Hepatocellular carcinoma after a sustained virological response by direct‐acting antivirals harbors TP53 inactivation

INTRODUCTION: The genomic characteristics of hepatocellular carcinoma (HCC) after a sustained virological response (SVR) and its differences according to whether an SVR was achieved by treatment with direct‐acting antivirals (DAA) or interferon (IFN) are still not fully understood. METHODS: Sixty‐ni...

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Autores principales: Imamura, Taisuke, Okamura, Yukiyasu, Ohshima, Keiichi, Uesaka, Katsuhiko, Sugiura, Teiichi, Ito, Takaaki, Yamamoto, Yusuke, Ashida, Ryo, Ohgi, Katsuhisa, Otsuka, Shimpei, Ohnami, Sumiko, Nagashima, Takeshi, Hatakeyama, Keiichi, Kakuda, Yuko, Sugino, Takashi, Urakami, Kenichi, Akiyama, Yasuto, Yamaguchi, Ken
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley and Sons Inc. 2022
Materias:
Clinical Cancer Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9041076/
https://www.ncbi.nlm.nih.gov/pubmed/35174643
http://dx.doi.org/10.1002/cam4.4571
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author Imamura, Taisuke
Okamura, Yukiyasu
Ohshima, Keiichi
Uesaka, Katsuhiko
Sugiura, Teiichi
Ito, Takaaki
Yamamoto, Yusuke
Ashida, Ryo
Ohgi, Katsuhisa
Otsuka, Shimpei
Ohnami, Sumiko
Nagashima, Takeshi
Hatakeyama, Keiichi
Kakuda, Yuko
Sugino, Takashi
Urakami, Kenichi
Akiyama, Yasuto
Yamaguchi, Ken
author_facet Imamura, Taisuke
Okamura, Yukiyasu
Ohshima, Keiichi
Uesaka, Katsuhiko
Sugiura, Teiichi
Ito, Takaaki
Yamamoto, Yusuke
Ashida, Ryo
Ohgi, Katsuhisa
Otsuka, Shimpei
Ohnami, Sumiko
Nagashima, Takeshi
Hatakeyama, Keiichi
Kakuda, Yuko
Sugino, Takashi
Urakami, Kenichi
Akiyama, Yasuto
Yamaguchi, Ken
author_sort Imamura, Taisuke
collection PubMed
description INTRODUCTION: The genomic characteristics of hepatocellular carcinoma (HCC) after a sustained virological response (SVR) and its differences according to whether an SVR was achieved by treatment with direct‐acting antivirals (DAA) or interferon (IFN) are still not fully understood. METHODS: Sixty‐nine surgically resected HCCs from patients with hepatitis C virus infection were analyzed by gene expression profiling and whole‐exome sequencing. RESULTS: Among the 69 HCC patients, 34 HCCs in which an SVR was not achieved at the time of surgery were classified as HCV‐positive, and 35 HCCs in which an SVR was achieved at the time of surgery were classified as HCV‐SVR. According to the HCV treatment, 35 HCV‐SVR HCCs were classified into two groups: eight tumors with DAA (HCV‐SVR‐DAA) and 24 tumors with interferon (HCV‐SVR‐IFN). The frequency of samples with ARID2 mutations was significantly lower in HCV‐SVR than in HCV‐positive tumors (p = 0.048). In contrast, the frequency of samples with PREX2 mutations was significantly higher in HCV‐SVR samples than in HCV‐positive samples (p = 0.048). Among the patients with HCV‐SVR, the frequency of samples with TP53 mutations was significantly higher in HCV‐SVR‐DAA tumors than in HCV‐SVR‐IFN tumors (p = 0.030). TP53 inactivation scores in HCV‐SVR‐DAA tumors were found to be significantly enhanced in comparison to HCV‐SVR‐IFN tumors (p = 0.022). In addition, chromosomal instability and PI3K/AKT/mTOR pathway signatures were enhanced in HCV‐SVR‐DAA tumors. HCV‐SVR‐DAA was significantly associated with portal vein invasion (p = 0.003) in comparison to HCV‐SVR‐IFN. CONCLUSION: Our dataset potentially serves as a fundamental resource for the genomic characteristics of HCV‐SVR‐DAA tumors. Our comprehensive genetic profiling by WES revealed significant differences in the mutation rate of several driver genes between HCV‐positive tumors and HCV‐SVR tumors. Furthermore, it was revealed that the frequency of samples with mutations in TP53 was significantly higher in HCV‐SVR‐DAA tumors than in HCV‐SVR‐IFN tumors.
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spelling pubmed-90410762022-04-28 Hepatocellular carcinoma after a sustained virological response by direct‐acting antivirals harbors TP53 inactivation Imamura, Taisuke Okamura, Yukiyasu Ohshima, Keiichi Uesaka, Katsuhiko Sugiura, Teiichi Ito, Takaaki Yamamoto, Yusuke Ashida, Ryo Ohgi, Katsuhisa Otsuka, Shimpei Ohnami, Sumiko Nagashima, Takeshi Hatakeyama, Keiichi Kakuda, Yuko Sugino, Takashi Urakami, Kenichi Akiyama, Yasuto Yamaguchi, Ken Cancer Med Clinical Cancer Research INTRODUCTION: The genomic characteristics of hepatocellular carcinoma (HCC) after a sustained virological response (SVR) and its differences according to whether an SVR was achieved by treatment with direct‐acting antivirals (DAA) or interferon (IFN) are still not fully understood. METHODS: Sixty‐nine surgically resected HCCs from patients with hepatitis C virus infection were analyzed by gene expression profiling and whole‐exome sequencing. RESULTS: Among the 69 HCC patients, 34 HCCs in which an SVR was not achieved at the time of surgery were classified as HCV‐positive, and 35 HCCs in which an SVR was achieved at the time of surgery were classified as HCV‐SVR. According to the HCV treatment, 35 HCV‐SVR HCCs were classified into two groups: eight tumors with DAA (HCV‐SVR‐DAA) and 24 tumors with interferon (HCV‐SVR‐IFN). The frequency of samples with ARID2 mutations was significantly lower in HCV‐SVR than in HCV‐positive tumors (p = 0.048). In contrast, the frequency of samples with PREX2 mutations was significantly higher in HCV‐SVR samples than in HCV‐positive samples (p = 0.048). Among the patients with HCV‐SVR, the frequency of samples with TP53 mutations was significantly higher in HCV‐SVR‐DAA tumors than in HCV‐SVR‐IFN tumors (p = 0.030). TP53 inactivation scores in HCV‐SVR‐DAA tumors were found to be significantly enhanced in comparison to HCV‐SVR‐IFN tumors (p = 0.022). In addition, chromosomal instability and PI3K/AKT/mTOR pathway signatures were enhanced in HCV‐SVR‐DAA tumors. HCV‐SVR‐DAA was significantly associated with portal vein invasion (p = 0.003) in comparison to HCV‐SVR‐IFN. CONCLUSION: Our dataset potentially serves as a fundamental resource for the genomic characteristics of HCV‐SVR‐DAA tumors. Our comprehensive genetic profiling by WES revealed significant differences in the mutation rate of several driver genes between HCV‐positive tumors and HCV‐SVR tumors. Furthermore, it was revealed that the frequency of samples with mutations in TP53 was significantly higher in HCV‐SVR‐DAA tumors than in HCV‐SVR‐IFN tumors. John Wiley and Sons Inc. 2022-02-17 /pmc/articles/PMC9041076/ /pubmed/35174643 http://dx.doi.org/10.1002/cam4.4571 Text en © 2022 The Authors. Cancer Medicine published by John Wiley & Sons Ltd. https://creativecommons.org/licenses/by/4.0/This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Clinical Cancer Research
Imamura, Taisuke
Okamura, Yukiyasu
Ohshima, Keiichi
Uesaka, Katsuhiko
Sugiura, Teiichi
Ito, Takaaki
Yamamoto, Yusuke
Ashida, Ryo
Ohgi, Katsuhisa
Otsuka, Shimpei
Ohnami, Sumiko
Nagashima, Takeshi
Hatakeyama, Keiichi
Kakuda, Yuko
Sugino, Takashi
Urakami, Kenichi
Akiyama, Yasuto
Yamaguchi, Ken
Hepatocellular carcinoma after a sustained virological response by direct‐acting antivirals harbors TP53 inactivation
title Hepatocellular carcinoma after a sustained virological response by direct‐acting antivirals harbors TP53 inactivation
title_full Hepatocellular carcinoma after a sustained virological response by direct‐acting antivirals harbors TP53 inactivation
title_fullStr Hepatocellular carcinoma after a sustained virological response by direct‐acting antivirals harbors TP53 inactivation
title_full_unstemmed Hepatocellular carcinoma after a sustained virological response by direct‐acting antivirals harbors TP53 inactivation
title_short Hepatocellular carcinoma after a sustained virological response by direct‐acting antivirals harbors TP53 inactivation
title_sort hepatocellular carcinoma after a sustained virological response by direct‐acting antivirals harbors tp53 inactivation
topic Clinical Cancer Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9041076/
https://www.ncbi.nlm.nih.gov/pubmed/35174643
http://dx.doi.org/10.1002/cam4.4571
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