Joint nonnegative matrix factorization based on sparse and graph Laplacian regularization for clustering and co-differential expression genes analysis (Q2225182)
From MaRDI portal
scientific article
Language | Label | Description | Also known as |
---|---|---|---|
English | Joint nonnegative matrix factorization based on sparse and graph Laplacian regularization for clustering and co-differential expression genes analysis |
scientific article |
Statements
Joint nonnegative matrix factorization based on sparse and graph Laplacian regularization for clustering and co-differential expression genes analysis (English)
0 references
5 February 2021
0 references
Summary: The explosion of multiomics data poses new challenges to existing data mining methods. Joint analysis of multiomics data can make the best of the complementary information that is provided by different types of data. Therefore, they can more accurately explore the biological mechanism of diseases. In this article, two forms of joint nonnegative matrix factorization based on the sparse and graph Laplacian regularization (SG-jNMF) method are proposed. In the method, the graph regularization constraint can preserve the local geometric structure of data. \(L_{2,1}\)-norm regularization can enhance the sparsity among the rows and remove redundant features in the data. First, SG-jNMF1 projects multiomics data into a common subspace and applies the multiomics fusion characteristic matrix to mine the important information closely related to diseases. Second, multiomics data of the same disease are mapped into the common sample space by SG-jNMF2, and the cluster structures are detected clearly. Experimental results show that SG-jNMF can achieve significant improvement in sample clustering compared with existing joint analysis frameworks. SG-jNMF also effectively integrates multiomics data to identify co-differentially expressed genes (Co-DEGs). SG-jNMF provides an efficient integrative analysis method for mining the biological information hidden in heterogeneous multiomics data.
0 references