Publication year
2007Source
Bioinformatics, 23, 13, (2007), pp. i195-204ISSN
Publication type
Article / Letter to editor
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Organization
CMBI
Molecular Biology
Journal title
Bioinformatics
Volume
vol. 23
Issue
iss. 13
Page start
p. i195
Page end
p. 204
Subject
IGMD 8: Mitochondrial medicine; Molecular Biology; NCMLS 4: Energy and redox metabolism; NCMLS 6: Genetics and epigenetic pathways of disease; UMCN 5.3: Cellular energy metabolismAbstract
MOTIVATION: Recent advances in microarray technologies have made it feasible to interrogate whole genomes with tiling arrays and this technique is rapidly becoming one of the most important high-throughput functional genomics assays. For large mammalian genomes, analyzing oligonucleotide tiling array data is complicated by the presence of non-unique sequences on the array, which increases the overall noise in the data and may lead to false positive results due to cross-hybridization. The ability to create custom microarrays using maskless array synthesis has led us to consider ways to optimize array design characteristics for improving data quality and analysis. We have identified a number of design parameters to be optimized including uniqueness of the probe sequences within the whole genome, melting temperature and self-hybridization potential. RESULTS: We introduce the uniqueness score, U, a novel quality measure for oligonucleotide probes and present a method to quickly compute it. We show that U is equivalent to the number of shortest unique substrings in the probe and describe an efficient greedy algorithm to design mammalian whole genome tiling arrays using probes that maximize U. Using the mouse genome, we demonstrate how several optimizations influence the tiling array design characteristics. With a sensible set of parameters, our designs cover 78% of the mouse genome including many regions previously considered 'untilable' due to the presence of repetitive sequence. Finally, we compare our whole genome tiling array designs with commercially available designs. AVAILABILITY: Source code is available under an open source license from http://www.ebi.ac.uk/~graef/arraydesign/.
This item appears in the following Collection(s)
- Academic publications [244084]
- Faculty of Medical Sciences [92872]
- Faculty of Science [36993]
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