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肺表面活性蛋白 SP-B 促进从单层到双层储库的形成以及界面与亚相之间的脂质传递。

Lung surfactant protein SP-B promotes formation of bilayer reservoirs from monolayer and lipid transfer between the interface and subphase.

机构信息

Department of Biological Sciences, University of Calgary, Calgary, Alberta, Canada.

出版信息

Biophys J. 2011 Apr 6;100(7):1678-87. doi: 10.1016/j.bpj.2011.02.019.

Abstract

We investigated the possible role of SP-B proteins in the function of lung surfactant. To this end, lipid monolayers at the air/water interface, bilayers in water, and transformations between them in the presence of SP-B were simulated. The proteins attached bilayers to monolayers, providing close proximity of the reservoirs with the interface. In the attached aggregates, SP-B mediated establishment of the lipid-lined connection similar to the hemifusion stalk. Via this connection, a lipid flow was initiated between the monolayer at the interface and the bilayer in water in a surface-tension-dependent manner. On interface expansion, the flow of lipids to the monolayer restored the surface tension to the equilibrium spreading value. SP-B induced formation of bilayer folds from the monolayer at positive surface tensions below the equilibrium. In the absence of proteins, lipid monolayers were stable at these conditions. Fold nucleation was initiated by SP-B from the liquid-expanded monolayer phase by local bending, and the proteins lined the curved perimeter of the growing fold. No effect on the liquid-condensed phase was observed. Covalently linked dimers resulted in faster kinetics for monolayer folding. The simulation results are in line with existing hypotheses on SP-B activity in lung surfactant and explain its molecular mechanism.

摘要

我们研究了 SP-B 蛋白在肺表面活性剂功能中的可能作用。为此,模拟了气/水界面处的单层脂、水中的双层以及 SP-B 存在下它们之间的转化。这些蛋白质将双层附着到单层上,使储层与界面接近。在附着的聚集体中,SP-B 介导了类似于半融合柄的脂质衬里连接的建立。通过这种连接,以表面张力依赖性的方式在界面处的单层和水中的双层之间引发了脂质流动。在界面扩展时,脂质流向单层将表面张力恢复到平衡扩展值。在正表面张力下低于平衡时,SP-B 诱导单层形成双层褶皱。在没有蛋白质的情况下,这些条件下的单层脂是稳定的。褶皱成核是由 SP-B 通过局部弯曲从液体膨胀的单层相发起的,蛋白质排列在不断增长的褶皱的弯曲周边。在液体冷凝相中没有观察到影响。共价连接的二聚体导致单层折叠的动力学更快。模拟结果与肺表面活性剂中 SP-B 活性的现有假说一致,并解释了其分子机制。

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