of serum amyloid P to laminin.

作者信息

Zahedi K

机构信息

Division of Nephrology, Children's Hospital Research Foundation and Department of Pediatrics, University of Cincinnati College of Medicine, Cincinnati, Ohio 45229-3039, USA.

出版信息

J Biol Chem. 1997 Jan 24;272(4):2143-8.

PMID:8999915
Abstract

Serum amyloid P (SAP) is a member of the pentraxin family. These are evolutionarily conserved proteins made up of five noncovalently bound identical subunits that are arranged in a flat pentameric disc. Although a variety of activities have been attributed to SAP and other pentraxins, their biological functions remain unclear. In humans SAP is a constitutive serum protein that is synthesized by hepatocytes. It is encoded by a single copy gene on chromosome 1. SAP is a component of all amyloid plaques and is also a normal component of a number of basement membranes including the glomerular basement membrane. The association and distribution of SAP within the glomerular basement membrane are altered or completely disrupted in a number of nephritides (e.g. Alport's Syndrome, type II membranoproliferative glomerulonephritis, and membranous glomerulonephritis). In the present study the binding of SAP to laminin was characterized. SAP binds to human laminin and merosin as well as mouse and rat laminins. The binding of SAP to mouse laminin is saturable and calcium-dependent. The Kd of this interaction is 2. 74 x 10(-7) M, with a SAP/laminin molar ratio of 1:7.1. Competition binding assays indicate that the binding of SAP to laminin is inhibited by both SAP and its analog, C-reactive protein, as well as phosphatidylethanolamine. In turbidity assays SAP enhanced the polymerization of laminin in a concentration-dependent manner. However, SAP did not alter the ability of laminin to serve as a cell adhesion substrate. Previous observations indicating that SAP binds to extracellular matrix components such as type IV collagen, proteoglycans, and fibronectin in concert with the data presented here suggest that SAP may play an important role in determining the structure of those basement membranes with which it is associated.

摘要

血清淀粉样蛋白P(SAP)是五聚素家族的成员。这些是进化上保守的蛋白质,由五个非共价结合的相同亚基组成,排列成扁平的五聚体盘状。尽管已将多种活性归因于SAP和其他五聚素,但其生物学功能仍不清楚。在人类中,SAP是一种由肝细胞合成的组成性血清蛋白。它由1号染色体上的单拷贝基因编码。SAP是所有淀粉样斑块的组成成分,也是包括肾小球基底膜在内的许多基底膜的正常成分。在一些肾炎(如阿尔波特综合征、II型膜增生性肾小球肾炎和膜性肾小球肾炎)中,SAP在肾小球基底膜内的结合和分布会发生改变或完全破坏。在本研究中,对SAP与层粘连蛋白的结合进行了表征。SAP与人层粘连蛋白和merosin以及小鼠和大鼠层粘连蛋白结合。SAP与小鼠层粘连蛋白的结合是可饱和的且依赖于钙。这种相互作用的解离常数(Kd)为2.74×10⁻⁷M,SAP/层粘连蛋白的摩尔比为1:7.1。竞争结合试验表明,SAP及其类似物C反应蛋白以及磷脂酰乙醇胺均可抑制SAP与层粘连蛋白的结合。在浊度测定中,SAP以浓度依赖的方式增强了层粘连蛋白的聚合。然而,SAP并未改变层粘连蛋白作为细胞粘附底物的能力。先前的观察表明,SAP与细胞外基质成分如IV型胶原、蛋白聚糖和纤连蛋白结合,结合本文提供的数据表明,SAP可能在决定与其相关的那些基底膜的结构中起重要作用。

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