β -淀粉样蛋白羧基末端区(残基34-42)的构象研究:酰胺骨架保护作为结构探针的战略性应用。

M Quibell, T Johnson, W G Turnell
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引用次数: 0

摘要

利用芴-9-基甲氧基羰基(Fmoc)-聚酰胺固相肽合成技术制备了含有N-(2-羟基-4-甲氧基苄基)(Hmb)酰胺不同位置主链取代的β -淀粉样蛋白(32-42)肽的类似物。装配过程中的N α - fmoc在线脱保护监测显示,在天然和β A(34-42, (Hmb)Gly38)模拟合成中释放受阻。在β A(34-42, (Hmb)Gly37)和β A(34-42, (Hmb)Val36)的合成过程中没有观察到这种阻碍。然而,后者包含一个异常缓慢的耦合反应。分析了裂解肽在各种溶剂中的溶解度,并对不溶性微球进行了亲嗜性染色试验。x射线分析Fmoc(和H-) β A(34-42)和相应的(Hmb)Gly38类似物作为二甲基甲酰胺肿胀凝胶的结构非常相似。二级结构预测和有序阵列模型的建立与我们的研究结果一致,表明β A(34-42)在溶液和树脂上形成β发夹结构,在Val36-Gly37-Gly38-Val39上形成相反的结构。
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Conformational studies on beta-amyloid protein carboxy-terminal region (residues 34-42): strategic use of amide backbone protection as a structural probe.

Analogues of beta-amyloid (32-42) peptide, containing N-(2-hydroxy-4-methoxybenzyl) (Hmb) amide backbone substitutions at various positions have been prepared using fluoren-9-ylmethoxycarbonyl (Fmoc)-polyamide based solid phase peptide synthesis. On-line N alpha-Fmoc deprotection monitoring during assembly exhibited hindered release in the native and beta A(34-42, (Hmb)Gly38) analogue syntheses. No such hindrance was observed during the synthesis of beta A(34-42, (Hmb)Gly37) nor beta A(34-42, (Hmb)Val36). However, the latter contained an exceptionally slow coupling reaction. Cleaved peptides were analysed for solubility in a variety of solvents and insoluble pellets tested for congophilic staining. X-ray analysis of Fmoc (and H-) beta A(34-42) and the corresponding (Hmb)Gly38 analogues as dimethylformamide swollen gels gave very similar structures. Secondary structure prediction and model-building of ordered arrays, compatible with our results, suggest that beta A(34-42) forms a beta-hairpin structure, with the reverse turn at Val36-Gly37-Gly38-Val39 both in solution and on the resin during synthesis.

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