# Comprehensive atlas of advanced adenomas and their surrounding primed colon: A multi-omics evaluation and clinical impact assessment

> **NIH NIH U54** · FRED HUTCHINSON CANCER CENTER · 2024 · $467,151

## Abstract

SUMMARY
Colon adenomas account for 80-85% of the CRC precancerous lesions and can progress to CRC. Yet, the
majority of these early lesions remain in an indolent early state, and only 5-10% are aggressive and progress to
CRC. Although the adenoma progression sequence was initially proposed to be driven mainly by the serial
accumulation of gene mutations and epigenetic alterations in colon epithelial cells, based on increasingly detailed
analyses of the ‘cancer-causing’ alterations that characterize CRC, it has becoming apparent that these same
alterations can also be found in indolent adenomas and even in the histologically normal colon epithelium. These
observations indicate that DNA alterations alone are not sufficient to drive adenoma progression. Emerging
studies indicate that factors that mediate adenoma progression can be derived from histologically normal colon
tissue ‘primed’ to foster adenoma progression into cancer. We hypothesize that the adenoma progression is
driven by both cell-autonomous and non-autonomous mechanisms and the ‘primed’ colon promotes adenoma
progression by providing a permissive tissue environment. We further hypothesize that the distinct features of
a ‘primed’ colon may be developed as biomarkers to predict the likelihood of adenoma progression to cancer.
AIM 1A: To identify molecular signatures of adenoma progression (‘aggressive’ or ‘indolent’) by performing a
mutli-omics evaluation of a unique collection of adenomas followed longitudinally with defined progression
outcomes; AIM 1B: To determine the ‘aggressiveness’ of adenomas in an independent cohort using the
molecular signature of progression derived from Aim 1A.
AIM 2: To directly determine the distinct features of a ‘primed’ colon that associate with adenoma progression.
(1) increased senescent fibroblast load and associated SASP factor expression; (2) oncogenic immune
microenvironment; (3) increased cancer driver gene mutation burden; (4) altered CRC associated methylome,
and (5) the dysbiotic CRC-associated microbiome state.
AIM 3A: To identify and evaluate DNA methylation-based tissue biomarkers to determine whether they predict
the risk of aggressive adenoma occurrence using a highly precise and sensitive droplet digital PCR method.
AIM 3B: To determine if the cancer driver gene mutation burden in the primed colon associates with aggressive
adenoma occurrence using a high fidelity and ultra-deep sequencing method.
This translational Project 1 will provide an unprecedented high-quality characterization of the early lesion and
the surrounding primed colon that enables its progression. This project aligns with the expertise of the
investigators involved, the access to precious sample biorepositories and the infrastructure provided by the U54
mechanism. The significance findings from Project 1 will be functionally interrogated in Project 2&3 and other
U54 projects, leading to an iterative process to advance our understanding of the adenoma biology and the
de...

## Key facts

- **NIH application ID:** 10926951
- **Project number:** 5U54CA274374-03
- **Recipient organization:** FRED HUTCHINSON CANCER CENTER
- **Principal Investigator:** William Mallory Grady
- **Activity code:** U54 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2024
- **Award amount:** $467,151
- **Award type:** 5
- **Project period:** 2022-09-20 → 2027-08-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10926951

## Citation

> US National Institutes of Health, RePORTER application 10926951, Comprehensive atlas of advanced adenomas and their surrounding primed colon: A multi-omics evaluation and clinical impact assessment (5U54CA274374-03). Retrieved via AI Analytics 2026-05-24 from https://api.ai-analytics.org/grant/nih/10926951. Licensed CC0.

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