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瓶中船:受限促进的自组装。

Ship in a bottle: confinement-promoted self-assembly.

作者信息

Lopez-Fontal Elkin, Grochmal Anna, Foran Tom, Milanesi Lilia, Tomas Salvador

机构信息

Institute of Structural and Molecular Biology , Department of Biological Sciences , School of Science , Birkbeck University of London , Malet Street , London WC1E 7HX , UK . Email:

School of Biological and Chemical Sciences , Queen Mary , University of London , Mile End Road , London E1 4NS , UK.

出版信息

Chem Sci. 2017 Dec 7;9(7):1760-1768. doi: 10.1039/c7sc04553k. eCollection 2018 Feb 21.

Abstract

Understanding self-assembly in confined spaces is essential to fully understand molecular processes in confined cell compartments and will offer clues on the behaviour of simple confined systems, such as protocells and lipid-vesicle based devices. Using a model system composed of lipid vesicles, a membrane impermeable receptor and a membrane-permeable ligand, we have studied in detail how compartmentalization modulates the interaction between the confined receptor and its ligand. We demonstrate that confinement of one of the building blocks stabilizes complex self-assembled structures to the extent that dilution leads, counterintuitively, to the formation of long range assemblies. The behaviour of the system can be explained by considering a confinement factor that is analogous, although not identical, to the effective molarity for intramolecular binding events. The confinement effect renders complex self-assembled species robust and persistent under conditions where they do not form in bulk solution. Moreover, we show that the formation of stable complex assemblies in systems compartmentalized by semi-permeable membranes does not require the prior confinement of all components, but only that of key membrane impermeable building blocks. To use a macroscopic analogy, lipid vesicles are like ship-in-a bottle constructs that are capable of directing the assembly of the confined ship following the confinement of a few key wooden planks. Therefore, we believe that the confinement effect described here would have played an important role in shaping the increase of chemical complexity within protocells during the first stages of abiogenesis. Additionally, we argue that this effect can be exploited to design increasingly efficient functional devices based on comparatively simple vesicles for applications in biosensing, nanoreactors and drug delivery vehicles.

摘要

了解受限空间中的自组装对于全面理解受限细胞区室中的分子过程至关重要,并且将为简单受限系统(如原始细胞和基于脂质囊泡的装置)的行为提供线索。我们使用由脂质囊泡、膜不可渗透受体和膜可渗透配体组成的模型系统,详细研究了区室化如何调节受限受体与其配体之间的相互作用。我们证明,其中一个构建模块的受限会使复杂的自组装结构稳定到一定程度,以至于稀释反而会导致形成长程组装,这与直觉相反。该系统的行为可以通过考虑一个受限因子来解释,该因子类似于但不完全等同于分子内结合事件的有效摩尔浓度。这种受限效应使复杂的自组装物种在本体溶液中不形成的条件下具有稳健性和持久性。此外,我们表明,在由半透膜分隔的系统中形成稳定的复合物组装体并不需要所有组分都预先受限,而只需要关键的膜不可渗透构建模块受限。用一个宏观的比喻来说,脂质囊泡就像瓶中船的构造,在一些关键木板受限之后,能够引导受限船的组装。因此,我们认为这里描述的受限效应在生命起源的最初阶段塑造原始细胞内化学复杂性的增加方面发挥了重要作用。此外,我们认为可以利用这种效应来设计基于相对简单囊泡的越来越高效的功能装置,用于生物传感、纳米反应器和药物递送载体等应用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4d4b/5885595/40e86dd87e14/c7sc04553k-f1.jpg

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