Regulation of inducible nitric oxide synthase expression in β cells by environmental factors:: heavy metals

被引：24

作者：

Eckhardt, W ^{[1
]}

Bellmann, K ^{[1
]}

Kolb, H ^{[1
]}

机构：

[1] Univ Dusseldorf, Diabet Res Inst, D-40225 Dusseldorf, Germany

来源：

BIOCHEMICAL JOURNAL | 1999年 / 338卷

关键词：

L-citrulline; insulinoma cells; lead; mercury; nitric oxide;

D O I：

10.1042/0264-6021:3380695

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 expression of inducible NO synthase (iNOS) in pancreatic islet beta cells modulates endocrine cell functions and, at very high levels of NO production causes beta-cell death. We tested the hypothesis that environmental factors such as heavy-metal salts modulate iNOS expression in beta cells. A rat beta-cell line (insulinoma RINm5F) was cultured in the presence of low-dose interleukin (IL)-1 beta for suboptimal induction of iNOS. PbCl2 (0.1-10 mu M) dose-dependently increased NO (measured as nitrite) formation (P < 0.001). In contrast, HgCl2 suppressed nitrite production (0.1-10 mu M, P < 0.05). Measurements of iNOS activity by determining citrulline levels confirmed the potentiating effect of PbCl2 (P < 0.05). There was a narrow time window of heavy-metal actions, ranging from -24 h (Hg2+) or -3 h (Pb2+) to +2 h, relative to the addition of IL-1By semi-quantitative reverse transcriptase-PCR, enhanced levels of iNOS mRNA were found in the presence of Pb2+ (P < 0.05) and decreased levels in the presence of Hg2+. The amount of iNOS protein as determined by Western blotting was increased in the presence of Pb2+. We conclude that Pb2+ upregulates and Hg2+ suppresses iNOS gene expression at the level of transcription, probably by acting on the signalling pathway. These observations may have important implications for understanding pathological effects of environmental factors on endocrine organ functions.beta.

引用

页码：695 / 700

页数：6

共 59 条

[1] ALBINA JE, 1991, J IMMUNOL, V147, P144
[2] EFFECT OF LEAD ACETATE ON NITRITE PRODUCTION BY MURINE BRAIN ENDOTHELIAL-CELL CULTURES
BLAZKA, ME
HARRY, GJ
LUSTER, MI
[J]. TOXICOLOGY AND APPLIED PHARMACOLOGY, 1994, 126 (01) : 191 - 194
[3] MACROPHAGE DEACTIVATION BY INTERLEUKIN-10
BOGDAN, C
VODOVOTZ, Y
NATHAN, C
[J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1991, 174 (06) : 1549 - 1555
[4] PHOSPHOLIPID-METABOLISM IN NEURAL MICROVASCULAR ENDOTHELIAL-CELLS AFTER EXPOSURE TO LEAD IN-VITRO
BRESSLER, J
FORMAN, S
GOLDSTEIN, GW
[J]. TOXICOLOGY AND APPLIED PHARMACOLOGY, 1994, 126 (02) : 352 - 360
[5] INDUCTION OF NITRIC-OXIDE SYNTHASE MESSENGER-RNA EXPRESSION - SUPPRESSION BY EXOGENOUS NITRIC-OXIDE
COLASANTI, M
PERSICHINI, T
MENEGAZZI, M
MARIOTTO, S
GIORDANO, E
CALDARERA, CM
SOGOS, V
LAURO, GM
SUZUKI, H
[J]. JOURNAL OF BIOLOGICAL CHEMISTRY, 1995, 270 (45) : 26731 - 26733
[6] INTERLEUKIN-1 IS POTENT MODULATOR OF INSULIN-SECRETION FROM ISOLATED RAT ISLETS OF LANGERHANS
COMENS, PG
WOLF, BA
UNANUE, ER
LACY, PE
MCDANIEL, ML
[J]. DIABETES, 1987, 36 (08) : 963 - 970
[7] NITRIC-OXIDE AND CYCLIC-GMP FORMATION INDUCED BY INTERLEUKIN-1-BETA IN ISLETS OF LANGERHANS - EVIDENCE FOR AN EFFECTOR ROLE OF NITRIC-OXIDE IN ISLET DYSFUNCTION
CORBETT, JA
WANG, JL
HUGHES, JH
WOLF, BA
SWEETLAND, MA
LANCASTER, JR
MCDANIEL, ML
[J]. BIOCHEMICAL JOURNAL, 1992, 287 : 229 - 235
[8] DOES NITRIC-OXIDE MEDIATE AUTOIMMUNE DESTRUCTION OF BETA-CELLS - POSSIBLE THERAPEUTIC INTERVENTIONS IN IDDM
CORBETT, JA
MCDANIEL, ML
[J]. DIABETES, 1992, 41 (08) : 897 - 903
[9] INTRAISLET RELEASE OF INTERLEUKIN-1 INHIBITS BETA-CELL FUNCTION BY INDUCING BETA-CELL EXPRESSION OF INDUCIBLE NITRIC-OXIDE SYNTHASE
CORBETT, JA
MCDANIEL, ML
[J]. JOURNAL OF EXPERIMENTAL MEDICINE, 1995, 181 (02) : 559 - 568
[10] A 1-HOUR PULSE WITH IL-1-BETA INDUCES FORMATION OF NITRIC-OXIDE AND INHIBITS INSULIN-SECRETION BY RAT ISLETS OF LANGERHANS - EVIDENCE FOR A TYROSINE KINASE SIGNALING MECHANISM
CORBETT, JA
SWEETLAND, MA
LANCASTER, JR
MCDANIEL, ML
[J]. FASEB JOURNAL, 1993, 7 (02) : 369 - 374

← 1 2 3 4 5 6 →