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Protection by αG‐Rutin, a Water‐soluble Antioxidant Flavonoid, against Renal Damage in Mice Treated with Ferric Nitrilotriacetate

The protective effect of aG‐Rutin against ferric nitrilotriacetate (Fe‐NTA)‐induced renal damage was studied in male ICR mice. Fe‐NTA induces renal lipid peroxidation, leading to a high incidence of renal cell carcinoma in rodents. Administration of αG‐Rutin (50 μmol as rut in/leg) by gastric intuba...

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Autores principales: Shimoi, Kayoko, Shen, Bingrong, Toyokuni, Shinya, Mochizuki, Rika, Furugori, Michiyo, Kinae, Naohide
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Blackwell Publishing Ltd 1997
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5921458/
https://www.ncbi.nlm.nih.gov/pubmed/9247601
http://dx.doi.org/10.1111/j.1349-7006.1997.tb00403.x
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author Shimoi, Kayoko
Shen, Bingrong
Toyokuni, Shinya
Mochizuki, Rika
Furugori, Michiyo
Kinae, Naohide
author_facet Shimoi, Kayoko
Shen, Bingrong
Toyokuni, Shinya
Mochizuki, Rika
Furugori, Michiyo
Kinae, Naohide
author_sort Shimoi, Kayoko
collection PubMed
description The protective effect of aG‐Rutin against ferric nitrilotriacetate (Fe‐NTA)‐induced renal damage was studied in male ICR mice. Fe‐NTA induces renal lipid peroxidation, leading to a high incidence of renal cell carcinoma in rodents. Administration of αG‐Rutin (50 μmol as rut in/leg) by gastric intubation 30 min after i.p. injection of Fe‐NTA (7 mg Fe/kg) most effectively suppressed renal lipid peroxidation. Repeated i.p. injection of Fe‐NTA (2 mg FeAg/day for the first 3 days and 3 mg Fe/ kg/day for 12 days, 5 days a week) causes subacute nephrotoxicity as revealed by induction of karyomegalic cells in renal proximal tubules. A protective effect was observed in mice given αG‐Rutin 30 min after each Fe‐NTA treatment. To elucidate the mechanism of protection by αG‐Rutin, the pharmacokinetics and hydroxyl radical‐scavenging effect of αG‐Rutin were investigated by HPLC analysis and by electron spin resonance (ESR) spin trapping with 5,5‐dimethyl‐l‐pyrroline‐N‐oxide (DMPO), respectively. When mice were given αG‐Rutin (50 μmol as rutin Ag) by gastric intubation, rapid absorption into the circulation was observed. The plasma concentration of äG‐Rutin reached the highest level 30 min after oral administration and then decreased to the control level within 60 min. äG‐Rutin inhibited the formation of DMPO‐OH in a concentration‐dependent manner. Further, chelating activity of äG‐Rutin to ferric ions was shown by spectrophotometric analysis. These results suggest that absorbed äG‐Rutin works as an antioxidant in vivo either by scavenging reactive oxygen species or by chelating ferric ions and this serves to prevent oxidative renal damage in mice treated with Fe‐NTA.
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spelling pubmed-59214582018-05-11 Protection by αG‐Rutin, a Water‐soluble Antioxidant Flavonoid, against Renal Damage in Mice Treated with Ferric Nitrilotriacetate Shimoi, Kayoko Shen, Bingrong Toyokuni, Shinya Mochizuki, Rika Furugori, Michiyo Kinae, Naohide Jpn J Cancer Res Article The protective effect of aG‐Rutin against ferric nitrilotriacetate (Fe‐NTA)‐induced renal damage was studied in male ICR mice. Fe‐NTA induces renal lipid peroxidation, leading to a high incidence of renal cell carcinoma in rodents. Administration of αG‐Rutin (50 μmol as rut in/leg) by gastric intubation 30 min after i.p. injection of Fe‐NTA (7 mg Fe/kg) most effectively suppressed renal lipid peroxidation. Repeated i.p. injection of Fe‐NTA (2 mg FeAg/day for the first 3 days and 3 mg Fe/ kg/day for 12 days, 5 days a week) causes subacute nephrotoxicity as revealed by induction of karyomegalic cells in renal proximal tubules. A protective effect was observed in mice given αG‐Rutin 30 min after each Fe‐NTA treatment. To elucidate the mechanism of protection by αG‐Rutin, the pharmacokinetics and hydroxyl radical‐scavenging effect of αG‐Rutin were investigated by HPLC analysis and by electron spin resonance (ESR) spin trapping with 5,5‐dimethyl‐l‐pyrroline‐N‐oxide (DMPO), respectively. When mice were given αG‐Rutin (50 μmol as rutin Ag) by gastric intubation, rapid absorption into the circulation was observed. The plasma concentration of äG‐Rutin reached the highest level 30 min after oral administration and then decreased to the control level within 60 min. äG‐Rutin inhibited the formation of DMPO‐OH in a concentration‐dependent manner. Further, chelating activity of äG‐Rutin to ferric ions was shown by spectrophotometric analysis. These results suggest that absorbed äG‐Rutin works as an antioxidant in vivo either by scavenging reactive oxygen species or by chelating ferric ions and this serves to prevent oxidative renal damage in mice treated with Fe‐NTA. Blackwell Publishing Ltd 1997-05 /pmc/articles/PMC5921458/ /pubmed/9247601 http://dx.doi.org/10.1111/j.1349-7006.1997.tb00403.x Text en
spellingShingle Article
Shimoi, Kayoko
Shen, Bingrong
Toyokuni, Shinya
Mochizuki, Rika
Furugori, Michiyo
Kinae, Naohide
Protection by αG‐Rutin, a Water‐soluble Antioxidant Flavonoid, against Renal Damage in Mice Treated with Ferric Nitrilotriacetate
title Protection by αG‐Rutin, a Water‐soluble Antioxidant Flavonoid, against Renal Damage in Mice Treated with Ferric Nitrilotriacetate
title_full Protection by αG‐Rutin, a Water‐soluble Antioxidant Flavonoid, against Renal Damage in Mice Treated with Ferric Nitrilotriacetate
title_fullStr Protection by αG‐Rutin, a Water‐soluble Antioxidant Flavonoid, against Renal Damage in Mice Treated with Ferric Nitrilotriacetate
title_full_unstemmed Protection by αG‐Rutin, a Water‐soluble Antioxidant Flavonoid, against Renal Damage in Mice Treated with Ferric Nitrilotriacetate
title_short Protection by αG‐Rutin, a Water‐soluble Antioxidant Flavonoid, against Renal Damage in Mice Treated with Ferric Nitrilotriacetate
title_sort protection by αg‐rutin, a water‐soluble antioxidant flavonoid, against renal damage in mice treated with ferric nitrilotriacetate
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5921458/
https://www.ncbi.nlm.nih.gov/pubmed/9247601
http://dx.doi.org/10.1111/j.1349-7006.1997.tb00403.x
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