4.6 Article

Multi-Omics Analysis of Glioblastoma Cells' Sensitivity to Oncolytic Viruses

Journal

CANCERS
Volume 13, Issue 21, Pages -

Publisher

MDPI
DOI: 10.3390/cancers13215268

Keywords

glioblastoma; interferon; antiviral mechanisms; oncolytic viruses; multi-omic approaches; pathway identification

Categories

Funding

  1. Russian Foundation [18-29-01059]
  2. Ministry of Science and Higher Education of the Russian Federation [075-15-2019-1660]
  3. VILLUM Center for Bioanalytical Sciences [7292]
  4. Danish National Mass Spectrometry Platform for Functional Proteomics [5072-00007B]

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Studies have shown that interferon-induced resistance may affect the sensitivity of tumor cells to viruses, but inhibiting a single ISG may not necessarily increase sensitivity. Silencing specific genes may negatively impact the internalization of certain viruses.
Oncolytic viruses have gained momentum in the last decades as a promising tool for cancer treatment. Despite the progress, only a fraction of patients show a positive response to viral therapy. One of the key variable factors contributing to therapy outcomes is interferon-dependent antiviral mechanisms in tumor cells. Here, we evaluated this factor using patient-derived glioblastoma multiforme (GBM) cultures. Cell response to the type I interferons' (IFNs) stimulation was characterized at mRNA and protein levels. Omics analysis revealed that GBM cells overexpress interferon-stimulated genes (ISGs) and upregulate their proteins, similar to the normal cells. A conserved molecular pattern unambiguously differentiates between the preserved and defective responses. Comparing ISGs' portraits with titration-based measurements of cell sensitivity to a panel of viruses, the strength of IFN-induced resistance acquired by GBM cells was ranked. The study demonstrates that suppressing a single ISG and encoding an essential antiviral protein, does not necessarily increase sensitivity to viruses. Conversely, silencing IFIT3 and PLSCR1 genes in tumor cells can negatively affect the internalization of vesicular stomatitis and Newcastle disease viruses. We present evidence of a complex relationship between the interferon response genes and other factors affecting the sensitivity of tumor cells to viruses.

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