A microarray study of MPP<sup>+</sup>-treated PC12 Cells: Mechanisms of toxicity (MOT) analysis using bioinformatics tools

A microarray study of MPP<sup>+</sup>-treated PC12 Cells: Mechanisms of toxicity (MOT) analysis using bioinformatics tools

<p>Abstract</p> <p>Background</p> <p>This paper describes a microarray study including data quality control, data analysis and the analysis of the mechanism of toxicity (MOT) induced by 1-methyl-4-phenylpyridinium (MPP<sup>+</sup>) in a rat adrenal pheochrom...

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Main Authors: Ali Syed F, Duhart Helen, Shi Leming, Han Tao, Wren Jonathan D, Patterson Tucker A, Xu Zengjun, Slikker William
Format: Article
Language:English
Published: BMC 2005-07-01
Series:BMC Bioinformatics
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spelling doaj-85983569d28a41d586af8bb1368016fc2020-11-25T02:46:16ZengBMCBMC Bioinformatics1471-21052005-07-016Suppl 2S810.1186/1471-2105-6-S2-S8A microarray study of MPP<sup>+</sup>-treated PC12 Cells: Mechanisms of toxicity (MOT) analysis using bioinformatics toolsAli Syed FDuhart HelenShi LemingHan TaoWren Jonathan DPatterson Tucker AXu ZengjunSlikker William<p>Abstract</p> <p>Background</p> <p>This paper describes a microarray study including data quality control, data analysis and the analysis of the mechanism of toxicity (MOT) induced by 1-methyl-4-phenylpyridinium (MPP<sup>+</sup>) in a rat adrenal pheochromocytoma cell line (PC12 cells) using bioinformatics tools. MPP<sup>+ </sup>depletes dopamine content and elicits cell death in PC12 cells. However, the mechanism of MPP<sup>+</sup>-induced neurotoxicity is still unclear.</p> <p>Results</p> <p>In this study, Agilent rat oligo 22K microarrays were used to examine alterations in gene expression of PC12 cells after 500 μM MPP<sup>+ </sup>treatment. Relative gene expression of control and treated cells represented by spot intensities on the array chips was analyzed using bioinformatics tools. Raw data from each array were input into the NCTR ArrayTrack database, and normalized using a Lowess normalization method. Data quality was monitored in ArrayTrack. The means of the averaged log ratio of the paired samples were used to identify the fold changes of gene expression in PC12 cells after MPP<sup>+ </sup>treatment. Our data showed that 106 genes and ESTs (Expressed Sequence Tags) were changed 2-fold and above with MPP<sup>+ </sup>treatment; among these, 75 genes had gene symbols and 59 genes had known functions according to the Agilent gene Refguide and ArrayTrack-linked gene library. The mechanism of MPP<sup>+</sup>-induced toxicity in PC12 cells was analyzed based on their genes functions, biological process, pathways and previous published literatures.</p> <p>Conclusion</p> <p>Multiple pathways were suggested to be involved in the mechanism of MPP<sup>+</sup>-induced toxicity, including oxidative stress, DNA and protein damage, cell cycling arrest, and apoptosis.</p>
collection DOAJ
language English
format Article
sources DOAJ
author Ali Syed F
Duhart Helen
Shi Leming
Han Tao
Wren Jonathan D
Patterson Tucker A
Xu Zengjun
Slikker William
spellingShingle Ali Syed F
Duhart Helen
Shi Leming
Han Tao
Wren Jonathan D
Patterson Tucker A
Xu Zengjun
Slikker William
A microarray study of MPP<sup>+</sup>-treated PC12 Cells: Mechanisms of toxicity (MOT) analysis using bioinformatics tools
BMC Bioinformatics
author_facet Ali Syed F
Duhart Helen
Shi Leming
Han Tao
Wren Jonathan D
Patterson Tucker A
Xu Zengjun
Slikker William
author_sort Ali Syed F
title A microarray study of MPP<sup>+</sup>-treated PC12 Cells: Mechanisms of toxicity (MOT) analysis using bioinformatics tools
title_short A microarray study of MPP<sup>+</sup>-treated PC12 Cells: Mechanisms of toxicity (MOT) analysis using bioinformatics tools
title_full A microarray study of MPP<sup>+</sup>-treated PC12 Cells: Mechanisms of toxicity (MOT) analysis using bioinformatics tools
title_fullStr A microarray study of MPP<sup>+</sup>-treated PC12 Cells: Mechanisms of toxicity (MOT) analysis using bioinformatics tools
title_full_unstemmed A microarray study of MPP<sup>+</sup>-treated PC12 Cells: Mechanisms of toxicity (MOT) analysis using bioinformatics tools
title_sort microarray study of mpp<sup>+</sup>-treated pc12 cells: mechanisms of toxicity (mot) analysis using bioinformatics tools
publisher BMC
series BMC Bioinformatics
issn 1471-2105
publishDate 2005-07-01
description <p>Abstract</p> <p>Background</p> <p>This paper describes a microarray study including data quality control, data analysis and the analysis of the mechanism of toxicity (MOT) induced by 1-methyl-4-phenylpyridinium (MPP<sup>+</sup>) in a rat adrenal pheochromocytoma cell line (PC12 cells) using bioinformatics tools. MPP<sup>+ </sup>depletes dopamine content and elicits cell death in PC12 cells. However, the mechanism of MPP<sup>+</sup>-induced neurotoxicity is still unclear.</p> <p>Results</p> <p>In this study, Agilent rat oligo 22K microarrays were used to examine alterations in gene expression of PC12 cells after 500 μM MPP<sup>+ </sup>treatment. Relative gene expression of control and treated cells represented by spot intensities on the array chips was analyzed using bioinformatics tools. Raw data from each array were input into the NCTR ArrayTrack database, and normalized using a Lowess normalization method. Data quality was monitored in ArrayTrack. The means of the averaged log ratio of the paired samples were used to identify the fold changes of gene expression in PC12 cells after MPP<sup>+ </sup>treatment. Our data showed that 106 genes and ESTs (Expressed Sequence Tags) were changed 2-fold and above with MPP<sup>+ </sup>treatment; among these, 75 genes had gene symbols and 59 genes had known functions according to the Agilent gene Refguide and ArrayTrack-linked gene library. The mechanism of MPP<sup>+</sup>-induced toxicity in PC12 cells was analyzed based on their genes functions, biological process, pathways and previous published literatures.</p> <p>Conclusion</p> <p>Multiple pathways were suggested to be involved in the mechanism of MPP<sup>+</sup>-induced toxicity, including oxidative stress, DNA and protein damage, cell cycling arrest, and apoptosis.</p>
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