首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >The effect of oxysterols on the interaction of Alzheimer's amyloid beta with model membranes
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The effect of oxysterols on the interaction of Alzheimer's amyloid beta with model membranes

机译:氧固醇对阿尔茨海默氏症淀粉样β与模型膜相互作用的影响

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摘要

The interaction of amyloid beta (Aβ) peptide with cell membranes has been shown to be influenced by Aβ conformation, membrane physicochemical properties and lipid composition. However, the effect of cholesterol and its oxidized derivatives, oxysterols, on Aβ-induced neurotoxicity to membranes is not fully understood. We employed here model membranes to investigate the localization of Aβ in membranes and the peptide-induced membrane dynamics in the presence of cholesterol and 7-ketocholesterol (7keto) or 25-hydroxycholesterol (25OH). Our results have indicated that oxysterols rendered membranes more sensitive to Aβ, in contrast to role of cholesterol in inhibiting Aβ/membrane interaction. We have demonstrated that two oxysterols had different impacts owing to distinct positions of the additional oxygen group in their structures. 7keto-containing cell-sized liposomes exhibited a high propensity toward association with Aβ, while 25OH systems were more capable of morphological changes in response to the peptide. Furthermore, we have shown that 42-amino acid Aβ (Aβ-42) pre-fibril species had higher association with membranes, and caused membrane fluctuation faster than 40-residue isoform (Aβ-40). These findings suggest the enhancing effect of oxysterols on interaction of Aβ with membranes and contribute to clarify the harmful impact of cholesterol on Aβ-induced neurotoxicity by means of its oxidation.
机译:淀粉样蛋白β(Aβ)肽与细胞膜的相互作用已显示受Aβ构象,膜理化性质和脂质组成的影响。然而,胆固醇及其氧化衍生物氧固醇对Aβ诱导的对膜的神经毒性的作用尚未完全了解。我们在这里使用模型膜来研究膜中Aβ的定位以及在胆固醇和7-酮胆固醇(7keto)或25-羟基胆固醇(25OH)存在下肽诱导的膜动力学。我们的结果表明,与胆固醇在抑制Aβ/膜相互作用中的作用相反,氧固醇使膜对Aβ更加敏感。我们已经证明,由于氧在其结构中的不同位置,两种氧固醇的影响不同。含7个酮的细胞大小的脂质体显示出与Aβ缔合的高度倾向,而25OH系统则更具有响应肽的形态变化的能力。此外,我们已经显示,42个氨基酸的Aβ(Aβ-42)前原纤维种与膜的结合更高,并且引起膜波动的速度快于40个残基的亚型(Aβ-40)。这些发现表明氧固醇对Aβ与膜相互作用的增强作用,并有助于阐明胆固醇通过其氧化对Aβ诱导的神经毒性的有害影响。

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