1. Academic Validation
  2. IRX4204 Induces Senescence and Cell Death in HER2-positive Breast Cancer and Synergizes with Anti-HER2 Therapy

IRX4204 Induces Senescence and Cell Death in HER2-positive Breast Cancer and Synergizes with Anti-HER2 Therapy

  • Clin Cancer Res. 2024 Apr 5. doi: 10.1158/1078-0432.CCR-23-3839.
Cassandra L Moyer 1 Amanda Lanier 1 Jing Qian 1 Darian Coleman 2 Jamal Hill 1 Vidyasagar Vuligonda 3 Martin E Sanders 4 Abhijit Mazumdar 1 Powel H Brown 1
Affiliations

Affiliations

  • 1 The University of Texas MD Anderson Cancer Center, Houston, TX, United States.
  • 2 The University of Texas MD Anderson Cancer Center, Houston, Texas, United States.
  • 3 Io Therapeutics, Inc., Spring, Texas, United States.
  • 4 Acousys Biodevices Inc, United States.
Abstract

Purpose: Rexinoids, agonists of nuclear retinoid X receptor (RXR), have been used for the treatment of cancers and are well-tolerated in both Animals and humans. However, the usefulness of rexinoids in treatment of breast Cancer remains unknown. This study examines the efficacy of IRX4204, a highly specific rexinoid, in breast Cancer cell lines and preclinical models to identify a biomarker for response and potential mechanism of action.

Experimental design: IRX4204 effects on breast Cancer cell growth and viability were determined using cell lines, syngeneic mouse models and primary PDX tumors. In vitro assays of cell cycle, Apoptosis, senescence, and lipid metabolism were used to uncover a potential mechanism of action. Standard anti-HER2 therapies were screened in combination with IRX4204 on a panel of breast Cancer cell lines to determine drug synergy.

Results: IRX4204 significantly inhibits the growth of HER2-positive breast Cancer cell lines, including trastuzumab and lapatinib resistant JIMT-1 and HCC1954. Treatment with IRX4204 reduced tumor growth rate in the MMTV-ErbB2 mouse and HER2-positive PDX model by 49% and 44% respectively. Mechanistic studies revealed IRX4204 modulates lipid metabolism and induces senescence of HER2-positive cells. In addition, IRX4204 demonstrates additivity and synergy with HER2 targeted monoclonal Antibodies, tyrosine kinase inhibitors, and antibody drug conjugates.

Conclusions: These findings identify HER2 as a biomarker for IRX4204 treatment response and demonstrate a novel use of RXR agonists to synergize with current anti-HER2 therapies. Furthermore, our results suggest that RXR agonists can be useful for the treatment of anti-HER2 resistant and metastatic HER2-positive breast Cancer.

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