Abstract
Single cell RNA-seq has fueled discovery and innovation in medicine over the past few years and is useful for studying cellular responses at individual cell resolution. But, due to paucity of starting RNA, the data acquired is highly sparse. To address this, We propose a deep matrix factorization based method, deepMc, to impute missing values in gene-expression data. For the deep architecture of our approach, We draw our motivation from great success of deep learning in solving various Machine learning problems. In this work, We support our method with positive results on several evaluation metrics like clustering of cell populations, differential expression analysis and cell type separability.
Copyright
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