Module dates/times: Monday, July 23; 8:30 a.m. -5 p.m.; Tuesday, July 24, 8:30 a.m.-5 p.m., and Wednesday, July 25, 8:30 a.m.-Noon

This course is full. If you wish to be placed on the waiting list, email uwbiost@uw.edu.

This module emphasizes how the theory and application of transcriptomics can be extended to include other types of omic analysis, and then integrated using statistical and machine learning tools.

It starts with the statistical basis of hypothesis testing covering the central role of normalization strategies and the specifics of differential expression analysis. Students will be given the opportunity to work examples using open source R code that is in standard use for RNASeq data.

The module then discusses options for downstream processing by clustering and module detection/comparison; extensions to methylation profiling, proteomics, and metabolomics; eQTL analysis including fine mapping of regulatory variation; and finally, integrative methodologies addressing the relationship between genomic, meta-genomic, and phenotypic variation.

This module deals primarily with upstream data processing methods that lead to the delineation of networks and pathways that are then considered in Module 19: Pathway & Network Analysis for Omics Data.

Greg Gibson is Professor and Director of the Center for Integrative Genomics at Georgia Tech. He conducts research on genomic approaches to human genetics; variability of gene expression; systems biology of disease; theory of canalization and biological robustness. He recently published “Constraints on eQTL fine mapping in the presence of multisite local regulation of gene expression.” G3-Genes,Genomes, Genetics7:2532-2544, 2017.