Hypoxia alters expression and activity of RNA modifying enzymes targeting cytidine in hepatocellular carcinoma cells

Hypoxia alters expression and activity of RNA modifying enzymes targeting cytidine in hepatocellular carcinoma cells

Cells adapt to environmental changes through a variety of biochemical processes. Some of these adaptations involve introducing chemical modifications to the molecules that make up their genetic material, which are the nucleic acid bases of DNA. While these changes do not alter the underlying DNA seq...

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Main Author: Lee, Benjamin Sian Teck
Other Authors: Valerie Lin
Format: Thesis-Doctor of Philosophy
Language:English
Published: Nanyang Technological University 2025
Subjects:
Chemistry
Medicine, Health and Life Sciences
Epitranscriptomics
Cancer
Hypoxia
RNA
Epigenetics
Online Access:https://hdl.handle.net/10356/182898
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Institution: Nanyang Technological University
Language: English
id sg-ntu-dr.10356-182898
record_format dspace
institution Nanyang Technological University
building NTU Library
continent Asia
country Singapore
Singapore
content_provider NTU Library
collection DR-NTU
language English
topic Chemistry
Medicine, Health and Life Sciences
Epitranscriptomics
Cancer
Hypoxia
RNA
Epigenetics
spellingShingle Chemistry
Medicine, Health and Life Sciences
Epitranscriptomics
Cancer
Hypoxia
RNA
Epigenetics
Lee, Benjamin Sian Teck
Hypoxia alters expression and activity of RNA modifying enzymes targeting cytidine in hepatocellular carcinoma cells
description Cells adapt to environmental changes through a variety of biochemical processes. Some of these adaptations involve introducing chemical modifications to the molecules that make up their genetic material, which are the nucleic acid bases of DNA. While these changes do not alter the underlying DNA sequence, they can influence how active the genes are by affecting the interactions between the DNA and other biomolecules. The bases of RNA can similarly be modified. Termed RNA epigenetics or epitranscriptomics, the mechanisms, processes, and functions of these modifications are a field of active research. Closely related to this is the study of the proteins that install, remove, and recognize these modifications. The objective of this PhD thesis is to study how the levels and activities of these proteins are affected by changes in microenvironmental oxygen concentration using both existing and novel techniques. It will be divided into three main parts. The first part of this thesis tests out various methods of isolating protein-RNA adducts formed by exposure of cultured cells to UV radiation. At the time this project began, the only method available for system-wide characterization of such adducts only targeted proteins bound to mRNA. This was due to its reliance on oligo-d(T) beads for pull-down of the adducts. Since then, however, multiple methods suitable for looking at the protein interactome of total RNA have become available. In my experiments, I have found silica-column based methods to be ineffective at accomplishing this task. On the other hand, methods exploiting phenol-chloroform organic phase separation performed very well, successfully enriching known RNA-binding proteins in UV crosslinked samples. The second part of this thesis uses orthogonal organic phase separation to profile changes in the RNA-binding proteome in hepatocellular carcinoma cells experiencing hypoxic stress. Whole proteome profiling was performed alongside this for comparison. Interestingly, western blot on whole cell lysate revealed the RNA modifying enzyme NAT10 to be downregulated in hypoxic conditions. Targeted epitranscriptomic sequencing experiments on a NAT10 target site on rRNA revealed cytidine acetylation to also be reduced upon hypoxia treatment, raising the question of what other RNA modifications could be affected by hypoxia. The third part of this thesis examines cytidine methylation in the context of hypoxia in hepatocellular carcinoma cells. Since there are multiple enzymes that can catalyse the formation of 5-methylcytidine on RNA, I was interested to know which of these enzymes would be dysregulated under hypoxia as this could potentially lead to a new therapeutic target for hepatocellular carcinoma. Using a novel method which I developed to profile the activity of these enzymes towards total RNA, I found that NSUN2 was more enzymatically active during hypoxia even though no changes in protein abundance was observed. Additionally, the activity of the rRNA methyltransferase NSUN1 was downregulated, which is noteworthy given the findings in the second part of this thesis. Taken together, these findings have shed new insights into the role of RNA modifications in the hypoxia response of hepatocellular carcinoma cells. Future work should strive to examine if inhibition of NSUN2 will have a noticeable effect on cancer survival or progression, and investigate the mechanisms underpinning the downregulation of rRNA modifying enzymes NAT10 and NSUN1 in the hopes of identifying other new druggable targets for hepatocellular carcinoma.
author2 Valerie Lin
author_facet Valerie Lin
Lee, Benjamin Sian Teck
format Thesis-Doctor of Philosophy
author Lee, Benjamin Sian Teck
author_sort Lee, Benjamin Sian Teck
title Hypoxia alters expression and activity of RNA modifying enzymes targeting cytidine in hepatocellular carcinoma cells
title_short Hypoxia alters expression and activity of RNA modifying enzymes targeting cytidine in hepatocellular carcinoma cells
title_full Hypoxia alters expression and activity of RNA modifying enzymes targeting cytidine in hepatocellular carcinoma cells
title_fullStr Hypoxia alters expression and activity of RNA modifying enzymes targeting cytidine in hepatocellular carcinoma cells
title_full_unstemmed Hypoxia alters expression and activity of RNA modifying enzymes targeting cytidine in hepatocellular carcinoma cells
title_sort hypoxia alters expression and activity of rna modifying enzymes targeting cytidine in hepatocellular carcinoma cells
publisher Nanyang Technological University
publishDate 2025
url https://hdl.handle.net/10356/182898
_version_ 1826362288602349568
spelling sg-ntu-dr.10356-1828982025-03-09T15:38:56Z Hypoxia alters expression and activity of RNA modifying enzymes targeting cytidine in hepatocellular carcinoma cells Lee, Benjamin Sian Teck Valerie Lin Interdisciplinary Graduate School (IGS) NTU Institute for Health Technologies CLLin@ntu.edu.sg Chemistry Medicine, Health and Life Sciences Epitranscriptomics Cancer Hypoxia RNA Epigenetics Cells adapt to environmental changes through a variety of biochemical processes. Some of these adaptations involve introducing chemical modifications to the molecules that make up their genetic material, which are the nucleic acid bases of DNA. While these changes do not alter the underlying DNA sequence, they can influence how active the genes are by affecting the interactions between the DNA and other biomolecules. The bases of RNA can similarly be modified. Termed RNA epigenetics or epitranscriptomics, the mechanisms, processes, and functions of these modifications are a field of active research. Closely related to this is the study of the proteins that install, remove, and recognize these modifications. The objective of this PhD thesis is to study how the levels and activities of these proteins are affected by changes in microenvironmental oxygen concentration using both existing and novel techniques. It will be divided into three main parts. The first part of this thesis tests out various methods of isolating protein-RNA adducts formed by exposure of cultured cells to UV radiation. At the time this project began, the only method available for system-wide characterization of such adducts only targeted proteins bound to mRNA. This was due to its reliance on oligo-d(T) beads for pull-down of the adducts. Since then, however, multiple methods suitable for looking at the protein interactome of total RNA have become available. In my experiments, I have found silica-column based methods to be ineffective at accomplishing this task. On the other hand, methods exploiting phenol-chloroform organic phase separation performed very well, successfully enriching known RNA-binding proteins in UV crosslinked samples. The second part of this thesis uses orthogonal organic phase separation to profile changes in the RNA-binding proteome in hepatocellular carcinoma cells experiencing hypoxic stress. Whole proteome profiling was performed alongside this for comparison. Interestingly, western blot on whole cell lysate revealed the RNA modifying enzyme NAT10 to be downregulated in hypoxic conditions. Targeted epitranscriptomic sequencing experiments on a NAT10 target site on rRNA revealed cytidine acetylation to also be reduced upon hypoxia treatment, raising the question of what other RNA modifications could be affected by hypoxia. The third part of this thesis examines cytidine methylation in the context of hypoxia in hepatocellular carcinoma cells. Since there are multiple enzymes that can catalyse the formation of 5-methylcytidine on RNA, I was interested to know which of these enzymes would be dysregulated under hypoxia as this could potentially lead to a new therapeutic target for hepatocellular carcinoma. Using a novel method which I developed to profile the activity of these enzymes towards total RNA, I found that NSUN2 was more enzymatically active during hypoxia even though no changes in protein abundance was observed. Additionally, the activity of the rRNA methyltransferase NSUN1 was downregulated, which is noteworthy given the findings in the second part of this thesis. Taken together, these findings have shed new insights into the role of RNA modifications in the hypoxia response of hepatocellular carcinoma cells. Future work should strive to examine if inhibition of NSUN2 will have a noticeable effect on cancer survival or progression, and investigate the mechanisms underpinning the downregulation of rRNA modifying enzymes NAT10 and NSUN1 in the hopes of identifying other new druggable targets for hepatocellular carcinoma. Doctor of Philosophy 2025-03-06T00:43:35Z 2025-03-06T00:43:35Z 2025 Thesis-Doctor of Philosophy Lee, B. S. T. (2025). Hypoxia alters expression and activity of RNA modifying enzymes targeting cytidine in hepatocellular carcinoma cells. Doctoral thesis, Nanyang Technological University, Singapore. https://hdl.handle.net/10356/182898 https://hdl.handle.net/10356/182898 en This work is licensed under a Creative Commons Attribution-NonCommercial 4.0 International License (CC BY-NC 4.0). application/pdf Nanyang Technological University

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