# Project 4: The role of codon bias in RAS tumorigenesis

> **NIH NIH P01** · UNIV OF NORTH CAROLINA CHAPEL HILL · 2020 · $667,732

## Abstract

ABSTRACT 
The RAS family of genes, comprised of KRAS, NRAS, and HRAS, are mutated in upwards of a third of 
all human cancers, yielding proteins that remain in a constitutively active, oncogenic state that are well 
established to cause this disease. The proteins encoded by these three genes are nearly identical, 
activated by and signal through the same proteins, and capable of causing cancer in mice. Despite this 
uniformity, KRAS is the most commonly mutated of the three, and the type of mutations in KRAS, as well 
as the other RAS genes, varies extensively in human cancers. To understand these phenomena, we 
compared the nucleotide sequence of the RAS genes, finding that KRAS has many rare codons that limit 
protein expression, HRAS has many common codons that foster protein expression, while NRAS has a 
mixture of rare and common codons and intermediate protein expression. Focusing on KRAS, the most 
commonly mutated RAS gene, we show that introducing silent mutations to convert rare codons to 
common in one exon of this gene reduced both the number of lung tumors and the mutations detected in 
Kras of mice exposed to a carcinogen. To determine the mechanism responsible for this result, in aim 1 
we will activate an inducible oncogenic Kras gene with common codons in the lungs of mice to identify 
the stage of tumorigenesis sensitive to perturbing the inherent rare codon bias of Kras. Once identified, 
we will then hone in on the cellular feature changed, and in turn, the molecular response underlying this 
effect. Converting rare codons to common also altered the type of oncogenic mutations recovered in 
Kras after carcinogen exposure. To determine the underlying mechanism, in aim 2 we will similarly 
engineer mice with an inducible Kras gene encoded by common versus native codons with different 
oncogenic mutations. As above, these Kras alleles will be activated in the lungs of mice to determine 
how different oncogenic mutations in the backdrop of altered codon usage impacts tumorigenesis, tumor 
cell characteristics, and cellular signaling. Completion of these two aims will elucidate the mechanism by 
which codon bias influences the frequency and type of mutations arising in Kras during tumorigenesis. 
Despite the advantage afforded to Kras by rare codons in early tumorigenesis, we show that established 
cancer cells overcome the poor translation of Kras mRNA imposed by rare codons to increase Kras 
protein expression, which was linked to increased tumorigenic activity and resistance to 
chemotherapeutics. To identify how cancer cells achieve this feat, we screened for and identified codon- 
dependent modifiers of oncogenic Ras in the model organism Drosophila. We will capitalize on these 
candidate modifiers in aim 3 to elucidate how cancer cells overcome poor translation of Kras, and in turn, 
whether such changes promote more malignant phenotypes. In summary, this research will reveal how 
this novel feature of KRAS, codon bias, impac...

## Key facts

- **NIH application ID:** 9982075
- **Project number:** 5P01CA203657-05
- **Recipient organization:** UNIV OF NORTH CAROLINA CHAPEL HILL
- **Principal Investigator:** CHRISTOPHER M COUNTER
- **Activity code:** P01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $667,732
- **Award type:** 5
- **Project period:** — → 2022-05-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/9982075

## Citation

> US National Institutes of Health, RePORTER application 9982075, Project 4: The role of codon bias in RAS tumorigenesis (5P01CA203657-05). Retrieved via AI Analytics 2026-05-23 from https://api.ai-analytics.org/grant/nih/9982075. Licensed CC0.

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