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Fluidization of a Dipalmitoyl Phosphatidylcholine Monolayer by Fluorocarbon Gases: Potential Use in Lung Surfactant Therapy

机译:碳氟化合物气体流化二棕榈酰磷脂酰胆碱单层:在肺表面活性剂治疗中的潜在用途。

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摘要

Fluorocarbon gases (gFCs) were found to inhibit the liquid-expanded (LE)/liquid-condensed (LC) phase transition of dipalmitoyl phosphatidylcholine (DPPC) Langmuir monolayers. The formation of domains of an LC phase, which typically occurs in the LE/LC coexistence region upon compression of DPPC, is prevented when the atmosphere above the DPPC monolayer is saturated with a gFC. When contacted with gFC, the DPPC monolayer remains in the LE phase for surface pressures lower than 38 mN m−1, as assessed by compression isotherms and fluorescence microscopy (FM). Moreover, gFCs can induce the dissolution of preexisting LC phase domains and facilitate the respreading of the DPPC molecules on the water surface, as shown by FM and grazing incidence x-ray diffraction. gFCs have thus a highly effective fluidizing effect on the DPPC monolayer. This gFC-induced fluidizing effect was compared with the fluidizing effect brought about by a mixture of unsaturated lipids and proteins, namely the two commercially available lung surfactant substitutes, Curosurf and Survanta, which are derived from porcine and bovine lung extracts, respectively. The candidate FCs were chosen among those already investigated for biomedical applications, and in particular for intravascular oxygen transport, i.e., perfluorooctyl bromide, perfluorooctylethane, bis(perfluorobutyl)ethene, perfluorodecalin, and perfluorooctane. The fluidizing effect is most effective with the linear FCs. This study suggests that FCs, whose biocompatibility is well documented, may be useful in lung surfactant substitute compositions.
机译:发现碳氟化合物气体(gFCs)抑制二棕榈酰磷脂酰胆碱(DPPC)Langmuir单层的液体膨胀(LE)/液体冷凝(LC)相变。当DPPC单层上方的气氛被gFC饱和时,可防止LC相域的形成(通常在DPPC压缩时出现在LE / LC共存区域中)。通过压缩等温线和荧光显微镜(FM)评估,当与gFC接触时,DPPC单层保持在LE相,表面压力低于38 mN m -1 。此外,gFM可诱导先前存在的LC相域的溶解,并促进DPPC分子在水表面的重新扩散,如FM和掠入射X射线衍射所示。因此,gFC对DPPC单层具有非常有效的流化作用。将这种gFC诱导的流化效果与不饱和脂质和蛋白质(即分别从猪和牛肺提取物中得到的两种市售肺表面活性剂替代品Curosurf和Survanta)带来的流化效果进行了比较。候选FCs是从已经研究用于生物医学应用,尤其是用于血管内氧气运输的那些中选择的,即全氟辛基溴化物,全氟辛基乙烷,双(全氟丁基)乙烯,全氟十氢化萘和全氟辛烷。线性FC的流化效果最有效。这项研究表明,具有良好生物相容性的FCs可能在肺表面活性剂替代品组合物中有用。

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