dtmrlogo dtmrlogo
homehomeresearchnewsdialogresourcesoutreachaboutuscontactus
RESEARCH
OUR SCIENTIFIC GOALS
CURRENT RESEARCH PROJECTS
SHARED TECHNICAL RESOURCES
ABSTRACTS AND TECHNICAL PAPERS
  2004
  2003
  2002
  2001
  2000
  1999
  1998
  1997
  1996

ABSTRACT: In vivo effects of ascorbate and glutathione on chromium uptake, formation of chromium(V), chromium-DNA binding and 8-OH-dG levels in liver and kidney of Ostegenic Disorder Shionogi (ODS) rats following treatment with chromium(VI).

Several previous in vitro studies have indicated that ascorbate and glutathione are the major reductants of Cr(VI) in cells. In order to evaluate the in vivo effects of ascorbate and glutathione on Cr(VI)-induced carcinogenesis, Cr uptake and the formation of Cr(V), Cr-DNA adducts and 8-hydroxy-2'-deoxyguanosine (8-OH-dG) were measured in the liver and kidney of Osteogenic Disorder Shionogi (ODS) rats that lack the ability to synthesize ascorbate. Despite a 10-fold difference in tissue ascorbate levels among different dietary ascorbate groups, the Cr(V) signal intensity, Cr uptake and total Cr-DNA binding were not affected in either organ. Treatment of ODS rats with Cr(VI) (10 mg/kg) had no substantial effect on the levels of ascorbate and glutathione in these tissues. The levels of Cr(V) and Cr-DNA binding were approximately 2-fold higher in the liver than in the kidney, although the levels of total Cr uptake were similar in both tissues. Cr uptake levels were significantly lower in the liver and kidney of ODS rats treated with high levels of ascorbate and a high dose of Cr(VI) (40 mg/kg), suggesting a detoxifying role played by plasma ascorbate. Similarly, modulation of glutathione levels by N-acetyl-L-cysteine, L-buthionine-S, R-sulfoximine or phorone in these animals by up to 2-fold had little or no consistent effect on Cr uptake, Cr-DNA binding, Cr(V) levels or 8-OH-dG formation in either organ. One possible explanation is that reduction of ascorbate and glutathione concentration to <10 and 50%, respectively, of normal in these two organs still provides threshold levels of these two reductants that are in excess of what is needed for significant reductive activation of Cr(VI). Alternatively, it is possible that ascorbate and glutathione do not play a major role in the formation of Cr(V), Cr-DNA binding or 8-OH-dG and that other cellular reductants, such as cysteine or other amino acids, might be more important reductants of Cr(VI) in vivo.

Yuann J-MP, Liu KJ, Hamilton JW and Wetterhahn KE. In vivo effects of ascorbate and glutathione on chromium uptake, formation of chromium(V), chromium-DNA binding and 8-OH-dG levels in liver and kidney of Ostegenic Disorder Shionogi (ODS) rats following treatment with chromium(VI). Carcinogenesis, 20:1267-1275, 1999.

 


top

Home | Toxic Metals | Research | News | Resources | Outreach | About Us | Contact Us | Site Map| Search

Dartmouth Home Page

Dartmouth Toxic Metals Research Program © 2001
This page was last modified on : Wednesday, 31-Mar-2004 14:10:52 EST

Web Administrator

Web design ©2001 Fairman Studios. All Rights Reserved.