Nag K, Perez-Gil J, Ruano M L, Worthman L A, Stewart J, Casals C, Keough K M
Department of Biochemistry, Memorial University of Newfoundland, St. John's, Canada.
Biophys J. 1998 Jun;74(6):2983-95. doi: 10.1016/S0006-3495(98)78005-1.
Pulmonary surfactant maintains a putative surface-active film at the air-alveolar fluid interface and prevents lung collapse at low volumes. Porcine lung surfactant extracts (LSE) were studied in spread and adsorbed films at 23 +/- 1 degrees C using epifluorescence microscopy combined with surface balance techniques. By incorporating small amounts of fluorescent probe 1-palmitoyl-2-nitrobenzoxadiazole dodecanoyl phosphatidylcholine (NBD-PC) in LSE films the expanded (fluid) to condensed (gel-like) phase transition was studied under different compression rates and ionic conditions. Films spread from solvent and adsorbed from vesicles both showed condensed (probe-excluding) domains dispersed in a background of expanded (probe-including) phase, and the appearance of the films was similar at similar surface pressure. In quasistatically compressed LSE films the appearance of condensed domains occurred at a surface pressure (pi) of 13 mN/m. Such domains increased in size and amounts as pi was increased to 35 mN/m, and their amounts appeared to decrease to 4% upon further compression to 45 mN/m. Above pi of 45 mN/m the LSE films had the appearance of filamentous materials of finely divided dark and light regions, and such features persisted up to a pi near 68 mN/m. Some of the condensed domains had typical kidney bean shapes, and their distribution was similar to those seen previously in films of dipalmitoylphosphatidylcholine (DPPC), the major component of surfactant. Rapid cyclic compression and expansion of LSE films resulted in features that indicated a possible small (5%) loss of fluid components from such films or an increase in condensation efficiency over 10 cycles. Calcium (5 mM) in the subphase of LSE films altered the domain distribution, decreasing the size and increasing the number and total amount of condensed phase domains. Calcium also caused an increase in the value of pi at which the maximum amount of independent condensed phase domains were observed to 45 mN/m. It also induced formation of large amounts of novel, nearly circular domains containing probe above pi of 50 mN/m, these domains being different in appearance than any seen at lower pressures with calcium or higher pressures in the absence of calcium. Surfactant protein-A (SP-A) adsorbed from the subphase onto solvent-spread LSE films, and aggregated condensed domains in presence of calcium. This study indicates that spread or adsorbed lung surfactant films can undergo expanded to condensed, and possibly other, phase transitions at the air-water interface as lateral packing density increases. These phase transitions are affected by divalent cations and SP-A in the subphase, and possibly by loss of material from the surface upon cyclic compression and expansion.
肺表面活性物质在气-肺泡液界面维持一层假定的表面活性膜,并防止肺在低容积时塌陷。使用落射荧光显微镜结合表面天平技术,在23±1℃下研究了猪肺表面活性物质提取物(LSE)在铺展和吸附膜中的情况。通过在LSE膜中加入少量荧光探针1-棕榈酰-2-硝基苯并恶二唑十二烷酰磷脂酰胆碱(NBD-PC),研究了在不同压缩速率和离子条件下从膨胀(流体)到凝聚(凝胶状)的相变。从溶剂铺展的膜和从囊泡吸附的膜都显示出凝聚(探针排斥)区域分散在膨胀(探针包含)相的背景中,并且在相似的表面压力下膜的外观相似。在准静态压缩的LSE膜中,凝聚区域在表面压力(π)为13 mN/m时出现。随着π增加到35 mN/m,这些区域的尺寸和数量增加,当进一步压缩到45 mN/m时,它们的数量似乎减少到4%。在π高于45 mN/m时,LSE膜呈现出由细分的暗区和亮区组成的丝状材料外观,并且这些特征一直持续到π接近68 mN/m。一些凝聚区域具有典型的菜豆形状,并且它们的分布与先前在表面活性物质的主要成分二棕榈酰磷脂酰胆碱(DPPC)膜中看到的相似。LSE膜的快速循环压缩和膨胀导致的特征表明,此类膜可能有少量(5%)的流体成分损失,或者在10个循环中凝聚效率增加。LSE膜亚相中5 mM的钙改变了区域分布,减小了凝聚相区域的尺寸,增加了其数量和总量。钙还使观察到最大量独立凝聚相区域时的π值增加到45 mN/m。它还在π高于50 mN/m时诱导形成大量含有探针的新型近圆形区域,这些区域的外观与在较低压力下有钙存在或在无钙时较高压力下看到的任何区域都不同。表面活性物质蛋白-A(SP-A)从亚相吸附到溶剂铺展的LSE膜上,并在有钙存在时使凝聚区域聚集。这项研究表明,随着横向堆积密度的增加,铺展或吸附的肺表面活性物质膜在气-水界面可经历从膨胀到凝聚以及可能的其他相变。这些相变受亚相中二价阳离子和SP-A的影响,并且可能受循环压缩和膨胀时表面物质损失的影响。
