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High-resolution investigation of nanoparticle interaction with a model pulmonary surfactant monolayer

机译:高分辨率研究模型肺表面活性剂单层纳米颗粒的相互作用

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The pulmonary surfactant film spanning the inner alveolar surface prevents alveolar collapse during the end-exhalation and reduces the work of breathing. Nanoparticles (NPs) present in the atmosphere or nanocarriers targeted through the pulmonary route for medical purposes challenge this biological barrier. During interaction with or passage of NPs through the alveolar surfactant, the biophysical functioning of the film may be altered. However, experimental evidence showing detailed biophysical interaction of NPs with the pulmonary surfactant film are scant. In this study, we have investigated the impact of a hydrophobic polyorganosiloxane (AmOrSil20) NPs on the integrity as well as on the structural organization of the model pulmonary surfactant film. Primarily, scanning force microscopic techniques and electron microscopy have been used to visualize the topology as well as to characterize the localization of nanoparticles within the compressed pulmonary surfactant film. We could show that the NPs partition in the fluid phase of the compressed film at lower surface pressure, and at higher surface pressure, such NPs interact extensively with the surface-associated structures. Major amounts of NPs are retained at the interface and are released slowly into the aqueous subphase during repeated compression/expansion cycles. Further, the process of vesicle insertion into the interfacial film was observed to slow down with increasing NP concentrations. The hydrophobic AmOrSil20 NPs up to a given concentration do not substantially affect the structural organization and functioning of pulmonary surfactant film; however, such NPs do show drastic impacts at higher concentrations.
机译:横跨肺泡内表面的肺表面活性剂膜可防止在呼气末期肺泡塌陷并减少呼吸功。大气中存在的纳米颗粒(NPs)或通过肺途径靶向的纳米载体(出于医学目的)挑战了这种生物屏障。在与NPs相互作用或通过其通过肺泡表面活性剂的过程中,膜的生物物理功能可能会改变。但是,很少有实验证据显示NP与肺表面活性剂膜的详细生物物理相互作用。在这项研究中,我们已经研究了疏水性聚有机硅氧烷(AmOrSil20)NPs对模型肺表面活性剂膜的完整性以及结构组织的影响。首先,扫描力显微镜技术和电子显微镜已用于可视化拓扑结构并表征纳米颗粒在压缩的肺表面活性剂膜内的定位。我们可以证明,在较低的表面压力和较高的表面压力下,NPs在压缩膜的液相中分配,这些NPs与表面相关的结构广泛相互作用。大量的NP保留在界面处,并在重复的压缩/膨胀循环中缓慢释放到水相中。此外,观察到囊泡插入界面膜的过程随着NP浓度的增加而减慢。达到给定浓度的疏水性AmOrSil20 NPs基本上不会影响肺表面活性剂膜的结构和功能。但是,这些NP在较高浓度下确实显示出剧烈的影响。

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