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首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >The specificity of monoglyceride-protein interactions and mechanism of the protein induced L_β to coagel phase transition
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The specificity of monoglyceride-protein interactions and mechanism of the protein induced L_β to coagel phase transition

机译:单酸甘油酯-蛋白质相互作用的特异性以及该蛋白质诱导的L_β到coagel相变的机制

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摘要

This study aims at gaining insight into the specificity and molecular mechanism of monoglyceride-protein interactions. We used β-lactoglobulin (β-LG) and lysozyme as model proteins and both monostearoylglycerol and monopalmitoylglycerol as defined gel phase monoglycerides. The monoglycerides were used in different combinations with the two negatively charged amphiphiles dicetylphosphate and distearylphosphate. The interactions were characterized using the monolayer technique, isothermal titration calorimetry, ~2H-nuclear magnetic resonance (NMR) using deuterium labelled monoglycerides and freeze fracture electron microscopy (EM). Our results show that lysozyme inserts efficiently into all monolayers tested, including pure monoglyceride layers. The insertion of β-LG depends on the lipid composition of the monolayer and is promoted when the acylchains of the negatively charged amphiphile are shorter than that of the monoglyceride. The binding parameters found for the interaction of β-LG and lysozyme with monoglyceride bilayers were generally similar. Moreover, in all cases a large exothermic binding enthalpy was observed which was found to depend on the nature of the monoglycerides but not of the proteins. ~2H-NMR and freeze fracture EM showed that this large enthalpy results from a protein mediated catalysis of the monoglyceride L_β to coagel phase transition. The mechanism of this phase transition consists of two steps, an initial protein mediated vesicle aggregation step which is followed by stacking and probably fusion of the bilayers.
机译:这项研究旨在深入了解甘油单酸酯-蛋白质相互作用的特异性和分子机制。我们使用β-乳球蛋白(β-LG)和溶菌酶作为模型蛋白,单硬脂酰甘油和单棕榈酰甘油均定义为凝胶相单甘油酯。甘油单酸酯与两种带负电荷的两亲性双十六烷基磷酸酯和磷酸二硬脂基酯以不同的组合使用。使用单层技术,等温滴定量热法,使用氘标记的甘油单酸酯的〜2H核磁共振(NMR)和冷冻断裂电子显微镜(EM)表征相互作用。我们的结果表明,溶菌酶可以有效地插入所有测试的单层中,包括纯甘油单酯层。 β-LG的插入取决于单层脂质的组成,并且当带负电荷的两亲物的酰基链短于单甘油酯的酰基链时,β-LG的插入会得到促进。对于β-LG和溶菌酶与甘油单酯双层的相互作用发现的结合参数通常是相似的。此外,在所有情况下均观察到大的放热结合焓,发现其依赖于甘油单酸酯的性质而不取决于蛋白质的性质。 〜2 H-NMR和冷冻断裂EM表明,这种大的焓是由蛋白质介导的单酸甘油酯L_β催化到Coagel相转变的结果。该相变的机理包括两个步骤,一个初始的蛋白质介导的囊泡聚集步骤,然后是双层的堆叠和可能的融合。

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