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Conopeptide-derived kappa-opioid agonists (conorphins): potent, selective, and metabolic stable dynorphin A mimetics with antinociceptive properties

机译:芋螺肽衍生的κ-阿片受体激动剂(conorphins):强效,选择性和代谢稳定的强啡肽a模拟物,具有抗伤害作用

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摘要

Opioid receptor screening of a conopeptide library led to a novel selective κ-opioid agonist peptide (conorphin T). Intensive medicinal chemistry, guided by potency, selectivity, and stability assays generated a pharmacophore model supporting rational design of highly potent and selective κ-opioid receptor (KOR) agonists (conorphins) with exceptional plasma stability. Conorphins are defined by a hydrophobic benzoprolyl moiety, a double arginine sequence, a spacer amino acid followed by a hydrophobic residue and a C-terminal vicinal disulfide moiety. The pharmacophore model was supported by computational docking studies, revealing receptor-ligand interactions similar to KOR agonist dynorphin A (1-8). A conorphin agonist inhibited colonic nociceptors in a mouse tissue model of chronic visceral hypersensitivity, suggesting the potential of KOR agonists for the treatment of chronic abdominal pain. This new conorphine KOR agonist class and pharmacophore model provide opportunities for future rational drug development and probes for exploring the role of the κ-opioid receptor.
机译:对阿片肽库的阿片样物质受体筛选产生了新型的选择性κ-阿片样物质激动剂肽(conorphin T)。在效能,选择性和稳定性测定的指导下,密集药物化学产生了一种药效团模型,该模型支持合理设计具有出色血浆稳定性的高效和选择性κ阿片受体(KOR)激动剂(伴肾上腺皮质激素)。伴肾上腺素的定义是疏水性苯并脯氨酰基部分,双精氨酸序列,间隔氨基酸和疏水性残基以及C端邻二硫键部分。该药效团模型得到计算对接研究的支持,揭示了与KOR激动剂强啡肽A(1-8)相似的受体-配体相互作用。伴肾上腺皮质激素激动剂在慢性内脏超敏反应的小鼠组织模型中抑制结肠伤害感受器,表明KOR激动剂具有治疗慢性腹痛的潜力。这种新的儿吗啡KOR激动剂类和药效团模型为未来的合理药物开发提供了机会,并为探索κ阿片受体的作用提供了探针。

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