An experimental loop design for the detection of constitutional chromosomal aberrations by array CGH

<p>Abstract</p> <p>Background</p> <p>Comparative genomic hybridization microarrays for the detection of constitutional chromosomal aberrations is the application of microarray technology coming fastest into routine clinical application. Through genotype-phenotype associ...

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Main Authors: De Moor Bart, Hannes Femke, Van Vooren Steven, Allemeersch Joke, Vermeesch Joris, Moreau Yves
Format: Article
Language:English
Published: BMC 2009-11-01
Series:BMC Bioinformatics
Online Access:http://www.biomedcentral.com/1471-2105/10/380
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spelling doaj-951d6c56e1a742aea49e55863cedd5952020-11-24T21:36:24ZengBMCBMC Bioinformatics1471-21052009-11-0110138010.1186/1471-2105-10-380An experimental loop design for the detection of constitutional chromosomal aberrations by array CGHDe Moor BartHannes FemkeVan Vooren StevenAllemeersch JokeVermeesch JorisMoreau Yves<p>Abstract</p> <p>Background</p> <p>Comparative genomic hybridization microarrays for the detection of constitutional chromosomal aberrations is the application of microarray technology coming fastest into routine clinical application. Through genotype-phenotype association, it is also an important technique towards the discovery of disease causing genes and genomewide functional annotation in human. When using a two-channel microarray of genomic DNA probes for array CGH, the basic setup consists in hybridizing a patient against a normal reference sample. Two major disadvantages of this setup are (1) the use of half of the resources to measure a (little informative) reference sample and (2) the possibility that deviating signals are caused by benign copy number variation in the "normal" reference instead of a patient aberration. Instead, we apply an experimental loop design that compares three patients in three hybridizations.</p> <p>Results</p> <p>We develop and compare two statistical methods (linear models of log ratios and mixed models of absolute measurements). In an analysis of 27 patients seen at our genetics center, we observed that the linear models of the log ratios are advantageous over the mixed models of the absolute intensities.</p> <p>Conclusion</p> <p>The loop design and the performance of the statistical analysis contribute to the quick adoption of array CGH as a routine diagnostic tool. They lower the detection limit of mosaicisms and improve the assignment of copy number variation for genetic association studies.</p> http://www.biomedcentral.com/1471-2105/10/380
collection DOAJ
language English
format Article
sources DOAJ
author De Moor Bart
Hannes Femke
Van Vooren Steven
Allemeersch Joke
Vermeesch Joris
Moreau Yves
spellingShingle De Moor Bart
Hannes Femke
Van Vooren Steven
Allemeersch Joke
Vermeesch Joris
Moreau Yves
An experimental loop design for the detection of constitutional chromosomal aberrations by array CGH
BMC Bioinformatics
author_facet De Moor Bart
Hannes Femke
Van Vooren Steven
Allemeersch Joke
Vermeesch Joris
Moreau Yves
author_sort De Moor Bart
title An experimental loop design for the detection of constitutional chromosomal aberrations by array CGH
title_short An experimental loop design for the detection of constitutional chromosomal aberrations by array CGH
title_full An experimental loop design for the detection of constitutional chromosomal aberrations by array CGH
title_fullStr An experimental loop design for the detection of constitutional chromosomal aberrations by array CGH
title_full_unstemmed An experimental loop design for the detection of constitutional chromosomal aberrations by array CGH
title_sort experimental loop design for the detection of constitutional chromosomal aberrations by array cgh
publisher BMC
series BMC Bioinformatics
issn 1471-2105
publishDate 2009-11-01
description <p>Abstract</p> <p>Background</p> <p>Comparative genomic hybridization microarrays for the detection of constitutional chromosomal aberrations is the application of microarray technology coming fastest into routine clinical application. Through genotype-phenotype association, it is also an important technique towards the discovery of disease causing genes and genomewide functional annotation in human. When using a two-channel microarray of genomic DNA probes for array CGH, the basic setup consists in hybridizing a patient against a normal reference sample. Two major disadvantages of this setup are (1) the use of half of the resources to measure a (little informative) reference sample and (2) the possibility that deviating signals are caused by benign copy number variation in the "normal" reference instead of a patient aberration. Instead, we apply an experimental loop design that compares three patients in three hybridizations.</p> <p>Results</p> <p>We develop and compare two statistical methods (linear models of log ratios and mixed models of absolute measurements). In an analysis of 27 patients seen at our genetics center, we observed that the linear models of the log ratios are advantageous over the mixed models of the absolute intensities.</p> <p>Conclusion</p> <p>The loop design and the performance of the statistical analysis contribute to the quick adoption of array CGH as a routine diagnostic tool. They lower the detection limit of mosaicisms and improve the assignment of copy number variation for genetic association studies.</p>
url http://www.biomedcentral.com/1471-2105/10/380
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