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土霉素治疗对遗传性糖尿病(db/db)小鼠肝脏糖原代谢酶的影响。

Effects of oxytetracycline treatment on enzymes of hepatic glycogen metabolism in genetically diabetic (db/db) mice.

作者信息

Benzo C A

出版信息

Biochem Med Metab Biol. 1987 Feb;37(1):42-50. doi: 10.1016/0885-4505(87)90008-9.

Abstract

The effects of daily oxytetracycline treatment on the activities of hepatic glycogen synthase, glycogen phosphorylase, plasma glucose, and insulin, and on liver glycogen, free fatty acid, and triglyceride levels were examined in 8- to 15-week-old genetically diabetic and lean mice. Oxytetracycline administration resulted in substantial reductions in the plasma glucose and immunoreactive-insulin levels in both diabetic and lean mice. The drug had no significant effect on the liver glycogen content in either phenotype, regardless of age, but it increased hepatic lipids and depressed body weights in lean animals. The most prominent effect of the drug was in markedly altering the activities of both glycogen synthase and phosphorylase in the liver of older diabetic mice. Oxytetracycline treatment produced a three-fold increase in the percentage of glycogen synthase I activity and reduced by one-third the percentage of glycogen phosphorylase a activity in 15-week-old diabetic mice. In age-matched lean mice treated with oxytetracycline, the percentage of glycogen synthase I activity increased significantly, but the percentage of phosphorylase a activity was unchanged. These data suggest that the drug may alter an aspect of hepatic glycogen metabolism which might lead to an inhibition of glycogenolysis and subsequent diminution of blood sugar levels in the diabetic. The present results show that, while oxytetracycline may be effective in reducing the severity of some of the diabetic symptoms associated with carbohydrate metabolism in this animal model of maturity-onset diabetes, the drug may have adverse effects on aspects of protein and lipid metabolism in these animals.

摘要

在8至15周龄的遗传性糖尿病小鼠和瘦小鼠中,研究了每日服用土霉素对肝糖原合酶、糖原磷酸化酶活性、血糖、胰岛素以及肝糖原、游离脂肪酸和甘油三酯水平的影响。给糖尿病小鼠和瘦小鼠服用土霉素后,其血糖和免疫反应性胰岛素水平均大幅降低。无论年龄大小,该药物对两种表型小鼠的肝糖原含量均无显著影响,但会增加瘦小鼠的肝脏脂质并降低其体重。该药物最显著的作用是明显改变老年糖尿病小鼠肝脏中糖原合酶和磷酸化酶的活性。在15周龄的糖尿病小鼠中,土霉素治疗使糖原合酶I活性百分比增加了两倍,糖原磷酸化酶a活性百分比降低了三分之一。在用土霉素治疗的年龄匹配的瘦小鼠中,糖原合酶I活性百分比显著增加,但磷酸化酶a活性百分比没有变化。这些数据表明,该药物可能改变了肝糖原代谢的一个方面,这可能导致糖尿病患者糖原分解受到抑制,进而血糖水平降低。目前的结果表明,虽然土霉素可能有效减轻这种成年型糖尿病动物模型中与碳水化合物代谢相关的一些糖尿病症状的严重程度,但该药物可能会对这些动物的蛋白质和脂质代谢产生不利影响。

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