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The synthesis of acid- and base-labile lipopeptides on solid support

机译:固体载体上对酸和碱不稳定的脂肽的合成

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Lipidated peptides, including characteristic partial structures of human Ras proteins, were synthesized by means of a new solid-phase technique in 22-68% yield. This technique gives access to farnesylated, palmitoylated, and doubly lipidated peptides as methyl esters or carboxylic acids carrying a fluorescent tag or a maleimide moiety for coupling to proteins. The peptide backbones were built up on the resin by using 9-fluorenylmethoxycarbonyl chemistry together with the oxidatively cleavable hydrazide linker. As a key step, the acid-labile farnesyl and basiclabile palmitoyl lipid groups were introduced onto the resin after the cleavage of appropriate acid-or reduction-sensitive protecting groups from the cysteine residues. Optional introduction of different fluorescent tags or a maleimide group into the peptide was followed by release of the resin-bound target peptide as the methyl ester or carboxylic acid by very mild copper(II)-mediated oxidation in slightly acidic or basic media. This new methodology should substantially facilitate the access to lipidated peptides for the study of important biological phenomena like biological signal transduction, localization, and versicular transport.
机译:利用新的固相技术合成了包括人Ras蛋白特征部分结构在内的脂化肽,收率为22-68%。该技术使法尼基化,棕榈酰化和双脂化的肽成为带有荧光标签或马来酰亚胺部分的甲酯或羧酸,可与蛋白质偶联。通过使用9-芴基甲氧基羰基化学以及可氧化裂解的酰肼连接基,在树脂上建立肽主链。作为关键步骤,在从半胱氨酸残基上切割适当的酸或还原敏感性保护基之后,将酸不稳定的法呢基和碱性不稳定的棕榈酰基脂质基团引入树脂。可选地将不同的荧光标签或马来酰亚胺基团引入肽中,然后在弱酸性或碱性介质中通过非常温和的铜(II)介导的氧化,释放出作为甲基酯或羧酸的树脂结合靶肽。这种新的方法学应大大促进脂化肽的获得,以研究重要的生物学现象,例如生物信号转导,定位和垂直运输。

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