METABOLIC, IONIC, AND SECRETORY RESPONSE TO D-GLUCOSE IN ISLETS FROM RATS WITH ACQUIRED OR INHERITED NON-INSULIN-DEPENDENT DIABETES

被引：40

作者：

GIROIX, MH ^{[1
]}

SENER, A ^{[1
]}

BAILBE, D ^{[1
]}

LECLERCQMEYER, V ^{[1
]}

PORTHA, B ^{[1
]}

MALAISSE, WJ ^{[1
]}

机构：

[1] FREE UNIV BRUSSELS,EXPTL MED LAB,B-1070 BRUSSELS,BELGIUM

来源：

BIOCHEMICAL MEDICINE AND METABOLIC BIOLOGY | 1993年 / 50卷 / 03期

关键词：

D O I：

10.1006/bmmb.1993.1072

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

The metabolic, ionic, and secretory response to D-glucose was investigated in islets of adult rats either injected with streptozotocin during the neonatal period (STZ rats) or presenting with inherited diabetes (GK rats). At a high concentration of D-glucose (16.7 mM), the ATP/ADP ratio was lower in islets from STZ and GK than control rats. This coincided with an impaired response of perifused islets to a rise in o-glucose concentration in terms of stimulation of insulin release, suppression of effluent radioactivity from islets prelabeled with [2-3H]adenosine, reduction in 86Rb efflux, and induction of a phosphate flush in islets prelabeled with 32Pi. The ratio in either D-[5-3H]glucose utilization or D-[2-14C]glucose oxidation at high/low hexose concentration, as well as the paired ratio between D-[2-14C]glucose oxidation and D-[5-3H]glucose utilization in islets incubated at a high concentration of the hexose, was also lower in STZ and GK rats than in control rats. Such was not the case, however, from the oxidation of [2-14C]pyruvate. Instead, the latter 2-keto acid, when tested at a 5.0 mM concentration, improved more efficiently the overall oxidative response of the islets to a rise in D-glucose concentration in STZ and GK rats than in control animals. It is proposed, therefore, that in both STZ and GK rats, the B-cell secretory defect is primarily attributable to an anomaly in oxidative glycolysis. In islets exposed to a high concentration of D-glucose, this metabolic deficiency results in impaired ATP generation, altered closing of ATP-responsive K+ channels, and, hence, diminished insulin output. © 1993 Academic Press. All rights reserved.

引用

页码：301 / 321

页数：21

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