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10.1109/JSTSP.2021.3061251

http://scihub22266oqcxt.onion/10.1109/JSTSP.2021.3061251
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suck abstract from ncbi


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pmid34812273      IEEE+J+Sel+Top+Signal+Process 2021 ; 15 (3): 746-758
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  • Application of Tensor Decomposition to Gene Expression of Infection of Mouse Hepatitis Virus Can Identify Critical Human Genes and Efffective Drugs for SARS-CoV-2 Infection #MMPMID34812273
  • Taguchi YH; Turki T
  • IEEE J Sel Top Signal Process 2021[Apr]; 15 (3): 746-758 PMID34812273show ga
  • To better understand the genes with altered expression caused by infection with the novel coronavirus strain SARS-CoV-2 causing COVID-19 infectious disease, a tensor decomposition (TD)-based unsupervised feature extraction (FE) approach was applied to a gene expression profile dataset of the mouse liver and spleen with experimental infection of mouse hepatitis virus, which is regarded as a suitable model of human coronavirus infection. TD-based unsupervised FE selected 134 altered genes, which were enriched in protein-protein interactions with orf1ab, polyprotein, and 3C-like protease that are well known to play critical roles in coronavirus infection, suggesting that these 134 genes can represent the coronavirus infectious process. We then selected compounds targeting the expression of the 134 selected genes based on a public domain database. The identified drug compounds were mainly related to known antiviral drugs, several of which were also included in those previously screened with an in silico method to identify candidate drugs for treating COVID-19.
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