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首页> 外文期刊>Nature Communications >Programmed spatial organization of biomacromolecules into discrete, coacervate-based protocells
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Programmed spatial organization of biomacromolecules into discrete, coacervate-based protocells

机译:将生物主义的空间组织编程为离散,共制的基于凝聚素的原始细胞

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摘要

The cell cytosol is crowded with high concentrations of many different biomacromolecules, which is difficult to mimic in bottom-up synthetic cell research and limits the functionality of existing protocellular platforms. There is thus a clear need for a general, biocompatible, and accessible tool to more accurately emulate this environment. Herein, we describe the development of a discrete, membrane-bound coacervate-based protocellular platform that utilizes the well-known binding motif between Ni 2 -nitrilotriacetic acid and His-tagged proteins to exercise a high level of control over the loading of biologically relevant macromolecules. This platform can accrete proteins in a controlled, efficient, and benign manner, culminating in the enhancement of an encapsulated two-enzyme cascade and protease-mediated cargo secretion, highlighting the potency of this methodology. This versatile approach for programmed spatial organization of biologically relevant proteins expands the protocellular toolbox, and paves the way for the development of the next generation of complex yet well-regulated synthetic cells.
机译:细胞胞嘧啶挤满了高浓度的许多不同的生物主量,这难以在自下而上的合成细胞研究中模仿并限制现有的生种平台的功能。因此,可以清楚地需要一般,生物相容性和可访问的工具来更准确地模拟这种环境。在此,我们描述了在Ni 2 - 腈酸和他标记的蛋白质之间使用众所周知的结合基序的离散的膜结合的凝聚晶细胞平台的发展,以在生物学相关的加载中运动高水平的控制大分子。该平台可以在受控,高效和良性的方式中粘附蛋白质,最终能够增强包封的双酶级联和蛋白酶介导的货物分泌,突出了该方法的效力。这种用于生物学相关蛋白质的程序空间组织的这种多功能方法扩展了生种致细胞工具箱,并为下一代复杂且调节的合成细胞进行了铺平道路。

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