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Histone deacetylase 6 inhibition enhances oncolytic viral replication in glioma
Hiroshi Nakashima, … , Timothy P. Cripe, E. Antonio Chiocca
Hiroshi Nakashima, … , Timothy P. Cripe, E. Antonio Chiocca
Published October 20, 2015
Citation Information: J Clin Invest. 2015;125(11):4269-4280. https://doi.org/10.1172/JCI80713.
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Research Article Oncology

Histone deacetylase 6 inhibition enhances oncolytic viral replication in glioma

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Abstract

Oncolytic viral (OV) therapy, which uses genetically engineered tumor-targeting viruses, is being increasingly used in cancer clinical trials due to the direct cytolytic effects of this treatment that appear to provoke a robust immune response against the tumor. As OVs enter tumor cells, intrinsic host defenses have the potential to hinder viral replication and spread within the tumor mass. In this report, we show that histone deacetylase 6 (HDAC6) in tumor cells appears to alter the trafficking of post-entry OVs from the nucleus toward lysosomes. In glioma cell lines and glioma-stem–like cells, HDAC6 inhibition (HDAC6i) by either pharmacologic or genetic means substantially increased replication of oncolytic herpes simplex virus type 1 (oHSV). Moreover, HDAC6i increased shuttling of post-entry oHSV to the nucleus. In addition, electron microscopic analysis revealed that post-entry oHSVs are preferentially taken up into glioma cells through the endosomal pathway rather than via fusion at the cell surface. Together, these findings illustrate a mechanism of glioma cell defense against an incoming infection by oHSV and identify possible approaches to enhance oHSV replication and subsequent lysis of tumor cells.

Authors

Hiroshi Nakashima, Johanna K. Kaufmann, Pin-Yi Wang, Tran Nguyen, Maria-Carmela Speranza, Kazue Kasai, Kazuo Okemoto, Akihiro Otsuki, Ichiro Nakano, Soledad Fernandez, William F. Goins, Paola Grandi, Joseph C. Glorioso, Sean Lawler, Timothy P. Cripe, E. Antonio Chiocca

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Figure 6

TEM analysis of oHSV uptake events in GBM83 and GBM326 GSCs and U251 glioma cells.

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TEM analysis of oHSV uptake events in GBM83 and GBM326 GSCs and U251 gli...
(A) GBM326 cells at 20 minutes after infection (p.i.) with rQNestin34.5. The inset shows an enveloped-virion–containing vesicle on the PM (arrowhead). N, nucleus. (B) GBM326 cells. The inset shows macropinocytosis of a virion on the PM. (C) GBM83 cells. The inset shows fusions with HSV-1 virions (arrowheads) and the PM. (D) GBM326 cells. The inset shows endocytic vesicles containing virions in the cytoplasm. Arrowheads indicate fusions of virions with vesicle membrane. (E) Summary of TEM analyses in GBM83, GBM326, and U251 cells at 2, 10, and 20 minutes after infection with rQNestin34.5 virus. PM, oHSV on PM; cytosol (vesicle), virions in the cytosolic endocytic vesicle; cytosol (naked), virions in cytosol without vesicles. Scale bar: 500 nm.

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ISSN: 0021-9738 (print), 1558-8238 (online)

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