Department of Pharmacology, Yale School of Medicine, New Haven, CT 06520, USA.
J Biol Chem. 2010 Jan 15;285(3):2165-73. doi: 10.1074/jbc.M109.018432. Epub 2009 Nov 10.
The amyloid beta-peptide deposit found in the brain tissue of patients with Alzheimer disease is derived from a large heparin-binding protein precursor APP. The biological function of APP and its homologs is not precisely known. Here we report the x-ray structure of the E2 domain of APL-1, an APP homolog in Caenorhabditis elegans, and compare it to the human APP structure. We also describe the structure of APL-1 E2 in complex with sucrose octasulfate, a highly negatively charged disaccharide, which reveals an unexpected binding pocket between the two halves of E2. Based on the crystal structure, we are able to map, using site-directed mutagenesis, a surface groove on E2 to which heparin may bind. Our biochemical data also indicate that the affinity of E2 for heparin is influenced by pH: at pH 5, the binding appears to be much stronger than that at neutral pH. This property is likely caused by histidine residues in the vicinity of the mapped heparin binding site and could be important for the proposed adhesive function of APL-1.
在阿尔茨海默病患者的脑组织中发现的淀粉样β肽沉积物源自一种大型肝素结合蛋白前体 APP。APP 及其同源物的生物学功能尚不清楚。在这里,我们报告了 APL-1(秀丽隐杆线虫中的一种 APP 同源物)E2 结构域的 X 射线结构,并将其与人类 APP 结构进行了比较。我们还描述了 APL-1 E2 与蔗糖八硫酸的复合物结构,蔗糖八硫酸是一种带高度负电荷的二糖,这揭示了 E2 两半之间一个意想不到的结合口袋。基于晶体结构,我们能够通过定点突变将 E2 上的一个表面凹槽映射到肝素可能结合的位置。我们的生化数据还表明,E2 与肝素的亲和力受 pH 值影响:在 pH5 时,结合似乎比中性 pH 时强得多。这种特性可能是由映射到肝素结合位点附近的组氨酸残基引起的,这对于 APL-1 提出的黏附功能可能很重要。
