Large scale analysis of positional effects of single-base mismatches on microarray gene expression data

<p>Abstract</p> <p>Background</p> <p>Affymetrix GeneChips utilize 25-mer oligonucleotides probes linked to a silica surface to detect targets in solution. Mismatches due to single nucleotide polymorphisms (SNPs) can affect the hybridization between probes and targets. P...

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Main Authors: Duan Fenghai, Pauley Mark A, Spindel Eliot R, Zhang Li, Norgren Robert B
Format: Article
Language:English
Published: BMC 2010-04-01
Series:BioData Mining
Online Access:http://www.biodatamining.org/content/3/1/2
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spelling doaj-2165cc2312da4ddd84ad12b8a24a1e4a2020-11-24T22:18:00ZengBMCBioData Mining1756-03812010-04-0131210.1186/1756-0381-3-2Large scale analysis of positional effects of single-base mismatches on microarray gene expression dataDuan FenghaiPauley Mark ASpindel Eliot RZhang LiNorgren Robert B<p>Abstract</p> <p>Background</p> <p>Affymetrix GeneChips utilize 25-mer oligonucleotides probes linked to a silica surface to detect targets in solution. Mismatches due to single nucleotide polymorphisms (SNPs) can affect the hybridization between probes and targets. Previous research has indicated that binding between probes and targets strongly depends on the positions of these mismatches. However, there has been substantial variability in the effect of mismatch type across studies.</p> <p>Methods</p> <p>By taking advantage of naturally occurring mismatches between rhesus macaque transcripts and human probes from the Affymetrix U133 Plus 2 GeneChip, we collected the largest 25-mer probes dataset with single-base mismatches at each of the 25 positions on the probe ever used in this type of analysis.</p> <p>Results</p> <p>A mismatch at the center of a probe led to a greater loss in signal intensity than a mismatch at the ends of the probe, regardless of the mismatch type. There was a slight asymmetry between the ends of a probe: effects of mismatches at the 3' end of a probe were greater than those at the 5' end. A cross study comparison of the effect of mismatch types revealed that results were not in good agreement among different reports. However, if the mismatch types were consolidated to purine or pyrimidine mismatches, cross study conclusions could be generated.</p> <p>Conclusion</p> <p>The comprehensive assessment of the effects of single-base mismatches on microarrays provided in this report can be useful for improving future versions of microarray platform design and the corresponding data analysis algorithms.</p> http://www.biodatamining.org/content/3/1/2
collection DOAJ
language English
format Article
sources DOAJ
author Duan Fenghai
Pauley Mark A
Spindel Eliot R
Zhang Li
Norgren Robert B
spellingShingle Duan Fenghai
Pauley Mark A
Spindel Eliot R
Zhang Li
Norgren Robert B
Large scale analysis of positional effects of single-base mismatches on microarray gene expression data
BioData Mining
author_facet Duan Fenghai
Pauley Mark A
Spindel Eliot R
Zhang Li
Norgren Robert B
author_sort Duan Fenghai
title Large scale analysis of positional effects of single-base mismatches on microarray gene expression data
title_short Large scale analysis of positional effects of single-base mismatches on microarray gene expression data
title_full Large scale analysis of positional effects of single-base mismatches on microarray gene expression data
title_fullStr Large scale analysis of positional effects of single-base mismatches on microarray gene expression data
title_full_unstemmed Large scale analysis of positional effects of single-base mismatches on microarray gene expression data
title_sort large scale analysis of positional effects of single-base mismatches on microarray gene expression data
publisher BMC
series BioData Mining
issn 1756-0381
publishDate 2010-04-01
description <p>Abstract</p> <p>Background</p> <p>Affymetrix GeneChips utilize 25-mer oligonucleotides probes linked to a silica surface to detect targets in solution. Mismatches due to single nucleotide polymorphisms (SNPs) can affect the hybridization between probes and targets. Previous research has indicated that binding between probes and targets strongly depends on the positions of these mismatches. However, there has been substantial variability in the effect of mismatch type across studies.</p> <p>Methods</p> <p>By taking advantage of naturally occurring mismatches between rhesus macaque transcripts and human probes from the Affymetrix U133 Plus 2 GeneChip, we collected the largest 25-mer probes dataset with single-base mismatches at each of the 25 positions on the probe ever used in this type of analysis.</p> <p>Results</p> <p>A mismatch at the center of a probe led to a greater loss in signal intensity than a mismatch at the ends of the probe, regardless of the mismatch type. There was a slight asymmetry between the ends of a probe: effects of mismatches at the 3' end of a probe were greater than those at the 5' end. A cross study comparison of the effect of mismatch types revealed that results were not in good agreement among different reports. However, if the mismatch types were consolidated to purine or pyrimidine mismatches, cross study conclusions could be generated.</p> <p>Conclusion</p> <p>The comprehensive assessment of the effects of single-base mismatches on microarrays provided in this report can be useful for improving future versions of microarray platform design and the corresponding data analysis algorithms.</p>
url http://www.biodatamining.org/content/3/1/2
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