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Artificial disulfide-rich peptide scaffolds with precisely defined disulfide patterns and a minimized number of isomers

机译:具有精确定义的二硫键模式和最少数量的异构体的富含二硫键的人工肽支架

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Disulfide-rich peptides are emerging as potential templates for drug design applications. However, the synthesis and reengineering of disulfide-rich peptides are challenging, owing to the complexity of the oxidative folding process involving a number of diverse isomeric structures. Novel disulfide-rich peptide scaffolds that are not besieged by their disulfide isomers are still greatly desired. In this work, we report the design and synthesis of a novel class of artificial disulfide-rich peptide scaffolds with precisely defined disulfide patterns and a minimized number of isomers. In theory, natural peptides with three disulfide bonds have 15 possible isomers. By rationally engineering the thiol-framework of a peptide containing six cysteines with penicillamines and a dithiol amino acid, we demonstrated, for the first time, that the total number of isomers formed after oxidative folding can be decreased to a minimum of two (i.e., from 15 to 2). As fewer isomeric folds are involved in the oxidative folding, the pathway of the folding becomes more concise and the yield of the artificial scaffolds is substantially increased compared to that of its six-cysteine-containing analogue, which makes the artificial disulfide-rich scaffolds (with only 2 predefined isomeric folds) extremely promising for being exploited as structurally complex templates for the design of peptide therapeutics and ligands.
机译:富含二硫键的肽正逐渐成为药物设计应用的潜在模板。然而,由于涉及许多不同异构体结构的氧化折叠过程的复杂性,富含二硫键的肽的合成和再工程具有挑战性。仍然非常需要不被其二硫键异构体包围的新颖的富含二硫键的肽支架。在这项工作中,我们报告了具有精确定义的二硫键模式和最少数量的异构体的新型一类新型的富含二硫键的人工肽支架的设计和合成。从理论上讲,具有三个二硫键的天然肽具有15种可能的异构体。通过合理地设计含有六个半胱氨酸和青霉胺和二硫醇氨基酸的肽的硫醇构架,我们首次证明了氧化折叠后形成的异构体总数可以减少到最少两个( ie ,从15到2)。由于氧化折叠涉及的异构体折叠较少,因此折叠的路径变得更加简洁,并且与包含六个半胱氨酸的类似物相比,人工支架的产量显着增加,这使得富含人工二硫的支架(仅具有2个预定义的异构体折叠)非常有希望被用作结构复杂的模板来设计肽治疗剂和配体。

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