Malondialdehyde Levels In Wilson′s Disease

Background: Copper ion is a pro-oxidant metal and may be responsible for free radical mediated damage in Wilson′s disease (WD). Estimation of serum malondialdehyde (MDA), a standard test to detect oxidative damage, may support this pathogenesis. Aim: The aim of the study was to analyze...

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Main Authors: Sinha Sanjib, Christopher R, Prashanth L K, Vidya N, Arunodaya G R, Rao S, Taly A B
Format: Article
Language:English
Published: Wolters Kluwer Medknow Publications 2004-01-01
Series:Annals of Indian Academy of Neurology
Online Access:http://www.annalsofian.org/article.asp?issn=0972-2327;year=2004;volume=7;issue=4;spage=507;epage=510;aulast=Sinha;type=0
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spelling doaj-e4d601c4bf9b48cdb80f603ab306e9902020-11-24T23:39:53ZengWolters Kluwer Medknow PublicationsAnnals of Indian Academy of Neurology0972-23271998-35492004-01-0174507510Malondialdehyde Levels In Wilson′s DiseaseSinha SanjibChristopher RPrashanth L KVidya NArunodaya G RRao STaly A BBackground: Copper ion is a pro-oxidant metal and may be responsible for free radical mediated damage in Wilson′s disease (WD). Estimation of serum malondialdehyde (MDA), a standard test to detect oxidative damage, may support this pathogenesis. Aim: The aim of the study was to analyze the serum levels of MDA and correlate with clinical status in patients of WD. Patients and Methods: Forty five patients, from a large cohort of proven WD at various stages of treatment were evaluated. Their clinical parameters were noted and assessment of disability and handicap were done. The laboratory tests were carried out using standard methods. Results: The mean age of patients was 21.1+9.1 years (range: 6-50 years) with M: F ratio of 1.6:1. The mean age at presentation was 14.4+6.9 years (range: 6-42 years) and the mean duration of treatment was 14.4+6.9 years (range: 0-24 years). Their mean serum copper and ceruloplasmin levels were 41.4+22.9 g/d1 (range: 4 -103 g/dl) and 5.8+3.4 mg/dl (range: 2-18 mg/dl) respectively. Thirty eight of them had neurological involvement, four had hepatic form, two had both hepatic and neurological involvement while one was presymptomatic sibling. Patients were assessed using CHU staging (mean: 1.5+0.6), modified schwab and England Activities of Daily Living (MSEADL) scale (mean: 94.44+19.55) and Neurologic symptom Score (NSS) (mean: 3.96+5.2). The mean serum MDA level was 0.65 + 0.34 moles/1 and only four (9.4%) patients had increased levels of MDA (mean: 1.32 + 0.05 moles/1), compared to control (mean: 0.56 + 0.36 moles/1) but it was not statistically significant. No significant correlation was noted between MDA levels and NSS, CHU score, MSEADL score and serum copper level. Conclusion: Increased levels of MDA were detected in only 4 out of 45 patients but those with or without increased MDA levels were not different in their clinical status. These patients were on long term treatment, which might alter the oxidative state. Mechanisms other than oxidative damage may underlie WD. Further studies, especially on newly diagnosed patients, need to be done to validate the mechanism of copper induced damage.http://www.annalsofian.org/article.asp?issn=0972-2327;year=2004;volume=7;issue=4;spage=507;epage=510;aulast=Sinha;type=0
collection DOAJ
language English
format Article
sources DOAJ
author Sinha Sanjib
Christopher R
Prashanth L K
Vidya N
Arunodaya G R
Rao S
Taly A B
spellingShingle Sinha Sanjib
Christopher R
Prashanth L K
Vidya N
Arunodaya G R
Rao S
Taly A B
Malondialdehyde Levels In Wilson′s Disease
Annals of Indian Academy of Neurology
author_facet Sinha Sanjib
Christopher R
Prashanth L K
Vidya N
Arunodaya G R
Rao S
Taly A B
author_sort Sinha Sanjib
title Malondialdehyde Levels In Wilson′s Disease
title_short Malondialdehyde Levels In Wilson′s Disease
title_full Malondialdehyde Levels In Wilson′s Disease
title_fullStr Malondialdehyde Levels In Wilson′s Disease
title_full_unstemmed Malondialdehyde Levels In Wilson′s Disease
title_sort malondialdehyde levels in wilson′s disease
publisher Wolters Kluwer Medknow Publications
series Annals of Indian Academy of Neurology
issn 0972-2327
1998-3549
publishDate 2004-01-01
description Background: Copper ion is a pro-oxidant metal and may be responsible for free radical mediated damage in Wilson′s disease (WD). Estimation of serum malondialdehyde (MDA), a standard test to detect oxidative damage, may support this pathogenesis. Aim: The aim of the study was to analyze the serum levels of MDA and correlate with clinical status in patients of WD. Patients and Methods: Forty five patients, from a large cohort of proven WD at various stages of treatment were evaluated. Their clinical parameters were noted and assessment of disability and handicap were done. The laboratory tests were carried out using standard methods. Results: The mean age of patients was 21.1+9.1 years (range: 6-50 years) with M: F ratio of 1.6:1. The mean age at presentation was 14.4+6.9 years (range: 6-42 years) and the mean duration of treatment was 14.4+6.9 years (range: 0-24 years). Their mean serum copper and ceruloplasmin levels were 41.4+22.9 g/d1 (range: 4 -103 g/dl) and 5.8+3.4 mg/dl (range: 2-18 mg/dl) respectively. Thirty eight of them had neurological involvement, four had hepatic form, two had both hepatic and neurological involvement while one was presymptomatic sibling. Patients were assessed using CHU staging (mean: 1.5+0.6), modified schwab and England Activities of Daily Living (MSEADL) scale (mean: 94.44+19.55) and Neurologic symptom Score (NSS) (mean: 3.96+5.2). The mean serum MDA level was 0.65 + 0.34 moles/1 and only four (9.4%) patients had increased levels of MDA (mean: 1.32 + 0.05 moles/1), compared to control (mean: 0.56 + 0.36 moles/1) but it was not statistically significant. No significant correlation was noted between MDA levels and NSS, CHU score, MSEADL score and serum copper level. Conclusion: Increased levels of MDA were detected in only 4 out of 45 patients but those with or without increased MDA levels were not different in their clinical status. These patients were on long term treatment, which might alter the oxidative state. Mechanisms other than oxidative damage may underlie WD. Further studies, especially on newly diagnosed patients, need to be done to validate the mechanism of copper induced damage.
url http://www.annalsofian.org/article.asp?issn=0972-2327;year=2004;volume=7;issue=4;spage=507;epage=510;aulast=Sinha;type=0
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