# Inflammation Induced Cytosine Deamination and the Initiation of Cancer

> **NIH NIH F30** · UNIVERSITY OF TEXAS MED BR GALVESTON · 2020 · $35,055

## Abstract

PROJECT SUMMARY/ABSTRACT
Cancer remains one of the leading causes of death in the United States and worldwide with more than 8.8
million cancer related deaths each year. To reduce this public health burden, investigation of the most
commonly observed substitution mutation, a cytosine to thymine transition, is crucial. An example of this
predominance is evident in inflammation driven colitis associated colorectal cancer (CAC). Development of
CAC involves an early critical p53 mutation dominated by cytosine to thymine transitions at 5’ cytosine, 3’
guanine (CpG) dinucleotides. These mutations arise from 5-methylcytosine deamination into thymine, forming
a T:G mispaired intermediate. Subsequent replication propagates the mutation to the opposing strand, forming
a T:A base pair. Although mutations in p53 have been demonstrated at the time of CAC diagnosis, little has
been done to detect the exact location of low frequency mutations and mispaired intermediates in
noncancerous tissues. It is also unknown how long a mutation is present before cancer diagnosis or how
inflammatory conditions can promote cytosine to thymine transitions. Current sequencing methodologies
involving standard PCR mask the presence of rare but potentially important mutations because amplification
exponentially increases the predominant sequence and reports only that sequence. To solve these
unanswered questions, we aim to mechanistically determine how inflammation increases the rate of these
critical mutations and develop novel methods to detect low frequency mispaired intermediates and mutations.
Given the critical role of inflammation in the etiology of CAC, we hypothesize that inflammation increases the
number of mutations by providing substrates for competing DNA repair pathways and that an inflammatory
environment will greatly increase the number of mutations and mispaired intermediates which leads to cancer
development. We will address this hypothesis by first proving our mechanistic hypothesis of competing DNA
repair and then developing methods to determine the number of global mispaired intermediates at a p53
mutation hotspot, described through three Specific Aims: 1) determine a potential mechanism by which
inflammatory mediators can induce characteristic cytosine to thymine transitions; 2) design a novel
glycosylase-mass spectrometry assay to measure global levels of mispaired intermediates and determine how
inflammation affects mispaired intermediate production; and 3) develop a novel method to scan p53 exon 7 for
cytosine deamination mutations and mispaired intermediates. By measuring low frequency mispaired
intermediates and mutations long before tumor formation, we will be able to estimate the number of cells in a
population that contains critical mutation and predict its prior DNA damage history. The mechanistic studies will
elucidate the role of inflammation on the beginning stages of tumorigenesis, and together, the results of this
proposal could lead to novel t...

## Key facts

- **NIH application ID:** 9928010
- **Project number:** 5F30CA225116-03
- **Recipient organization:** UNIVERSITY OF TEXAS MED BR GALVESTON
- **Principal Investigator:** Chia Wei Hsu
- **Activity code:** F30 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $35,055
- **Award type:** 5
- **Project period:** 2018-07-01 → 2022-06-30

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9928010

## Citation

> US National Institutes of Health, RePORTER application 9928010, Inflammation Induced Cytosine Deamination and the Initiation of Cancer (5F30CA225116-03). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/9928010. Licensed CC0.

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