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Structural insights for fatty acid binding in a Lys49-phospholipase A(2): crystal structure of myotoxin II from Bothrops molojeni complexed with stearic acid

机译:Lys49磷脂酶A(2)中的脂肪酸结合的结构见解:结合硬脂酸的Bothrops molojeni的肌毒素II的晶体结构

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The crystal structure of dimeric Lys49-phospholipase A2 myotoxin-II from Bothrops moojeni (MjTX-II) co-crystallized with stearic acid (C18H36O2) has been determined at a resolution of 1.8 angstrom. The electron density maps permitted the unambiguous inclusion of six stearic acid molecules in the refinement. Two stearic acid molecules could be located in the substrate-binding cleft of each monomer in positions, which favor the interaction of their carboxyl groups with active site residues. The way of binding of stearic acids to this Lys49-PLA(2)s is analogous to phospholipids and transition state analogues to catalytically active PLA(2)s. Two additional stearic acid molecules were located at the dimer interface region, defining a hitherto unidentified acyl-binding site on the protein surface. The strictly conserved Lys122 for Lys49-PLA(2)s may play a fundamental role for stabilization of legend-protein complex. The comparison of MjTX-II/satiric acid complex with other Lys-PLA(2)s structures whose putative fatty acids were located at their active site is also analysed. Molecular details of the stearic acid/protein interactions provide insights to binding in croup I/II PLA(2)s and to the possible interactions of Lys49-PLA(2)s with target membranes. (c) 2004 Elsevier SAS. All rights reserved.
机译:已确定与硬脂酸(C18H36O2)共结晶的来自Bothrops moojeni(MjTX-II)的二聚Lys49-磷脂酶A2肌毒素II的晶体结构,分辨率为1.8埃。电子密度图允许在精制中明确包含六个硬脂酸分子。两个硬脂酸分子可以位于每个单体的底物结合裂隙中的位置,这有利于它们的羧基与活性位点残基的相互作用。硬脂酸与此Lys49-PLA(2)s的结合方式类似于磷脂,而过渡态类似物则具有催化活性的PLA(2)s。两个额外的硬脂酸分子位于二聚体界面区域,在蛋白质表面上定义了迄今尚未确定的酰基结合位点。严格保守的Lys49-PLA(2)的Lys122可能在稳定图例蛋白复合体中起重要作用。还分析了MjTX-II /饱和脂肪酸与其他假定脂肪酸位于其活性位点的Lys-PLA(2)s结构的比较。硬脂酸/蛋白质相互作用的分子详细信息提供了对在臀部I / II PLA(2)中结合以及Lys49-PLA(2)与靶膜可能相互作用的见解。 (c)2004年Elsevier SAS。版权所有。

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