GIMscan: a new statistical method for analyzing whole-genome array CGH data
RECOMB'07 Proceedings of the 11th annual international conference on Research in computational molecular biology
Detection of chromosomal abnormalities using high resolution arrays in clinical cancer research
Journal of Biomedical Informatics
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Motivation: Comparative genomic hybridization array experiments that investigate gene copy number changes present new challenges for statistical analysis and call for methods that incorporate spatial dependence between sequences along the chromosome. For this purpose, we propose a novel method called CGHmix. It is based on a spatially structured mixture model with three states corresponding to genomic sequences that are either unmodified, deleted or amplified. Inference is performed in a Bayesian framework. From the output, posterior probabilities of belonging to each of the three states are estimated for each genomic sequence and used to classify them. Results: Using simulated data, CGHmix is validated and compared with both a conventional unstructured mixture model and with a recently proposed data mining method. We demonstrate the good performance of CGHmix for classifying copy number changes. In Addition, the method provides a good estimate of the false discovery rate. We also present the analysis of a cancer related dataset. Supplementary information: http://www.bgx.org.uk/papers.html Contact: broet@vjf.inserm.fr