HDAC6 Regulates Radiosensitivity of Non-Small Cell Lung Cancer by Promoting Degradation of Chk1

HDAC6 Regulates Radiosensitivity of Non-Small Cell Lung Cancer by Promoting Degradation of Chk1

We have previously discovered that HDAC6 regulates the DNA damage response (DDR) via modulating the homeostasis of a DNA mismatch repair protein, MSH2, through HDAC6’s ubiquitin E3 ligase activity. Here, we have reported HDAC6’s second potential E3 ligase substrate, a critical cell cycle checkpoint...

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Main Authors: Niko Moses, Mu Zhang, Jheng-Yu Wu, Chen Hu, Shengyan Xiang, Xinran Geng, Yue Chen, Wenlong Bai, You-Wei Zhang, Gerold Bepler, Xiaohong Mary Zhang
Format: Article
Language:English
Published: MDPI AG 2020-10-01
Series:Cells
Subjects:
histone deacetylase 6 (HDAC6)
checkpoint kinase 1 (Chk1)
ubiquitination
ubiquitin E3 ligase
ionizing radiation (IR)
DNA damage response (DDR)
Online Access:https://www.mdpi.com/2073-4409/9/10/2237
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spelling doaj-9609134495974755a0e6983a9f6471762020-11-25T01:27:44ZengMDPI AGCells2073-44092020-10-0192237223710.3390/cells9102237HDAC6 Regulates Radiosensitivity of Non-Small Cell Lung Cancer by Promoting Degradation of Chk1Niko Moses0Mu Zhang1Jheng-Yu Wu2Chen Hu3Shengyan Xiang4Xinran Geng5Yue Chen6Wenlong Bai7You-Wei Zhang8Gerold Bepler9Xiaohong Mary Zhang10Cancer Biology Graduate Program, Department of Oncology, Wayne State University School of Medicine, Karmanos Cancer Institute, Detroit, MI 48201, USAMolecular Therapeutics Program, Department of Oncology, Karmanos Cancer Institute, Wayne State University School of Medicine, 4100 John R. Street Detroit, MI 48201, USAMolecular Therapeutics Program, Department of Oncology, Karmanos Cancer Institute, Wayne State University School of Medicine, 4100 John R. Street Detroit, MI 48201, USAMolecular Therapeutics Program, Department of Oncology, Karmanos Cancer Institute, Wayne State University School of Medicine, 4100 John R. Street Detroit, MI 48201, USADepartment of Pathology & Cell Biology, Morsani College of Medicine, University of South Florida, 12901 Bruce B. Downs Blvd., Tampa, FL 33612, USADepartment of Pharmacology, Case Comprehensive Cancer Center, School of Medicine, Case Western Reserve University,2109 Adelbert Road, Wood Building W343A, Cleveland, OH 44106, USADepartment of Biochemistry, Molecular Biology and Biophysics, The University of Minnesota at Twin Cities, Minneapolis, MN 55455, USADepartment of Pathology & Cell Biology, Morsani College of Medicine, University of South Florida, 12901 Bruce B. Downs Blvd., Tampa, FL 33612, USADepartment of Pharmacology, Case Comprehensive Cancer Center, School of Medicine, Case Western Reserve University,2109 Adelbert Road, Wood Building W343A, Cleveland, OH 44106, USAMolecular Therapeutics Program, Department of Oncology, Karmanos Cancer Institute, Wayne State University School of Medicine, 4100 John R. Street Detroit, MI 48201, USAMolecular Therapeutics Program, Department of Oncology, Karmanos Cancer Institute, Wayne State University School of Medicine, 4100 John R. Street Detroit, MI 48201, USAWe have previously discovered that HDAC6 regulates the DNA damage response (DDR) via modulating the homeostasis of a DNA mismatch repair protein, MSH2, through HDAC6’s ubiquitin E3 ligase activity. Here, we have reported HDAC6’s second potential E3 ligase substrate, a critical cell cycle checkpoint protein, Chk1. We have found that HDAC6 and Chk1 directly interact, and that HDAC6 ubiquitinates Chk1 in vivo and in vitro. Specifically, HDAC6 interacts with Chk1 via the DAC1 domain, which contains its ubiquitin E3 ligase activity. During the cell cycle, Chk1 protein levels fluctuate, peaking at the G2 phase, subsequently resolving via the ubiquitin-proteasome pathway, and thereby allowing cells to progress to the M phase. However, in HDAC6 knockdown non-small cell lung cancer (NSCLC) cells, Chk1 is constitutively active and fails to resolve post-ionizing radiation (IR), and this enhanced Chk1 activity leads to preferential G2 arrest in HDAC6 knockdown cells accompanied by a reduction in colony formation capacity and viability. Depletion or pharmacological inhibition of Chk1 in HDAC6 knockdown cells reverses this radiosensitive phenotype, suggesting that the radiosensitivity of HDAC6 knockdown cells is dependent on increased Chk1 kinase activity. Overall, our results highlight a novel mechanism of Chk1 regulation at the post-translational level, and a possible strategy for sensitizing NSCLC to radiation via inhibiting HDAC6’s E3 ligase activity.https://www.mdpi.com/2073-4409/9/10/2237histone deacetylase 6 (HDAC6)checkpoint kinase 1 (Chk1)ubiquitinationubiquitin E3 ligaseionizing radiation (IR)DNA damage response (DDR)
collection DOAJ
language English
format Article
sources DOAJ
author Niko Moses
Mu Zhang
Jheng-Yu Wu
Chen Hu
Shengyan Xiang
Xinran Geng
Yue Chen
Wenlong Bai
You-Wei Zhang
Gerold Bepler
Xiaohong Mary Zhang
spellingShingle Niko Moses
Mu Zhang
Jheng-Yu Wu
Chen Hu
Shengyan Xiang
Xinran Geng
Yue Chen
Wenlong Bai
You-Wei Zhang
Gerold Bepler
Xiaohong Mary Zhang
HDAC6 Regulates Radiosensitivity of Non-Small Cell Lung Cancer by Promoting Degradation of Chk1
Cells
histone deacetylase 6 (HDAC6)
checkpoint kinase 1 (Chk1)
ubiquitination
ubiquitin E3 ligase
ionizing radiation (IR)
DNA damage response (DDR)
author_facet Niko Moses
Mu Zhang
Jheng-Yu Wu
Chen Hu
Shengyan Xiang
Xinran Geng
Yue Chen
Wenlong Bai
You-Wei Zhang
Gerold Bepler
Xiaohong Mary Zhang
author_sort Niko Moses
title HDAC6 Regulates Radiosensitivity of Non-Small Cell Lung Cancer by Promoting Degradation of Chk1
title_short HDAC6 Regulates Radiosensitivity of Non-Small Cell Lung Cancer by Promoting Degradation of Chk1
title_full HDAC6 Regulates Radiosensitivity of Non-Small Cell Lung Cancer by Promoting Degradation of Chk1
title_fullStr HDAC6 Regulates Radiosensitivity of Non-Small Cell Lung Cancer by Promoting Degradation of Chk1
title_full_unstemmed HDAC6 Regulates Radiosensitivity of Non-Small Cell Lung Cancer by Promoting Degradation of Chk1
title_sort hdac6 regulates radiosensitivity of non-small cell lung cancer by promoting degradation of chk1
publisher MDPI AG
series Cells
issn 2073-4409
publishDate 2020-10-01
description We have previously discovered that HDAC6 regulates the DNA damage response (DDR) via modulating the homeostasis of a DNA mismatch repair protein, MSH2, through HDAC6’s ubiquitin E3 ligase activity. Here, we have reported HDAC6’s second potential E3 ligase substrate, a critical cell cycle checkpoint protein, Chk1. We have found that HDAC6 and Chk1 directly interact, and that HDAC6 ubiquitinates Chk1 in vivo and in vitro. Specifically, HDAC6 interacts with Chk1 via the DAC1 domain, which contains its ubiquitin E3 ligase activity. During the cell cycle, Chk1 protein levels fluctuate, peaking at the G2 phase, subsequently resolving via the ubiquitin-proteasome pathway, and thereby allowing cells to progress to the M phase. However, in HDAC6 knockdown non-small cell lung cancer (NSCLC) cells, Chk1 is constitutively active and fails to resolve post-ionizing radiation (IR), and this enhanced Chk1 activity leads to preferential G2 arrest in HDAC6 knockdown cells accompanied by a reduction in colony formation capacity and viability. Depletion or pharmacological inhibition of Chk1 in HDAC6 knockdown cells reverses this radiosensitive phenotype, suggesting that the radiosensitivity of HDAC6 knockdown cells is dependent on increased Chk1 kinase activity. Overall, our results highlight a novel mechanism of Chk1 regulation at the post-translational level, and a possible strategy for sensitizing NSCLC to radiation via inhibiting HDAC6’s E3 ligase activity.
topic histone deacetylase 6 (HDAC6)
checkpoint kinase 1 (Chk1)
ubiquitination
ubiquitin E3 ligase
ionizing radiation (IR)
DNA damage response (DDR)
url https://www.mdpi.com/2073-4409/9/10/2237
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