Prolonged hypoxia promotes enrichment of cytosolic EZH2 in breast cancer stem cells via a HIF-1α-independent mechanism

Prolonged hypoxia promotes enrichment of cytosolic EZH2 in breast cancer stem cells via a HIF-1α-independent mechanism

Cancer stem cells (CSCs) make up a small subpopulation of the entire tumour. They have the ability to self-renew as well as differentiate into the cells that make up the bulk tumour. Previously, we have demonstrated that EZH2 is highly enriched in the cytosol of breast cancer stem cells (BCSCs), res...

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Main Author: Law, Daniel Cheng Lui
Other Authors: Su I-Hsin
Format: Final Year Project
Language:English
Published: Nanyang Technological University 2020
Subjects:
Science::Biological sciences::Molecular biology
Online Access:https://hdl.handle.net/10356/142015
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Institution: Nanyang Technological University
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spelling sg-ntu-dr.10356-1420152023-02-28T18:07:57Z Prolonged hypoxia promotes enrichment of cytosolic EZH2 in breast cancer stem cells via a HIF-1α-independent mechanism Law, Daniel Cheng Lui Su I-Hsin School of Biological Sciences IHSu@ntu.edu.sg Science::Biological sciences::Molecular biology Cancer stem cells (CSCs) make up a small subpopulation of the entire tumour. They have the ability to self-renew as well as differentiate into the cells that make up the bulk tumour. Previously, we have demonstrated that EZH2 is highly enriched in the cytosol of breast cancer stem cells (BCSCs), resulting in EZH2-dependent methylation of Talin1 and subsequent hyperactivation of STAT3. We also identified a subpopulation within BCSCs that highly expressed cytosolic EZH2 (60-80%). Since the tumour microenvironment has been revealed to be a suitable niche for CSCs, we sought to evaluate whether the hypoxic tumour microenvironment could result in further enrichment of cytosolic EZH2 in BCSCs. We discovered that our in vitro CSC-like model exhibited significantly higher cytosolic EZH2 under prolonged hypoxia in a HIF-1α-independent manner. Paradoxically, HIF-1α, EZH2 and STAT3 activation levels were decreased upon acute and prolonged hypoxia, indicating that HIF-2α may be responsible for the observed changes. The activation of PI3K-mTORC2 and biphasic activation pattern of ERK1/2 further supported the preference of HIF-2α over HIF-1α under prolonged hypoxia. In conclusion, this study highlighted a potential HIF-1α-independent hypoxic adaptive response which may have played a role in the further enrichment of cytosolic EZH2 in BCSCs. Bachelor of Science in Biological Sciences 2020-06-15T02:38:53Z 2020-06-15T02:38:53Z 2020 Final Year Project (FYP) https://hdl.handle.net/10356/142015 en application/pdf Nanyang Technological University
institution Nanyang Technological University
building NTU Library
continent Asia
country Singapore
Singapore
content_provider NTU Library
collection DR-NTU
language English
topic Science::Biological sciences::Molecular biology
spellingShingle Science::Biological sciences::Molecular biology
Law, Daniel Cheng Lui
Prolonged hypoxia promotes enrichment of cytosolic EZH2 in breast cancer stem cells via a HIF-1α-independent mechanism
description Cancer stem cells (CSCs) make up a small subpopulation of the entire tumour. They have the ability to self-renew as well as differentiate into the cells that make up the bulk tumour. Previously, we have demonstrated that EZH2 is highly enriched in the cytosol of breast cancer stem cells (BCSCs), resulting in EZH2-dependent methylation of Talin1 and subsequent hyperactivation of STAT3. We also identified a subpopulation within BCSCs that highly expressed cytosolic EZH2 (60-80%). Since the tumour microenvironment has been revealed to be a suitable niche for CSCs, we sought to evaluate whether the hypoxic tumour microenvironment could result in further enrichment of cytosolic EZH2 in BCSCs. We discovered that our in vitro CSC-like model exhibited significantly higher cytosolic EZH2 under prolonged hypoxia in a HIF-1α-independent manner. Paradoxically, HIF-1α, EZH2 and STAT3 activation levels were decreased upon acute and prolonged hypoxia, indicating that HIF-2α may be responsible for the observed changes. The activation of PI3K-mTORC2 and biphasic activation pattern of ERK1/2 further supported the preference of HIF-2α over HIF-1α under prolonged hypoxia. In conclusion, this study highlighted a potential HIF-1α-independent hypoxic adaptive response which may have played a role in the further enrichment of cytosolic EZH2 in BCSCs.
author2 Su I-Hsin
author_facet Su I-Hsin
Law, Daniel Cheng Lui
format Final Year Project
author Law, Daniel Cheng Lui
author_sort Law, Daniel Cheng Lui
title Prolonged hypoxia promotes enrichment of cytosolic EZH2 in breast cancer stem cells via a HIF-1α-independent mechanism
title_short Prolonged hypoxia promotes enrichment of cytosolic EZH2 in breast cancer stem cells via a HIF-1α-independent mechanism
title_full Prolonged hypoxia promotes enrichment of cytosolic EZH2 in breast cancer stem cells via a HIF-1α-independent mechanism
title_fullStr Prolonged hypoxia promotes enrichment of cytosolic EZH2 in breast cancer stem cells via a HIF-1α-independent mechanism
title_full_unstemmed Prolonged hypoxia promotes enrichment of cytosolic EZH2 in breast cancer stem cells via a HIF-1α-independent mechanism
title_sort prolonged hypoxia promotes enrichment of cytosolic ezh2 in breast cancer stem cells via a hif-1α-independent mechanism
publisher Nanyang Technological University
publishDate 2020
url https://hdl.handle.net/10356/142015
_version_ 1759855125163147264

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