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Strong antitumor efficacy of a pancreatic tumor‐targeting oncolytic adenovirus for neuroendocrine tumors

Although oncolytic adenoviruses are promising cancer therapy agents, for effective oncolytic activity, viruses need to specifically infect and effectively replicate in cancer cells but not in normal cells. We have previously identified a pancreatic cancer‐targeting ligand, SYENFSA (SYE), by screenin...

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Autores principales: Yamamoto, Yuki, Nagasato, Masaki, Rin, Yosei, Henmi, Marina, Ino, Yoshinori, Yachida, Shinichi, Ohki, Rieko, Hiraoka, Nobuyoshi, Tagawa, Masatoshi, Aoki, Kazunori
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2017
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5633550/
https://www.ncbi.nlm.nih.gov/pubmed/28941156
http://dx.doi.org/10.1002/cam4.1185
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author Yamamoto, Yuki
Nagasato, Masaki
Rin, Yosei
Henmi, Marina
Ino, Yoshinori
Yachida, Shinichi
Ohki, Rieko
Hiraoka, Nobuyoshi
Tagawa, Masatoshi
Aoki, Kazunori
author_facet Yamamoto, Yuki
Nagasato, Masaki
Rin, Yosei
Henmi, Marina
Ino, Yoshinori
Yachida, Shinichi
Ohki, Rieko
Hiraoka, Nobuyoshi
Tagawa, Masatoshi
Aoki, Kazunori
author_sort Yamamoto, Yuki
collection PubMed
description Although oncolytic adenoviruses are promising cancer therapy agents, for effective oncolytic activity, viruses need to specifically infect and effectively replicate in cancer cells but not in normal cells. We have previously identified a pancreatic cancer‐targeting ligand, SYENFSA (SYE), by screening an adenovirus library displaying random peptides against human pancreatic cancer cells and reported that a survivin promoter‐regulated adenovirus, displaying the SYE ligand (AdSur‐SYE), provided effective oncolysis of pancreatic ductal adenocarcinoma (PDAC) in a preclinical study. As we examined the infectivity of AdSur‐SYE in human surgical specimens of various pancreatic tumors, we unexpectedly found that AdSur‐SYE showed high gene transduction efficiency for pancreatic neuroendocrine tumors (PNETs) as well as for PDAC, 9.1‐ and 6.2‐fold, respectively, compared to that of the nontargeting virus (AdSur). The infectivity of both vectors was almost the same in other cancers and organs such as the pancreas. Immunostaining indicated that the cells infected with AdSur‐SYE were PNET cells but not stromal cells. AdSur‐SYE showed a significantly higher oncolytic potency than that of AdSur in human PNET cell lines, and intratumoral infection with AdSur‐SYE completely diminished subcutaneous tumors in a murine model, in which AdSur‐SYE effectively proliferated and spread. AdSur‐SYE exerted a stronger oncolytic effect in primary PNET cells cocultured with mouse embryonic fibroblasts than AdSur did. Thus, AdSur‐SYE shows promise as a next‐generation therapy for PNET.
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spelling pubmed-56335502017-10-17 Strong antitumor efficacy of a pancreatic tumor‐targeting oncolytic adenovirus for neuroendocrine tumors Yamamoto, Yuki Nagasato, Masaki Rin, Yosei Henmi, Marina Ino, Yoshinori Yachida, Shinichi Ohki, Rieko Hiraoka, Nobuyoshi Tagawa, Masatoshi Aoki, Kazunori Cancer Med Cancer Biology Although oncolytic adenoviruses are promising cancer therapy agents, for effective oncolytic activity, viruses need to specifically infect and effectively replicate in cancer cells but not in normal cells. We have previously identified a pancreatic cancer‐targeting ligand, SYENFSA (SYE), by screening an adenovirus library displaying random peptides against human pancreatic cancer cells and reported that a survivin promoter‐regulated adenovirus, displaying the SYE ligand (AdSur‐SYE), provided effective oncolysis of pancreatic ductal adenocarcinoma (PDAC) in a preclinical study. As we examined the infectivity of AdSur‐SYE in human surgical specimens of various pancreatic tumors, we unexpectedly found that AdSur‐SYE showed high gene transduction efficiency for pancreatic neuroendocrine tumors (PNETs) as well as for PDAC, 9.1‐ and 6.2‐fold, respectively, compared to that of the nontargeting virus (AdSur). The infectivity of both vectors was almost the same in other cancers and organs such as the pancreas. Immunostaining indicated that the cells infected with AdSur‐SYE were PNET cells but not stromal cells. AdSur‐SYE showed a significantly higher oncolytic potency than that of AdSur in human PNET cell lines, and intratumoral infection with AdSur‐SYE completely diminished subcutaneous tumors in a murine model, in which AdSur‐SYE effectively proliferated and spread. AdSur‐SYE exerted a stronger oncolytic effect in primary PNET cells cocultured with mouse embryonic fibroblasts than AdSur did. Thus, AdSur‐SYE shows promise as a next‐generation therapy for PNET. John Wiley and Sons Inc. 2017-09-21 /pmc/articles/PMC5633550/ /pubmed/28941156 http://dx.doi.org/10.1002/cam4.1185 Text en © 2017 The Authors. Cancer Medicine published by John Wiley & Sons Ltd. This is an open access article under the terms of the Creative Commons Attribution (http://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Cancer Biology
Yamamoto, Yuki
Nagasato, Masaki
Rin, Yosei
Henmi, Marina
Ino, Yoshinori
Yachida, Shinichi
Ohki, Rieko
Hiraoka, Nobuyoshi
Tagawa, Masatoshi
Aoki, Kazunori
Strong antitumor efficacy of a pancreatic tumor‐targeting oncolytic adenovirus for neuroendocrine tumors
title Strong antitumor efficacy of a pancreatic tumor‐targeting oncolytic adenovirus for neuroendocrine tumors
title_full Strong antitumor efficacy of a pancreatic tumor‐targeting oncolytic adenovirus for neuroendocrine tumors
title_fullStr Strong antitumor efficacy of a pancreatic tumor‐targeting oncolytic adenovirus for neuroendocrine tumors
title_full_unstemmed Strong antitumor efficacy of a pancreatic tumor‐targeting oncolytic adenovirus for neuroendocrine tumors
title_short Strong antitumor efficacy of a pancreatic tumor‐targeting oncolytic adenovirus for neuroendocrine tumors
title_sort strong antitumor efficacy of a pancreatic tumor‐targeting oncolytic adenovirus for neuroendocrine tumors
topic Cancer Biology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5633550/
https://www.ncbi.nlm.nih.gov/pubmed/28941156
http://dx.doi.org/10.1002/cam4.1185
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