Knebel D, Sieber M, Reichelt R, Galla H-J, Amrein M
Institut für Biochemie, Westfälische Wilhelms-Universität, D-48149 Münster, Germany.
Biophys J. 2002 Jul;83(1):547-55. doi: 10.1016/S0006-3495(02)75190-4.
The structural dynamics of pulmonary surfactant was studied by epifluorescence light microscopy at the air-water interface of a bubble as a model close to nature for an alveolus. Small unilamellar vesicles of dipalmitoylphosphatidylcholine, dipalmitoylphosphatidylglycerol, a small amount of a fluorescent dipalmitoylphosphatidylcholine-analog, and surfactant-associated protein C were injected into the buffer solution. They aggregated to large clusters in the presence of Ca(2+) and adsorbed from these units to the interface. This gave rise to an interfacial film that eventually became fully condensed with dark, polygonal domains in a fluorescent matrix. When now the bubble size was increased or decreased, respectively, the film expanded or contracted. Upon expansion of the bubble, the dark areas became larger to the debit of the bright matrix and reversed upon contraction. We were able to observe single domains during the whole process. The film remained condensed, even when the interface was increased to twice its original size. From comparison with scanning force microscopy directly at the air-water interface, the fluorescent areas proved to be lipid bilayers associated with the (dark) monolayer. In the lung, such multilayer phase acts as a reservoir that guarantees a full molecular coverage of the alveolar interface during the breathing cycle and provides mechanical stability to the film.
以气泡的气-水界面作为接近肺泡自然状态的模型,通过落射荧光显微镜研究了肺表面活性剂的结构动力学。将二棕榈酰磷脂酰胆碱、二棕榈酰磷脂酰甘油、少量荧光二棕榈酰磷脂酰胆碱类似物和表面活性剂相关蛋白C的小单层囊泡注入缓冲溶液中。它们在Ca(2+)存在下聚集形成大的聚集体,并从这些聚集体吸附到界面上。这产生了一种界面膜,最终在荧光基质中形成完全凝聚的暗多边形区域。当气泡尺寸分别增大或减小时,膜会扩张或收缩。气泡扩张时,暗区变大,亮基质减少,收缩时则相反。在整个过程中我们能够观察到单个区域。即使界面增大到原来的两倍,膜仍保持凝聚状态。通过与直接在气-水界面的扫描力显微镜比较,荧光区域被证明是与(暗)单层相关的脂质双层。在肺中,这种多层相作为一个储存库,可确保在呼吸周期中肺泡界面得到完全的分子覆盖,并为膜提供机械稳定性。