Cell-generated nitric oxide inactivates rat hepatocyte mitochondria in vitro but reacts with hemoglobin in vivo

被引：31

作者：

Fisch, C

Robin, MA

Letteron, P

Fromenty, B

Berson, A

Renault, S

Chachaty, C

Pessayre, D

机构：

[1] HOP BEAUJON, INSERM, U24, F-92118 CLICHY, FRANCE

[2] HOP BEAUJON, CTR RECH PHYSIOPATHOL HEPAT, ASSOC CLAUDE BERNARD, F-92118 CLICHY, FRANCE

来源：

GASTROENTEROLOGY | 1996年 / 110卷 / 01期

关键词：

D O I：

10.1053/gast.1996.v110.pm8536859

中图分类号：

R57 [消化系及腹部疾病];

学科分类号：

摘要：

Background & Aims: Nitric oxide forms inactive iron-nitrosyl complexes within hepatic mitochondria in vitro, However, when formed in vivo, NO might react instead with hemoglobin. The aim of this study was to compare the effects of cell-derived NO on rat hepatocyte mitochondria in vitro and in vivo. Methods: First, hepatocytes were cultured in vitro for 24 hours under a porous membrane supporting macrophages that were stimulated by endotoxin. Second, hepatic macrophage hyperplasia was induced in vivo by preadministration of killed Corynebacterium parvum; 7 days later, rats received endotoxin and were killed after 6 hours, Third, mitochondria were exposed to sodium nitroprusside in vitro, washed, mixed with blood, and recovered. Results: Iron-nitrosyl complexes and hepatocyte mitochondrial dysfunction were observed in the in vitro model and prevented by an NO synthase inhibitor. In the in vivo model, however, despite a 130-fold increase in plasma nitrate levels and formation of hemoglobin-NO complexes in blood, no iron-nitrosyl complex was detected in hepatic mitochondria, and hepatic mitochondrial function was not impaired. In the third model, mitochondria lost preformed iron-nitrosyl complexes when exposed to blood. Conclusions: Although NO reacts with hepatocyte mitochondria in vitro, in vivo it reacts with sinusoidal hemoglobin without detectable impairment of hepatic mitochondrial function.

引用

页码：210 / 220

页数：11

共 31 条

[21] EFFECTS OF COLD ENVIRONMENT ON MITOCHONDRIAL GENOME EXPRESSION IN THE RAT - EVIDENCE FOR A TISSUE-SPECIFIC INCREASE IN THE LIVER, INDEPENDENT OF CHANGES IN MITOCHONDRIAL GENE ABUNDANCE
MARTIN, I
VINAS, O
MAMPEL, T
IGLESIAS, R
VILLARROYA, F
[J]. BIOCHEMICAL JOURNAL, 1993, 296 : 231 - 234
[22] ACTION OF BACTERIAL LIPOPOLYSACCHARIDE ON THE RESPIRATION OF MOUSE-LIVER MITOCHONDRIA
MCGIVNEY, A
BRADLEY, SG
[J]. INFECTION AND IMMUNITY, 1980, 27 (01) : 102 - 106
[23] MONCADA S, 1991, PHARMACOL REV, V43, P109
[24] Rickwood D., 1987, Mitochondria: a pratical approach, P1
[25] MEASUREMENT OF PROTEIN USING BICINCHONINIC ACID
SMITH, PK
KROHN, RI
HERMANSON, GT
MALLIA, AK
GARTNER, FH
PROVENZANO, MD
FUJIMOTO, EK
GOEKE, NM
OLSON, BJ
KLENK, DC
[J]. ANALYTICAL BIOCHEMISTRY, 1985, 150 (01) : 76 - 85
[26] EFFECT OF EXOGENOUS AND ENDOGENOUS NITRIC-OXIDE ON MITOCHONDRIAL RESPIRATION OF RAT HEPATOCYTES
STADLER, J
BILLIAR, TR
CURRAN, RD
STUEHR, DJ
OCHOA, JB
SIMMONS, RL
[J]. AMERICAN JOURNAL OF PHYSIOLOGY, 1991, 260 (05): : C910 - C916
[27] NONHEME IRON NITROSYL COMPLEX-FORMATION IN RAT HEPATOCYTES - DETECTION BY ELECTRON-PARAMAGNETIC RESONANCE SPECTROSCOPY
STADLER, J
BERGONIA, HA
DISILVIO, M
SWEETLAND, MA
BILLIAR, TR
SIMMONS, RL
LANCASTER, JR
[J]. ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS, 1993, 302 (01) : 4 - 11
[28] BIOCHEMISTRY OF NITRIC-OXIDE AND ITS REDOX-ACTIVATED FORMS
STAMLER, JS
SINGEL, DJ
LOSCALZO, J
[J]. SCIENCE, 1992, 258 (5090) : 1898 - 1902
[29] TRACEY WR, 1995, J PHARMACOL EXP THER, V272, P1011
[30] TUMOR-NECROSIS-FACTOR-ALPHA PRODUCES HEPATOCELLULAR DYSFUNCTION DESPITE NORMAL CARDIAC-OUTPUT AND HEPATIC MICROCIRCULATION
WANG, P
AYALA, A
BA, ZF
ZHOU, M
PERRIN, MM
CHAUDRY, IH
[J]. AMERICAN JOURNAL OF PHYSIOLOGY, 1993, 265 (01): : G126 - G132

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