An integrated view of beta-cell dysfunction in type-II diabetes

被引:0
作者
Poitout, V
Robertson, RP
机构
来源
ANNUAL REVIEW OF MEDICINE | 1996年 / 47卷
关键词
non-insulin-dependent diabetes; insulin secretion; pancreatic beta-cell;
D O I
暂无
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
Type-II (non-insulin-dependent) diabetes mellitus (NIDDM) is a heterogeneous disease resulting from insulin resistance and beta-cell dysfunction. beta-Cell dysfunction in Type-II diabetes is characterized by a specific lack of first-phase glucose-induced insulin secretion. This defect is readily reversible upon normalization of blood glucose levels. Chronic hyperglycemia itself is harmful to the beta-cell and affects both insulin biosynthesis and exocytosis. No unique intracellular defect has been demonstrated to be responsible for all common forms of the disease. However, mutations of the glucokinase gene have been identified in maturity onset diabetes in the young, a particular form of NIDDM.
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页码:69 / 83
页数:15
相关论文
共 42 条
[1]   INCREASED SECRETORY DEMAND RATHER THAN A DEFECT IN THE PROINSULIN CONVERSION MECHANISM CAUSES HYPERPROINSULINEMIA IN A GLUCOSE-INFUSION RAT MODEL OF NON-INSULIN-DEPENDENT DIABETES-MELLITUS [J].
ALARCON, C ;
LEAHY, JL ;
SCHUPPIN, GT ;
RHODES, CJ .
JOURNAL OF CLINICAL INVESTIGATION, 1995, 95 (03) :1032-1039
[2]   GLUCOSE INDUCES CLOSURE OF SINGLE POTASSIUM CHANNELS IN ISOLATED RAT PANCREATIC BETA-CELLS [J].
ASHCROFT, FM ;
HARRISON, DE ;
ASHCROFT, SJH .
NATURE, 1984, 312 (5993) :446-448
[3]   PROTEIN-PHOSPHORYLATION IN THE REGULATION OF INSULIN-SECRETION AND BIOSYNTHESIS [J].
ASHCROFT, SJH ;
HUGHES, SJ .
BIOCHEMICAL SOCIETY TRANSACTIONS, 1990, 18 (01) :116-118
[4]   INSULIN SECRETORY RESPONSE TO SECRETAGOGUES BY PERIFUSED ISLETS FROM CHRONICALLY GLUCOSE-INFUSED RATS [J].
BEDOYA, FJ ;
JEANRENAUD, B .
DIABETES, 1991, 40 (01) :15-19
[5]   RELATIONSHIPS BETWEEN FASTING PLASMA GLUCOSE LEVELS AND INSULIN-SECRETION DURING INTRAVENOUS GLUCOSE-TOLERANCE TESTS [J].
BRUNZELL, JD ;
ROBERTSON, RP ;
LERNER, RL ;
HAZZARD, WR ;
ENSINCK, JW ;
BIERMAN, EL ;
PORTE, D .
JOURNAL OF CLINICAL ENDOCRINOLOGY & METABOLISM, 1976, 42 (02) :222-229
[6]   INSULIN SECRETORY ABNORMALITIES IN SUBJECTS WITH HYPERGLYCEMIA DUE TO GLUCOKINASE MUTATIONS [J].
BYRNE, MM ;
STURIS, J ;
CLEMENT, K ;
VIONNET, N ;
PUEYO, ME ;
STOFFEL, L ;
TAKEDA, J ;
PASSA, P ;
COHEN, D ;
BELL, GI ;
VELHO, G ;
FROGUEL, P ;
POLONSKY, KS .
JOURNAL OF CLINICAL INVESTIGATION, 1994, 93 (03) :1120-1130
[7]   ABNORMAL SENSITIVITY TO GLUCOSE OF HUMAN ISLETS CULTURED IN A HIGH GLUCOSE MEDIUM - PARTIAL REVERSIBILITY AFTER AN ADDITIONAL CULTURE IN A NORMAL GLUCOSE MEDIUM [J].
DAVALLI, AM ;
RICORDI, C ;
SOCCI, C ;
BRAGHI, S ;
BERTUZZI, F ;
FATTOR, B ;
DICARLO, V ;
PONTIROLI, AE ;
POZZA, G .
JOURNAL OF CLINICAL ENDOCRINOLOGY & METABOLISM, 1991, 72 (01) :202-208
[8]  
ELZIRIK DL, 1992, J CLIN INVEST, V90, P1263
[9]   FAMILIAL HYPERGLYCEMIA DUE TO MUTATIONS IN GLUCOKINASE - DEFINITION OF A SUBTYPE OF DIABETES-MELLITUS [J].
FROGUEL, P ;
ZOUALI, H ;
VIONNET, N ;
VELHO, G ;
VAXILLAIRE, M ;
SUN, F ;
LESAGE, S ;
STOFFEL, M ;
TAKEDA, J ;
PASSA, P ;
PERMUTT, MA ;
BECKMANN, JS ;
BELL, GI ;
COHEN, D .
NEW ENGLAND JOURNAL OF MEDICINE, 1993, 328 (10) :697-702
[10]   EVIDENCE THAT GLUCOSE CAN CONTROL INSULIN RELEASE INDEPENDENTLY FROM ITS ACTION ON ATP-SENSITIVE K+ CHANNELS IN MOUSE B-CELLS [J].
GEMBAL, M ;
GILON, P ;
HENQUIN, JC .
JOURNAL OF CLINICAL INVESTIGATION, 1992, 89 (04) :1288-1295
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