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Transient Nanoscopic Phase Separation in Biological Lipid Membranes Resolved by Planar Plasmonic Antennas

机译:通过平面等离子体天线解决的生物脂质膜中的瞬时纳米镜分离

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Nanoscale membrane assemblies of sphingolipids, cholesterol, and certain proteins, also known as lipid rafts, play a crucial role in facilitating a broad range of important cell functions. Whereas on living cell membranes lipid rafts have been postulated to have nanoscopic dimensions and to be highly transient, the existence of a similar type of dynamic nanodomains in multicomponent lipid bilayers has been questioned. Here, we perform fluorescence correlation spectroscopy on planar plasmonic antenna arrays with different nanogap sizes to assess the dynamic nanoscale organization of mimetic biological membranes. Our approach takes advantage of the highly enhanced and confined excitation light provided by the nanoantennas together with their outstanding planarity to investigate membrane regions as small as 10 mu in size with microsecond time resolution. Our diffusion data are consistent with the coexistence of transient nanoscopic domains in both the liquid-ordered and the liquid-disordered microscopic phases of multicomponent lipid bilayers. These nanodomains have characteristic residence times between 30 and 150 mu s and sizes around 10 nm, as inferred from the diffusion data. Thus, although microscale phase separation occurs on mimetic membranes, nanoscopic domains also coexist, suggesting that these transient assemblies might be similar to those occurring in living cells, which in the absence of raft-stabilizing proteins are poised to be short-lived. Importantly, our work underscores the high potential of photonic nanoantennas to interrogate the nanoscale heterogeneity of native biological membranes with ultrahigh spatiotemporal resolution.
机译:含鞘脂素,胆固醇和某些蛋白质的纳米级膜组件,也称为脂质筏,在促进广泛的重要细胞功能方面发挥至关重要的作用。然而,在活细胞膜上已经假设脂质筏具有纳米镜尺寸并且是高瞬态的,并且存在类似类型的多组分脂质双层在多组分脂质双层的存在。这里,我们在具有不同纳米剧尺寸的平面等离子体天线阵列上进行荧光相关光谱,以评估模拟生物膜的动态纳米级组织。我们的方法利用了纳米环绕的高度增强和狭窄的激发光,以及它们出色的平面性,以调查膜区域,以微秒的时间分辨率调查大约10μm的10μm。我们的扩散数据与多组分脂质双层的液体有序和液体无序微观相中的瞬时纳米镜域的共存一致。这些纳米弥射具有30至150μs的特征停留时间,并且尺寸约为10nm,从扩散数据推断。因此,尽管在模拟膜上发生微米相分离,但是纳米镜域也共存,表明这些瞬态组件可能与活细胞中发生的那些相似,在没有筏稳定的蛋白质的情况下,这在没有筏子稳定的蛋白质的情况下被达到短暂的蛋白质。重要的是,我们的工作强调了光子纳米环绕的高潜力,以询问天然生物膜的纳米级异质性,具有超高的时空分辨率。

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