Abstract
Due to the high cost of sequencing-based genomics assays such as ChIP-seq and DNase-seq, the epigenomic characterization of a cell type is typically carried out using a small panel of assay types. Deciding a priori which assays to perform is, thus, a critical step in many studies. We present the submodular selection of assays (SSA), a method for choosing a diverse panel of genomic assays that leverages methods from submodular optimization. More generally, this application serves as a model for how submodular optimization can be applied to other discrete problems in biology.
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Wei, K., Libbrecht, M. W., Bilmes, J. A., & Noble, W. S. (2016). Choosing panels of genomics assays using submodular optimization. Genome Biology, 17(1). https://doi.org/10.1186/s13059-016-1089-7
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