Arsenic nano complex induced degradation of YAP sensitized ESCC cancer cells to radiation and chemotherapy

Arsenic nano complex induced degradation of YAP sensitized ESCC cancer cells to radiation and chemotherapy

Abstract Background Increased reactive oxygen species (ROS) production by arsenic treatment in solid tumors showed to be effective to sensitize cancer cells to chemotherapies. Arsenic nano compounds are known to increase the ROS production in solid tumors. Methods In this study we developed arsenic–...

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Main Authors: Wei Zhou, Meiyue Liu, Xia Li, Peng Zhang, Jiong Li, Yue Zhao, Guogui Sun, Weimin Mao
Format: Article
Language:English
Published: BMC 2020-12-01
Series:Cell & Bioscience
Subjects:
Arsenic nano complex
YAP
ESCC
ROS
Radiation therapy
Chemotherapy
Online Access:https://doi.org/10.1186/s13578-020-00508-x
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spelling doaj-22e66394ac5d404fa4ff44a9615dff542020-12-27T12:19:19ZengBMCCell & Bioscience2045-37012020-12-0110111510.1186/s13578-020-00508-xArsenic nano complex induced degradation of YAP sensitized ESCC cancer cells to radiation and chemotherapyWei Zhou0Meiyue Liu1Xia Li2Peng Zhang3Jiong Li4Yue Zhao5Guogui Sun6Weimin Mao7Cancer Hospital of University of Chinese Academy of Sciences (Zhejiang Cancer Hospital), Institute of Cancer and Basic Medicine of Chinese Academy of SciencesSchool of Public Health, North China University of Science and Technology Affiliated People’s Hospital, North China University of Science and TechnologyCancer Hospital of University of Chinese Academy of Sciences (Zhejiang Cancer Hospital), Institute of Cancer and Basic Medicine of Chinese Academy of SciencesCancer Hospital of University of Chinese Academy of Sciences (Zhejiang Cancer Hospital), Institute of Cancer and Basic Medicine of Chinese Academy of SciencesDepartment of Medicinal Chemistry, Massey Cancer Center, Philips Institute for Oral Health Research , Virginia Commonwealth UniversityCancer Hospital of University of Chinese Academy of Sciences (Zhejiang Cancer Hospital), Institute of Cancer and Basic Medicine of Chinese Academy of SciencesSchool of Public Health, North China University of Science and Technology Affiliated People’s Hospital, North China University of Science and TechnologyCancer Hospital of University of Chinese Academy of Sciences (Zhejiang Cancer Hospital), Institute of Cancer and Basic Medicine of Chinese Academy of SciencesAbstract Background Increased reactive oxygen species (ROS) production by arsenic treatment in solid tumors showed to be effective to sensitize cancer cells to chemotherapies. Arsenic nano compounds are known to increase the ROS production in solid tumors. Methods In this study we developed arsenic–ferrosoferric oxide conjugated Nano Complex (As2S2–Fe3O4, AFCNC) to further promote the ROS induction ability of arsenic reagent in solid tumors. We screen for the molecular pathways that are affect by arsenic treatment in ESCC cancer cells. And explored the underlying molecular mechanism for the arsenic mediated degradations of the key transcription factor we identified in the gene microarray screen. Mouse xenograft model were used to further verify the synthetic effects of AFCNC with chemo and radiation therapies, and the molecular target of arsenic treatment is verified with IHC analysis. Results With gene expression microarray analysis we found Hippo signaling pathway is specifically affected by arsenic treatment, and induced ubiquitination mediated degradation of YAP in KYSE-450 esophageal squamous cell carcinoma (ESCC) cells. Mechanistically we proved PML physically interacted with YAP, and arsenic induced degradation PML mediated the degradation of YAP in ESCC cells. As a cancer stem cell related transcription factor, YAP 5SA over expressions in cancer cells are correlated with resistance to chemo and radiation therapies. We found AFCNC treatment inhibited the increased invasion and migration ability of YAP 5SA overexpressing KYSE-450 cells. AFCNC treatment also effectively reversed protective effects of YAP 5SA overexpression against cisplatin induced apoptosis in KYSE-450 cells. Lastly, with ESCC mouse xenograft model we found AFCNC combined with cisplatin treatment or radiation therapy significantly reduced the tumor volumes in vivo in the xenograft ESCC tumors. Conclusions Together, these findings suggested besides ROS, YAP is a potential target for arsenic based therapy in ESCC, which should play an important role in the synthetic effects of arsenic nano complex with chemo and radiation therapy.https://doi.org/10.1186/s13578-020-00508-xArsenic nano complexYAPESCCROSRadiation therapyChemotherapy
collection DOAJ
language English
format Article
sources DOAJ
author Wei Zhou
Meiyue Liu
Xia Li
Peng Zhang
Jiong Li
Yue Zhao
Guogui Sun
Weimin Mao
spellingShingle Wei Zhou
Meiyue Liu
Xia Li
Peng Zhang
Jiong Li
Yue Zhao
Guogui Sun
Weimin Mao
Arsenic nano complex induced degradation of YAP sensitized ESCC cancer cells to radiation and chemotherapy
Cell & Bioscience
Arsenic nano complex
YAP
ESCC
ROS
Radiation therapy
Chemotherapy
author_facet Wei Zhou
Meiyue Liu
Xia Li
Peng Zhang
Jiong Li
Yue Zhao
Guogui Sun
Weimin Mao
author_sort Wei Zhou
title Arsenic nano complex induced degradation of YAP sensitized ESCC cancer cells to radiation and chemotherapy
title_short Arsenic nano complex induced degradation of YAP sensitized ESCC cancer cells to radiation and chemotherapy
title_full Arsenic nano complex induced degradation of YAP sensitized ESCC cancer cells to radiation and chemotherapy
title_fullStr Arsenic nano complex induced degradation of YAP sensitized ESCC cancer cells to radiation and chemotherapy
title_full_unstemmed Arsenic nano complex induced degradation of YAP sensitized ESCC cancer cells to radiation and chemotherapy
title_sort arsenic nano complex induced degradation of yap sensitized escc cancer cells to radiation and chemotherapy
publisher BMC
series Cell & Bioscience
issn 2045-3701
publishDate 2020-12-01
description Abstract Background Increased reactive oxygen species (ROS) production by arsenic treatment in solid tumors showed to be effective to sensitize cancer cells to chemotherapies. Arsenic nano compounds are known to increase the ROS production in solid tumors. Methods In this study we developed arsenic–ferrosoferric oxide conjugated Nano Complex (As2S2–Fe3O4, AFCNC) to further promote the ROS induction ability of arsenic reagent in solid tumors. We screen for the molecular pathways that are affect by arsenic treatment in ESCC cancer cells. And explored the underlying molecular mechanism for the arsenic mediated degradations of the key transcription factor we identified in the gene microarray screen. Mouse xenograft model were used to further verify the synthetic effects of AFCNC with chemo and radiation therapies, and the molecular target of arsenic treatment is verified with IHC analysis. Results With gene expression microarray analysis we found Hippo signaling pathway is specifically affected by arsenic treatment, and induced ubiquitination mediated degradation of YAP in KYSE-450 esophageal squamous cell carcinoma (ESCC) cells. Mechanistically we proved PML physically interacted with YAP, and arsenic induced degradation PML mediated the degradation of YAP in ESCC cells. As a cancer stem cell related transcription factor, YAP 5SA over expressions in cancer cells are correlated with resistance to chemo and radiation therapies. We found AFCNC treatment inhibited the increased invasion and migration ability of YAP 5SA overexpressing KYSE-450 cells. AFCNC treatment also effectively reversed protective effects of YAP 5SA overexpression against cisplatin induced apoptosis in KYSE-450 cells. Lastly, with ESCC mouse xenograft model we found AFCNC combined with cisplatin treatment or radiation therapy significantly reduced the tumor volumes in vivo in the xenograft ESCC tumors. Conclusions Together, these findings suggested besides ROS, YAP is a potential target for arsenic based therapy in ESCC, which should play an important role in the synthetic effects of arsenic nano complex with chemo and radiation therapy.
topic Arsenic nano complex
YAP
ESCC
ROS
Radiation therapy
Chemotherapy
url https://doi.org/10.1186/s13578-020-00508-x
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AT yuezhao arsenicnanocomplexinduceddegradationofyapsensitizedescccancercellstoradiationandchemotherapy
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