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α 细胞在小鼠胰腺胰岛的出生后形态发生和成熟过程中是可有可无的。

α-Cells are dispensable in postnatal morphogenesis and maturation of mouse pancreatic islets.

机构信息

Division of Pediatric General and Thoracic Surgery, Children's Hospital of Pittsburgh of UPMC, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania.

出版信息

Am J Physiol Endocrinol Metab. 2013 Oct 15;305(8):E1030-40. doi: 10.1152/ajpendo.00022.2013. Epub 2013 Aug 27.

Abstract

Glucagon-producing α-cells are the second-most abundant cell type in the islet. Whereas α-cells make up less than 20% of the cells in a mature mouse islet, they occupy a much larger proportion of the pancreatic endocrine cell population during the early postnatal period, the time when morphological and functional maturation occurs to form adult islets. To determine whether α-cells have a role in postnatal islet development, a diphtheria toxin-mediated α-cell ablation mouse model was established. Rapid and persistent depletion of α-cells was achieved by daily injection of the toxin for 2 wk starting at postnatal day 1 (P1). Total pancreatic glucagon content in the α-cell-ablated mice was undetectable at P14 and still less than 0.3% of that of the control mice at 4 mo of age. Histological analyses revealed that formation of spherical islets occurred normally, and the islet size distribution was not changed despite the near-total lack of α-cells. Furthermore, there were no differences in expression of β-cell maturation marker proteins, including urocortin 3 and glucose transporter 2, in the α-cell-ablated islets at P14. Mice lacking α-cells grew normally and appeared healthy. Both glucose and insulin tolerance tests demonstrated that the α-cell-ablated mice had normal glucose homeostasis. These results indicate that α-cells do not play a critical role in postnatal islet morphogenesis or functional maturation of β-cells.

摘要

胰岛中含量第二丰富的细胞类型是产生胰高血糖素的α细胞。虽然α细胞在成熟胰岛中的比例不到 20%,但在出生后早期,即形态和功能成熟形成成年胰岛的时期,它们在胰腺内分泌细胞群体中占有更大的比例。为了确定α细胞是否在胰岛的出生后发育中起作用,建立了一种白喉毒素介导的α细胞消融小鼠模型。通过在出生后第 1 天(P1)开始每天注射毒素 2 周,迅速且持续地消耗α细胞。在 4 月龄时,α细胞消融小鼠的胰腺总胰高血糖素含量仍无法检测到,仍不到对照组的 0.3%。组织学分析表明,尽管几乎完全缺乏α细胞,但球形胰岛的形成仍正常发生,胰岛大小分布没有改变。此外,在 P14 时,α细胞消融胰岛中β细胞成熟标志物蛋白的表达,包括 Ucn3 和 Glut2,没有差异。缺乏α细胞的小鼠正常生长,且健康状况良好。葡萄糖和胰岛素耐量试验均表明,α细胞消融小鼠的葡萄糖稳态正常。这些结果表明,α细胞在胰岛的出生后形态发生或β细胞的功能成熟过程中不起关键作用。

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