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Stochastic modeling of nanoparticle internalization and expulsion through receptor-mediated transcytosis

机译:随机建模的纳米颗粒内化和驱逐受体介导transcytosis

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Receptor-mediated transcytosis (RMT) is a fundamental mechanism for the transcellular transport of nanoparticles. RMT is a complex process, during which the nanoparticles actively interact with the membrane and the membrane profile undergoes extreme deformations for particle internalization and expulsion. In this work, we developed a stochastic model to study the endocytosis and exocytosis of nanoparticles across soft membranes. The model is based on the combination of a stochastic particle binding model with a membrane model, and accounts for both clathrin-mediated endocytosis for internalization and actin-mediated exocytosis for expulsion. Our results showed that nanoparticles must have certain avidity with enough ligand density and ligand-receptor binding affinity to be taken up, while too high avidity limited the particle release from the cell surface. We further explored the functional roles of actin during exocytosis, which has been a topic under active debate. Our simulations indicated that the membrane compression due to the actin induced tension tended to break the ligand-receptor bonds and to shrink the fusion pore. Therefore, an intermediate tension promoted the fusion pore expansion and nanoparticle release, while high tension prohibits particle release. Our model provides new and critical mechanistic insights into RMT, and represents a powerful platform for aiding the rational design of nanocarriers for controlled drug delivery.
机译:受体介导transcytosis (RMT)transcellular基本机制运输的纳米粒子。过程,在这个过程中纳米颗粒的积极参与与膜和膜配置文件经历极端变形粒子内化和驱逐。工作,我们建立了一个随机模型研究纳米颗粒的内吞作用和胞外分泌在软膜。结合随机粒子绑定模型与膜模型,占两个clathrin-mediated内吞作用的内化和actin-mediated胞外分泌驱逐。必须有一定的活动性与足够的配体吗中的密度和亲和力了,而高活动性有限从细胞表面粒子释放。进一步探讨了肌动蛋白的功能角色在胞外分泌,下一个话题活跃的辩论。由于肌动蛋白诱导膜压缩紧张倾向于打破中的债券和收缩毛孔融合。中间张力促进了融合孔隙扩张和纳米粒子释放,而高张力禁止粒子释放。提供了新的和关键机械的见解RMT,代表了一个强大的平台帮助人们的理性设计控制药物输送。

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