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疏水表面活性蛋白对肺表面活性物质单分子层塌陷的影响。

Effects of hydrophobic surfactant proteins on collapse of pulmonary surfactant monolayers.

作者信息

Lhert Florence, Yan Wenfei, Biswas Samares C, Hall Stephen B

机构信息

Department of Biochemistry and Molecular Biology, Oregon Health & Science University, Portland, Oregon 97239, USA.

出版信息

Biophys J. 2007 Dec 15;93(12):4237-43. doi: 10.1529/biophysj.107.111823. Epub 2007 Aug 24.

Abstract

To determine if hydrophobic surfactant proteins affect the stability of pulmonary surfactant monolayers at an air/water interface, the studies reported here compared the kinetics of collapse for the complete set of lipids in calf surfactant with and without the proteins. Monomolecular films spread at the surface of captive bubbles were compressed at 37 degrees C to surface pressures above 46 mN/m, at which collapse first occurred. The rate of area-compression required to maintain a constant surface pressure was measured to directly determine the rate of collapse. For films with and without the proteins, higher surface pressures initially produced faster collapse, but the rates then reached a maximum and decreased to values <0.04 min(-1) above 53 mN/m. The maximum rate for the lipids with the proteins (1.22 +/- 0.28 min(-1)) was almost twice the value for the lipids alone (0.71 +/- 0.15 min(-1)). Because small increments in surface pressure produced large shifts in the rate close to the fastest collapse, compressions at a series of constant speeds also established the threshold rate required to achieve high surface pressure as an indirect indication of the fastest collapse. Both samples produced a sharply defined threshold that occurred at slightly faster compression with the proteins present, supporting the conclusion of the direct measurements that the proteins produce a faster maximum rate of collapse. Our results indicate that at 47-53 mN/m, the hydrophobic surfactant proteins destabilize the compressed monolayers and tend to limit access to the higher surface pressures at which the lipid films become metastable.

摘要

为了确定疏水性表面活性剂蛋白是否会影响肺表面活性剂单分子层在空气/水界面的稳定性,本文报道的研究比较了含有和不含这些蛋白的小牛表面活性剂中全套脂质的塌陷动力学。在捕获气泡表面铺展的单分子膜在37℃下被压缩至表面压力高于46 mN/m,此时首次发生塌陷。测量维持恒定表面压力所需的面积压缩速率,以直接确定塌陷速率。对于含蛋白和不含蛋白的膜,较高的表面压力最初会导致更快的塌陷,但随后速率达到最大值,并在高于53 mN/m时降至<0.04 min⁻¹的值。含蛋白脂质的最大速率(1.22±0.28 min⁻¹)几乎是仅脂质的两倍(0.71±0.15 min⁻¹)。由于表面压力的微小增加会在接近最快塌陷时使速率产生较大变化,以一系列恒定速度进行压缩也确定了达到高表面压力所需的阈值速率,作为最快塌陷的间接指标。两个样品都产生了一个明确界定的阈值,在有蛋白存在时压缩速度稍快时出现,这支持了直接测量的结论,即蛋白产生更快的最大塌陷速率。我们的结果表明,在47 - 53 mN/m时,疏水性表面活性剂蛋白会使压缩的单分子层不稳定,并倾向于限制达到脂质膜变得亚稳的更高表面压力。

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