无热量甜味剂雷鲍迪甙A刺激胰高血糖素样肽1的释放并增加来自肠道不同位置的二维小鼠类器官的肠内分泌细胞数量。

The Journal of Nutrition Health and Aging Pub Date : 2016-10-26 DOI:10.3945/JN.116.232678

Nikkie van der Wielen, J. T. ten Klooster, Susanne Muckenschnabl, R. Pieters, H. Hendriks, R. Witkamp, J. Meijerink

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引用次数: 28

摘要

胰高血糖素样肽1 (GLP-1)有助于饱腹感，并在胰岛素分泌和葡萄糖稳态中起关键作用。与GLP-1类似，肽YY (PYY)和胆囊收缩素也影响食物摄入。肠道内分泌细胞沿肠道分泌这些激素是受营养物质调节的。从甜菊糖苷植物中提取的制剂，包括甜菊糖苷A，越来越多地被用作无热量甜味剂。目的研究雷鲍迪苷A对类器官模型肠内分泌细胞数量和分泌能力的影响。方法建立C57BL/6J小鼠十二指肠、空肠和回肠隐窝的二维类器官模型，采用基因表达和免疫荧光技术对模型进行表征。我们用10 mmol/L雷鲍迪苷A刺激这些类器官1小时，并测量它们的GLP-1、PYY和胆囊收缩素的释放。我们还分析了雷鲍迪甙A在孵育18小时后对肠内分泌细胞基因表达的影响。结果二维类器官包含隐窝细胞和分化的绒毛细胞，包括肠细胞、杯状细胞和肠内分泌细胞。这些肠内分泌细胞GLP-1、PYY和血清素染色阳性。培养的二维类器官保持其位置特异性基因表达模式。与对照组相比，雷鲍迪苷A诱导十二指肠、空肠和回肠GLP-1分泌分别增加1.7倍(P < 0.01)、2.2倍(P < 0.01)和4.3倍(P < 0.001)。与对照组相比，雷鲍迪甙A可使回肠PYY释放量增加3倍(P < 0.05)。长期(18小时)刺激可诱导肠内分泌特异性标志物嗜铬粒蛋白A、胰高血糖素、Pyy和胆囊收缩素的表达分别为3.5倍(P < 0.001)、3.5倍(P < 0.001)、3.8倍(P < 0.05)和6.5倍(P < 0.001)。结论利鲍迪糖苷A对小鼠小肠肠内分泌细胞具有新的体外作用，在代谢性疾病治疗中具有潜在的新应用前景。

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The Noncaloric Sweetener Rebaudioside A Stimulates Glucagon-Like Peptide 1 Release and Increases Enteroendocrine Cell Numbers in 2-Dimensional Mouse Organoids Derived from Different Locations of the Intestine.

BACKGROUND Glucagon-like peptide 1 (GLP-1) contributes to satiety and plays a pivotal role in insulin secretion and glucose homeostasis. Similar to GLP-1, peptide YY (PYY) and cholecystokinin also influence food intake. The secretion of these hormones by enteroendocrine cells along the intestine is modulated by nutrients. Preparations from the Stevia rebaudiana plant, including rebaudioside A, are increasingly being used as noncaloric sweeteners. OBJECTIVE We investigated the effects of rebaudioside A on enteroendocrine cells by assessing both cell numbers as well as their secretory capacity in an organoid model. METHODS A 2-dimensional organoid model derived from duodenal, jejunal, and ileal crypts of a C57BL/6J mouse was developed and characterized with the use of gene expression and immunofluorescence. We stimulated these organoids with 10 mmol/L rebaudioside A for 1 h and measured their GLP-1, PYY, and cholecystokinin release. We also analyzed the effects of rebaudioside A on gene expression in enteroendocrine cells after an 18-h incubation. RESULTS The 2-dimensional organoids contained crypt cells and differentiated villus cells, including enterocytes and goblet and enteroendocrine cells. These enteroendocrine cells stained positive for GLP-1, PYY, and serotonin. The cultured 2-dimensional organoids maintained their location-specific gene expression patterns. Compared with the control, rebaudioside A induced GLP-1 secretion 1.7-fold in the duodenum (P < 0.01), 2.2-fold in the jejunum (P < 0.01), and 4.3-fold in the ileum (P < 0.001). PYY release was increased by rebaudioside A 3-fold in the ileum compared with the control (P < 0.05). Long-term (18-h) stimulation with the sweetener induced the expression of the enteroendocrine-specific markers chromogranin A, glucagon, Pyy, and cholecystokinin 3.5- (P < 0.001), 3.5- (P < 0.001), 3.8- (P < 0.05), and 6.5-fold (P < 0.001), respectively. CONCLUSIONS These results show novel ex vivo effects of rebaudioside A on enteroendocrine cells of the mouse small intestine and highlight potentially new applications for rebaudioside A in metabolic diseases.

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The Journal of Nutrition Health and Aging

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