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外周结合肽沿外膜和内膜小叶的耦合扩散。

Coupled diffusion of peripherally bound peptides along the outer and inner membrane leaflets.

作者信息

Horner Andreas, Antonenko Yuri N, Pohl Peter

机构信息

Institut für Biophysik, Johannes Kepler Universität Linz, Linz, Austria.

出版信息

Biophys J. 2009 Apr 8;96(7):2689-95. doi: 10.1016/j.bpj.2008.12.3931.

Abstract

Transmembrane signaling implies that peripheral protein binding to one leaflet be detected by the opposite leaflet. Therefore, protein recruitment into preexisting cholesterol and sphingolipid rich platforms may be required. However, no clear molecular picture has evolved about how these rafts in both leaflets are connected. By using planar lipid bilayers, we show that the peripheral binding of a charged molecule (poly-lysine, PLL) is detected at the other side of the bilayer without involvement of raft lipids. The diffusion coefficient, D(P), of PLL differed by a factor of radical2 when PLL absorbed to one or to both leaflets of planar membranes. Fluorescence correlation spectroscopy showed that the changes of the lipid diffusion coefficient, D(M), were even more pronounced. Although D(M) remained larger than D(P) on PLL binding to the first membrane leaflet, D(M) dropped to D(P) on PLL binding to both leaflets, which indicated that the lipids sandwiched between two PLL molecules had formed a nanodomain. Due to its small area of approximately 20 nm(2) membrane electrostriction or leaflet interaction at bilayer midplane can only make a small contribution to interleaflet coupling. The tendency of the system to maximize the area where the membrane is free to undulate seems to be more important. As a spot with increased bending stiffness, the PLL bound patch in one leaflet attracts a stiffening additive on the other leaflet. That is to say, instead of suppressing undulations in two spots, two opposing PLL molecules migrate along a membrane at matching positions and suppress these undulations in a single spot. The gain in undulation energy is larger than the energy required for the alignment of two small PLL domains in opposite leafs and their coordinated diffusion. We propose that this type of mechanical interaction between two membrane separated ligands generally contributes to transmembrane signaling.

摘要

跨膜信号传导意味着外周蛋白与一个脂单层的结合要被相对的另一个脂单层所检测到。因此,可能需要将蛋白质募集到预先存在的富含胆固醇和鞘脂的平台中。然而,关于两个脂单层中的这些筏是如何连接的,尚未形成清晰的分子图景。通过使用平面脂质双层,我们发现带电荷分子(聚赖氨酸,PLL)的外周结合能在双层的另一侧被检测到,而无需筏脂的参与。当PLL吸附到平面膜的一个或两个脂单层时,PLL的扩散系数D(P)相差根号2倍。荧光相关光谱表明,脂质扩散系数D(M)的变化更为显著。虽然在PLL与第一个膜脂单层结合时D(M)仍大于D(P),但在PLL与两个脂单层都结合时D(M)降至D(P),这表明夹在两个PLL分子之间的脂质形成了一个纳米结构域。由于其面积小,约为20 nm²,膜电致收缩或双层中间平面处的脂单层相互作用对层间偶联的贡献很小。系统使膜自由起伏的面积最大化的趋势似乎更为重要。作为一个弯曲刚度增加的位点,一个脂单层中结合PLL的斑块会吸引另一个脂单层上的硬化添加剂。也就是说,两个相对的PLL分子不是在两个位点抑制起伏,而是在匹配位置沿着膜迁移,并在单个位点抑制这些起伏。起伏能量的增加大于两个小PLL结构域在相对叶中对齐及其协同扩散所需的能量。我们提出,两个膜分离配体之间的这种机械相互作用通常有助于跨膜信号传导。

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