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首页> 美国卫生研究院文献>PLoS Clinical Trials >Orexin-1 Receptor Co-Localizes with Pancreatic Hormones in Islet Cells and Modulates the Outcome of Streptozotocin-Induced Diabetes Mellitus
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Orexin-1 Receptor Co-Localizes with Pancreatic Hormones in Islet Cells and Modulates the Outcome of Streptozotocin-Induced Diabetes Mellitus

机译:Orexin-1受体与胰岛细胞胰激素共定位并调节链脲佐菌素诱导的糖尿病的结果。

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Recent studies have shown that orexins play a critical role in the regulation of sleep/wake states, feeding behaviour, and reward processes. The exocrine and endocrine pancreas are involved in the regulation of food metabolism and energy balance. This function is deranged in diabetes mellitus. This study examined the pattern of distribution of orexin-1 receptor (OX1R) in the endocrine cells of the pancreas of normal and diabetic Wistar (a model of type 1 diabetes), Goto-Kakizaki (GK, a model of type 2 diabetes) rats and in orexin-deficient (OX−/−) and wild type mice. Diabetes mellitus (DM) was induced in Wistar rats and mice by streptozotocin (STZ). At different time points (12 h, 24 h, 4 weeks, 8 months and 15 months) after the induction of DM, pancreatic fragments of normal and diabetic rats were processed for immunohistochemistry and Western blotting. OX1R-immunoreactive nerves were observed in the pancreas of normal and diabetic Wistar rats. OX1R was also discernible in the pancreatic islets of normal and diabetic Wistar and GK rats, and wild type mice. OX1R co-localized with insulin (INS) and glucagon (GLU) in the pancreas of Wistar and GK rats. The number of OX1R-positive cells in the islets increased markedly (p<0.0001) after the onset of DM. The increase in the number of OX1R-positive cells is associated with a high degree of co-localization with GLU. The number of GLU- positive cells expressing OX1R was significantly (p<0.0001) higher after the onset of DM. The tissue level of OX1R protein increased with the duration of DM especially in type 1 diabetes where it co-localized with cleaved caspase 3 in islet cells. In comparison to STZ-treated wild type mice, STZ-treated OX−/− animals exhibited reduced hyperglycemia and handled glucose more efficiently in glucose tolerance test. The findings suggest an important role for the OX-OX1R pathway in STZ-induced experimental diabetes.
机译:最近的研究表明,食欲素在调节睡眠/觉醒状态,进食行为和奖励过程中起着至关重要的作用。外分泌和内分泌胰腺参与食物代谢和能量平衡的调节。该功能在糖尿病中是紊乱的。这项研究检查了正常和糖尿病Wistar(1型糖尿病模型),五岛崎崎(GK,2型糖尿病模型)大鼠胰腺内分泌细胞中orexin-1受体(OX1R)的分布模式和缺乏orexin的小鼠(OX -/-)和野生型小鼠。在Wistar大鼠和小鼠中,链脲佐菌素(STZ)诱导了糖尿病(DM)。在诱导DM后的不同时间点(12小时,24小时,4周,8个月和15个月),对正常和糖尿病大鼠的胰腺片段进行免疫组织化学和蛋白质印迹分析。在正常和糖尿病Wistar大鼠的胰腺中观察到OX1R免疫反应性神经。在正常和糖尿病Wistar和GK大鼠和野生型小鼠的胰岛中,OX1R也很明显。 OX1R与胰岛素(INS)和胰高血糖素(GLU)在Wistar和GK大鼠的胰腺中共定位。 DM发作后,胰岛中OX1R阳性细胞的数量显着增加(p <0.0001)。 OX1R阳性细胞数量的增加与与GLU的高度共定位有关。 DM发病后,表达OX1R的GLU阳性细胞数量显着增加(p <0.0001)。 OX1R蛋白的组织水平随DM持续时间的增加而增加,特别是在1型糖尿病中,它与裂解的caspase 3共定位于胰岛细胞中。与STZ处理的野生型小鼠相比,STZ处理的OX -/-动物表现出降低的高血糖症,并且在葡萄糖耐量测试中更有效地处理了葡萄糖。这些发现表明,OX-OX1R途径在STZ诱导的实验性糖尿病中具有重要作用。

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