Newcastle Disease Virus (NDV) Oncolytic Activity in Human Glioma Tumors Is Dependent on CDKN2A-Type I IFN Gene Cluster Codeletion.
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2020
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Cells
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Abstract
Glioblastoma (GBM) is the most aggressive and frequent primary brain tumor in adults
with a median overall survival of 15 months. Tumor recurrence and poor prognosis are related to
cancer stem cells (CSCs), which drive resistance to therapies. A common characteristic in GBM is
CDKN2A gene loss, located close to the cluster of type I IFN genes at Ch9p21. Newcastle disease
virus (NDV) is an avian paramyxovirus with oncolytic and immunostimulatory properties that has
been proposed for the treatment of GBM. We have analyzed the CDKN2A-IFN I gene cluster in
1018 glioma tumors and evaluated the NDV oncolytic e ect in six GBM CSCs ex vivo and in a mouse
model. Our results indicate that more than 50% of GBM patients have some IFN deletion. Moreover,
GBM susceptibility to NDV is dependent on the loss of the type I IFN. Infection of GBM with an
NDV-expressing influenza virus NS1 protein can overcome the resistance to oncolysis by NDV of type
I-competent cells. These results highlight the potential of using NDV vectors in antitumor therapies.
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Glioblastoma, Oncolytic virotherapy, Newcastle disease virus (NDV), Interferon I