Continuous intravenous infusion of deferoxamine reduces mortality by paraquat in vitamin E-deficient rats.

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Standard

Continuous intravenous infusion of deferoxamine reduces mortality by paraquat in vitamin E-deficient rats. / B.S., van Asbeck; F.C., Hillen; C.M., Boonen Harrie; Y., de Jong; J.A., Dormans; N.A., van der Wal; J.J., Marx; B., Sangster.

I: The American review of respiratory disease, Bind 139, Nr. 3, 1989, s. 769-773.

Publikation: Bidrag til tidsskriftTidsskriftartikelForskningfagfællebedømt

Harvard

B.S., VA, F.C., H, C.M., BH, Y., DJ, J.A., D, N.A., VDW, J.J., M & B., S 1989, 'Continuous intravenous infusion of deferoxamine reduces mortality by paraquat in vitamin E-deficient rats.', The American review of respiratory disease, bind 139, nr. 3, s. 769-773.

APA

B.S., V. A., F.C., H., C.M., B. H., Y., D. J., J.A., D., N.A., V. D. W., J.J., M., & B., S. (1989). Continuous intravenous infusion of deferoxamine reduces mortality by paraquat in vitamin E-deficient rats. The American review of respiratory disease, 139(3), 769-773.

Vancouver

B.S. VA, F.C. H, C.M. BH, Y. DJ, J.A. D, N.A. VDW o.a. Continuous intravenous infusion of deferoxamine reduces mortality by paraquat in vitamin E-deficient rats. The American review of respiratory disease. 1989;139(3):769-773.

Author

B.S., van Asbeck ; F.C., Hillen ; C.M., Boonen Harrie ; Y., de Jong ; J.A., Dormans ; N.A., van der Wal ; J.J., Marx ; B., Sangster. / Continuous intravenous infusion of deferoxamine reduces mortality by paraquat in vitamin E-deficient rats. I: The American review of respiratory disease. 1989 ; Bind 139, Nr. 3. s. 769-773.

Bibtex

@article{425059d0f9e611de825d000ea68e967b,
title = "Continuous intravenous infusion of deferoxamine reduces mortality by paraquat in vitamin E-deficient rats.",
abstract = "Paraquat, an oxygen radical-generating agent, is a widely used agrochemical that is also toxic for humans, in whom it may cause respiratory failure. In the present study, we investigated the effect of deferoxamine (DF), an iron chelator with antioxidant capacity, on paraquat toxicity in vitamin E-deficient rats. After the administration of paraquat at a dose of 20 mg/kg the animals were treated with a continuous intravenous infusion of DF for 14 days. In a dose-response study, four of six animals receiving 100 mg DF/kg/24 h survived the study period of 14 days compared with none in the saline-treated control group (n = 6), and three and two animals in the groups receiving 50 (n = 6) and 200 mg DF/kg/24 h (n = 6), respectively. In another series of experiments, animals were monitored for a total period of 35 days, at which time any survivors were killed, and lung histologic examination was carried out. Deferoxamine treatment was started simultaneously (n = 21), 6 h (n = 18), and 16 h (n = 18) after paraquat poisoning. Percent survival in the various time-point groups was 47.7 (p less than 0.01), 38.9 (p less than 0.02), and 22.2 (not significant), respectively, compared with 7.1 (n = 14) in the control group. The presence of lung damage was seen only in those of the surviving rats where DF was started at the 16 h time point after paraquat administration. In ancillary in vitro studies, where Escherichia coli was used as a source of enzymic activity for the redox-cycling of paraquat, DF completely inhibited the formation of hydroxyl radical Udgivelsesdato: 1989",
author = "B.S., {van Asbeck} and Hillen F.C. and C.M., {Boonen Harrie} and Y., {de Jong} and Dormans J.A. and N.A., {van der Wal} and Marx J.J. and Sangster B.",
year = "1989",
language = "English",
volume = "139",
pages = "769--773",
journal = "American Review of Respiratory Disease",
issn = "0003-0805",
publisher = "American Thoracic Society; American Lung Association",
number = "3",

}

RIS

TY - JOUR

T1 - Continuous intravenous infusion of deferoxamine reduces mortality by paraquat in vitamin E-deficient rats.

AU - B.S., van Asbeck

AU - F.C., Hillen

AU - C.M., Boonen Harrie

AU - Y., de Jong

AU - J.A., Dormans

AU - N.A., van der Wal

AU - J.J., Marx

AU - B., Sangster

PY - 1989

Y1 - 1989

N2 - Paraquat, an oxygen radical-generating agent, is a widely used agrochemical that is also toxic for humans, in whom it may cause respiratory failure. In the present study, we investigated the effect of deferoxamine (DF), an iron chelator with antioxidant capacity, on paraquat toxicity in vitamin E-deficient rats. After the administration of paraquat at a dose of 20 mg/kg the animals were treated with a continuous intravenous infusion of DF for 14 days. In a dose-response study, four of six animals receiving 100 mg DF/kg/24 h survived the study period of 14 days compared with none in the saline-treated control group (n = 6), and three and two animals in the groups receiving 50 (n = 6) and 200 mg DF/kg/24 h (n = 6), respectively. In another series of experiments, animals were monitored for a total period of 35 days, at which time any survivors were killed, and lung histologic examination was carried out. Deferoxamine treatment was started simultaneously (n = 21), 6 h (n = 18), and 16 h (n = 18) after paraquat poisoning. Percent survival in the various time-point groups was 47.7 (p less than 0.01), 38.9 (p less than 0.02), and 22.2 (not significant), respectively, compared with 7.1 (n = 14) in the control group. The presence of lung damage was seen only in those of the surviving rats where DF was started at the 16 h time point after paraquat administration. In ancillary in vitro studies, where Escherichia coli was used as a source of enzymic activity for the redox-cycling of paraquat, DF completely inhibited the formation of hydroxyl radical Udgivelsesdato: 1989

AB - Paraquat, an oxygen radical-generating agent, is a widely used agrochemical that is also toxic for humans, in whom it may cause respiratory failure. In the present study, we investigated the effect of deferoxamine (DF), an iron chelator with antioxidant capacity, on paraquat toxicity in vitamin E-deficient rats. After the administration of paraquat at a dose of 20 mg/kg the animals were treated with a continuous intravenous infusion of DF for 14 days. In a dose-response study, four of six animals receiving 100 mg DF/kg/24 h survived the study period of 14 days compared with none in the saline-treated control group (n = 6), and three and two animals in the groups receiving 50 (n = 6) and 200 mg DF/kg/24 h (n = 6), respectively. In another series of experiments, animals were monitored for a total period of 35 days, at which time any survivors were killed, and lung histologic examination was carried out. Deferoxamine treatment was started simultaneously (n = 21), 6 h (n = 18), and 16 h (n = 18) after paraquat poisoning. Percent survival in the various time-point groups was 47.7 (p less than 0.01), 38.9 (p less than 0.02), and 22.2 (not significant), respectively, compared with 7.1 (n = 14) in the control group. The presence of lung damage was seen only in those of the surviving rats where DF was started at the 16 h time point after paraquat administration. In ancillary in vitro studies, where Escherichia coli was used as a source of enzymic activity for the redox-cycling of paraquat, DF completely inhibited the formation of hydroxyl radical Udgivelsesdato: 1989

M3 - Journal article

VL - 139

SP - 769

EP - 773

JO - American Review of Respiratory Disease

JF - American Review of Respiratory Disease

SN - 0003-0805

IS - 3

ER -

ID: 16784164