Iglesias-Osma María Carmen, Garcia-Barrado Maria José, Visentin Virgile, Pastor-Mansilla Maria Francisca, Bour Sandy, Prévot Danielle, Valet Philippe, Moratinos Julio, Carpéné Christian
Unité de recherches sur les obésités, Institut National de la Santé et de la Recherche Médicale U586, Centre Hospitalier Universitaire de Toulouse, Université Paul Sabatier, France.
J Pharmacol Exp Ther. 2004 Jun;309(3):1020-8. doi: 10.1124/jpet.103.063636. Epub 2004 Feb 20.
Benzylamine, a substrate of semicarbazide-sensitive amine oxidase (SSAO), stimulates glucose transport in rat adipocytes and improves glucose disposal in diabetic rats only in the presence of vanadate. These effects have been described to result from a synergism between the hydrogen peroxide formed during amine oxidation and vanadate, via the generation of pervanadate, a powerful insulin mimicker. However, it has also been reported that benzylamine alone can stimulate glucose uptake and inhibit lipolysis in human fat cells. In this work, we therefore investigated whether benzylamine on its own was able to induce both in vivo and in vitro insulin-like responses in animal models other than rat. In rabbits, the i.v. infusion of 7 micromol/kg benzylamine before a glucose tolerance test resulted in a net reduction of the hyperglycemic response without a change in insulin secretion. Benzylamine also improved glucose tolerance and reduced lipid mobilization in hyperglycemic/obese mice. In vitro, 0.1 mM benzylamine stimulated glucose transport and inhibited lipolysis in mouse and rabbit adipocytes. These effects were blocked by previous treatments with semicarbazide, a SSAO inhibitor. Levels of benzylamine oxidation were more elevated in mouse than in rabbit adipose tissues, whereas the reverse was observed for skeletal muscles. Finally, benzylamine was unable to stimulate insulin secretion by isolated pancreatic islets from both species and SSAO activity was hardly detectable in pancreas. Together, our results bring evidence that benzylamine on its own can improve glucose tolerance in rabbit and mouse, likely by stimulating glucose uptake via amine oxidase activation in insulin-sensitive tissues.
苄胺是氨基脲敏感胺氧化酶(SSAO)的一种底物,仅在有钒酸盐存在的情况下,它能刺激大鼠脂肪细胞的葡萄糖转运,并改善糖尿病大鼠的葡萄糖代谢。据描述,这些作用是由胺氧化过程中形成的过氧化氢与钒酸盐之间的协同作用导致的,通过生成过氧钒酸盐,一种强大的胰岛素模拟物。然而,也有报道称苄胺单独就能刺激人脂肪细胞的葡萄糖摄取并抑制脂肪分解。因此,在这项研究中,我们调查了苄胺自身是否能够在大鼠以外的动物模型中诱导体内和体外的胰岛素样反应。在兔子中,在葡萄糖耐量试验前静脉注射7微摩尔/千克苄胺导致高血糖反应净减少,而胰岛素分泌没有变化。苄胺还改善了高血糖/肥胖小鼠的葡萄糖耐量并减少了脂质动员。在体外,0.1毫摩尔/升苄胺刺激小鼠和兔子脂肪细胞的葡萄糖转运并抑制脂肪分解。这些作用被氨基脲(一种SSAO抑制剂)预先处理所阻断。小鼠脂肪组织中苄胺氧化水平比兔子脂肪组织中更高,而在骨骼肌中观察到的情况则相反。最后,苄胺不能刺激这两个物种的分离胰岛分泌胰岛素,并且在胰腺中几乎检测不到SSAO活性。总之,我们的结果证明苄胺自身可以改善兔子和小鼠的葡萄糖耐量,可能是通过在胰岛素敏感组织中激活胺氧化酶来刺激葡萄糖摄取。
