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Change of dynamics of raft-model membrane induced by amyloid-β protein binding

机译:淀粉样β蛋白结合诱导的筏模型膜动力学变化

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While the steady-state existence in the size and shape of liquid-ordered microdomains in cell membranes, the so-called"lipid rafts", still remain the subject of debate, glycosphingolipid-cholesterol rich regions in plasma membranes have been considered to have a function as platforms for signaling and sorting. In addition, recent spectroscopic studies show that the interaction between monosialoganglioside and amyloid beta (Aβ) protein promotes the transition of Aβ from the native structure to the cross-beta fold in amyloid aggregates. However, there is few evidence on the dynamics of lipid "rafts" membranes. As the neutron spin-echo (NSE) technique is well known to detect directly slow dynamics of membrane systems in situ, by the combination of NSE and small-angle X-ray scattering we have studied the effect of the interaction between raft-model membrane and amyloid Aβ proteins on the structure and dynamics of a large uni-lamellar vesicle (LUV) consisting of monosialoganglioside-cholesterol-phospholipid ternary mixtures as a model of lipid-raft membrane. We have found that the interaction between the Aβ proteins and the model membrane at the liquid crystal phase significantly suppresses a bending-diffusion motion with a minor effect on the LUV structure. The present results would suggest a possibility of non-receptormediated disorder in signaling through a modulation of a membrane dynamics induced by the association of amyloidogenic peptides on a plasma membrane.
机译:尽管细胞膜中液体有序微区的大小和形状处于稳态,所谓的“脂质筏”仍然是争论的话题,但人们认为质膜中富含糖鞘脂-胆固醇的区域具有用作信令和分类的平台。此外,最近的光谱研究表明,单唾液酸神经节苷脂和淀粉样β(Aβ)蛋白之间的相互作用促进了淀粉样聚集体中Aβ从天然结构过渡到交叉β折叠。但是,关于脂质“筏”膜动力学的证据很少。由于众所周知,中子自旋回波(NSE)技术可直接检测原位膜系统的慢动力学,因此,通过结合NSE和小角度X射线散射,我们研究了筏式膜之间相互作用的影响和淀粉样蛋白Aβ蛋白对大单层囊泡(LUV)的结构和动力学的影响,该囊泡由单唾液酸神经节苷脂-胆固醇-磷脂三元混合物组成,为脂质筏膜的模型。我们发现,在液晶相中,Aβ蛋白与模型膜之间的相互作用可显着抑制弯曲扩散运动,而对LUV结构的影响较小。本结果提示通过调节由质膜上淀粉样蛋白生成肽的缔合而引起的膜动力学,信号传导中非受体介导的疾病的可能性。

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