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The antigen-antibody unbinding process through steered molecular dynamics of a complex of an Fv fragment and lysozyme

机译:通过Fv片段和溶菌酶复合物的分子动力学控制来进行抗原-抗体解除结合过程

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We have investigated the antigen-antibody unbinding process using steered molecular dynamics (SMD) simulations. We focus on a complex system consisting of an Fv fragment of an antibody molecule and a lysozyme as an antigen molecule. The Fv fragment consists of a VL and VH chain. The results show that the VH chain is unbound earlier than the VL chain, which is confirmed by the ensemble average of the distance profile obtained from 40 unbinding trajectories. The use of lysozyme as an antigen molecule instead of a small hapten molecule reveals the fact that the induced fit, estimated by the deformation accompanying the unbinding process, is more noticeable for the antigen molecule than for the antibody molecule. The SMD also reveals the non-Gaussian distribution of maximum force necessary for the unbinding process.
机译:我们已经研究了使用转向分子动力学(SMD)模拟的抗原抗体解结合过程。我们专注于一个复杂的系统,该系统由抗体分子的Fv片段和作为抗原分子的溶菌酶组成。 Fv片段由VL和VH链组成。结果表明,VH链比VL链更早地未结合,这由从40条未结合的轨迹获得的距离分布的整体平均值所证实。溶菌酶作为抗原分子而不是小的半抗原分子的使用揭示了这样的事实,即通过伴随解离过程的变形来估计的诱导拟合,对抗原分子比对抗体分子更引人注意。 SMD还揭示了解除绑定过程所需的最大力的非高斯分布。

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