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胰岛素与地塞米松在调控绵羊脂肪组织丙酮酸激酶活性及葡萄糖代谢中的相互作用

Interactions of insulin and dexamethasone in the control of pyruvate kinase activity and glucose metabolism in sheep adipose tissue.

作者信息

Plested C P, Taylor E, Brindley D N, Vernon R G

机构信息

Department of Biochemistry, University of Nottingham Medical School, Queen's Medical Centre, U.K.

出版信息

Biochem J. 1987 Oct 15;247(2):459-65. doi: 10.1042/bj2470459.

Abstract
  1. The Vmax. activity of pyruvate kinase of sheep adipose tissue increased during tissue culture up to 48 h; the increase was blocked by actinomycin D (an inhibitor of transcription) and was promoted by insulin and antagonized by dexamethasone. 2. In contrast with their effects on pyruvate kinase, insulin and dexamethasone acted synergistically to increase the activity of glucose-6-phosphate dehydrogenase of sheep adipose tissue maintained in culture. 3. Insulin stimulated, whereas dexamethasone inhibited, glucose utilization by sheep adipose tissue maintained in culture; the two agents were mutually antagonistic, and their effects were prevented by actinomycin D. 4. Antimycin A (an inhibitor of the electron-transport chain) stimulated glucose uptake and lactate output by sheep adipose tissue in the presence of dexamethasone and insulin, suggesting that the effects of dexamethasone on glucose utilization by sheep adipose tissue were not due to an inhibition of glucose transport. 5. Comparison of these findings with previous studies on the endocrine control of hepatic pyruvate kinase shows that there are major differences in the control of these Vmax. activities in liver and adipose tissue. 6. Although glucocorticoid hormones inhibit glucose utilization themselves and can antagonize the stimulatory effects of insulin on glucose utilization in adipose tissue from both sheep and rats, there appear to be major differences in the sites of action of these hormones in the two species.
摘要
  1. 绵羊脂肪组织丙酮酸激酶的最大反应速度(Vmax)活性在组织培养长达48小时的过程中增加;这种增加被放线菌素D(一种转录抑制剂)阻断,被胰岛素促进,并被地塞米松拮抗。2. 与它们对丙酮酸激酶的作用相反,胰岛素和地塞米松协同作用以增加培养的绵羊脂肪组织中葡萄糖-6-磷酸脱氢酶的活性。3. 胰岛素刺激培养的绵羊脂肪组织的葡萄糖利用,而地塞米松抑制;这两种药物相互拮抗,且它们的作用被放线菌素D阻止。4. 抗霉素A(一种电子传递链抑制剂)在存在地塞米松和胰岛素的情况下刺激绵羊脂肪组织的葡萄糖摄取和乳酸输出,表明地塞米松对绵羊脂肪组织葡萄糖利用的作用不是由于抑制葡萄糖转运。5. 将这些发现与先前关于肝丙酮酸激酶内分泌控制的研究进行比较表明,肝脏和脂肪组织中这些最大反应速度(Vmax)活性的控制存在主要差异。6. 尽管糖皮质激素本身抑制葡萄糖利用并且可以拮抗胰岛素对绵羊和大鼠脂肪组织中葡萄糖利用的刺激作用,但这些激素在两个物种中的作用位点似乎存在主要差异。

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