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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Cholesterol modulates the exposure and orientation of pulmonary surfactant protein SP-C in model surfactant membranes.
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Cholesterol modulates the exposure and orientation of pulmonary surfactant protein SP-C in model surfactant membranes.

机译:胆固醇可调节模型表面活性剂膜中肺表面活性剂蛋白SP-C的暴露和方向。

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Cholesterol is the major neutral lipid in lung surfactant, accounting for up to 8-10% of surfactant mass, while surfactant protein SP-C ( approximately 4.2 kDa) accounts for no more than 1-1.5% of total surfactant weight but plays critical roles in formation and stabilization of pulmonary surfactant films. It has been reported that surfactant protein SP-C interacts with cholesterol in lipid/protein interfacial films and this interaction could have a potential role on modulating surfactant function. In the present study, we have analyzed the effect of cholesterol on the structure, orientation and dynamic properties of SP-C embedded in physiologically relevant model membranes. The presence of cholesterol does not induce substantial changes in the secondary structure of SP-C, as analyzed by Attenuated Reflection Fourier Transformed Infrared spectroscopy (ATR-FTIR). However, the presence of cholesterol modifies the orientation of the transmembrane helix and the dynamic properties of the protein, as demonstrated by hydrogen/deuterium exchange kinetics. The effect of cholesterol on SP-C reconstituted in zwitterionic, entirely fluid, membranes made of POPC (palmitoyloleoylphospatidylcholine) or in anionic membranes with coexistence of ordered and disordered phases, such as those made of dipalmitoylphosphatidylcholine (DPPC):POPC:Palmitoyloleoylphosphatidylglycerol (POPG) (50:25:15) is dual. Cholesterol decreases the exposure of the protein to the aqueous environment and the tilt of its transmembrane helical segment up to a ratio Cholesterol:SP-C of 4.8 and 2.4 (mol/mol) in the two lipid systems tested, respectively, and it increases the exposure and tilt at higher cholesterol proportions. The results presented here suggest the existence of an interaction between SP-C and cholesterol-enriched phases, with consequences on the behavior of the protein, which could be of relevance for cholesterol-dependent structure-function relationships in pulmonary surfactant membranes and films.
机译:胆固醇是肺表面活性剂中的主要中性脂质,占表面活性剂质量的8-10%,而表面活性剂蛋白SP-C(约4.2 kDa)不超过表面活性剂总重量的1-1.5%,但起着至关重要的作用在形成和稳定肺表面活性剂膜方面。据报道,表面活性剂蛋白SP-C与脂质/蛋白界面膜中的胆固醇相互作用,这种相互作用可能对调节表面活性剂功能具有潜在作用。在本研究中,我们已经分析了胆固醇对嵌入生理相关模型膜中的SP-C的结构,取向和动力学性质的影响。如通过衰减反射傅里叶变换红外光谱(ATR-FTIR)分析,胆固醇的存在不会引起SP-C二级结构的实质性变化。然而,胆固醇的存在改变了跨膜螺旋的方向和蛋白质的动态特性,如氢/氘交换动力学所证明的。胆固醇对SP-C的影响在由POPC(棕榈酰油酰磷脂酰胆碱)制成的两性离子,完全流动的膜中重构,或在有序相和无序相共存的阴离子膜中重构,例如由二棕榈酰磷脂酰胆碱(DPPC):POPC:Palmitoyloleoylphospholylphosphatid (50:25:15)是双重的。在两个测试的脂质体系中,胆固醇降低了蛋白质在水性环境中的暴露量以及其跨膜螺旋段的倾斜度,分别达到4.8:2.4(mol / mol)的胆固醇:SP-C比率,并增加了在较高的胆固醇比例下暴露和倾斜。此处显示的结果表明,SP-C与胆固醇富集相之间存在相互作用,从而影响蛋白质的行为,这可能与肺表面活性剂膜和膜中胆固醇依赖的结构-功能关系有关。

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