Diverse signaling pathways in the cellular actions of insulin

被引：135

作者：

Saltiel, AR

机构：

来源：

AMERICAN JOURNAL OF PHYSIOLOGY-ENDOCRINOLOGY AND METABOLISM | 1996年 / 270卷 / 03期

关键词：

protein phosphorylation; intermediary metabolism; protein phosphatase; src homology domain;

D O I：

10.1152/ajpendo.1996.270.3.E375

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

Insulin is one of the most important regulators of glucose and Lipid homeostasis. Many of its cellular actions are mediated by changes in protein phosphorylation. The consequences of these phosphorylation events extend from a series of different short-term metabolic actions to longer-term effects of the hormone on cellular growth and differentiation. Although the insulin receptor itself is a tyrosine kinase that is activated upon hormone binding, the ensuing changes in phosphorylation occur predominantly on serine and threonine residues. Moreover, insulin can simultaneously stimulate the phosphorylation of some proteins and the dephosphorylation of others. These paradoxical effects of insulin suggest that separate signal transduction pathways may emanate from the receptor itself to produce the pleiotropic actions of the hormone.

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页码：E375 / E385

页数：11

相关论文

共 97 条

[1] REQUIREMENT FOR INTEGRATION OF SIGNALS FROM 2 DISTINCT PHOSPHORYLATION PATHWAYS FOR ACTIVATION OF MAP KINASE [J].

ANDERSON, NG ;

MALLER, JL ;

TONKS, NK ;

STURGILL, TW .

NATURE, 1990, 343 (6259) :651-653

[2] ALTERNATIVE PATHWAY OF INSULIN SIGNALING IN MICE WITH TARGETED DISRUPTION OF THE IRS-1 GENE [J].

ARAKI, E ;

LIPES, MA ;

PATTI, ME ;

BRUNING, JC ;

HAAG, B ;

JOHNSON, RS ;

KAHN, CR .

NATURE, 1994, 372 (6502) :186-190

[3]

AVRUCH J, 1982, FED PROC, V41, P2629

[4] THE NATURE OF THE DECREASED ACTIVITY OF GLYCOGEN-SYNTHASE PHOSPHATASE IN THE LIVER OF THE ADRENALECTOMIZED STARVED RAT [J].

BOLLEN, M ;

DOPERE, F ;

GORIS, J ;

MERLEVEDE, W ;

STALMANS, W .

EUROPEAN JOURNAL OF BIOCHEMISTRY, 1984, 144 (01) :57-63

[5] DIABETES-INDUCED FUNCTIONAL AND STRUCTURAL-CHANGES IN INSULIN-RECEPTORS FROM RAT SKELETAL-MUSCLE [J].

BURANT, CF ;

TREUTELAAR, MK ;

BUSE, MG .

JOURNAL OF CLINICAL INVESTIGATION, 1986, 77 (01) :260-270

[6]

BURGESS JW, 1992, J BIOL CHEM, V267, P10077

[7] ONCOGENES AND SIGNAL TRANSDUCTION [J].

CANTLEY, LC ;

AUGER, KR ;

CARPENTER, C ;

DUCKWORTH, B ;

GRAZIANI, A ;

KAPELLER, R ;

SOLTOFF, S .

CELL, 1991, 64 (02) :281-302

[8] INSULIN-RECEPTOR KINASE IN HUMAN SKELETAL-MUSCLE FROM OBESE SUBJECTS WITH AND WITHOUT NONINSULIN DEPENDENT DIABETES [J].

CARO, JF ;

SINHA, MK ;

RAJU, SM ;

ITTOOP, O ;

PORIES, WJ ;

FLICKINGER, EG ;

MEELHEIM, D ;

DOHM, GL .

JOURNAL OF CLINICAL INVESTIGATION, 1987, 79 (05) :1330-1337

[9] ACTIVATION OF PROTEIN-KINASE C-ALPHA INHIBITS INSULIN-STIMULATED TYROSINE PHOSPHORYLATION OF INSULIN-RECEPTOR SUBSTRATE-1 [J].

CHIN, JE ;

LIU, F ;

ROTH, RA .

MOLECULAR ENDOCRINOLOGY, 1994, 8 (01) :51-58

[10] MICROINJECTION OF A PROTEIN-TYROSINE-PHOSPHATASE INHIBITS INSULIN ACTION IN XENOPUS OOCYTES [J].

CICIRELLI, MF ;

TONKS, NK ;

DILTZ, CD ;

WEIEL, JE ;

FISCHER, EH ;

KREBS, EG .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1990, 87 (14) :5514-5518

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