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葡萄糖对肥胖型(fa/fa) Zucker大鼠培养胰岛中胰岛素分泌及葡萄糖磷酸化活性的调节作用

Modulation by glucose of insulin secretion and glucose phosphorylating activity in cultured pancreatic islets from obese (fa/fa) Zucker rats.

作者信息

Chan C B, Lowe J M, Debertin W J

机构信息

Department of Anatomy and Physiology, Atlantic Veterinary College, University of Prince Edward Island, Charlottetown, Canada.

出版信息

Int J Obes Relat Metab Disord. 1996 Feb;20(2):175-84.

PMID:8646255
Abstract

OBJECTIVE

In normal B-cells, glucokinase activity is regulated by glucose. We hypothesized that chronic exposure to low or high glucose levels would regulate glucokinase function and insulin secretion differently in islets of fa/fa compared with lean rats. SUBJECTS, DESIGN, and

MEASUREMENTS

Islets isolated from lean and fa/fa rats (8-12 wk old) were cultured for 1-7 days in low (3.3 mM), moderate (12.5 mM) or supraphysiological (25.0 mM) glucose-supplemented medium. Sensitivity to glucose of hexokinase, glucokinase (by enzyme assay and kinetic analysis), and the insulin response (by radioimmunoassay) were assessed in each group of islets.

RESULTS

Islets of fa/fa rats cultured in 12.5 mM glucose for 1-7 days demonstrated a left-shift in both the EC50 of the insulin response and the Km of glucokinase to glucose. The glucokinase Vmax of fa/fa rat islets was lower under all conditions tested, thereby limiting the potential increase in insulin secretion. When cultured in 3.3 mM glucose for 1-7 days, fa/fa rat islets retained responsiveness to glucose longer and the estimated EC50 for glucose actually declined. However, the glucokinase Km for glucose increased three-fold in both phenotypes cultured in low glucose. Lean and fa/fa rat islets cultured in 25.0 mM glucose demonstrated a paradoxical hypersecretion of insulin to basal glucose concentrations and desensitization to stimulation by high concentrations of glucose. Islets from fa/fa rats were more easily desensitized, with significant effects in 25.0 mM glucose by 3 days compared with 7 days for the lean rat islets. Culture in high glucose erased the phenotype differences in glucokinase Km that were observed in 12.5 mM glucose cultured islets.

CONCLUSIONS

Differences in fa/fa rat islet glucokinase were observed only at moderate, near physiological glucose conditions. Glucokinase activity was similarly affected by low or high glucose in the two phenotypes, although differences in insulin secretion pattern were still detected, leading to the conclusion that factors other than glucokinase contribute to altered insulin secretion in the fa/fa rat. Further study of the glucose desensitization phenomenon in fa/fa rat islets might help unravel the factors that increase susceptibility to development of diabetes mellitus in some phenotypes.

摘要

目的

在正常B细胞中,葡萄糖激酶活性受葡萄糖调节。我们推测,与瘦大鼠相比,长期暴露于低或高葡萄糖水平会对fa/fa大鼠胰岛中的葡萄糖激酶功能和胰岛素分泌产生不同的调节作用。

对象、设计和测量:从瘦大鼠和fa/fa大鼠(8 - 12周龄)分离的胰岛在补充了低(3.3 mM)、中等(12.5 mM)或超生理(25.0 mM)葡萄糖的培养基中培养1 - 7天。通过酶测定和动力学分析评估每组胰岛中己糖激酶、葡萄糖激酶对葡萄糖的敏感性,以及通过放射免疫测定评估胰岛素反应。

结果

在12.5 mM葡萄糖中培养1 - 7天的fa/fa大鼠胰岛,其胰岛素反应的半数有效浓度(EC50)和葡萄糖激酶对葡萄糖的米氏常数(Km)均向左偏移。在所有测试条件下,fa/fa大鼠胰岛的葡萄糖激酶最大反应速度(Vmax)均较低,从而限制了胰岛素分泌的潜在增加。当在3.3 mM葡萄糖中培养1 - 7天时,fa/fa大鼠胰岛对葡萄糖的反应性保持更长时间,且葡萄糖的估计EC50实际上下降。然而,在低葡萄糖培养条件下,两种表型的胰岛中葡萄糖激酶对葡萄糖的Km均增加了三倍。在25.0 mM葡萄糖中培养的瘦大鼠和fa/fa大鼠胰岛对基础葡萄糖浓度表现出反常的高胰岛素分泌,并且对高浓度葡萄糖刺激脱敏。fa/fa大鼠的胰岛更容易脱敏,在25.0 mM葡萄糖中培养3天时就有显著影响,而瘦大鼠胰岛则需要7天。在高葡萄糖中培养消除了在12.5 mM葡萄糖培养的胰岛中观察到的葡萄糖激酶Km的表型差异。

结论

仅在中等、接近生理葡萄糖条件下观察到fa/fa大鼠胰岛葡萄糖激酶的差异。两种表型中,低或高葡萄糖对葡萄糖激酶活性的影响相似,尽管仍检测到胰岛素分泌模式的差异,这表明除葡萄糖激酶外的其他因素导致了fa/fa大鼠胰岛素分泌的改变。对fa/fa大鼠胰岛中葡萄糖脱敏现象的进一步研究可能有助于揭示在某些表型中增加糖尿病易感性的因素。

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