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NPY激素家族:在胃肠疾病中的临床相关性及潜在应用

NPY family of hormones: clinical relevance and potential use in gastrointestinal disease.

作者信息

Vona-Davis L C, McFadden D W

机构信息

Department of Surgery, West Virginia University, PO Box 9238, Morgantown, West Virginia 26506, USA.

出版信息

Curr Top Med Chem. 2007;7(17):1710-20. doi: 10.2174/156802607782340966.

Abstract

The neuropeptide Y (NPY), peptide YY (PYY) and pancreatic polypeptide (PP) family of hormones exhibit a wide variety of biological actions on the mammalian gastrointestinal tract through known G-protein coupled receptor pathways. At least four receptor subtypes, denoted as Y(1), Y(2), Y(4) an Y(5), each with specific affinities to NPY ligands, serve as regulators of mucosal function, gastrointestinal motility and secretion. Investigations to date, however, have implicated the NPY peptides as mediators in the pathogenesis of numerous gastrointestinal disorders, including malabsorption, short gut, inflammatory bowel diseases, and forms of pancreatitis. Our understanding of these diseases and the interactions of NPY peptides have been advanced by the development of receptor agonists and antagonists that can be used experimentally in animal models. Potent selective PYY agonists have been developed that exhibit clinical potential as proabsorptive agents. NPY receptor agonists and antagonists as well as mice harboring null mutations in the Y(1) and Y(4) receptors have provided novel approaches in preventing intestinal inflammation and diarrhea. The use of competitive antagonists and Y(2) receptor knockouts have also aided in understanding secretory tone and electrogenic ion transport in the colon. In the pancreas, PYY suppresses amylase and cytokine release, which would be desirable in the clinical therapy of pancreatitis. Protein/DNA array analysis has revealed that PYY reduces transcription factor binding activity and disrupts signal transduction pathways activated by TNF-alpha in acinar cells. The present review gives an overview of NPY research in gastrointestinal disease and discusses its clinical relevance and potential use as therapy.

摘要

神经肽Y(NPY)、肽YY(PYY)和胰多肽(PP)激素家族通过已知的G蛋白偶联受体途径,对哺乳动物胃肠道发挥多种生物学作用。至少有四种受体亚型,分别称为Y(1)、Y(2)、Y(4)和Y(5),它们对NPY配体各有特定亲和力,可作为黏膜功能、胃肠动力和分泌的调节因子。然而,迄今为止的研究表明,NPY肽在多种胃肠道疾病的发病机制中起介导作用,包括吸收不良、短肠综合征、炎症性肠病和某些形式的胰腺炎。能够在动物模型中进行实验性应用的受体激动剂和拮抗剂的开发,推动了我们对这些疾病以及NPY肽相互作用的认识。已经开发出强效选择性PYY激动剂,它们作为促吸收剂具有临床应用潜力。NPY受体激动剂和拮抗剂以及Y(1)和Y(4)受体存在无效突变的小鼠,为预防肠道炎症和腹泻提供了新方法。竞争性拮抗剂的使用和Y(2)受体基因敲除也有助于了解结肠的分泌张力和电生性离子转运。在胰腺中,PYY可抑制淀粉酶和细胞因子释放,这在胰腺炎的临床治疗中是可取的。蛋白质/DNA阵列分析显示,PYY可降低腺泡细胞中转录因子的结合活性,并破坏由肿瘤坏死因子-α激活的信号转导途径。本综述概述了NPY在胃肠道疾病方面的研究,并讨论了其临床相关性以及作为治疗手段的潜在用途。

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