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神经肽Y的表达标志着小鼠和人类中部分分化的β细胞。

Neuropeptide Y expression marks partially differentiated β cells in mice and humans.

作者信息

Rodnoi Pope, Rajkumar Mohan, Moin Abu Saleh Md, Georgia Senta K, Butler Alexandra E, Dhawan Sangeeta

机构信息

Larry L. Hillblom Islet Research Center, David Geffen School of Medicine, UCLA, Los Angeles, California, USA.

Children's Hospital Los Angeles (CHLA), Keck School of Medicine, University of Southern California (USC), Los Angeles, California, USA.

出版信息

JCI Insight. 2017 Jun 15;2(12). doi: 10.1172/jci.insight.94005.

Abstract

β Cells are formed in embryonic life by differentiation of endocrine progenitors and expand by replication during neonatal life, followed by transition into functional maturity. In this study, we addressed the potential contribution of neuropeptide Y (NPY) in pancreatic β cell development and maturation. We show that NPY expression is restricted from the progenitor populations during pancreatic development and marks functionally immature β cells in fetal and neonatal mice and humans. NPY expression is epigenetically downregulated in β cells upon maturation. Neonatal β cells that express NPY are more replicative, and knockdown of NPY expression in neonatal mouse islets reduces replication and enhances insulin secretion in response to high glucose. These data show that NPY expression likely promotes replication and contributes to impaired glucose responsiveness in neonatal β cells. We show that NPY expression reemerges in β cells in mice fed with high-fat diet as well as in diabetes in mice and humans, establishing a potential new mechanism to explain impaired β cell maturity in diabetes. Together, these studies highlight the contribution of NPY in the regulation of β cell differentiation and have potential applications for β cell supplementation for diabetes therapy.

摘要

β细胞在胚胎期由内分泌祖细胞分化形成,并在新生期通过复制进行扩增,随后转变为功能成熟状态。在本研究中,我们探讨了神经肽Y(NPY)在胰腺β细胞发育和成熟过程中的潜在作用。我们发现,在胰腺发育过程中,NPY的表达在祖细胞群体中受到限制,并且在胎儿和新生儿小鼠及人类中标记功能不成熟的β细胞。β细胞成熟时,NPY的表达通过表观遗传机制下调。表达NPY的新生β细胞具有更强的复制能力,在新生小鼠胰岛中敲低NPY的表达会减少复制,并增强对高葡萄糖的胰岛素分泌反应。这些数据表明,NPY的表达可能促进复制,并导致新生β细胞葡萄糖反应性受损。我们发现,在高脂饮食喂养的小鼠以及小鼠和人类糖尿病模型中,β细胞中NPY的表达会再次出现,这为解释糖尿病中β细胞成熟受损建立了一种潜在的新机制。总之,这些研究突出了NPY在β细胞分化调控中的作用,并为糖尿病治疗中β细胞补充疗法提供了潜在应用。

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