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Identification of platform-independent gene expression markers of cisplatin nephrotoxicity.

Within the International Life Sciences Institute Committee on Genomics, a working group was formed to focus on the application of microarray technology to preclinical assessments of drug-induced nephrotoxicity. As part of this effort, Sprague-Dawley rats were treated with the nephrotoxicant cisplati...

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Autores principales: Thompson, Karol L, Afshari, Cynthia A, Amin, Rupesh P, Bertram, Timothy A, Car, Bruce, Cunningham, Michael, Kind, Clive, Kramer, Jeffrey A, Lawton, Michael, Mirsky, Michael, Naciff, Jorge M, Oreffo, Victor, Pine, P Scott, Sistare, Frank D
Formato: Texto
Lenguaje:English
Publicado: 2004
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1241903/
https://www.ncbi.nlm.nih.gov/pubmed/15033599
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author Thompson, Karol L
Afshari, Cynthia A
Amin, Rupesh P
Bertram, Timothy A
Car, Bruce
Cunningham, Michael
Kind, Clive
Kramer, Jeffrey A
Lawton, Michael
Mirsky, Michael
Naciff, Jorge M
Oreffo, Victor
Pine, P Scott
Sistare, Frank D
author_facet Thompson, Karol L
Afshari, Cynthia A
Amin, Rupesh P
Bertram, Timothy A
Car, Bruce
Cunningham, Michael
Kind, Clive
Kramer, Jeffrey A
Lawton, Michael
Mirsky, Michael
Naciff, Jorge M
Oreffo, Victor
Pine, P Scott
Sistare, Frank D
author_sort Thompson, Karol L
collection PubMed
description Within the International Life Sciences Institute Committee on Genomics, a working group was formed to focus on the application of microarray technology to preclinical assessments of drug-induced nephrotoxicity. As part of this effort, Sprague-Dawley rats were treated with the nephrotoxicant cisplatin at doses of 0.3-5 mg/kg over a 4- to 144-hr time course. RNA prepared from these animals was run on a variety of microarray formats at multiple sites. A set of 93 differentially expressed genes associated with cisplatin-induced renal injury was identified on the National Institute of Environmental Health Sciences (NIEHS) custom cDNA microarray platform using quadruplicate measurements of pooled animal RNA. The reproducibility of this profile of statistically significant gene changes on other platforms, in pooled and individual animal replicate samples, and in an independent study was investigated. A good correlation in response between platforms was found among the 48 genes in the NIEHS data set that could be matched to probes on the Affymetrix RGU34A array by UniGene identifier or sequence alignment. Similar results were obtained with genes that could be linked between the NIEHS and Incyte or PHASE-1 arrays. The degree of renal damage induced by cisplatin in individual animals was commensurate with the number of differentially expressed genes in this data set. These results suggest that gene profiles linked to specific types of tissue injury or mechanisms of toxicity and identified in well-performed replicated microarray experiments may be extrapolatable across platform technologies, laboratories, and in-life studies.
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spelling pubmed-12419032005-11-08 Identification of platform-independent gene expression markers of cisplatin nephrotoxicity. Thompson, Karol L Afshari, Cynthia A Amin, Rupesh P Bertram, Timothy A Car, Bruce Cunningham, Michael Kind, Clive Kramer, Jeffrey A Lawton, Michael Mirsky, Michael Naciff, Jorge M Oreffo, Victor Pine, P Scott Sistare, Frank D Environ Health Perspect Research Article Within the International Life Sciences Institute Committee on Genomics, a working group was formed to focus on the application of microarray technology to preclinical assessments of drug-induced nephrotoxicity. As part of this effort, Sprague-Dawley rats were treated with the nephrotoxicant cisplatin at doses of 0.3-5 mg/kg over a 4- to 144-hr time course. RNA prepared from these animals was run on a variety of microarray formats at multiple sites. A set of 93 differentially expressed genes associated with cisplatin-induced renal injury was identified on the National Institute of Environmental Health Sciences (NIEHS) custom cDNA microarray platform using quadruplicate measurements of pooled animal RNA. The reproducibility of this profile of statistically significant gene changes on other platforms, in pooled and individual animal replicate samples, and in an independent study was investigated. A good correlation in response between platforms was found among the 48 genes in the NIEHS data set that could be matched to probes on the Affymetrix RGU34A array by UniGene identifier or sequence alignment. Similar results were obtained with genes that could be linked between the NIEHS and Incyte or PHASE-1 arrays. The degree of renal damage induced by cisplatin in individual animals was commensurate with the number of differentially expressed genes in this data set. These results suggest that gene profiles linked to specific types of tissue injury or mechanisms of toxicity and identified in well-performed replicated microarray experiments may be extrapolatable across platform technologies, laboratories, and in-life studies. 2004-03 /pmc/articles/PMC1241903/ /pubmed/15033599 Text en
spellingShingle Research Article
Thompson, Karol L
Afshari, Cynthia A
Amin, Rupesh P
Bertram, Timothy A
Car, Bruce
Cunningham, Michael
Kind, Clive
Kramer, Jeffrey A
Lawton, Michael
Mirsky, Michael
Naciff, Jorge M
Oreffo, Victor
Pine, P Scott
Sistare, Frank D
Identification of platform-independent gene expression markers of cisplatin nephrotoxicity.
title Identification of platform-independent gene expression markers of cisplatin nephrotoxicity.
title_full Identification of platform-independent gene expression markers of cisplatin nephrotoxicity.
title_fullStr Identification of platform-independent gene expression markers of cisplatin nephrotoxicity.
title_full_unstemmed Identification of platform-independent gene expression markers of cisplatin nephrotoxicity.
title_short Identification of platform-independent gene expression markers of cisplatin nephrotoxicity.
title_sort identification of platform-independent gene expression markers of cisplatin nephrotoxicity.
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC1241903/
https://www.ncbi.nlm.nih.gov/pubmed/15033599
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