Multiomic Profiling Identified EGF Receptor Signaling as a Potential Inhibitor of Type I Interferon Response in Models of Oncolytic Therapy by Vesicular Stomatitis Virus

Anastasia S. Nikitina; Anastasia V. Lipatova; Anton O. Goncharov; Anna A. Kliuchnikova; Mikhail A. Pyatnitskiy; Ksenia G. Kuznetsova; Azzam Hamad; Pavel O. Vorobyev; Olga N. Alekseeva; Marah Mahmoud; Yasmin Shakiba; Ksenia S. Anufrieva; Georgy P. Arapidi; Mark V. Ivanov; Irina A. Tarasova; Mikhail V. Gorshkov; Peter M. Chumakov; Sergei A. Moshkovskii

doi:10.3390/ijms23095244

International Journal of Molecular Sciences (May 2022)

Multiomic Profiling Identified EGF Receptor Signaling as a Potential Inhibitor of Type I Interferon Response in Models of Oncolytic Therapy by Vesicular Stomatitis Virus

Anastasia S. Nikitina,
Anastasia V. Lipatova,
Anton O. Goncharov,
Anna A. Kliuchnikova,
Mikhail A. Pyatnitskiy,
Ksenia G. Kuznetsova,
Azzam Hamad,
Pavel O. Vorobyev,
Olga N. Alekseeva,
Marah Mahmoud,
Yasmin Shakiba,
Ksenia S. Anufrieva,
Georgy P. Arapidi,
Mark V. Ivanov,
Irina A. Tarasova,
Mikhail V. Gorshkov,
Peter M. Chumakov,
Sergei A. Moshkovskii

Affiliations

Anastasia S. Nikitina: Federal Research and Clinical Center of Physical-Chemical Medicine, 119435 Moscow, Russia
Anastasia V. Lipatova: Engelhardt Institute of Molecular Biology, Russian Academy of Sciences, 119991 Moscow, Russia
Anton O. Goncharov: Federal Research and Clinical Center of Physical-Chemical Medicine, 119435 Moscow, Russia
Anna A. Kliuchnikova: Federal Research and Clinical Center of Physical-Chemical Medicine, 119435 Moscow, Russia
Mikhail A. Pyatnitskiy: Federal Research and Clinical Center of Physical-Chemical Medicine, 119435 Moscow, Russia
Ksenia G. Kuznetsova: Federal Research and Clinical Center of Physical-Chemical Medicine, 119435 Moscow, Russia
Azzam Hamad: Engelhardt Institute of Molecular Biology, Russian Academy of Sciences, 119991 Moscow, Russia
Pavel O. Vorobyev: Engelhardt Institute of Molecular Biology, Russian Academy of Sciences, 119991 Moscow, Russia
Olga N. Alekseeva: Engelhardt Institute of Molecular Biology, Russian Academy of Sciences, 119991 Moscow, Russia
Marah Mahmoud: Moscow Institute of Physics and Technology, 141700 Dolgoprudniy, Russia
Yasmin Shakiba: Moscow Institute of Physics and Technology, 141700 Dolgoprudniy, Russia
Ksenia S. Anufrieva: Federal Research and Clinical Center of Physical-Chemical Medicine, 119435 Moscow, Russia
Georgy P. Arapidi: Federal Research and Clinical Center of Physical-Chemical Medicine, 119435 Moscow, Russia
Mark V. Ivanov: V.L. Talrose Institute for Energy Problems of Chemical Physics, N.N. Semenov Federal Research Center for Chemical Physics, Russian Academy of Sciences, 119334 Moscow, Russia
Irina A. Tarasova: V.L. Talrose Institute for Energy Problems of Chemical Physics, N.N. Semenov Federal Research Center for Chemical Physics, Russian Academy of Sciences, 119334 Moscow, Russia
Mikhail V. Gorshkov: V.L. Talrose Institute for Energy Problems of Chemical Physics, N.N. Semenov Federal Research Center for Chemical Physics, Russian Academy of Sciences, 119334 Moscow, Russia
Peter M. Chumakov: Engelhardt Institute of Molecular Biology, Russian Academy of Sciences, 119991 Moscow, Russia
Sergei A. Moshkovskii: Federal Research and Clinical Center of Physical-Chemical Medicine, 119435 Moscow, Russia

DOI: https://doi.org/10.3390/ijms23095244
Journal volume & issue: Vol. 23, no. 9
p. 5244

Abstract

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Cancer cell lines responded differentially to type I interferon treatment in models of oncolytic therapy using vesicular stomatitis virus (VSV). Two opposite cases were considered in this study, glioblastoma DBTRG-05MG and osteosarcoma HOS cell lines exhibiting resistance and sensitivity to VSV after the treatment, respectively. Type I interferon responses were compared for these cell lines by integrative analysis of the transcriptome, proteome, and RNA editome to identify molecular factors determining differential effects observed. Adenosine-to-inosine RNA editing was equally induced in both cell lines. However, transcriptome analysis showed that the number of differentially expressed genes was much higher in DBTRG-05MG with a specific enrichment in inflammatory proteins. Further, it was found that two genes, EGFR and HER2, were overexpressed in HOS cells compared with DBTRG-05MG, supporting recent reports that EGF receptor signaling attenuates interferon responses via HER2 co-receptor activity. Accordingly, combined treatment of cells with EGF receptor inhibitors such as gefitinib and type I interferon increases the resistance of sensitive cell lines to VSV. Moreover, sensitive cell lines had increased levels of HER2 protein compared with non-sensitive DBTRG-05MG. Presumably, the level of this protein expression in tumor cells might be a predictive biomarker of their resistance to oncolytic viral therapy.

Published in International Journal of Molecular Sciences

ISSN: 1661-6596 (Print); 1422-0067 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Science: Biology (General); Science: Chemistry
Website: http://www.mdpi.com/journal/ijms

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