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Synaptic arrangement of the neuroligin/beta-neurexin complex revealed by X-ray and neutron scattering

机译:X射线和中子散射揭示神经胶蛋白/β-神经毒素复合物的突触排列

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摘要

Neuroligins are postsynaptic cell-adhesion proteins that associate with their presynaptic partners, the neurexins. Using small-angle X-ray scattering, we determined the shapes of the extracellular region of several neuroligin isoforms in solution. We conclude that the neuroligins dimerize via the characteristic four-helix bundle observed in cholinesterases, and that the connecting sequence between the globular lobes of the dimer and the cell membrane is elongated, projecting away from the dimer interface. X-ray scattering and neutron contrast variation data show that two neurexin monomers, separated by 107 A, bind at symmetric locations on opposite sides of the long axis of the neuroligin dimer. Using these data, we developed structural models that delineate the spatial arrangements of different neuroligin domains and their partnering molecules. As mutations of neurexin and neuroligin genes appear to be linked to autism, these models provide a structural framework for understanding altered recognition by these proteins in neurodevelopmental disorders.
机译:神经胶蛋白是突触后细胞粘附蛋白,与它们的突触前伴侣神经毒素相关。使用小角度X射线散射,我们确定了溶液中几种神经胶蛋白同工型的细胞外区域的形状。我们得出结论,神经胶蛋白通过在胆碱酯酶中观察到的特征性四螺旋束而二聚化,并且二聚体的球状小叶和细胞膜之间的连接序列延长了,突出了远离二聚体的界面。 X射线散射和中子对比度变化数据显示,两个神经氨酸单体(以107 A隔开)在神经素二聚体长轴相对侧的对称位置结合。利用这些数据,我们开发了结构模型,描述了不同神经胶蛋白域及其伙伴分子的空间排列。由于神经毒素和神经胶蛋白基因的突变似乎与孤独症有关,因此这些模型为理解这些蛋白在神经发育障碍中识别的改变提供了结构框架。

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