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'Frozen' Block Copolymer Nanomembranes with Light-Driven Proton Pumping Performance

机译:具有光驱动质子泵送性能的“冷冻”嵌段共聚物纳米膜

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摘要

Cellular membranes are natural nanoengineering devices, where matter transport, information processing, and energy conversion across the nanoscale boundaries are mediated by membrane proteins (MPs). Despite the great potential of MPs for nanotechnologies, their broad utility in engineered systems is limited by the fluidic and often labile nature of MP-supporting membranes. Little is known on how to direct spontaneous reconstitution of MPs into robust synthetic nanomembranes or how to tune MP functions through rational design of these membranes. Here we report that proteorhodopsin (PR), a lightdriven proton pump, can be spontaneously reconstituted into "frozen" (i.e., glassy state) amphiphilic block copolymer membranes via a charge-interactiondirected reconstitution mechanism. We show that PR is not enslaved by a fluidic or lipid-based membrane environment. Rather, well-defined block copolymer nanomembranes, with their tunable membrane moduli, act as allosteric regulators to support the structural integrity and function of PR. Versatile membrane designs exist to modulate the conformational energetics of reconstituted MPs, therefore optimizing proteomembrane stability and performance in synthetic systems.
机译:细胞膜是天然的纳米工程设备,物质运输,信息处理和跨纳米级边界的能量转换由膜蛋白(MPs)介导。尽管MP在纳米技术中具有巨大的潜力,但它们在工程系统中的广泛应用受到MP支持膜的流动性和不稳定特性的限制。关于如何将MP的自发重组成坚固的合成纳米膜,或者如何通过合理设计这些膜来调节MP功能,人们所知甚少。在这里,我们报道蛋白视紫红质(PR),一种光驱动的质子泵,可以通过电荷相互作用导向的重构机制自发地重构为“冻结的”(即玻璃态)两亲嵌段共聚物膜。我们表明,PR不被流体或基于脂质的膜环境所奴役。相反,定义明确的嵌段共聚物纳米膜及其可调的膜模量可作为变构调节剂,以支持PR的结构完整性和功能。存在通用的膜设计来调节重构MP的构象能量,因此优化了合成系统中蛋白膜的稳定性和性能。

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