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含肺表面活性物质蛋白C的脂质膜在气-水界面作为肺泡表面的模型。

Pulmonary surfactant protein C containing lipid films at the air-water interface as a model for the surface of lung alveoli.

作者信息

Post A, Nahmen A V, Schmitt M, Ruths J, Riegler H, Sieber M, Galla H J

机构信息

Institute of Biochemistry, Westfälische Wilhelms-Universität Münster, Germany.

出版信息

Mol Membr Biol. 1995 Jan-Mar;12(1):93-9. doi: 10.3109/09687689509038502.

DOI:10.3109/09687689509038502
PMID:7767391
Abstract

The pulmonary surfactant lines as a complex monolayer of lipids and proteins the alveolar epithelial surface. The monolayer dynamically adapts the surface tension of this interface to the varying surface areas during inhalation and exhalation. Its presence in the alveoli is thus a prerequisite for a proper lung function. The lipid moiety represents about 90% of the surfactant and contains mainly dipalmitoylphosphatidylcholine (DPPC) and phosphatidylglycerol (PG). The surfactant proteins involved in the surface tension adaption are called SP-A, SP-B and SP-C. The aim of the present investigation is to analyse the properties of monolayer films made from pure SP-C and from mixtures of DPPC, DPPG and SP-C in order to mimic the surfactant monolayer with minimal compositional requirement. Pressure-area diagrams were taken. Ellipsometric measurements at the air-water interface of a Langmuir film balance allowed measurement of the changes in monolayer thickness upon compression. Isotherms of pure SP-C monolayers exhibit a plateau between 22 and 25 mN/m. A further plateau is reached at higher compression. Structures of the monolayer formed during compression are reversible during expansion. Together with ellipsometric data which show a stepwise increase in film thickness (coverage) during compression, we conclude that pure SP-C films rearrange reversibly into multilayers of homogenous thickness. Lipid monolayers collapse locally and irreversibly if films are compressed to approximately 0.4 nm2/molecule. In contrast, mixed DPPG/SP-C monolayers with less than 5 mol% protein collapse in a controlled and reversible way. The pressure-area diagrams exhibit a plateau at 20 mN/m, indicating partial demixing of SP-C and DPPG.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

肺表面活性剂以脂质和蛋白质的复杂单分子层形式覆盖肺泡上皮表面。在吸气和呼气过程中,该单分子层动态调节此界面的表面张力以适应不同的表面积。因此,其在肺泡中的存在是肺功能正常的先决条件。脂质部分约占表面活性剂的90%,主要包含二棕榈酰磷脂酰胆碱(DPPC)和磷脂酰甘油(PG)。参与表面张力调节的表面活性剂蛋白称为SP - A、SP - B和SP - C。本研究的目的是分析由纯SP - C以及DPPC、DPPG和SP - C混合物制成的单分子层膜的特性,以便以最少的成分要求模拟表面活性剂单分子层。绘制了压力 - 面积图。在Langmuir膜天平的气 - 水界面进行椭偏测量,可测量压缩过程中单分子层厚度的变化。纯SP - C单分子层的等温线在22至25 mN/m之间呈现一个平台期。在更高压缩程度下会达到另一个平台期。压缩过程中形成的单分子层结构在膨胀时是可逆的。结合椭偏数据显示压缩过程中膜厚度(覆盖率)逐步增加,我们得出结论,纯SP - C膜可逆地重排成均匀厚度的多层结构。如果将膜压缩至约0.4 nm2/分子,脂质单分子层会局部不可逆地塌陷。相比之下,蛋白质含量低于5 mol%的DPPG/SP - C混合单分子层以可控且可逆的方式塌陷。压力 - 面积图在20 mN/m处呈现一个平台期,表明SP - C和DPPG发生了部分分离。(摘要截选至250字)

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