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首页> 外文期刊>American Journal of Physiology >Intraportal administration of neuropeptide Y and hepatic glucose metabolism
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Intraportal administration of neuropeptide Y and hepatic glucose metabolism

机译:门静脉内施用神经肽Y和肝糖代谢

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We examined whether intraportal delivery of neuropeptide Y (NPY) affects glucose metabolism in 42-h-fasted conscious dogs using arteriovenous difference methodology. The experimental period was divided into three subperiods (P1, P2, and P3). During all subperiods, the dogs received infusions of somatostatin, intraportal insulin (threefold basal), intraportal glucagon (basal), and peripheral intravenous glucose to increase the hepatic glucose load twofold basal. Following P1, in the NPY group (n = 7), NPY was infused intraportally at 0.2 and 5.1 pmol centre dot kg~(-1) centre dot min~(-1) during P2 and P3, respectively. The control group (n = 7) received intraportal saline infusion without NPY. There were no significant changes in hepatic blood flow in NPY vs. control. The lower infusion rate of NPY (P2) did not enhance net hepatic glucose uptake. During P3, the increment in net hepatic glucose uptake (compared with P1) was 4 +- 1 and 10 +- 2 mumol centre dot kg~(-1) centre dot min~(-1) in control and NPY, respectively (P < 0.05). The increment in net hepatic fractional glucose extraction during P3 was 0.015 +- 0.005 and 0.039 +- 0.008 in control and NPY, respectively (P < 0.05). Net hepatic carbon retention was enhanced in NPY vs. control (22 +- 2 vs. 14 +- 2 mumol centre dot kg~(-1) centre dot min~(-1), P < 0.05). There were no significant differences between groups in the total glucose infusion rate. Thus, intraportal NPY stimulates net hepatic glucose uptake without significantly altering whole body glucose disposal in dogs.
机译:我们检查了动静脉差异方法是否门内传递神经肽Y(NPY)会影响禁食42小时的清醒犬的葡萄糖代谢。实验期分为三个子时段(P1,P2和P3)。在所有亚周期中,犬接受生长抑素,门静脉内胰岛素(基础剂量的三倍),门静脉内胰高血糖素(基础的)和外周静脉葡萄糖的输注,以使肝葡萄糖负荷增加两倍。在P1之后,在NPY组(n = 7)中,在P2和P3期间分别以0.2和5.1 pmol中心点kg〜(-1)中心点min〜(-1)经门静脉内注入NPY。对照组(n = 7)接受门静脉输注生理盐水而无NPY。与对照组相比,NPY的肝血流量无明显变化。较低的NPY(P2)输注速率不会增加肝净葡萄糖摄取。在P3期间,对照组和NPY的净肝葡萄糖摄取增量(与P1相比)分别为4 +/- 1和10 +/- 2μmol中心点kg〜(-1)中心点min〜(-1)(P <0.05)。在对照和NPY中,P3期间净肝分数葡萄糖提取的增量分别为0.015±0.005和0.039±0.008(P <0.05)。与对照组相比,NPY的净肝碳保留量增加(22±2 vs. 14±2 mumol中心点kg〜(-1)中心点min〜(-1),P <0.05)。两组之间的总葡萄糖输注速率没有显着差异。因此,门静脉内NPY刺激肝净葡萄糖摄取,而不会显着改变犬体内的全身葡萄糖处置。

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