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Effect of portal glucose sensing on incretin hormone secretion in a canine model

机译:门静脉葡萄糖感应对犬类模型肠促胰岛素激素分泌的影响

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It is unknown whether activation of hepato-portal vein (PV) glucose sensors plays a role in incretin hormone amplification of oral glucose-stimulated insulin secretion (GSIS). In previous studies, PV glucose infusion increased GSIS through unknown mechanisms, perhaps neural stimulation of pancreatic P-cells and/or stimulation of gut incretin hormone release. Thus, there could be a difference in the incretin effect when comparing GSIS with portal rather than leg vein (LV) glucose infusion. Plasma insulin and incretin hormones were studied in six overnight-fasted dogs. An oral glucose tolerance test (OGTT) was administered, and then 1 and 2 wk later the arterial plasma glucose profile from the OGTT was mimicked by infusing glucose into either the PV or a LV. The arterial glucose levels were nearly identical between groups (AUCs within 1 of each other). Oral glucose administration increased arterial GLP-I and GIP levels by more than sixfold, whereas they were not elevated by PV or LV glucose infusion. Oral glucose delivery was associated with only a small incretin effect (arterial insulin and C-peptide were 21 ±23 and 24 ± 17 greater, respectively, during the 1st hour with oral compared with PV glucose and 14 ± 37 and 13 ± 35 greater, respectively, in oral versus LV; PV versus LV responses were not significantly different from each other). Thus, following an OGTT incretin hormone release did not depend on activation of PV glucose sensors, and the insulin response was not greater with PV compared with LV glucose infusion in the dog. The small incretin effect points to species peculiarities, which is perhaps related to diet.
机译:目前尚不清楚肝门静脉 (PV) 葡萄糖传感器的激活是否在口服葡萄糖刺激胰岛素分泌 (GSIS) 的肠促胰岛素激素扩增中发挥作用。在之前的研究中,PV葡萄糖输注通过未知的机制增加了GSIS,可能是胰腺P细胞的神经刺激和/或肠道肠促胰岛素激素释放的刺激。因此,将 GSIS 与门静脉而不是腿静脉 (LV) 葡萄糖输注进行比较时,肠促胰岛素效应可能存在差异。在六只过夜禁食的狗中研究了血浆胰岛素和肠促胰岛素激素。进行口服葡萄糖耐量试验 (OGTT),然后在 1 周和 2 周后通过将葡萄糖注入 PV 或 LV 来模拟来自 OGTT 的动脉血浆葡萄糖谱。各组之间的动脉葡萄糖水平几乎相同(AUCs彼此相差1%以内)。口服葡萄糖使动脉 GLP-I 和 GIP 水平增加 6 倍以上,而 PV 或 LV 葡萄糖输注并未升高。口服葡萄糖递送仅与小的肠促胰岛素效应相关(与 PV 葡萄糖相比,口服葡萄糖的第 1 小时内动脉胰岛素和 C 肽分别高 21 ±23 和 24 ± 17%,口服葡萄糖和 13 ± 35% 分别高 14 ± 37% 和 13 35%;PV与LV反应彼此之间没有显著差异)。因此,OGTT 肠促胰岛素激素释放后不依赖于 PV 葡萄糖传感器的激活,并且与狗的 LV 葡萄糖输注相比,PV 的胰岛素反应并不大。小肠促胰岛素效应指向物种特性,这可能与饮食有关。

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