L-ARGININE STIMULATES CYCLIC GUANOSINE 3',5'-MONOPHOSPHATE FORMATION IN RAT ISLETS OF LANGERHANS AND RINM5F INSULINOMA CELLS - EVIDENCE FOR L-ARGININE-NITRIC OXIDE SYNTHASE

被引：128

作者：

LAYCHOCK, SG ^{[1
]}

MODICA, ME ^{[1
]}

CAVANAUGH, CT ^{[1
]}

机构：

[1] SUNY BUFFALO, SCH MED & BIOMED SC, DEPT PHARMACOL & THERAPEUT, BUFFALO, NY 14214 USA

来源：

ENDOCRINOLOGY | 1991年 / 129卷 / 06期

关键词：

D O I：

10.1210/endo-129-6-3043

中图分类号：

R5 [内科学];

学科分类号：

1002 ; 100201 ;

摘要：

L-Arginine (L-Arg) is metabolized by nitric oxide synthase to the reactive intermediate nitric oxide. Since nitric oxide stimulates guanylyl cyclase and cGMP synthesis, L-Arg effects on cGMP accumulation in isolated pancreatic islets of the rat and RINm5F insulinoma cells were determined. Both L-Arg and glucose stimulation increased islet cGMP levels, and glucose potentiated the response to L-Arg alone. A competitive inhibitor of L-Arg metabolism to nitric oxide, N(G)-monomethyl-L-arginine, reduced glucose- and L-Arg-stimulated insulin release and glucose-induced increases in cGMP; however, basal insulin release was slightly increased. D-Arg and L-ornithine did not affect islet cGMP levels, although insulin release was stimulated. RINm5F cell cGMP levels and insulin release increased in response to L-Arg in a concentration- and time-related manner, whereas glucose and L-histidine were without effect. 8-Bromo-cGMP also slightly increased RINm5F cell insulin release. Sodium nitroprusside as a source of nitric oxide increased RINm5F cell cGMP production. Methylene blue and LY83583, inhibitors of soluble guanylyl cyclase activation, reduced RINm5F cell cGMP levels in the presence and absence of L-Arg; LY83583 also reduced glucose-stimulated cGMP levels in islets. Insulin release by glucose and L-Arg was also inhibited by methylene blue and LY83583 in islets. We conclude that glucose and L-Arg stimulate guanylyl cyclase activity and cGMP formation in beta-cells at least in part through metabolism to the reactive intermediate nitric oxide. However, neither nitric oxide nor cGMP synthesis is obligatory for insulin secretion.

引用

页码：3043 / 3052

页数：10

共 58 条

[31] STIMULUS-SECRETION COUPLING OF ARGININE-INDUCED INSULIN RELEASE - METABOLISM OF L-ARGININE AND L-ORNITHINE IN TUMORAL ISLET CELLS [J].

MALAISSE, WJ ;

BLACHIER, F ;

MOURTADA, A ;

CAMARA, J ;

ALBOR, A ;

VALVERDE, I ;

SENER, A .

MOLECULAR AND CELLULAR ENDOCRINOLOGY, 1989, 67 (01) :81-91

[32] STIMULUS-SECRETION COUPLING OF ARGININE-INDUCED INSULIN RELEASE - METABOLISM OF L-ARGININE AND L-ORNITHINE IN PANCREATIC-ISLETS [J].

MALAISSE, WJ ;

BLACHIER, F ;

MOURTADA, A ;

CAMARA, J ;

ALBOR, A ;

VALVERDE, I ;

SENER, A .

BIOCHIMICA ET BIOPHYSICA ACTA, 1989, 1013 (02) :133-143

[33]

MALTA E, 1988, N-S ARCH PHARMACOL, V337, P459

[34] MACROPHAGE OXIDATION OF L-ARGININE TO NITRITE AND NITRATE - NITRIC-OXIDE IS AN INTERMEDIATE [J].

MARLETTA, MA ;

YOON, PS ;

IYENGAR, R ;

LEAF, CD ;

WISHNOK, JS .

BIOCHEMISTRY, 1988, 27 (24) :8706-8711

[35] BIOSYNTHESIS OF ENDOTHELIUM-DERIVED RELAXING FACTOR - A CYTOSOLIC ENZYME IN PORCINE AORTIC ENDOTHELIAL-CELLS CA-2+-DEPENDENTLY CONVERTS L-ARGININE INTO AN ACTIVATOR OF SOLUBLE GUANYLYL CYCLASE [J].

MAYER, B ;

SCHMIDT, K ;

HUMBERT, P ;

BOHME, E .

BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS, 1989, 164 (02) :678-685

[36] SELECTIVE BLOCKADE OF RECEPTOR-MEDIATED CYCLIC-GMP FORMATION IN NIE-115 NEUROBLASTOMA-CELLS BY AN INHIBITOR OF NITRIC-OXIDE SYNTHESIS [J].

MCKINNEY, M ;

BOLDEN, C ;

SMITH, C ;

JOHNSON, A ;

RICHELSON, E .

EUROPEAN JOURNAL OF PHARMACOLOGY, 1990, 178 (01) :139-140

[37]

MITTAL CK, 1977, J CYCLIC NUCL PROT, V3, P381

[38] BIOSYNTHESIS OF NITRIC-OXIDE FROM L-ARGININE - A PATHWAY FOR THE REGULATION OF CELL-FUNCTION AND COMMUNICATION [J].

MONCADA, S ;

PALMER, RMJ ;

HIGGS, EA .

BIOCHEMICAL PHARMACOLOGY, 1989, 38 (11) :1709-1715

[39] DIETARY ARGININE, INSULIN-SECRETION, GLUCOSE-TOLERANCE AND LIVER LIPIDS DURING REPLETION OF PROTEIN-DEPLETED RATS [J].

MULLOY, AL ;

KARI, FW ;

VISEK, WJ .

HORMONE AND METABOLIC RESEARCH, 1982, 14 (09) :471-475

[40]

MULSCH A, 1988, J PHARMACOL EXP THER, V247, P283

← 1 2 3 4 5 6 →