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在小鼠 β 细胞再生模型中,通过激活胰岛前体细胞中胰高血糖素样肽 1(GLP-1)原激素转化酶 1/3 来实现胰岛内 GLP-1 的产生。

Intraislet production of GLP-1 by activation of prohormone convertase 1/3 in pancreatic α-cells in mouse models of ß-cell regeneration.

机构信息

Department of Medicine, The University of Chicago, Chicago, IL USA.

出版信息

Islets. 2010 May-Jun;2(3):149-55. doi: 10.4161/isl.2.3.11396.

Abstract

The islet of Langerhans is a highly vascularized micro-organ consisting of not only ß-cells but multiple cell types such as α-, delta-, pancreatic polypeptide- and epsilon-cells that work together to regulate glucose homeostatis. We have recently proposed a new model of the neonatal islet formation in mice by a process of fission following contiguous endocrine cell proliferation in the form of branched cord-like structures in embryos and newborns. There exist large stretches of interconnected islet structures along large blood vessels in the neonatal pancreas, which, upon further development, segregate into smaller fragments (i.e., islets) that eventually become more spherical by internal proliferation as seen in the adult pancreas. α-cells span these elongated islet-like structures in the developing pancreas, which we hypothesize represent sites of fission and facilitate the eventual formation of discrete islets. The α-cells express both prohormone convertase 2 and 1/3 (PC 2 and PC 1/3, respectively), which resulted in the processing of the proglucagon precursor into glucagon-like peptide 1, thereby leading to local production of this important ß-cell growth factor. Furthermore, while α-cells in the adult basically only express PC 2, significant activation of PC 1/3 is also observed in mouse models of insulin resistance such as pregnant, ob/ ob, db/db and prediabetic NOD mice, which may be a common mechanism in proliferating ß-cells. Our study suggests an important role of α-cells for ß-cell proliferation and further for the endocrine cell network within an islet.

摘要

胰岛是一个高度血管化的微器官,不仅包含β细胞,还包含多种细胞类型,如α、δ、胰多肽和ε细胞,它们共同作用以调节葡萄糖稳态。我们最近提出了一种新的小鼠胰岛形成模型,即通过胚胎和新生儿中分支状条索样结构的连续内分泌细胞增殖来实现分裂。新生胰腺中的大血管周围存在大量相互连接的胰岛结构,这些结构在进一步发育过程中会分离成更小的片段(即胰岛),最终通过内部增殖变得更加球形,这与成年胰腺中的情况相似。α细胞跨越发育中胰腺中的这些拉长的胰岛样结构,我们假设这些结构代表分裂的部位,并有助于最终形成离散的胰岛。α细胞表达前激素转化酶 2 和 1/3(分别为 PC 2 和 PC 1/3),这导致前胰高血糖素原被加工成胰高血糖素样肽 1,从而导致这种重要的β细胞生长因子的局部产生。此外,虽然成年α细胞基本上只表达 PC 2,但在胰岛素抵抗的小鼠模型中,如妊娠、ob/ob、db/db 和糖尿病前期 NOD 小鼠中,也观察到 PC 1/3 的显著激活,这可能是增殖β细胞的共同机制。我们的研究表明,α细胞在β细胞增殖以及进一步在胰岛内的内分泌细胞网络中发挥重要作用。

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