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An engineered cyclic peptide alleviates symptoms of inflammation in a murine model of inflammatory bowel disease

机译:工程化的环肽缓解了炎症性肠病的小鼠模型中的炎症症状

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摘要

Inflammatory bowel diseases (IBDs) are a set of complex and debilitating diseases for which there is no satisfactory treatment. Recent studies have shown that small peptides show promise for reducing inflammation in models of IBD. However, these small peptides are likely to be unstable and rapidly cleared from the circulation, and therefore, if not modified for better stability, represent non-viable drug leads. We hypothesized that improving the stability of these peptides by grafting them into a stable cyclic peptide scaffold may enhance their therapeutic potential. Using this approach, we have designed a novel cyclic peptide that comprises a small bioactive peptide from the annexin A1 protein grafted into a sunflower trypsin inhibitor cyclic scaffold. We used native chemical ligation to synthesize the grafted cyclic peptide. This engineered cyclic peptide maintained the overall fold of the naturally occurring cyclic peptide, was more effective at reducing inflammation in a mouse model of acute colitis than the bioactive peptide alone, and showed enhanced stability in human serum. Our findings suggest that the use of cyclic peptides as structural backbones offers a promising approach for the treatment of IBD and potentially other chronic inflammatory conditions.
机译:炎症性肠病(IBDs)是一类复杂且令人衰弱的疾病,目前尚无令人满意的治疗方法。最近的研究表明,小肽有望在IBD模型中减轻炎症。但是,这些小肽可能不稳定并迅速从循环中清除,因此,如果不进行修饰以获得更好的稳定性,则表示无效的药物前导。我们假设通过将它们嫁接到稳定的环状肽支架中来改善这些肽的稳定性可能会增强其治疗潜力。使用这种方法,我们设计了一种新型的环肽,该环肽包含来自膜联蛋白A1蛋白的小生物活性肽,该小生物活性肽被嫁接到向日葵胰蛋白酶抑制剂的环状支架中。我们使用天然化学连接来合成接枝的环肽。这种工程化的环状肽保持了天然环状肽的整体折叠,在急性结肠炎的小鼠模型中减轻炎症的作用比单独的生物活性肽更有效,并且在人血清中显示出增强的稳定性。我们的发现表明,使用环肽作为结构骨架可为IBD和其他潜在的慢性炎症性疾病的治疗提供有希望的方法。

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