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首页> 外文期刊>Journal of diabetes and its complications >Effects of mitemcinal (GM-611), an orally active erythromycin-derived prokinetic agent, on delayed gastric emptying and postprandial glucose in a new minipig model of diabetes.
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Effects of mitemcinal (GM-611), an orally active erythromycin-derived prokinetic agent, on delayed gastric emptying and postprandial glucose in a new minipig model of diabetes.

机译:口服活性红霉素衍生的动能素(GM-611)对新型糖尿病迷你猪模型中延迟胃排空和餐后葡萄糖的影响。

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摘要

AIMS: This study was conducted to evaluate the suitability of a new minipig model for investigating aspects of diabetes such as delayed gastric emptying and glucose metabolism abnormalities, and to test the effects of mitemcinal (GM-611), an orally active erythromycin-derived motilin receptor agonist, on gastric emptying and postprandial glucose in normal and diabetic minipigs. METHODS AND RESULTS: Intravenous injection of 300 mg/kg streptozotocin (STZ) to 5-week-old minipigs induced moderate hyperglycemia (about 200 mg/dl) for >80 weeks without insulin treatment. Decreased insulin production (P<.05), increased area under the glucose curve (P<.05), and slower glucose disappearance (P<.05) were demonstrated, and there was no severe inhibition of body weight gain, liver failure, or renal failure. Gastric emptying was significantly delayed in diabetic minipigs (P<.05) at 80 weeks, but not at 40 weeks, post-STZ. Oral administration of mitemcinal (5 mg/kg) at 80 weeks accelerated gastric emptying and induced a similar postprandial glucose profile in normal and diabetic minipigs with delayed gastric emptying. CONCLUSIONS: The new diabetic minipig model showed suitability for investigating diabetes, gastric emptying, and plasma glucose excursions. Since delayed gastric emptying and irregular plasma glucose excursions are characteristic of diabetic gastroparesis, the accelerating and regulating effects of mitemcinal on this model add to the existing evidence that mitemcinal is likely to be useful for treating diabetic gastroparesis.
机译:目的:本研究旨在评估新的小型猪模型在研究糖尿病方面的适用性,例如延迟排空胃液和葡萄糖代谢异常,并测试口服活性红霉素衍生的胃动素米他辛(GM-611)的作用受体激动剂,对正常和糖尿病小型猪的胃排空和餐后葡萄糖产生影响。方法和结果:未经胰岛素治疗的5周龄小型猪静脉注射300 mg / kg链脲佐菌素(STZ)导致中度高血糖(约200 mg / dl),持续时间超过80周。结果显示胰岛素产生减少(P <.05),葡萄糖曲线下面积增加(P <.05)和葡萄糖消失缓慢(P <.05),并且没有严重抑制体重增加,肝衰竭,或肾功能衰竭。 STZ后,糖尿病小型猪的胃排空明显延迟(P <.05),但在80周时没有延迟(P <.05)。在80周时口服咪替米宁(5 mg / kg)可加速正常和糖尿病小型猪的胃排空,并引起类似的餐后葡萄糖分布,并延迟胃排空。结论:新的糖尿病小型猪模型显示出适用于研究糖尿病,胃排空和血浆葡萄糖偏移的研究。由于延迟的胃排空和血浆葡萄糖不规则偏移是糖尿病性胃轻瘫的特征,因此米替米康对该模型的加速和调节作用增加了现有证据,表明米替米康可能用于治疗糖尿病性胃轻瘫。

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