maSigPro: a method to identify significantly differential expression profiles in time-course microarray experiments

doi:10.1093/bioinformatics/btl056

Bioinformatics Advance Access originally published online on February 15, 2006
Bioinformatics 2006 22(9):1096-1102; doi:10.1093/bioinformatics/btl056

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maSigPro: a method to identify significantly differential expression profiles in time-course microarray experiments

Ana Conesa ¹^,^,*, María José Nueda ²^,, Alberto Ferrer ³ and Manuel Talón ¹

¹ Centro de Genómica. Instituto Valenciano de Investigaciones Agrarias, Apartado Oficial 46113 Moncada, Valencia, Spain
² Departamento de Estadística e Investigación Operativa. Universidad de Alicante Apartado 03080, Alicante Spain
³ Departamento de Estadística e Investigación Operativa Aplicadas y Calidad, Universidad Politécnica de Valencia Apartado 46022, Valencia, Spain

^*To whom correspondence should be addressed.

Motivation: Multi-series time-course microarray experimentsare useful approaches for exploring biological processes. Inthis type of experiments, the researcher is frequently interestedin studying gene expression changes along time and in evaluatingtrend differences between the various experimental groups. Thelarge amount of data, multiplicity of experimental conditionsand the dynamic nature of the experiments poses great challengesto data analysis.

Results: In this work, we propose a statistical procedure toidentify genes that show different gene expression profilesacross analytical groups in time-course experiments. The methodis a two-regression step approach where the experimental groupsare identified by dummy variables. The procedure first adjustsa global regression model with all the defined variables toidentify differentially expressed genes, and in second a variableselection strategy is applied to study differences between groupsand to find statistically significant different profiles. Themethodology is illustrated on both a real and a simulated microarraydataset.

Availability: The method has been implemented in the statisticallanguage R and is freely available from the Bioconductor contributedpackages repository and from http://www.ivia.es/centrogenomica/bioinformatics.htm

Contact: aconesa{at}ivia.es; mj.nueda{at}ua.es

Received on November 9, 2005; revised on February 1, 2006; accepted on February 10, 2006

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