ID1 promotes hepatocellular carcinoma proliferation and confers chemoresistance to oxaliplatin by activating pentose phosphate pathway

ID1 promotes hepatocellular carcinoma proliferation and confers chemoresistance to oxaliplatin by activating pentose phosphate pathway

Abstract Background Drug resistance is one of the major concerns in the treatment of hepatocellular carcinoma (HCC). The aim of the present study was to determine whether aberrant high expression of the inhibitor of differentiation 1(ID1) confers oxaliplatin-resistance to HCC by activating the pento...

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Main Authors: Xin Yin, Bei Tang, Jing-Huan Li, Yan Wang, Lan Zhang, Xiao-Ying Xie, Bo-Heng Zhang, Shuang-Jian Qiu, Wei-Zhong Wu, Zheng-Gang Ren
Format: Article
Language:English
Published: BMC 2017-11-01
Series:Journal of Experimental & Clinical Cancer Research
Subjects:
Hepatocellular carcinoma
ID1 (inhibitor of differentiation and DNA binding-1)
Pentose phosphate pathway
Chemoresistance
Online Access:http://link.springer.com/article/10.1186/s13046-017-0637-7
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spelling doaj-a57cb9a8228247ada8f126a4cdb21ee62020-11-25T00:42:46ZengBMCJournal of Experimental & Clinical Cancer Research1756-99662017-11-0136111310.1186/s13046-017-0637-7ID1 promotes hepatocellular carcinoma proliferation and confers chemoresistance to oxaliplatin by activating pentose phosphate pathwayXin Yin0Bei Tang1Jing-Huan Li2Yan Wang3Lan Zhang4Xiao-Ying Xie5Bo-Heng Zhang6Shuang-Jian Qiu7Wei-Zhong Wu8Zheng-Gang Ren9Liver Cancer Institute & Zhong Shan Hospital, Fudan UniversityLiver Cancer Institute & Zhong Shan Hospital, Fudan UniversityLiver Cancer Institute & Zhong Shan Hospital, Fudan UniversityLiver Cancer Institute & Zhong Shan Hospital, Fudan UniversityLiver Cancer Institute & Zhong Shan Hospital, Fudan UniversityLiver Cancer Institute & Zhong Shan Hospital, Fudan UniversityLiver Cancer Institute & Zhong Shan Hospital, Fudan UniversityKey Laboratory of Carcinogenesis and Cancer Invasion, Ministry of EducationKey Laboratory of Carcinogenesis and Cancer Invasion, Ministry of EducationLiver Cancer Institute & Zhong Shan Hospital, Fudan UniversityAbstract Background Drug resistance is one of the major concerns in the treatment of hepatocellular carcinoma (HCC). The aim of the present study was to determine whether aberrant high expression of the inhibitor of differentiation 1(ID1) confers oxaliplatin-resistance to HCC by activating the pentose phosphate pathway (PPP). Methods Aberrant high expression of ID1 was detected in two oxaliplatin-resistant cell lines MHCC97H–OXA(97H–OXA) and Hep3B–OXA(3B–OXA). The lentiviral shRNA or control shRNA was introduced into the two oxaliplatin-resistant cell lines. The effects of ID1 on cell proliferation, apoptosis and chemoresistance were evaluated in vitro and vivo. The molecular signaling mechanism underlying the induction of HCC proliferation and oxaliplatin resistance by ID1 was explored. The prognostic value of ID1/G6PD signaling in HCC patients was assessed using the Cancer Genome Atlas (TCGA) database. Results ID1 was upregulated in oxaliplaitin-resistant HCC cells and promoted HCC cell proliferation and oxaliplatin resistance. Silencing ID1 expression in oxaliplaitin-resistant HCC cell lines inhibited cell proliferation and sensitized oxaliplaitin-resistant cells to death. ID1 knockdown significantly decreased the expression of glucose-6-phosphate dehydrogenase (G6PD), a key enzyme of the PPP. Silencing ID1 expression blocked the activation of G6PD, decreased the production of PPP NADPH, and augmented reactive oxygen and species (ROS), thus inducing cell apoptosis. Study of the molecular mechanism showed that ID1 induced G6PD promoter transcription and activated PPP through Wnt/β-catenin/c-MYC signaling. In addition, ID1/G6PD signaling predicted unfavorable prognosis of HCC patients on the basis of TCGA. Conclusions Our study provided the first evidence that ID1 conferred oxaliplatin resistance in HCC by activating the PPP. This newly defined pathway may have important implications in the research and development of new more effective anti-cancer drugs.http://link.springer.com/article/10.1186/s13046-017-0637-7Hepatocellular carcinomaID1 (inhibitor of differentiation and DNA binding-1)Pentose phosphate pathwayChemoresistance
collection DOAJ
language English
format Article
sources DOAJ
author Xin Yin
Bei Tang
Jing-Huan Li
Yan Wang
Lan Zhang
Xiao-Ying Xie
Bo-Heng Zhang
Shuang-Jian Qiu
Wei-Zhong Wu
Zheng-Gang Ren
spellingShingle Xin Yin
Bei Tang
Jing-Huan Li
Yan Wang
Lan Zhang
Xiao-Ying Xie
Bo-Heng Zhang
Shuang-Jian Qiu
Wei-Zhong Wu
Zheng-Gang Ren
ID1 promotes hepatocellular carcinoma proliferation and confers chemoresistance to oxaliplatin by activating pentose phosphate pathway
Journal of Experimental & Clinical Cancer Research
Hepatocellular carcinoma
ID1 (inhibitor of differentiation and DNA binding-1)
Pentose phosphate pathway
Chemoresistance
author_facet Xin Yin
Bei Tang
Jing-Huan Li
Yan Wang
Lan Zhang
Xiao-Ying Xie
Bo-Heng Zhang
Shuang-Jian Qiu
Wei-Zhong Wu
Zheng-Gang Ren
author_sort Xin Yin
title ID1 promotes hepatocellular carcinoma proliferation and confers chemoresistance to oxaliplatin by activating pentose phosphate pathway
title_short ID1 promotes hepatocellular carcinoma proliferation and confers chemoresistance to oxaliplatin by activating pentose phosphate pathway
title_full ID1 promotes hepatocellular carcinoma proliferation and confers chemoresistance to oxaliplatin by activating pentose phosphate pathway
title_fullStr ID1 promotes hepatocellular carcinoma proliferation and confers chemoresistance to oxaliplatin by activating pentose phosphate pathway
title_full_unstemmed ID1 promotes hepatocellular carcinoma proliferation and confers chemoresistance to oxaliplatin by activating pentose phosphate pathway
title_sort id1 promotes hepatocellular carcinoma proliferation and confers chemoresistance to oxaliplatin by activating pentose phosphate pathway
publisher BMC
series Journal of Experimental & Clinical Cancer Research
issn 1756-9966
publishDate 2017-11-01
description Abstract Background Drug resistance is one of the major concerns in the treatment of hepatocellular carcinoma (HCC). The aim of the present study was to determine whether aberrant high expression of the inhibitor of differentiation 1(ID1) confers oxaliplatin-resistance to HCC by activating the pentose phosphate pathway (PPP). Methods Aberrant high expression of ID1 was detected in two oxaliplatin-resistant cell lines MHCC97H–OXA(97H–OXA) and Hep3B–OXA(3B–OXA). The lentiviral shRNA or control shRNA was introduced into the two oxaliplatin-resistant cell lines. The effects of ID1 on cell proliferation, apoptosis and chemoresistance were evaluated in vitro and vivo. The molecular signaling mechanism underlying the induction of HCC proliferation and oxaliplatin resistance by ID1 was explored. The prognostic value of ID1/G6PD signaling in HCC patients was assessed using the Cancer Genome Atlas (TCGA) database. Results ID1 was upregulated in oxaliplaitin-resistant HCC cells and promoted HCC cell proliferation and oxaliplatin resistance. Silencing ID1 expression in oxaliplaitin-resistant HCC cell lines inhibited cell proliferation and sensitized oxaliplaitin-resistant cells to death. ID1 knockdown significantly decreased the expression of glucose-6-phosphate dehydrogenase (G6PD), a key enzyme of the PPP. Silencing ID1 expression blocked the activation of G6PD, decreased the production of PPP NADPH, and augmented reactive oxygen and species (ROS), thus inducing cell apoptosis. Study of the molecular mechanism showed that ID1 induced G6PD promoter transcription and activated PPP through Wnt/β-catenin/c-MYC signaling. In addition, ID1/G6PD signaling predicted unfavorable prognosis of HCC patients on the basis of TCGA. Conclusions Our study provided the first evidence that ID1 conferred oxaliplatin resistance in HCC by activating the PPP. This newly defined pathway may have important implications in the research and development of new more effective anti-cancer drugs.
topic Hepatocellular carcinoma
ID1 (inhibitor of differentiation and DNA binding-1)
Pentose phosphate pathway
Chemoresistance
url http://link.springer.com/article/10.1186/s13046-017-0637-7
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