ROLE OF IRON AND SUPEROXIDE IN MEDIATING HYDROGEN-PEROXIDE INJURY TO CULTURED RAT GASTRIC CELLS

被引：25

作者：

HIRAISHI, H

TERANO, A

RAZANDI, M

SUGIMOTO, T

HARADA, T

IVEY, KJ

机构：

[1] VET AFFAIRS MED CTR, DEPT MED, LONG BEACH, CA USA

[2] UNIV CALIF IRVINE, IRVINE, CA 92717 USA

[3] UNIV TOKYO, FAC MED, DEPT INTERNAL MED 2, TOKYO 113, JAPAN

[4] DOKKYO UNIV, SCH MED, DEPT INTERNAL MED 2, MIBU, TOCHIGI 32102, JAPAN

来源：

GASTROENTEROLOGY | 1993年 / 104卷 / 03期

关键词：

D O I：

10.1016/0016-5085(93)91013-8

中图分类号：

R57 [消化系及腹部疾病];

学科分类号：

摘要：

Background: Gastric epithelium is exposed to toxic, reactive oxygen species generated within the lumen. The present study examined the role of cellular iron and superoxide (O2-) in mediating hydrogen peroxide (H2O2)-induced damage to cultured gastric mucosal cells. Methods: H2O2 was generated by glucose oxidase acting on b-d(+)glucose. Cytotoxicity was assessed by 51Cr release from prelabeled cells. Results: Deferoxamine (a chelator of Fe3+) prevented injury induced by H2O2, whether present before or during H2O2 production. In contrast, whereas the presence of phenanthroline (a chelator of Fe2+) during the cytotoxicity assay prevented damage, prior treatment with the agent did not; this suggested that cellular Fe3+ reduced to Fe2+ upon exposure to H2O2 is responsible for damage. Neither extracellular superoxide dismutase nor inhibitors of xanthine oxidase (a possible source of cellular O2- production) protected against H2O2. Further, protection by iron chelators was not associated with modulation of endogenous antioxidants. Conclusions: Deferoxamine and phenanthroline protect cells from H2O2 by chelating stored iron (Fe3+) or reduced iron (Fe2+), respectively. Reduction of cellular Fe3+ appears to be a prerequisite for mediation of damage, but this reduction is independent of extracellular O2- or cellular xanthine oxidase-derived O2-. © 1993.

引用

页码：780 / 788

页数：9

共 50 条

[41] THE ROLE OF THE SUPEROXIDE RADICAL IN THE OSO4-CATALYZED DECOMPOSITION OF HYDROGEN-PEROXIDE
NAGY, L
GALBACS, ZM
CSANYI, LJ
HORVATH, L
MAGYAR KEMIAI FOLYOIRAT, 1983, 89 (04): : 162 - 166
[42] THE ROLE OF THE SUPEROXIDE RADICAL IN THE OSO4-CATALYZED DECOMPOSITION OF HYDROGEN-PEROXIDE
NAGY, L
GALBACS, ZM
CSANYI, LJ
JOURNAL OF THE CHEMICAL SOCIETY-DALTON TRANSACTIONS, 1982, (05): : 859 - 863
[43] DIFFERENTIAL RESPONSIVENESS OF CULTURED RAT MYOCARDIAL-CELLS TO ISOPRENALINE AND PHENYLEPHRINE AFTER INCUBATION WITH HYDROGEN-PEROXIDE
HEYDECK, D
WALLUKAT, G
PAPIES, B
SCHIMKE, I
FRESENIUS JOURNAL OF ANALYTICAL CHEMISTRY, 1992, 343 (01): : 71 - 72
[44] A STARRING ROLE FOR HYDROGEN-PEROXIDE
HAIRSTON, D
CHEMICAL ENGINEERING, 1995, 102 (07) : 67 - +
[45] NITRIC-OXIDE ENHANCES CYTOTOXICITY OF CULTURED RABBIT GASTRIC-MUCOSAL CELLS INDUCED BY HYDROGEN-PEROXIDE
HATA, Y
OTA, S
TERANO, A
RAZANDI, M
IVEY, KJ
GASTROENTEROLOGY, 1995, 108 (04) : A110 - A110
[46] EFFECT OF THIOCYANATE AND HYDROGEN-PEROXIDE IN CULTURED PRODUCTS
ZALL, RR
CHEN, JH
DZUREC, DJ
MILCHWISSENSCHAFT-MILK SCIENCE INTERNATIONAL, 1983, 38 (05): : 264 - 266
[47] CARCINOGENIC DNA-DAMAGE IS INDUCED IN CULTURED GASTRIC EPITHELIAL-CELLS EXPOSED TO HYDROGEN-PEROXIDE AND MONOCHLORAMINE
SUZUKI, M
MORI, M
MIURA, S
ISHII, H
GASTROENTEROLOGY, 1995, 108 (04) : A229 - A229
[48] ALBUMIN DECREASES HYDROGEN-PEROXIDE AND REPERFUSION INJURY IN ISOLATED RAT HEARTS
BROWN, JM
BEEHLER, CJ
BERGER, EM
GROSSO, MA
WHITMAN, GJ
TERADA, LS
LEFF, JA
HARKEN, AH
REPINE, JE
INFLAMMATION, 1989, 13 (05) : 583 - 589
[49] REPERFUSION INJURY AND EXHALED HYDROGEN-PEROXIDE
WILSON, WC
LABORDE, PR
BENUMOF, JL
TAYLOR, R
SWETLAND, JF
ANESTHESIA AND ANALGESIA, 1993, 77 (05): : 963 - 970
[50] HYDROGEN-PEROXIDE MEDIATES REPERFUSION INJURY IN THE ISOLATED RAT-HEART
BROWN, JM
TERADA, LS
GROSSO, MA
WHITMAN, GJ
VELASCO, SE
PATT, A
HARKEN, AH
REPINE, JE
MOLECULAR AND CELLULAR BIOCHEMISTRY, 1988, 84 (02) : 173 - 175

← 1 2 3 4 5 →