Institute of Biochemistry, Biocenter, Goethe-University Frankfurt, Max-von Laue-Straße 9, 60438 Frankfurt a.M., Germany.
ACS Nano. 2021 Apr 27;15(4):6747-6755. doi: 10.1021/acsnano.0c10139. Epub 2021 Mar 16.
Cellular life depends on transport and communication across membranes, which is emphasized by the fact that membrane proteins are prime drug targets. The cell-like environment of membrane proteins has gained increasing attention based on its important role in function and regulation. As a versatile scaffold for bottom-up synthetic biology and nanoscience, giant liposomes represent minimalistic models of living cells. Nevertheless, the incorporation of fragile multiprotein membrane complexes still remains a major challenge. Here, we report on an approach for the functional reconstitution of membrane assemblies exemplified by human and bacterial ATP-binding cassette (ABC) transporters. We reveal that these nanomachineries transport substrates unidirectionally against a steep concentration gradient. Active substrate transport can be spatiotemporally resolved in single cell-like compartments by light, enabling real-time tracking of substrate export and import in individual liposomes. This approach will help to construct delicate artificial cell-like systems.
细胞的生命依赖于跨膜的运输和通讯,这一点在膜蛋白是主要的药物靶点这一事实上得到了强调。基于膜蛋白在功能和调节中的重要作用,其类似细胞的环境越来越受到关注。巨大的脂质体作为自下而上的合成生物学和纳米科学的通用支架,代表了最简单的活细胞模型。然而,脆弱的多蛋白膜复合物的掺入仍然是一个主要的挑战。在这里,我们报告了一种功能重建膜组件的方法,以人和细菌的 ATP 结合盒(ABC)转运蛋白为例。我们揭示了这些纳米机器可以沿着陡峭的浓度梯度单向运输底物。通过光可以在单细胞样隔室中空间和时间分辨地解析活性底物的运输,从而能够实时跟踪单个脂质体中底物的输出和输入。这种方法将有助于构建精细的人工细胞样系统。
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