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Divide Conquer: Surfactant Protein SP-C and Cholesterol Modulate Phase Segregation in Lung Surfactant

机译:分而治之:表面活性剂蛋白SP-C和胆固醇调节肺表面活性剂中的相分离

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摘要

Lung surfactant (LS) is an essential system supporting the respiratory function. Cholesterol can be deleterious for LS function, a condition that is reversed by the presence of the lipopeptide SP-C. In this work, the structure of LS-mimicking membranes has been analyzed under the combined effect of SP-C and cholesterol by deuterium NMR and phosphorus NMR and by electron spin resonance. Our results show that SP-C induces phase segregation at 37°C, resulting in an ordered phase with spectral features resembling an interdigitated state enriched in dipalmitoylphosphatidylcholine, a liquid-crystalline bilayer phase, and an extremely mobile phase consistent with small vesicles or micelles. In the presence of cholesterol, POPC and POPG motion seem to be more hindered by SP-C than dipalmitoylphosphatidylcholine. The use of deuterated cholesterol did not show signs of specific interactions that could be attributed to SP-C or to the other hydrophobic surfactant protein SP-B. Palmitoylation of SP-C had an indirect effect on the extent of protein-lipid perturbations by stabilizing SP-C structure, and seemed to be important to maximize differences among the lipids participating in each phase. These results shed some light on how SP-C-induced lipid perturbations can alter membrane structure to sustain LS functionality at the air-liquid interface.
机译:肺表面活性剂(LS)是支持呼吸功能的重要系统。胆固醇可能对LS功能有害,这种情况会因脂肽SP-C的存在而逆转。在这项工作中,通过氘核磁共振和磷核磁共振以及电子自旋共振分析了在SP-C和胆固醇共同作用下模拟LS的膜的结构。我们的研究结果表明,SP-C在37°C诱导相分离,导致具有类似光谱特征的有序相,该相特征富含二棕榈酰磷脂酰胆碱,液晶双层相以及与小囊泡或胶束一致的极易流动的相。在存在胆固醇的情况下,SP-C似乎比二棕榈酰磷脂酰胆碱更能阻止POPC和POPG的运动。氘化胆固醇的使用没有显示出特定相互作用的迹象,该相互作用可能归因于SP-C或其他疏水性表面活性剂蛋白SP-B。通过稳定SP-C结构,SP-C的棕榈酰化对蛋白质-脂质扰动的程度具有间接影响,并且对于最大化参与每个阶段的脂质之间的差异似乎很重要。这些结果为SP-C诱导的脂质扰动如何改变膜结构以在气液界面维持LS功能提供了一些启示。

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