Lipid oxidative damage and distribution of inorganic arsenic and its metabolites in the rat nervous system after arsenite exposure: Influence of alpha tocopherol supplementation

García-Chávez, E; Jiménez, I; Segura, B; Del Razo, LM

HERO ID

627186

Reference Type

Journal Article

Year

2006

Language

English

PMID

16797074

HERO ID 627186
In Press No
Year 2006
Title Lipid oxidative damage and distribution of inorganic arsenic and its metabolites in the rat nervous system after arsenite exposure: Influence of alpha tocopherol supplementation
Authors García-Chávez, E; Jiménez, I; Segura, B; Del Razo, LM
Journal NeuroToxicology
Volume 27
Issue 6
Page Numbers 1024-1031
Abstract Inorganic arsenic (iAs) exposure causes peripheral neuropathy. Oxidative effects caused by iAs exposure in peripheral nerves have been incompletely characterized. This study analyzed arsenic and lipid oxidative damage in the brain, spinal cord, and sciatic and sensory sural nerves following arsenite exposure. This study also explored whether alpha tocopherol (alpha-TOC) administration mitigates arsenite-induced oxidative damage. Thiobarbituric acid-reactive substance (TBARS) levels and distributions of iAs and its metabolites were evaluated in male Wistar rats following 30d of sodium arsenite exposure (10mg/kg bodyweight (bw)/d, by gavage). A second group also received alpha-TOC (125mg/kg bw/d, by gavage) during the final 20d of arsenite administration. Arsenite exposure caused increased TBARS levels within each region of the nervous system; oxidative stress was most pronounced in the sural and sciatic nerves. In addition there was a positive quadratic relationship between TBARS levels and the concentration of arsenicals found in the nervous system (r(2)=0.878, p<0.001). Dimethylarsenic was the predominant metabolite of iAs found. Animals alpha-TOC-treated had a 1.7-5.2-fold reduction in TBARS levels when compared with rats that received iAs alone. These results suggest that oxidative damage may be the main mechanism of toxicity induced by exposure of the peripheral nervous system to arsenite and that such damage could be attenuated by alpha-TOC-supplementation.
Doi 10.1016/j.neuro.2006.05.001
Pmid 16797074
Wosid WOS:000243211300010
Is Certified Translation No
Dupe Override No
Comments |WOS:000243211300010
Is Public Yes
Language Text English
Keyword arsenic; neurotoxicity; oxidative damage; peripheral nervous system
Is Qa No
Tags
IRIS
Arsenic (Inorganic)
  1. Literature
  PubMed
  Toxline, TSCATS, & DART
  Web of Science
  Identified during manual review of authoritative sources
  3. Hazard ID Screening
  Other potentially supporting studies
  4. Adverse Outcome Pathways/Networks Screening
  Relevant
  5. Susceptibility Screening
  Excluded/Not relevant
Arsenic MOA
  1. MOA Literature Screening
  MOA Cluster
  Susceptibility Screening
  MOA Seeds
  5. Health Effect
  Nervous System Effects
  4. Adverse Outcome Pathways
  Oxidative stress related effects (includes non-specific SH reactions)
Arsenic Susceptibility
  3. References Identified During Review
  1. Susceptibility Literature Screening
  Supplemental Search
  2. Excluded
  MOA/Mechanistic
  5. Health Effect
  Nervous System Effects
Inorganic Arsenic (7440-38-2) [Final 2025]
  1. Initial Lit Search
  PubMed
  WOS
  ToxNet
  4. Considered through Oct 2015
  6. Cluster Filter through Oct 2015
  7. Other Studies through Oct 2015