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Identification of putative gene based markers of renal toxicity.

This study, designed and conducted as part of the International Life Sciences Institute working group on the Application of Genomics and Proteomics, examined the changes in the expression profile of genes associated with the administration of three different nephrotoxicants--cisplatin, gentamicin, a...

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Autores principales: Amin, Rupesh P, Vickers, Alison E, Sistare, Frank, Thompson, Karol L, Roman, Richard J, Lawton, Michael, Kramer, Jeffrey, Hamadeh, Hisham K, Collins, Jennifer, Grissom, Sherry, Bennett, Lee, Tucker, C Jeffrey, Wild, Stacie, Kind, Clive, Oreffo, Victor, Davis, John W, Curtiss, Sandra, Naciff, Jorge M, Cunningham, Michael, Tennant, Raymond, Stevens, James, Car, Bruce, Bertram, Timothy A, Afshari, Cynthia A
Formato: Texto
Lenguaje:English
Publicado: 2004
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1241901/
https://www.ncbi.nlm.nih.gov/pubmed/15033597
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author Amin, Rupesh P
Vickers, Alison E
Sistare, Frank
Thompson, Karol L
Roman, Richard J
Lawton, Michael
Kramer, Jeffrey
Hamadeh, Hisham K
Collins, Jennifer
Grissom, Sherry
Bennett, Lee
Tucker, C Jeffrey
Wild, Stacie
Kind, Clive
Oreffo, Victor
Davis, John W
Curtiss, Sandra
Naciff, Jorge M
Cunningham, Michael
Tennant, Raymond
Stevens, James
Car, Bruce
Bertram, Timothy A
Afshari, Cynthia A
author_facet Amin, Rupesh P
Vickers, Alison E
Sistare, Frank
Thompson, Karol L
Roman, Richard J
Lawton, Michael
Kramer, Jeffrey
Hamadeh, Hisham K
Collins, Jennifer
Grissom, Sherry
Bennett, Lee
Tucker, C Jeffrey
Wild, Stacie
Kind, Clive
Oreffo, Victor
Davis, John W
Curtiss, Sandra
Naciff, Jorge M
Cunningham, Michael
Tennant, Raymond
Stevens, James
Car, Bruce
Bertram, Timothy A
Afshari, Cynthia A
author_sort Amin, Rupesh P
collection PubMed
description This study, designed and conducted as part of the International Life Sciences Institute working group on the Application of Genomics and Proteomics, examined the changes in the expression profile of genes associated with the administration of three different nephrotoxicants--cisplatin, gentamicin, and puromycin--to assess the usefulness of microarrays in the understanding of mechanism(s) of nephrotoxicity. Male Sprague-Dawley rats were treated with daily doses of puromycin (5-20 mg/kg/day for 21 days), gentamicin (2-240 mg/kg/day for 7 days), or a single dose of cisplatin (0.1-5 mg/kg). Groups of rats were sacrificed at various times after administration of these compounds for standard clinical chemistry, urine analysis, and histological evaluation of the kidney. RNA was extracted from the kidney for microarray analysis. Principal component analysis and gene expression-based clustering of compound effects confirmed sample separation based on dose, time, and degree of renal toxicity. In addition, analysis of the profile components revealed some novel changes in the expression of genes that appeared to be associated with injury in specific portions of the nephron and reflected the mechanism of action of these various nephrotoxicants. For example, although puromycin is thought to specifically promote injury of the podocytes in the glomerulus, the changes in gene expression after chronic exposure of this compound suggested a pattern similar to the known proximal tubular nephrotoxicants cisplatin and gentamicin; this prediction was confirmed histologically. We conclude that renal gene expression profiling coupled with analysis of classical end points affords promising opportunities to reveal potential new mechanistic markers of renal toxicity.
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spelling pubmed-12419012005-11-08 Identification of putative gene based markers of renal toxicity. Amin, Rupesh P Vickers, Alison E Sistare, Frank Thompson, Karol L Roman, Richard J Lawton, Michael Kramer, Jeffrey Hamadeh, Hisham K Collins, Jennifer Grissom, Sherry Bennett, Lee Tucker, C Jeffrey Wild, Stacie Kind, Clive Oreffo, Victor Davis, John W Curtiss, Sandra Naciff, Jorge M Cunningham, Michael Tennant, Raymond Stevens, James Car, Bruce Bertram, Timothy A Afshari, Cynthia A Environ Health Perspect Research Article This study, designed and conducted as part of the International Life Sciences Institute working group on the Application of Genomics and Proteomics, examined the changes in the expression profile of genes associated with the administration of three different nephrotoxicants--cisplatin, gentamicin, and puromycin--to assess the usefulness of microarrays in the understanding of mechanism(s) of nephrotoxicity. Male Sprague-Dawley rats were treated with daily doses of puromycin (5-20 mg/kg/day for 21 days), gentamicin (2-240 mg/kg/day for 7 days), or a single dose of cisplatin (0.1-5 mg/kg). Groups of rats were sacrificed at various times after administration of these compounds for standard clinical chemistry, urine analysis, and histological evaluation of the kidney. RNA was extracted from the kidney for microarray analysis. Principal component analysis and gene expression-based clustering of compound effects confirmed sample separation based on dose, time, and degree of renal toxicity. In addition, analysis of the profile components revealed some novel changes in the expression of genes that appeared to be associated with injury in specific portions of the nephron and reflected the mechanism of action of these various nephrotoxicants. For example, although puromycin is thought to specifically promote injury of the podocytes in the glomerulus, the changes in gene expression after chronic exposure of this compound suggested a pattern similar to the known proximal tubular nephrotoxicants cisplatin and gentamicin; this prediction was confirmed histologically. We conclude that renal gene expression profiling coupled with analysis of classical end points affords promising opportunities to reveal potential new mechanistic markers of renal toxicity. 2004-03 /pmc/articles/PMC1241901/ /pubmed/15033597 Text en
spellingShingle Research Article
Amin, Rupesh P
Vickers, Alison E
Sistare, Frank
Thompson, Karol L
Roman, Richard J
Lawton, Michael
Kramer, Jeffrey
Hamadeh, Hisham K
Collins, Jennifer
Grissom, Sherry
Bennett, Lee
Tucker, C Jeffrey
Wild, Stacie
Kind, Clive
Oreffo, Victor
Davis, John W
Curtiss, Sandra
Naciff, Jorge M
Cunningham, Michael
Tennant, Raymond
Stevens, James
Car, Bruce
Bertram, Timothy A
Afshari, Cynthia A
Identification of putative gene based markers of renal toxicity.
title Identification of putative gene based markers of renal toxicity.
title_full Identification of putative gene based markers of renal toxicity.
title_fullStr Identification of putative gene based markers of renal toxicity.
title_full_unstemmed Identification of putative gene based markers of renal toxicity.
title_short Identification of putative gene based markers of renal toxicity.
title_sort identification of putative gene based markers of renal toxicity.
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1241901/
https://www.ncbi.nlm.nih.gov/pubmed/15033597
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