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Controlling Cargo Trafficking in Multicomponent Membranes

机译:控制多组分膜的货物贩运

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Biological membranes typically contain a large number of different components dispersed in small concentrations in the main membrane phase, including proteins, sugars, and lipids of varying geometrical properties. Most of these components do not bind the cargo. Here, we show that such "inert" components can be crucial for the precise control of cross-membrane trafficking. Using a statistical mechanics model and molecular dynamics simulations, we demonstrate that the presence of inert membrane components of small isotropic curvatures dramatically influences cargo endocytosis, even if the total spontaneous curvature of such a membrane remains unchanged. Curved lipids, such as cholesterol, as well as asymmetrically included proteins and tethered sugars can, therefore, actively participate in the control of the membrane trafficking of nanoscopic cargo. We find that even a low-level expression of curved inert membrane components can determine the membrane selectivity toward the cargo size and can be used to selectively target membranes of certain compositions. Our results suggest a robust and general method of controlling cargo trafficking by adjusting the membrane composition without needing to alter the concentration of receptors or the average membrane curvature. This study indicates that cells can prepare for any trafficking event by incorporating curved inert components in either of the membrane leaflets.
机译:生物膜通常含有大量不同的组分,分散在主膜相中的小浓度,包括蛋白质,糖和不同几何特性的脂质。这些组件中的大多数都没有绑定货物。在这里,我们表明这种“惰性”组件对于精确控制跨膜运输可能是至关重要的。使用统计力学模型和分子动力学模拟,我们证明了小各向同性曲率的惰性膜组分显着影响货物内吞作用,即使这种膜的总自发曲率保持不变。因此,诸如胆固醇以及不对称的蛋白质和束缚糖的弯曲脂质可以积极参与控制纳米镜货物的膜运输的控制。我们发现即使是弯曲惰性膜组分的低水平表达也可以确定膜选择性朝向货物尺寸,并且可用于选择性地靶向某些组合物的膜。我们的研究结果表明,通过调节膜组合物而不需要改变受体浓度或平均膜曲率来控制货物贩运的稳健和一般方法。该研究表明,通过在任一膜小叶中掺入弯曲的惰性组分,细胞可以为任何贩运事件做好准备。

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