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首页> 外文期刊>International Scholarly Research Notices >Mechanism of Protein-Z-Mediated Inhibition of Coagulation Factor Xa by Z-Protein-Dependent Inhibitor: A Molecular Dynamic Approach
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Mechanism of Protein-Z-Mediated Inhibition of Coagulation Factor Xa by Z-Protein-Dependent Inhibitor: A Molecular Dynamic Approach

机译:Z蛋白依赖性抑制剂的蛋白Z介导的凝血因子Xa抑制机制:分子动力学方法

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Protein Z is a plasma protein functioning as a carrier for ZPI. Protein Z also accelerates inhibitory effect of ZPI on factor Xa by 1000-fold. Inhibition of coagulation cascade via FXa by ZPI and other serpins is very important safety factor for normal homeostasis protecting human life against unwanted thrombosis. In the present work using native structure of PZ, ZPI, FXa and in a dynamic simulation, using NAMD software, the ternary complex was studied in an up to 10 nanoseconds protocol. Rely on trajectory analyses, we postulated that PZ binds ZPI by using its SP-like domain and through noncovalent forces. PZ then transfers ZPI through-out the blood, and by using its GLA domain and a bivalent cation of calcium, PZ binds to phospholipid bilayers (e.g., platelet) where the FXa is preallocated. In case of PZ-ZPI binding to plasma membrane, a series of complementary interactions take place between FXa, and PZ-ZPI complex including interactions between RCL loop of ZPI and catalytic site of FXa and some take place between long arm of PZ (composed of GLA, EGF1, and EGF2 domains) and GLA domain of FXa. In our claim these complementary interactions lead PZ to bind correctly to prelocated FXa.
机译:Z蛋白是血浆蛋白,可作为ZPI的载体。 Z蛋白还可以将ZPI对Xa因子的抑制作用提高1000倍。 ZPI和其他丝氨酸蛋白酶抑制剂通过FXa抑制凝血级联反应是正常体内平衡的重要安全系数,可保护人类生命免受不必要的血栓形成。在当前使用PZ,ZPI,FXa的本机结构的工作中,以及在使用NAMD软件进行的动态仿真中,以高达10纳秒的协议研究了三元复合物。依靠轨迹分析,我们推测PZ通过使用其SP样域和非共价力与ZPI结合。然后PZ将ZPI转移到整个血液中,通过使用其GLA结构域和钙的二价阳离子,PZ与FXa预先分配的磷脂双层(例如血小板)结合。如果PZ-ZPI与质膜结合,则FXa与PZ-ZPI络合物之间会发生一系列互补相互作用,包括ZPI的RCL环与FXa催化位点之间的相互作用以及PZ的长臂之间的相互作用。 FXa的GLA,EGF1和EGF2域)和GLA域。在我们的主张中,这些互补的相互作用导致PZ正确绑定到预先定位的FXa。

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