首页> 外文OA文献 >Effect of Leucine to Phenylalanine Substitution on the Nonpolar Face of a Class A Amphipathic Helical Peptide on Its Interaction with Lipid: HIGH RESOLUTION SOLUTION NMR STUDIES OF 4F-DIMYRISTOYLPHOSPHATIDYLCHOLINE DISCOIDAL COMPLEX*S⃞
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Effect of Leucine to Phenylalanine Substitution on the Nonpolar Face of a Class A Amphipathic Helical Peptide on Its Interaction with Lipid: HIGH RESOLUTION SOLUTION NMR STUDIES OF 4F-DIMYRISTOYLPHOSPHATIDYLCHOLINE DISCOIDAL COMPLEX*S⃞

机译:亮氨酸对苯丙氨酸取代的非极性表面的影响。 A类两亲性螺旋肽与脂质的相互作用:高 4F-二甲硫代磷脂酰胆碱二旋体的拆分溶液NMR研究 复杂*S⃞

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摘要

Model class A amphipathic helical peptides mimic several properties of apolipoprotein A-I (apoA-I), the major protein component of high density lipoproteins. Previously, we reported the NMR structures of Ac-18A-NH2 (renamed as 2F because of two phenylalanines), the base-line model class A amphipathic helical peptide in the presence of lipid (Mishra, V. K., Anantharamaiah, G. M., Segrest, J. P., Palgunachari, M. N., Chaddha, M., Simon Sham, S. W., and Krishna, N. R. (2006) J Biol. Chem. 281, 6511-651916407255). Substitution of two Leu residues on the nonpolar face (Leu3 and Leu14) with Phe residues produced the peptide 4F (so named because of four phenylalanines), which has been extensively studied for its anti-inflammatory and antiatherogenic properties. Like 2F, 4F also forms discoidal nascent high density lipoprotein-like particles with 1,2-dimyristoyl-sn-glycero-3-phosphocholine (DMPC). Since subtle structural changes in the peptide-lipid complexes have been shown to be responsible for their antiatherogenic properties, we undertook high resolution NMR studies to deduce detailed structure of 4F in 4F·DMPC discs. Like 2F, 4F adopts a well defined amphipathic α-helical structure in association with the lipid at a 1:1 peptide/lipid weight ratio. Nuclear Overhauser effect (NOE) spectroscopy revealed a number of intermolecular close contacts between the aromatic residues in the hydrophobic face of the helix and the lipid acyl chain protons. Similar to 2F, the pattern of observed peptide-lipid NOEs is consistent with a parallel orientation of the amphipathic α helix, with respect to the plane of the lipid bilayer, on the edge of the disc (the belt model). However, in contrast to 2F in 2F·DMPC, 4F in the 4F·DMPC complex is located closer to the lipid headgroup as evidenced by a number of NOEs between 4F and DMPC headgroup protons. These NOEs are absent in the 2F·DMPC complex. In addition, the conformation of the DMPC sn-3 chain in 4F·DMPC complex is different than in the 2F·DMPC complex as evidenced by the NOE between lipid 2.CH and βCH2 protons in 4F·DMPC, but not in 2F·DMPC, complex. Based on the results of this study, we infer that the antiatherogenic properties of 4F may result from its preferential interaction with lipid headgroups.
机译:模型A类两亲性螺旋肽模拟载脂蛋白A-I(apoA-I)的几种特性,载脂蛋白A-I是高密度脂蛋白的主要蛋白成分。以前,我们报道了在脂质存在下,基线模型A类两亲性螺旋肽Ac-18A-NH2(由于两个苯基丙氨酸而更名为2F)的NMR结构(Mishra,VK,Anantharamaiah,GM,Segrest,JP ,MN,Palgunachari,M.Chaddha,SW,Simon Sham,和NR,Krishna(2006)J Biol.Chem.281,6511-651916407255)。非极性表面上的两个Leu残基(Leu3和Leu14)被Phe残基取代产生了4F肽(由于四个苯丙氨酸而得名),该肽已被广泛研究其抗炎和抗动脉粥样硬化特性。像2F一样,4F也与1,2-二肉豆蔻酰基-sn-甘油-3-磷酸胆碱(DMPC)形成盘状新生高密度脂蛋白样颗粒。由于已显示肽-脂质复合物的细微结构变化是其抗动脉粥样硬化特性的原因,我们进行了高分辨率NMR研究,以推断4F·DMPC光盘中4F的详细结构。像2F一样,4F与脂质以1:1的肽/脂质重量比结合采用定义明确的两亲性α螺旋结构。核Overhauser效应(NOE)光谱显示,在螺旋疏水面的芳族残基与脂质酰基链质子之间存在许多分子间紧密接触。与2F相似,观察到的肽-脂质NOE的模式与两亲性α螺旋相对于脂双层的平面在椎间盘边缘上的平行方向一致(皮带模型)。但是,与2F·DMPC中的2F相比,4F·DMPC复合物中的4F位置更靠近脂质头基,这由4F和DMPC头基质子之间的许多NOE所证明。这些NOE在2F·DMPC复合物中不存在。此外,4F·DMPC复合物中DMPC sn-3链的构象与2F·DMPC复合物中的构象不同,这是由4F·DMPC中脂质2.CH和βCH2质子之间的NOE所证明的,而在2F·DMPC中则没有。 ,复杂。根据这项研究的结果,我们推断4F的抗动脉粥样硬化特性可能是由于其与脂质头基的优先相互作用所致。

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