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棕榈酰化作为调节肺表面活性物质膜多层结构中SP-C-脂质相互作用的关键因素。

Palmitoylation as a key factor to modulate SP-C-lipid interactions in lung surfactant membrane multilayers.

作者信息

Roldan Nuria, Goormaghtigh Erik, Pérez-Gil Jesús, Garcia-Alvarez Begoña

机构信息

Department of Biochemistry and Molecular Biology I, Faculty of Biological Sciences, Universidad Complutense de Madrid, Spain.

Laboratory for the Structure and Function of Biological Membranes, Center for Structural Biology and Bioinformatics, Université Libre de Bruxelles (ULB), Belgium.

出版信息

Biochim Biophys Acta. 2015 Jan;1848(1 Pt A):184-91. doi: 10.1016/j.bbamem.2014.10.009. Epub 2014 Oct 12.

DOI:10.1016/j.bbamem.2014.10.009
PMID:25306965
Abstract

Surfactant protein C (SP-C) has been regarded as the most specific protein linked to development of mammalian lungs, and great efforts have been done to understand its structure-function relationships. Previous evidence has outlined the importance of SP-C palmitoylation to sustain the proper dynamics of lung surfactant, but the mechanism by which this posttranslational modification aids SP-C to stabilize the interfacial surfactant film along the compression-expansion breathing cycles, is still unrevealed. In this work we have compared the structure, orientation and lipid-protein interactions of a native palmitoylated SP-C with those of a non-palmitoylated recombinant SP-C (rSP-C) form in air-exposed multilayer membrane environments, by means of ATR-FTIR spectroscopy. Palmitoylation does not affect the secondary structure of the protein, which exhibits a full α-helical conformation in partly dehydrated phospholipid multilayer films. However, differences between the Amide I band of the IR spectrum of palmitoylated and non-palmitoylated proteins suggest subtle differences affecting the environment of their helical component. These differences are accompanied by differential effects on the IR bands from phospholipid phosphates, indicating that palmitoylation modulates lipid-protein interactions at the headgroup region of phospholipid layers. On the other hand, the relative dichroic absorption of polarized IR has allowed calculating that the palmitoylated protein adopts a more tilted transmembrane orientation than the non-palmitoylated SP-C, likely contributing to more compact, dehydrated and possibly stable multilayer lipid-protein films. As a whole, the behavior of multilayer films containing palmitoylated SP-C may reflect favorable structural properties for surfactant reservoirs at the air-liquid respiratory interface.

摘要

表面活性蛋白C(SP-C)被认为是与哺乳动物肺发育相关的最具特异性的蛋白质,人们已经付出了巨大努力来了解其结构与功能的关系。先前的证据已经阐明了SP-C棕榈酰化对于维持肺表面活性剂正常动态的重要性,但是这种翻译后修饰帮助SP-C在呼吸的压缩-膨胀循环中稳定界面表面活性剂膜的机制仍未揭示。在这项工作中,我们通过衰减全反射傅里叶变换红外光谱(ATR-FTIR),比较了天然棕榈酰化的SP-C与非棕榈酰化重组SP-C(rSP-C)在暴露于空气的多层膜环境中的结构、取向和脂-蛋白相互作用。棕榈酰化不影响蛋白质的二级结构,该蛋白质在部分脱水的磷脂多层膜中呈现出完整的α-螺旋构象。然而,棕榈酰化和非棕榈酰化蛋白质红外光谱的酰胺I带之间的差异表明,其螺旋成分的环境存在细微差异。这些差异伴随着对磷脂磷酸盐红外波段的不同影响,表明棕榈酰化调节了磷脂层头部区域的脂-蛋白相互作用。另一方面,偏振红外的相对二向色吸收使得我们能够计算出,棕榈酰化蛋白质比非棕榈酰化的SP-C具有更倾斜的跨膜取向,这可能有助于形成更致密、脱水且可能更稳定的多层脂-蛋白膜。总体而言,含有棕榈酰化SP-C的多层膜的行为可能反映了气液呼吸界面处表面活性剂储库的有利结构特性。

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