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Enterovirus A71 Oncolysis of Malignant Gliomas

Xiaowei Zhang, Hanzhong Wang, Yuhan Sun, Mi Qi, Wei Li, Zhiping Zhang, Xian‐En Zhang, Zongqiang Cui

2020Molecular Therapy25 citationsDOIOpen Access PDF

Abstract

Malignant gliomas, the most lethal type of primary brain tumor, continue to be a major therapeutic challenge. Here, we found that enterovirus A71 (EV-A71) can be developed as a novel oncolytic agent against malignant gliomas. EV-A71 preferentially infected and killed malignant glioma cells relative to normal glial cells. The virus receptor human scavenger receptor class B, member 2 (SCARB2), and phorbol-12-myristate-13-acetate-induced protein 1 (PMAIP1)-mediated cell death were involved in EV-A71-induced oncolysis. In mice with implanted subcutaneous gliomas, intraneoplastic inoculation of EV-A71 caused significant tumor growth inhibition. Furthermore, in mice bearing intracranial orthotopic gliomas, intraneoplastic inoculation of EV-A71 substantially prolonged survival. By insertion of brain-specific microRNA-124 (miR124) response elements into the viral genome, we improved the tumor specificity of EV-A71 oncolytic therapy by reducing its neurotoxicity while maintaining its replication potential and oncolytic capacity in gliomas. Our study reveals that EV-A71 is a potent oncolytic agent against malignant gliomas and may have a role in treating this tumor in the clinical setting.

Topics & Concepts

Oncolytic virusGliomaCancer researchApoptosisVirusVirologyVirotherapyBiologyMedicineImmunologyBiochemistryVirus-based gene therapy researchViral Infections and Immunology ResearchRNA regulation and disease
Enterovirus A71 Oncolysis of Malignant Gliomas | Litcius