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Effect of Lung Surfactant Protein SP-C and SP-C-Promoted Membrane Fragmentation on Cholesterol Dynamics

机译:肺表面活性剂蛋白SP-C和SP-C促进的膜碎裂对胆固醇动力学的影响

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摘要

To allow breathing and prevent alveolar collapse, lung surfactant (LS) develops a complex membranous system at the respiratory surface. LS is defined by a specific protein and lipid composition, including saturated and unsaturated phospholipid species and cholesterol. Surfactant protein C (SP-C) has been suggested to be an essential element for sustaining the presence of cholesterol in surfactant without functional impairment. In this work, we used a fluorescent sterol-partitioning assay to assess the effect of the surfactant proteins SP-B and SP-C on cholesterol distribution in membranes. Our results suggest that in the LS context, the combined action of SP-B and SP-C appears to facilitate cholesterol dynamics, whereas SP-C does not seem to establish a direct interaction with cholesterol that could increase the partition of free cholesterol into membranes. Interestingly, SP-C exhibits a membrane-fragmentation behavior, leading to the conversion of large unilamellar vesicles into highly curved vesicles ∼25 nm in diameter. Sterol partition was observed to be sensitive to the bending of bilayers, indicating that the effect of SP-C to mobilize cholesterol could be indirectly associated with SP-C-mediated membrane remodeling. Our results suggest a potential role for SP-C in generating small surfactant structures that may participate in cholesterol mobilization and pulmonary surfactant homeostasis at the alveolar interfaces.
机译:为了允许呼吸并防止肺泡塌陷,肺表面活性剂(LS)在呼吸表面形成了复杂的膜系统。 LS由特定的蛋白质和脂质组成定义,包括饱和和不饱和磷脂种类和胆固醇。表面活性剂蛋白C(SP-C)被认为是在表面活性剂中维持胆固醇存在而又不损害功能的必要元素。在这项工作中,我们使用了荧光固醇分配测定法来评估表面活性剂蛋白SP-B和SP-C对膜中胆固醇分布的影响。我们的结果表明,在LS背景下,SP-B和SP-C的联合作用似乎促进了胆固醇的动态变化,而SP-C似乎并未与胆固醇建立直接相互作用,从而可能增加游离胆固醇在膜中的分配。有趣的是,SP-C表现出膜碎片行为,导致大的单层囊泡转变为直径约25 nm的高度弯曲的囊泡。观察到甾醇分配对双层的弯曲敏感,表明SP-C调动胆固醇的作用可能与SP-C介导的膜重塑间接相关。我们的结果表明SP-C在产生可能参与胆固醇动员和肺泡界面处肺表面活性剂稳态的小的表面活性剂结构中的潜在作用。

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