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Engineering of an Anti-Inflammatory Peptide Based on the Disulfide-Rich Linaclotide Scaffold

机译:基于富含二硫化物的利那洛肽支架的抗炎肽的工程设计

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Inflammatory bowel diseases are a set of complex and debilitating diseases, for which there is no satisfactory treatment. Peptides as small as three amino acids have been shown to have anti-inflammatory activity in mouse models of colitis, but they are likely to be unstable, limiting their development as drug leads. Here, we have grafted a tripeptide from the annexin A1 protein into linaclotide, a 14-amino-acid peptide with three disulfide bonds, which is currently in clinical use for patients with chronic constipation or irritable bowel syndrome. This engineered disulfide-rich peptide maintained the overall fold of the original synthetic guanylate cyclase C agonist peptide, and reduced inflammation in a mouse model of acute colitis. This is the first study to show that this disulfide-rich peptide can be used as a scaffold to confer a new bioactivity.
机译:炎性肠病是一系列复杂且使人衰弱的疾病,目前尚无令人满意的治疗方法。在结肠炎的小鼠模型中,已显示小至3个氨基酸的肽具有抗炎活性,但它们可能不稳定,限制了其作为药物前导的发展。在这里,我们将膜联蛋白A1蛋白的三肽移植到了具有三个二硫键的14个氨基酸的肽linaclotide上,目前正在临床上用于患有慢性便秘或肠易激综合症的患者。这种工程化的富含二硫键的肽保持了原始合成鸟苷酸环化酶C激动剂肽的整体折叠,并减轻了急性结肠炎小鼠模型的炎症。这是第一项显示该富含二硫键的肽可用作赋予新生物活性的支架的研究。

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