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The effects of GLP-1 infusion in the hepatic portal region on food intake.

机译:肝门区GLP-1输注对食物摄入的影响。

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A wide range of evidence points to a role for GLP-1 to regulate food intake. Anorectic effects of GLP-1 are most apparent when the peptide is administered directly into the central nervous system (CNS), but suppression of food intake has also been noted in some cases with peripheral administration. It is unclear which GLP-1 receptor (GLP-1r) population mediates the effects of plasma GLP-1, although direct actions to activate CNS neurons have been demonstrated. More recently several groups have demonstrated that GLP-1 can activate peripheral nerves in the hepatic portal vein to regulate glucose metabolism. To test the hypothesis that GLP-1 receptors on nerve terminals in the hepatic portal affect feeding behavior, we compared the effects of direct infusions into hepatic portal and jugular veins in rats. Jugular GLP-1 decreased food intake at doses as low as 10 microg from 0.5-4 h into the dark cycle, whereas portal GLP-1 decreased food intake only at the highest dose tested (100 microg). The blockade of endogenous GLP-1 action before or during eating by infusing dH-Ex, GLP-1 receptor antagonist, into either jugular or portal vein did not cause any change in food intake during either the dark or light cycles. Taken together, these data suggest that while peripheral GLP-1 may be involved in the regulation of food intake, the key GLP-1 receptors are unlikely to be those associated with vagal afferent nerves innervating the hepatic portal vein.
机译:大量证据表明,GLP-1可以调节食物摄入量。当将肽直接给药至中枢神经系统(CNS)时,GLP-1的厌食作用最为明显,但在某些情况下,外周给药也可抑制食物摄入。尚不清楚哪种GLP-1受体(GLP-1r)介导血浆GLP-1的作用,尽管已经证明了激活CNS神经元的直接作用。最近,几个研究小组证明了GLP-1可以激活肝门静脉的周围神经来调节葡萄糖代谢。为了检验肝门神经末梢上的GLP-1受体影响进食行为的假设,我们比较了直接输注大鼠肝门和颈静脉的作用。在黑暗周期中,从0.5-4小时到低剂量,颈静脉GLP-1减少食物摄入,而门极GLP-1仅在最高测试剂量(100微克)下减少食物摄入。在黑暗或明亮的周期中,通过将dH-Ex,GLP-1受体拮抗剂注入颈静脉或门静脉来阻止进食前或进食期间内源性GLP-1的作用不会引起食物摄入量的任何变化。综上所述,这些数据表明,虽然外周GLP-1可能参与食物摄入的调节,但关键的GLP-1受体不太可能与支配肝门静脉的迷走神经有关。

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