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餐中肝门静脉输注葡萄糖可减少大鼠的自发进食量。

Intrameal hepatic-portal infusion of glucose reduces spontaneous meal size in rats.

作者信息

Langhans W, Grossmann F, Geary N

机构信息

Institute of Animal Sciences, Swiss Federal Institute of Technology, Zurich, Switzerland.

出版信息

Physiol Behav. 2001 Jul;73(4):499-507. doi: 10.1016/s0031-9384(01)00479-6.

Abstract

To test whether glucose (GLC) or insulin (INS) acutely reduces spontaneous meal size, we tested the effects of remotely controlled, intrameal hepatic-portal vein infusions of GLC or INS on rats' spontaneous feeding patterns. Experiment 1 included four blocks of three test infusions and one control infusion. The test infusions in each block were 0.25, 0.5, 1.0 or 1.5 mmol GLC; 2, 4, 6, or 8 mU INS; or the four combinations with dose ratios of 1 mmol GLC/8 mU INS, respectively. Control infusions and the INS vehicle were saline infusions that were equiosmotic to the GLC infusion used in that block. Infusions (0.1 ml x 5 min) were done during the first spontaneous dark-phase meal. None of the test infusions affected meal size, meal duration or the duration of the subsequent intermeal interval. In Experiment 2, a similar design was used to test infusions of 1 mmol GLC, 2 mU INS and GLC/INS. Both GLC alone and GLC/INS reduced the size and duration of the first spontaneous dark-phase meal. The subsequent intermeal interval was unaffected, but GLC alone also increased the satiety ratio (min/g) of the meal. The size and duration of the second dark-phase meal were unaffected. INS alone did not affect any meal parameters. In Experiment 3, infusions of 1 mmol GLC and 2 mU INS were repeated during each of the first three meals of the dark phase. These infusions reduced the size and duration of each meal, as well as 6-h cumulative food intake, but did not affect any other meal parameter. These experiments demonstrate for the first time that intrameal hepatic-portal infusions of GLC or of GLC and INS is sufficient to acutely and selectively reduce spontaneous meal size in the rat. The findings are consistent with the idea that meal-contingent changes in hepatic-portal GLC concentration contribute to satiation.

摘要

为了测试葡萄糖(GLC)或胰岛素(INS)是否能急性降低自发进食量,我们通过远程控制、在进食期间经肝门静脉输注GLC或INS,来测试其对大鼠自发进食模式的影响。实验1包括四个组块,每个组块有三次测试输注和一次对照输注。每个组块中的测试输注分别为0.25、0.5、1.0或1.5 mmol GLC;2、4、6或8 mU INS;或剂量比为1 mmol GLC/8 mU INS的四种组合。对照输注和INS溶媒为与该组块中使用的GLC输注等渗的生理盐水输注。输注(0.1 ml×5分钟)在第一次自发暗期进食期间进行。没有任何测试输注影响进食量、进食持续时间或随后的餐间间隔时间。在实验2中,采用类似设计测试1 mmol GLC、2 mU INS和GLC/INS的输注。单独的GLC和GLC/INS均减小了第一次自发暗期进食的量和持续时间。随后的餐间间隔未受影响,但单独的GLC也增加了该餐的饱腹感比率(分钟/克)。第二次暗期进食的量和持续时间未受影响。单独的INS不影响任何进食参数。在实验3中,在暗期的前三餐每餐期间重复输注1 mmol GLC和2 mU INS。这些输注减小了每餐的量和持续时间,以及6小时累积食物摄入量,但不影响任何其他进食参数。这些实验首次证明,在进食期间经肝门静脉输注GLC或GLC与INS足以急性且选择性地降低大鼠的自发进食量。这些发现与肝门静脉GLC浓度随餐变化有助于产生饱腹感的观点一致。

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