Abstract 17P
Background
Esophageal adenocarcinoma (EAC) is a lethal cancer type rapidly increasing worldwide. Overexpression of the human epidermal growth factor receptor 2 (HER2) occurs in approximately one third of patients. However, small-molecule tyrosine kinase inhibitors, like lapatinib, show limited clinical benefits due to fast-developed drug unresponsiveness. The evolutionary driver of resistance remains largely unknown.
Methods
We generated reversible drug-tolerant persister and stable resistant cell lines through short- and long-term drug exposure. Time-course matched ATAC-seq and RNA-seq analysis were performed to dynamically decipher drivers for resistance development. Functional validation in vitro and in vivo using genetic and pharmacological approaches was conducted in both drug-sensitive and resistant cells. Furthermore, we detected the metabolic spectrum via flow cytometry and compared metabolic vulnerability through pharmacological disruption of critical enzymes involved between sensitive and resistant cells.
Results
Integrated multi-omics analysis revealed a high degree of NRF2 dependency during resistance acquisition. Inhibition of NRF2 incapacitated drug-tolerant persister development, and both naturally occurring and developed resistant cell lines showed consistent vulnerability to NRF2 inhibition. Conversely, NRF2 overexpression/activation promoted survival of sensitive cell lines from lapatinib toxicity by reprogramming metabolism to glutathione. Glutathione precursor supplementation rescued sensitive cells from lapatinib treatment, while disrupting the glutathione-conversion enzyme, GPX4, rapidly triggered cell death in resistant cell lines. In vivo, NRF2 inhibitor substantially suppressed the growth of lapatinib-resistant EAC xenografts, but tumor growth persisted in lapatinib-sensitive EAC-bearing mice, confirming the NRF2 vulnerability.
Conclusions
NRF2 is essential for acquiring resistance to ERBB2 inhibition, and it promotes a switch to glutathione dependency. These results offer a promising opportunity to tackle cellular adaptation and ensuing drug resistance in incurable EAC.
Editorial acknowledgement
Clinical trial identification
Legal entity responsible for the study
The authors.
Funding
Wellcome Trust.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
125P - Combination of navitoclax with alpelisib and trametinib to synergistically impair cell viability in high-grade ovarian cancer
Presenter: Lisa Wozelka-Oltjan
Session: Cocktail & Poster Display session
Resources:
Abstract
126P - Effect of sequential antitumoral treatment with immune checkpoint blockade and tyrosine kinase inhibitors in hepatocellular carcinoma
Presenter: Vincenza Ciaramella
Session: Cocktail & Poster Display session
Resources:
Abstract
127P - Novel bone-targeting of activatable sirolimus for targeted therapy of bone-resident cancers
Presenter: Alistare Sadra
Session: Cocktail & Poster Display session
Resources:
Abstract
128P - Network medicine approach identifies small molecule drugs as immune checkpoint inhibitors repurposable for rectal cancer
Presenter: Faheem Ahmed
Session: Cocktail & Poster Display session
Resources:
Abstract
129P - Repurposing existing therapies for adrenal cancer: Unlocking new possibilities
Presenter: Anupama Samantasinghar
Session: Cocktail & Poster Display session
Resources:
Abstract
130P - Restoration of the mutant p53 protein upon treatment with small molecule modulators
Presenter: Elvina Gilyazova
Session: Cocktail & Poster Display session
Resources:
Abstract
131P - Trop 2 and its overexpression in metastatic colorectal cancer patients (mCRCp): Biological, clinical and therapeutic implications
Presenter: Andrea Mancuso Petricca
Session: Cocktail & Poster Display session
Resources:
Abstract
132P - Novel small molecule modulators for activation of mutant tumor suppressor p53
Presenter: Damir Davletshin
Session: Cocktail & Poster Display session
Resources:
Abstract
133P - Cytotoxic efficacy of artificial vesicles obtained from CAR-T cells by ultrasonication
Presenter: Ekaterina Zmievskaya
Session: Cocktail & Poster Display session
Resources:
Abstract
134P - Doxorubicin and olaparib (OLA) synergism in high-grade serous ovarian (HGOC) and triple-negative breast cancer (TNBC) cell lines with olaparib-resistance
Presenter: Jose Alejandro Perez Fidalgo
Session: Cocktail & Poster Display session
Resources:
Abstract