# Overcoming adaptive feedback resistance to KRAS inhibition in colorectal cancer

> **NIH NIH R01** · MASSACHUSETTS GENERAL HOSPITAL · 2022 · $728,990

## Abstract

Project Summary/Abstract
Although KRAS is mutated in 20% of all cancers and 40% of colorectal cancer (CRC), it has long been
considered an “undruggable” target 1. Recently, novel covalent inhibitors selective for KRASG12C have entered
the clinic, offering the unprecedented opportunity to target KRAS directly, and other mutation-specific KRAS
inhibitors (i.e. G12D) are under development 2,3. However, prior efforts to target the RAS-MAPK pathway have
been hampered by adaptive feedback, which drives pathway reactivation and resistance, particularly in CRC.
For example, BRAF inhibition in BRAFV600 CRC leads to loss of ERK-dependent negative feedback and RTK-
mediated pathway reactivation, leading to response rates of only ~5%, compared to ~35% in lung cancer and
>50% in melanoma 4,5. Similarly, while early clinical data with KRASG12C inhibitors show promising response rates
of >35% in lung cancer, response rates in CRC appear much lower (~10%) with limited durability, suggesting a
similar mode of adaptive resistance may be operant in KRASG12C CRC 2,3. In support of this hypothesis, our
preliminary studies have suggested that robust adaptive feedback signals lead to rapid pathway reactivation and
lack of response in KRASG12C CRC models 6. However, prior studies in BRAFV600 CRC—including preclinical and
clinical collaborations between Drs. Corcoran and Kopetz—have demonstrated that combination therapies
targeting adaptive feedback signaling (e.g. EGFR) can improve clinical outcome, with the first such combination
FDA-approved this year (Corcoran et al, Cancer Discovery 2018; Kopetz et al, NEJM, 2019)7-10. Similarly, our
preliminary data support the importance of targeting adaptive feedback in KRASG12C CRC, but suggest complex
feedback signaling that will require strategies beyond targeting EGFR to optimize outcome.
Here, we propose to define the key mechanisms of resistance to KRAS inhibition in CRC and devise therapeutic
strategies to overcome resistance. To accomplish this goal, we propose to leverage a unique collection of ~100
patient-derived CRC organoids and a bank of ~300 CRC PDXs, generated through the MGH/MIT/Broad U54
DRSC and the MDACC U54 PDXNet teams, respectively. We will deploy these novel tools to comprehensively
map the adaptive feedback response to KRASG12C inhibition in vivo using clinically-relevant PDX and patient-
derived organoid xenografts (PDOX) CRC models. In parallel, we will model the evolution of resistance in vivo
to evaluate the potential role of RTK plasticity in driving resistance to specific KRAS inhibitor combinations and
will identify candidate mechanisms of acquired resistance through genomic analysis of serial tumor biopsies and
cfDNA from CRC patients on KRAS inhibitor combination trials. Utilizing this enhanced mechanistic
understanding, we will devise and test novel therapeutic strategies in vivo in our patient-derived models.

## Key facts

- **NIH application ID:** 10440792
- **Project number:** 1R01CA262805-01A1
- **Recipient organization:** MASSACHUSETTS GENERAL HOSPITAL
- **Principal Investigator:** Ryan Bruce Corcoran
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2022
- **Award amount:** $728,990
- **Award type:** 1
- **Project period:** 2022-04-01 → 2027-03-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10440792

## Citation

> US National Institutes of Health, RePORTER application 10440792, Overcoming adaptive feedback resistance to KRAS inhibition in colorectal cancer (1R01CA262805-01A1). Retrieved via AI Analytics 2026-05-22 from https://api.ai-analytics.org/grant/nih/10440792. Licensed CC0.

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