Mathews I I, Vanderhoff-Hanaver P, Castellino F J, Tulinsky A
Department of Chemistry, Michigan State University, East Lansing, Michigan 48824, USA.
Biochemistry. 1996 Feb 27;35(8):2567-76. doi: 10.1021/bi9521351.
The X-ray crystal structures of the complexes of the recombinant kringle 1 domain of human plasminogen (Klpg) with the ligands epsilon-aminocaproic acid (EACA) and trans-4-(aminomethyl)cyclohexane-1-carboxylic acid (AMCHA), which are representative of a class of in vivo antifibrinolytic agents, have been determined at 2.1 angstroms resolution. Each Klpg/ligand unit cell contained a dimer of the complexes, and some small differences were noted in the kringle/ligand interatomic distances within the monomeric components of the dimers. The structures obtained allowed predictions to be made of the amino acid residues of Klpg that are likely important to ligand binding. In the crystal structure, the anionic center of Klpg responsible for coordinating the amino group of the ligands is composed of both Asp54 and Asp56, and the cationic center that stabilizes binding of the carboxylate moiety of the ligands is Arg70, with a possible contribution from Arg34. A hydrogen bond between the carboxylate of the ligand to the hydroxyl group of Tyr63 also appears to contribute to the kringle/ligand binding energies. The methylene groups of the ligand are stablized in the binding pocket by van der Waals contacts with side-chain atoms of Trp61 and Tyr71. These conclusions are in general agreement with site-directed mutagenesis results that implicate many of the same amino acid residues in the binding process, thus showing that the crystal and solution structures are in basic accord with each other. Further comparisons of the X-ray crystal structures of the Klpg/ligand complexes with each other and with apo-Klpg show that while small differences in Klpg side-chain geometries may exist in the three structures, the binding pocket can be considered to be preformed in the apokringle and not substantially altered by the nature of the omega-amino acid ligand that is inserted into the site. From the similar geometries of the binding of EACA and AMCHA, it appears that the kon is an important component to the tighter binding of AMCHA to Klpg, as compared to EACA. Ordered solvation effects of the bound AMCHA may contribute to its longer lifetime on Klpg, thereby retarding koff, both effects thus accounting for the higher binding energy of AMCHA as compared to EACA.
已在2.1埃分辨率下测定了人纤溶酶原重组kringle 1结构域(Klpg)与配体ε-氨基己酸(EACA)和反式-4-(氨甲基)环己烷-1-羧酸(AMCHA)复合物的X射线晶体结构,这两种配体是一类体内抗纤维蛋白溶解剂的代表。每个Klpg/配体晶胞包含复合物的二聚体,并且在二聚体单体组分内的kringle/配体原子间距离中观察到一些小的差异。所获得的结构使得能够对Klpg中可能对配体结合很重要的氨基酸残基进行预测。在晶体结构中,负责配位配体氨基的Klpg阴离子中心由Asp54和Asp56组成,稳定配体羧酸盐部分结合的阳离子中心是Arg70,Arg34可能也有贡献。配体羧酸盐与Tyr63羟基之间的氢键似乎也对kringle/配体结合能有贡献。配体的亚甲基通过与Trp61和Tyr71侧链原子的范德华接触而稳定在结合口袋中。这些结论与定点诱变结果总体一致,定点诱变结果表明许多相同的氨基酸残基参与了结合过程,从而表明晶体结构和溶液结构基本一致。Klpg/配体复合物的X射线晶体结构彼此之间以及与脱辅基Klpg的进一步比较表明,虽然在这三种结构中Klpg侧链几何形状可能存在小的差异,但结合口袋在脱辅基kringle中可以认为是预先形成的,并且不会因插入该位点的ω-氨基酸配体的性质而发生实质性改变。从EACA和AMCHA结合的相似几何形状来看,与EACA相比,kon似乎是AMCHA与Klpg更紧密结合的一个重要因素。结合的AMCHA的有序溶剂化效应可能有助于其在Klpg上的寿命延长,从而延缓koff,这两种效应因此解释了AMCHA与EACA相比具有更高的结合能。
