Home Medicine Combining markers of nephrotoxicity and hepatotoxicity for improved monitoring and detection of chronic alcohol abuse
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Combining markers of nephrotoxicity and hepatotoxicity for improved monitoring and detection of chronic alcohol abuse

  • Ewa Taracha , Bogusław Habrat , Stanisław J. Chrapusta , Małgorzata Lehner , Aleksandra Wisłowska , Bohdan T. Woronowicz , Marta Bogulas , Jolanta Charewicz , Cezary Markuszewski and Adam Płaźnik
Published/Copyright: December 13, 2006
Clinical Chemistry and Laboratory Medicine (CCLM)
From the journal Clinical Chemistry and Laboratory Medicine (CCLM) Volume 44 Issue 12

Abstract

Background: Most of the commonly used markers of chronic alcohol abuse reflect alcohol hepatotoxicity; however, such abuse is deleterious to the kidneys as well. Combined use of serum markers of liver origin and urinary markers of kidney origin may be of diagnostic advantage.

Methods: The study was performed in 73 male alcoholics undergoing detoxification and 36 male alcoholics who had maintained abstinence for ≥6weeks. Factor analysis, discriminant analysis and receiver operating characteristic (ROC) analysis were used to assess the discriminative power of two urinary markers of alcohol nephrotoxicity, namely β-N-acetylhexosaminidase (Hex, EC 3.2.1.52) and alanine aminopeptidase (EC 3.4.11.2), and of three serum markers of alcohol hepatotoxicity, namely aspartate aminotransferase (EC 2.6.1.1), alanine aminotransferase (EC 2.6.1.2) and γ-glutamyltransferase (GGT, EC 2.3.2.2), and of their quantitative combinations.

Results: The discriminative power of the urinary markers matched that of the serum markers. Hex and GGT appeared to be the best for discriminating the study groups. Their combination given by the equation G&H=0.62×ln(GGT)+0.72×ln(Hex) showed excellent discriminative ability (ROC area under the curve 0.92) that was significantly higher than that of any single marker in this report, indicating superior diagnostic accuracy of the compound marker.

Conclusions: Kidney-derived urinary markers, particularly Hex, can complement or replace, if necessary, serum markers of chronic alcohol abuse that relate to alcohol hepatotoxicity. The compound marker proposed seems a promising tool for the monitoring and perhaps detection of chronic alcohol abuse and warrants further studies.

Clin Chem Lab Med 2006;44:1446–52.

Keywords: β-N-acetylhexosaminidase; biomarker; γ-glutamyltransferase; sensitivity; serum enzyme; specificity; urinary enzyme
Corresponding author: Ewa Taracha, PhD, Department of Neurochemistry, Institute of Psychiatry and Neurology, 9 Sobieskiego St, 02-957 Warsaw, Poland Phone: +48-22-458-26-19, Fax: +48-22-321-34-71,

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Received: 2006-7-27
Accepted: 2006-9-11
Published Online: 2006-12-13
Published in Print: 2006-12-1

©2006 by Walter de Gruyter Berlin New York

Articles in the same Issue

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  14. Analytical performance and clinical utility of the INNOTEST® PHOSPHO-TAU(181P) assay for discrimination between Alzheimer's disease and dementia with Lewy bodies
  15. Variations in assay protocol for the Dako cystatin C method may change patient results by 50% without changing the results for controls
  16. Approved IFCC recommendation on reporting results for blood glucose: International Federation of Clinical Chemistry and Laboratory Medicine Scientific Division, Working Group on Selective Electrodes and Point-of-Care Testing (IFCC-SD-WG-SEPOCT)
  17. National survey on the pre-analytical variability in a representative cohort of Italian laboratories
  18. 10% CV concentration for the fourth generation Roche cardiac troponin T assay derived from Internal Quality Control data
  19. Biological variation of non-SI traceable biological quantities: example of proteins
  20. Effect of tibolone therapy on lipids and coagulation indices
  21. Acknowledgement
  22. Contents Volume 44, 2006
  23. Author Index
  24. Subject Index
https://doi.org/10.1515/CCLM.2006.263
Keywords for this article
β-N-acetylhexosaminidase; biomarker; γ-glutamyltransferase; sensitivity; serum enzyme; specificity; urinary enzyme

Articles in the same Issue

  1. Initiation and progression of atherosclerosis – enzymatic or oxidative modification of low-density lipoprotein?
  2. Blood transfusions in athletes. Old dogmas, new tricks
  3. Molecular detection of tyrosinase transcripts in peripheral blood from patients with malignant melanoma: correlation of PCR sensitivity threshold with clinical and pathologic disease characteristics
  4. Increase in and clearance of cell-free plasma DNA in hemodialysis quantified by real-time PCR
  5. Lipoprotein lipase gene polymorphism at the PvuII locus and serum lipid levels in Guangxi Hei Yi Zhuang and Han populations
  6. Interpretation of cardiac troponin T behaviour in size-exclusion chromatography
  7. Point-of-care C-reactive protein testing in febrile children in general practice
  8. Improvement in HPLC separation of porphyrin isomers and application to biochemical diagnosis of porphyrias
  9. Measurement of late-night salivary cortisol with an automated immunoassay system
  10. Combining markers of nephrotoxicity and hepatotoxicity for improved monitoring and detection of chronic alcohol abuse
  11. Stone or stricture as a cause of extrahepatic cholestasis – do liver function tests predict the diagnosis?
  12. Insulin resistance and enhanced protein glycation in men with prehypertension
  13. Prevalence-dependent decision limits for the early detection of type 2 diabetes mellitus in venous blood, venous plasma and capillary blood during glucose challenge
  14. Analytical performance and clinical utility of the INNOTEST® PHOSPHO-TAU(181P) assay for discrimination between Alzheimer's disease and dementia with Lewy bodies
  15. Variations in assay protocol for the Dako cystatin C method may change patient results by 50% without changing the results for controls
  16. Approved IFCC recommendation on reporting results for blood glucose: International Federation of Clinical Chemistry and Laboratory Medicine Scientific Division, Working Group on Selective Electrodes and Point-of-Care Testing (IFCC-SD-WG-SEPOCT)
  17. National survey on the pre-analytical variability in a representative cohort of Italian laboratories
  18. 10% CV concentration for the fourth generation Roche cardiac troponin T assay derived from Internal Quality Control data
  19. Biological variation of non-SI traceable biological quantities: example of proteins
  20. Effect of tibolone therapy on lipids and coagulation indices
  21. Acknowledgement
  22. Contents Volume 44, 2006
  23. Author Index
  24. Subject Index
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