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10.3390/biom12050690

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suck abstract from ncbi


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pmid35625619      Biomolecules 2022 ; 12 (5): ä
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  • Immune-Related Protein Interaction Network in Severe COVID-19 Patients toward the Identification of Key Proteins and Drug Repurposing #MMPMID35625619
  • Sagulkoo P; Suratanee A; Plaimas K
  • Biomolecules 2022[May]; 12 (5): ä PMID35625619show ga
  • Coronavirus disease 2019 (COVID-19) is still an active global public health issue. Although vaccines and therapeutic options are available, some patients experience severe conditions and need critical care support. Hence, identifying key genes or proteins involved in immune-related severe COVID-19 is necessary to find or develop the targeted therapies. This study proposed a novel construction of an immune-related protein interaction network (IPIN) in severe cases with the use of a network diffusion technique on a human interactome network and transcriptomic data. Enrichment analysis revealed that the IPIN was mainly associated with antiviral, innate immune, apoptosis, cell division, and cell cycle regulation signaling pathways. Twenty-three proteins were identified as key proteins to find associated drugs. Finally, poly (I:C), mitomycin C, decitabine, gemcitabine, hydroxyurea, tamoxifen, and curcumin were the potential drugs interacting with the key proteins to heal severe COVID-19. In conclusion, IPIN can be a good representative network for the immune system that integrates the protein interaction network and transcriptomic data. Thus, the key proteins and target drugs in IPIN help to find a new treatment with the use of existing drugs to treat the disease apart from vaccination and conventional antiviral therapy.
  • |*COVID-19 Drug Treatment[MESH]
  • |*Protein Interaction Maps[MESH]
  • |Antiviral Agents/pharmacology/therapeutic use[MESH]
  • |Drug Repositioning[MESH]
  • |Humans[MESH]
  • |Signal Transduction[MESH]


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