Enhanced oncolytic adenoviral production by downregulation of death-domain associated protein and overexpression of precursor terminal protein

Abstract Adequate viral replication in tumor cells is the key to improving the anti-cancer effects of oncolytic adenovirus therapy. In this study, we introduced short hairpin RNAs against death-domain associated protein (Daxx), a repressor of adenoviral replication, and precursor terminal protein (p...

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Main Authors: Jihyun Lee, Geun-Hyeok Oh, Jeong A. Hong, Soojin Choi, Hye Jin Choi, Jae J. Song
Format: Article
Language:English
Published: Nature Publishing Group 2021-01-01
Series:Scientific Reports
Online Access:https://doi.org/10.1038/s41598-020-79998-1
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spelling doaj-6a774af5ee9d4227a13925858eb8e2472021-01-17T12:37:24ZengNature Publishing GroupScientific Reports2045-23222021-01-0111112310.1038/s41598-020-79998-1Enhanced oncolytic adenoviral production by downregulation of death-domain associated protein and overexpression of precursor terminal proteinJihyun Lee0Geun-Hyeok Oh1Jeong A. Hong2Soojin Choi3Hye Jin Choi4Jae J. Song5Institute for Cancer Research, Yonsei University College of MedicineInstitute for Cancer Research, Yonsei University College of MedicineInstitute for Cancer Research, Yonsei University College of MedicineInstitute for Cancer Research, Yonsei University College of MedicineDepartment of Internal Medicine, Yonsei University College of MedicineInstitute for Cancer Research, Yonsei University College of MedicineAbstract Adequate viral replication in tumor cells is the key to improving the anti-cancer effects of oncolytic adenovirus therapy. In this study, we introduced short hairpin RNAs against death-domain associated protein (Daxx), a repressor of adenoviral replication, and precursor terminal protein (pTP), an initiator of adenoviral genome replication, into adenoviral constructs to determine their contributions to viral replication. Both Daxx downregulation and pTP overexpression increased viral production in variety of human cancer cell lines, and the enhanced production of virus progeny resulted in more cell lysis in vitro, and tumor regression in vivo. We confirmed that increased virus production by Daxx silencing, or pTP overexpression, occurred using different mechanisms by analyzing levels of adenoviral protein expression and virus production. Specifically, Daxx downregulation promoted both virus replication and oncolysis in a consecutive manner by optimizing IVa2-based packaging efficiency, while pTP overexpression by increasing both infectious and total virus particles but their contribution to increased viral production may have been damaged to some extent by their another contribution to apoptosis and autophagy. Therefore, introducing both Daxx shRNA and pTP in virotherapy may be a suitable strategy to increase apoptotic tumor-cell death and to overcome poor viral replication, leading to meaningful reductions in tumor growth in vivo.https://doi.org/10.1038/s41598-020-79998-1
collection DOAJ
language English
format Article
sources DOAJ
author Jihyun Lee
Geun-Hyeok Oh
Jeong A. Hong
Soojin Choi
Hye Jin Choi
Jae J. Song
spellingShingle Jihyun Lee
Geun-Hyeok Oh
Jeong A. Hong
Soojin Choi
Hye Jin Choi
Jae J. Song
Enhanced oncolytic adenoviral production by downregulation of death-domain associated protein and overexpression of precursor terminal protein
Scientific Reports
author_facet Jihyun Lee
Geun-Hyeok Oh
Jeong A. Hong
Soojin Choi
Hye Jin Choi
Jae J. Song
author_sort Jihyun Lee
title Enhanced oncolytic adenoviral production by downregulation of death-domain associated protein and overexpression of precursor terminal protein
title_short Enhanced oncolytic adenoviral production by downregulation of death-domain associated protein and overexpression of precursor terminal protein
title_full Enhanced oncolytic adenoviral production by downregulation of death-domain associated protein and overexpression of precursor terminal protein
title_fullStr Enhanced oncolytic adenoviral production by downregulation of death-domain associated protein and overexpression of precursor terminal protein
title_full_unstemmed Enhanced oncolytic adenoviral production by downregulation of death-domain associated protein and overexpression of precursor terminal protein
title_sort enhanced oncolytic adenoviral production by downregulation of death-domain associated protein and overexpression of precursor terminal protein
publisher Nature Publishing Group
series Scientific Reports
issn 2045-2322
publishDate 2021-01-01
description Abstract Adequate viral replication in tumor cells is the key to improving the anti-cancer effects of oncolytic adenovirus therapy. In this study, we introduced short hairpin RNAs against death-domain associated protein (Daxx), a repressor of adenoviral replication, and precursor terminal protein (pTP), an initiator of adenoviral genome replication, into adenoviral constructs to determine their contributions to viral replication. Both Daxx downregulation and pTP overexpression increased viral production in variety of human cancer cell lines, and the enhanced production of virus progeny resulted in more cell lysis in vitro, and tumor regression in vivo. We confirmed that increased virus production by Daxx silencing, or pTP overexpression, occurred using different mechanisms by analyzing levels of adenoviral protein expression and virus production. Specifically, Daxx downregulation promoted both virus replication and oncolysis in a consecutive manner by optimizing IVa2-based packaging efficiency, while pTP overexpression by increasing both infectious and total virus particles but their contribution to increased viral production may have been damaged to some extent by their another contribution to apoptosis and autophagy. Therefore, introducing both Daxx shRNA and pTP in virotherapy may be a suitable strategy to increase apoptotic tumor-cell death and to overcome poor viral replication, leading to meaningful reductions in tumor growth in vivo.
url https://doi.org/10.1038/s41598-020-79998-1
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