首页> 外文期刊>General Pharmacology >Effect of acute and sub-chronic administration of the imidazoline compound S 22068 on in vivo glucose and insulin responses in normal lean CBA/Ca mice.
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Effect of acute and sub-chronic administration of the imidazoline compound S 22068 on in vivo glucose and insulin responses in normal lean CBA/Ca mice.

机译:咪唑啉化合物S 22068的急性和亚慢性给药对正常瘦CBA / Ca小鼠体内葡萄糖和胰岛素反应的影响。

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摘要

Acute S 22068 (24 mg/kg po) improved glucose tolerance and increased insulin sensitivity, assessed as the acute blood glucose response to exogenous insulin. The same acute dose did not stimulate insulin secretion or induce hypoglycemia in fed animals. Comparison of acute S 22068 to equipotent doses (with respect to effect on glucose tolerance) of gliclazide (2 mg/kg) and metformin (60 mg/kg) found S 22068 to be similar to metformin with respect to its effects on basal glucose levels (BGL) and insulin sensitivity. This also suggests that S 22068 acts by a mechanism which does not involve insulin release. Acute or sub-chronic S 22068 (14 days at 25 mg/day) had no effect on brown adipose tissue (BAT) or white adipose tissue (WAT) lipogenesis, an insulin-sensitive metabolic pathway. Sub-chronic treatment with S 22068 did not alter body weight (BW) or food intake, and resulted in tolerance to its effects on glucose metabolism and insulin sensitivity. These findings suggest that S 22068 is similar in effect to metformin, and is not insulinogenic, in contrast to the sulfonylureas or putative I(3) imidazoline site ligands.
机译:急性S 22068(24 mg / kg po)改善了葡萄糖耐量,并提高了胰岛素敏感性,被评估为对外源胰岛素的急性血糖反应。相同的急性剂量不会刺激喂养动物的胰岛素分泌或引起低血糖。将急性S 22068与格列齐特(2 mg / kg)和二甲双胍(60 mg / kg)的等效剂量(就其对葡萄糖耐量的影响有关)进行比较发现,S 22068在对基础葡萄糖水平的影响方面与二甲双胍相似(BGL)和胰岛素敏感性。这也表明S 22068通过不涉及胰岛素释放的机制起作用。急性或亚慢性S 22068(25毫克/天,可持续14天)对棕色脂肪组织(BAT)或白色脂肪组织(WAT)脂肪生成(一种胰岛素敏感的代谢途径)没有影响。用S 22068进行的亚慢性治疗不会改变体重(BW)或食物摄入量,并导致其对葡萄糖代谢和胰岛素敏感性的影响具有耐受性。这些发现表明,与磺酰脲类或推定的I(3)咪唑啉位点配体相反,S 22068的作用与二甲双胍相似,且不致胰岛素。

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