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Coarse-grained molecular dynamics studies of the translocation mechanism of polyarginines across asymmetric membrane under tension

机译:张力下聚精氨酸跨不对称膜移位机理的粗粒分子动力学研究

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Understanding interactions between cell-penetrating peptides and biomembrane under tension can help improve drug delivery and elucidate mechanisms underlying fundamental cellular events. As far as the effect of membrane tension on translocation, it is generally thought that tension should disorder the membrane structure and weaken its strength, thereby facilitating penetration. However, our coarse-grained molecular dynamics simulation results showed that membrane tension can restrain polyarginine translocation across the asymmetric membrane and that this effect increases with increasing membrane tension. We also analyzed the structural properties and lipid topology of the tensed membrane to explain the phenomena. Simulation results provide important molecular information on the potential translocation mechanism of peptides across the asymmetric membrane under tension as well as new insights in drug and gene delivery.
机译:了解在张力下细胞穿透肽和生物膜之间的相互作用可以帮助改善药物递送并阐明基础细胞事件的机制。至于膜张力对易位的影响,通常认为张力会扰乱膜结构并削弱其强度,从而促进渗透。然而,我们的粗粒分子动力学模拟结果表明,膜张力可以抑制聚精氨酸在不对称膜上的移位,并且这种影响随着膜张力的增加而增加。我们还分析了张力膜的结构特性和脂质拓扑结构,以解释这种现象。仿真结果提供了重要的分子信息,这些信息涉及在张力下肽跨不对称膜的潜在转运机制,以及在药物和基因传递方面的新见解。

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