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Pharmacology and clinical potential of guanylyl cyclase C agonists in the treatment of ulcerative colitis.

机译:鸟苷酸环化酶C激动剂在治疗溃疡性结肠炎中的药理学和临床潜力。

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摘要

Agonists of the transmembrane intestinal receptor guanylyl cyclase C (GCC) have recently attracted interest as promising human therapeutics. Peptide ligands that can specifically induce GCC signaling in the intestine include endogenous hormones guanylin and uroguanylin, diarrheagenic bacterial enterotoxins (ST), and synthetic drugs linaclotide, plecanatide, and SP-333. These agonists bind to GCC at intestinal epithelial surfaces and activate the receptoru27s intracellular catalytic domain, an event initiating discrete biological responses upon conversion of guanosine-5u27-triphosphate to cyclic guanosine monophosphate. A principal action of GCC agonists in the colon is the promotion of mucosal homeostasis and its dependent barrier function. Herein, GCC agonists are being developed as new medications to treat inflammatory bowel diseases, pathological conditions characterized by mucosal barrier hyperpermeability, abnormal immune reactions, and chronic local inflammation. This review will present important concepts underlying the pharmacology and therapeutic utility of GCC agonists for patients with ulcerative colitis, one of the most prevalent inflammatory bowel disease disorders.
机译:跨膜肠受体鸟苷酰环化酶C(GCC)的激动剂作为一种有前途的人类疗法最近引起了人们的兴趣。可以在肠道中特异性诱导GCC信号传导的肽配体包括内源性鸟苷蛋白和尿鸟苷蛋白,腹泻性细菌肠毒素(ST)和合成药物利那洛肽,普卡那肽和SP-333。这些激动剂在肠上皮表面与GCC结合并激活受体的细胞内催化结构域,该事件在鸟苷5 u27-三磷酸转化为环状鸟苷单磷酸时引发离散的生物反应。 GCC激动剂在结肠中的主要作用是促进粘膜稳态及其依赖的屏障功能。在此,GCC激动剂被开发为治疗炎性肠疾病,以粘膜屏障高通透性为特征的病理状况,异常的免疫反应和慢性局部炎症的新药。这篇综述将介绍GCC激动剂对溃疡性结肠炎(最常见的炎性肠疾病之一)患者的药理学和治疗效用的重要概念。

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    Pitari Giovanni M;

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