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Dynamic and reversible control of 2D membrane protein concentration in a droplet interface bilayer

机译:动态和可逆控制液滴界面双层中二维膜蛋白浓度

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摘要

We form an artificial lipid bilayer between a nanolitre aqueous droplet and a supporting hydrogel immersed in an oil/lipid solution. Manipulation of the axial position of the droplet relative to the hydrogel controls the size of the bilayer formed at the interface; this enables the surface density of integral membrane proteins to be controlled. We are able to modulate the surface density of the β-barrel pore-forming toxin α-hemolysin over a range of 4 orders of magnitude within a time frame of a few seconds. The concentration changes are fully reversible. Membrane protein function and diffusion are unaltered, as measured by single molecule microscopy and single channel electrical recording.
机译:我们在纳升的水液滴和浸入油/脂溶液中的支持水凝胶之间形成人工脂质双层。液滴相对于水凝胶的轴向位置的控制控制了在界面处形成的双层的大小;这使得整合膜蛋白的表面密度得以控制。我们能够在几秒钟的时间内在4个数量级范围内调节β桶成孔毒素α-溶血素的表面密度。浓度变化是完全可逆的。通过单分子显微镜和单通道电记录测量,膜蛋白的功能和扩散没有改变。

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