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与皮下注射相比,慢性腹腔内胰岛素给药可改善链脲佐菌素诱导的糖尿病大鼠的肝脏葡萄糖代谢。

Chronic intraperitoneal insulin delivery, as compared with subcutaneous delivery, improves hepatic glucose metabolism in streptozotocin diabetic rats.

作者信息

Mason T M, Gupta N, Goh T, El-Bahrani B, Zannis J, van de Werve G, Giacca A

机构信息

Department of Physiology and Medicine, University of Toronto, Canada.

出版信息

Metabolism. 2000 Nov;49(11):1411-6. doi: 10.1053/meta.2000.17731.

Abstract

We have previously shown that chronic insulin treatment by the intraperitoneal route normalizes the elevated glucose production (GP) in streptozotocin (STZ) diabetic rats, while insulin delivered by the subcutaneous route only partially normalizes GP. To investigate the biochemical mechanism of the effect of chronic insulin delivery by either route on hepatic glucose metabolism, we measured the hepatic activity of glucose 6-phosphatase (G6Pase) and glucokinase (GK). Four groups of rats were used: (1) nondiabetic rats (N, n = 7), (2) untreated STZ diabetic rats (D, n = 8), (3) diabetic rats treated intraperitoneally (IP, n = 6), or (4) subcutaneously (SC, n = 8) (both 3 U of insulin/d). Glucose levels, higher in D, were normalized by insulin treatment regardless of route. Peripheral insulin levels were lowest in D and highest in SC as expected (N, 162 +/- 18 pmol/L; D, 66 +/- 12; IP, 360 +/- 96; SC, 798 +/- 198). STZ diabetes resulted in a 10-fold decrease in GK (P < .001), and a 2-fold increase in G6Pase activity (P < .01). Both intraperitoneal and subcutaneous treatments normalized G6Pase activity. In contrast, with subcutaneous but not intraperitoneal treatment, GK activity was still 35% less than normal (SC v N, P < .05). Glucose 6-phosphate (G6P) levels did not differ among the groups. In summary: (1) the increase in GP in D reflected increased activity of G6Pase and reduced activity of GK, (2) the partial suppression of GP with subcutaneous insulin treatment reflected correction of increased G6Pase activity, but only partial correction of low GK activity, and (3) the normalization of GP with intraperitoneal insulin treatment reflected correction of both increased G6Pase activity and low GK activity. Our current studies indicate that chronic intraperitoneal insulin treatment is superior to subcutaneous treatment with regard to hepatic glucose metabolism.

摘要

我们之前已经表明,通过腹腔途径进行慢性胰岛素治疗可使链脲佐菌素(STZ)诱导的糖尿病大鼠升高的葡萄糖生成(GP)恢复正常,而通过皮下途径给予胰岛素只能部分使GP恢复正常。为了研究通过这两种途径进行慢性胰岛素给药对肝脏葡萄糖代谢影响的生化机制,我们测量了葡萄糖6磷酸酶(G6Pase)和葡萄糖激酶(GK)的肝脏活性。使用了四组大鼠:(1)非糖尿病大鼠(N,n = 7),(2)未治疗的STZ糖尿病大鼠(D,n = 8),(3)腹腔注射治疗的糖尿病大鼠(IP,n = 6),或(4)皮下注射治疗的糖尿病大鼠(SC,n = 8)(均为胰岛素3 U/d)。D组的血糖水平较高,胰岛素治疗无论通过何种途径均可使其恢复正常。外周胰岛素水平在D组中最低,在SC组中最高,正如预期的那样(N组,162±18 pmol/L;D组,66±12;IP组,360±96;SC组,798±198)。STZ糖尿病导致GK降低了10倍(P <.001),G6Pase活性增加了2倍(P <.01)。腹腔注射和皮下注射治疗均使G6Pase活性恢复正常。相比之下,皮下注射而非腹腔注射治疗后,GK活性仍比正常水平低35%(SC组与N组相比,P <.05)。各组之间的葡萄糖6磷酸(G6P)水平没有差异。总之:(1)D组中GP的增加反映了G6Pase活性增加和GK活性降低,(2)皮下胰岛素治疗对GP的部分抑制反映了G6Pase活性增加的纠正,但仅部分纠正了GK活性降低,(3)腹腔胰岛素治疗使GP恢复正常反映了G6Pase活性增加和GK活性降低两者均得到纠正。我们目前的研究表明,就肝脏葡萄糖代谢而言,慢性腹腔胰岛素治疗优于皮下治疗。

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