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Influence of polar support for the synthesis of large C-terminal peptide aldehyde: application to chemoselective ligation

机译:极性载体对合成大型C端肽醛的影响:在化学选择性连接中的应用

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Efficient conditions have been developed for the synthesis of large peptide aldehydes from solid support through nucleophilic displacement. Aminolysis of the ester bond between a deprotected peptide and the phenylacetamidomethyl linker with aminoacetaldehyde-dimethylacetal leads to a peptide aldehyde masked as an acetal. Besides the optimization of parameters such as solvents, workup procedure and temperature, the influence of the nature of the polymeric support was crucial. Among the solid supports tested, the poly(ethylene glycol)poly(acrylamide) resin proved to afford the best cleavage yield. This work underlines that the solid support has to be considered as a co-solvent rather than an inert carrier. Our methodology was further applied to the synthesis of a 33-mer with T-helper activity from the fusion protein of measles virus. The 33-mer peptide aldehyde was then chemoselectively ligated via an oxime bond to an (aminooxy) acetyl peptide with T-cytotoxic activity. (C) 2002 Elsevier Science Ltd. All rights reserved. [References: 41]
机译:已经开发了通过固相支持通过亲核置换从大分子醛合成大肽醛的有效条件。用氨基乙醛-二甲基乙缩醛对脱保护的肽和苯基乙酰胺基甲基接头之间的酯键进行氨解会导致被掩盖为缩醛的肽醛。除了优化诸如溶剂,后处理程序和温度等参数外,聚合物载体性质的影响也至关重要。在所测试的固体载体中,聚(乙二醇)聚(丙烯酰胺)树脂被证明具有最佳的裂解产率。这项工作强调必须将固体载体视为助溶剂而不是惰性载体。我们的方法被进一步应用于由麻疹病毒融合蛋白合成具有T辅助活性的33-mer。然后将33聚体的肽醛通过肟键化学选择性地连接至具有T细胞毒性活性的(氨氧基)乙酰基肽上。 (C)2002 Elsevier ScienceLtd。保留所有权利。 [参考:41]

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