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肺表面活性剂及其对薄膜稳定性的不同作用。

Lung surfactants and different contributions to thin film stability.

作者信息

Hermans Eline, Bhamla M Saad, Kao Peter, Fuller Gerald G, Vermant Jan

机构信息

Department of Chemical Engineering, KU Leuven, Belgium.

出版信息

Soft Matter. 2015 Nov 7;11(41):8048-57. doi: 10.1039/c5sm01603g.

Abstract

The surfactant lining the walls of the alveoli in the lungs increases pulmonary compliance and prevents collapse of the lung at the end of expiration. In premature born infants, surfactant deficiency causes problems, and lung surfactant replacements are instilled to facilitate breathing. These pulmonary surfactants, which form complex structured fluid-fluid interfaces, need to spread with great efficiency and once in the alveolus they have to form a thin stable film. In the present work, we investigate the mechanisms affecting the stability of surfactant-laden thin films during spreading, using drainage flows from a hemispherical dome. Three commercial lung surfactant replacements Survanta, Curosurf and Infasurf, along with the phospholipid dipalmitoylphosphatidylcholine (DPPC), are used. The surface of the dome can be covered with human alveolar epithelial cells and experiments are conducted at the physiological temperature. Drainage is slowed down due to the presence of all the different lung surfactant replacements and therefore the thin films show enhanced stability. However, a scaling analysis combined with visualization experiments demonstrates that different mechanisms are involved. For Curosurf and Infasurf, Marangoni stresses are essential to impart stability and interfacial shear rheology does not play a role, in agreement with what is observed for simple surfactants. Survanta, which was historically the first natural surfactant used, is rheologically active. For DPPC the dilatational properties play a role. Understanding these different modes of stabilization for natural surfactants can benefit the design of effective synthetic surfactant replacements for treating infant and adult respiratory disorders.

摘要

肺部肺泡壁内衬的表面活性剂可增加肺顺应性,并防止肺在呼气末塌陷。对于早产婴儿,表面活性剂缺乏会引发问题,因此需注入肺表面活性剂替代品以促进呼吸。这些肺表面活性剂形成复杂的结构化液-液界面,需要高效铺展,并且一旦进入肺泡,它们必须形成一层薄而稳定的膜。在本研究中,我们利用半球形穹顶的排水流来研究影响铺展过程中含表面活性剂薄膜稳定性的机制。我们使用了三种商业肺表面活性剂替代品Survanta、珂立苏(Curosurf)和固尔苏(Infasurf),以及磷脂二棕榈酰磷脂酰胆碱(DPPC)。穹顶表面可覆盖人肺泡上皮细胞,并在生理温度下进行实验。由于所有不同的肺表面活性剂替代品的存在,排水速度减慢,因此薄膜显示出增强的稳定性。然而,结合可视化实验的标度分析表明涉及不同的机制。对于珂立苏和固尔苏,马兰戈尼应力对于赋予稳定性至关重要,而界面剪切流变学不起作用,这与简单表面活性剂的观察结果一致。Survanta是历史上最早使用的天然表面活性剂,具有流变活性。对于DPPC,膨胀特性起作用。了解天然表面活性剂这些不同的稳定模式有助于设计用于治疗婴儿和成人呼吸系统疾病的有效合成表面活性剂替代品。

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