# Elucidating and Leveraging the mTOR Negative Feedback Pathway in Breast Cancer

> **NIH NIH R01** · CLEVELAND CLINIC LERNER COM-CWRU · 2020 · $304,945

## Abstract

PROJECT SUMMARY
Targeted therapies have considerably improved survival from many cancers, including breast cancer. A major
limitation of such therapies is resistance that occurs as a consequence of the extreme molecular evolution and
adaptability of tumor cells. For targeted therapies to achieve their full potential of inducing sustained cures,
they must be paired with additional agents that preclude activation of alternative growth and survival pathways.
Identifying the most appropriate combinations requires a concerted effort to uncover mechanisms underlying
activation of compensatory pathways. The PI3K/AKT/mTOR pathway is commonly activated in breast cancer.
This proposal focuses on discovering new intermediaries of this signaling loop that can be targeted to improve
the efficacy of mTOR inhibitors. Of the two mTOR complexes, rapalogs inhibit mTORC1 and protein
translation. As single agents, rapalogs have limited efficacy in breast cancer, primarily due to feedback
activation of AKT and induction of survival signals. Inhibitors of both mTORC1 and mTORC2 also cause AKT
activation. Lastly, while dual inhibitors of PI3K and mTOR block this feedback pathway, they suffer from dose-
limiting toxicities. These outcomes indicate that strictly targeting PI3K/AKT/mTOR is insufficient. We postulate
that discerning the key elements within the negative feedback pathway that extends from mTOR to AKT will
reveal novel targetable proteins for impeding rebound activation of AKT in response to mTOR inhibition. This
should improve therapeutic outcomes without increasing toxicity. We used a computational method to reveal
dasatinib, an inhibitor of Src Family Kinases (SFK) and Abl kinase, as a drug that may be highly synergistic
with rapalogs. In breast cancer cells, dasatinib completely blocked the rebound activation of AKT that occurred
with the rapalog, rapamycin. These two drugs also synergistically inhibited growth of triple negative breast
cancer cells in vitro, and elicited tumor regression in multiple mouse models of breast cancer. These and other
data revealed that at least one SFK resides within the pathway leading from mTOR to AKT and suggests that
dual mTOR/SFK inhibition may be a novel approach to curtail resistance to mTOR inhibitors. Using phospho-
proteomics and transcriptomics, we also found that focal adhesion signaling may be a major gateway for
mTOR negative feedback signaling to AKT. We propose three aims to address these possibilities. In Aim 1, we
will assess whether simultaneous blockade of SFKs and mTOR inhibits growth of patient derived xenografts of
breast cancers as well as tumors that are resistant to current targeted therapies for HER2 and estrogen
receptor. In Aim 2, we will interrogate the role of focal adhesion signaling in mediating mTOR feedback with the
goal of leveraging this pathway for therapeutic benefit. Lastly, Aim 3 will uncover molecular signatures of
resistance to mTOR/SFK inhibitors with the goal of revealing additiona...

## Key facts

- **NIH application ID:** 10278978
- **Project number:** 7R01CA213843-05
- **Recipient organization:** CLEVELAND CLINIC LERNER COM-CWRU
- **Principal Investigator:** RUTH A. KERI
- **Activity code:** R01 (R01, R21, SBIR, etc.)
- **Funding institute:** NIH
- **Fiscal year:** 2020
- **Award amount:** $304,945
- **Award type:** 7
- **Project period:** 2017-08-01 → 2022-07-31

## Primary source

NIH RePORTER: https://reporter.nih.gov/project-details/10278978

## Citation

> US National Institutes of Health, RePORTER application 10278978, Elucidating and Leveraging the mTOR Negative Feedback Pathway in Breast Cancer (7R01CA213843-05). Retrieved via AI Analytics 2026-05-23 from https://api.ai-analytics.org/grant/nih/10278978. Licensed CC0.

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