AI Article Synopsis
- Epigenetic changes play a significant role in breast cancer progression, particularly in the aggressive subtype known as triple-negative breast cancer (TNBC), where EZH2 is identified as a key epigenetic modulator.
- Inhibiting EZH2 can reduce the ability of cancer cells to spread and also helps them adopt a less aggressive, more treatable state by promoting the expression of GATA3, making them more responsive to hormone therapies.
- The research highlights that certain subtypes of TNBC, especially EZH2 basal-like 1 and mesenchymal subtypes, are particularly sensitive to EZH2 inhibition, suggesting the potential for EZH2-targeted therapies in treating metastatic TNBC.
Article Abstract
Epigenetic changes are increasingly being appreciated as key events in breast cancer progression. However, breast cancer subtype-specific epigenetic regulation remains poorly investigated. Here we report that EZH2 is a leading candidate of epigenetic modulators associated with the TNBC subtype and that it predicts poor overall survival in TNBC patients. We demonstrate that specific pharmacological or genetic inhibition of EZH2 catalytic activity impairs distant metastasis. We further define a specific EZH2 population with enhanced invasion, mammosphere formation, and metastatic potential that exhibits marked sensitivity to EZH2 inhibition. Mechanistically, EZH2 inhibition differentiates EZH2 basal cells to a luminal-like phenotype by derepressing GATA3 and renders them sensitive to endocrine therapy. Furthermore, dissection of human TNBC heterogeneity shows that EZH2 basal-like 1 and mesenchymal subtypes have exquisite sensitivity to EZH2 inhibition compared with the EZH2 luminal androgen receptor subtype. These preclinical findings provide a rationale for clinical development of EZH2 as a targeted therapy against TNBC metastasis.
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| http://dx.doi.org/10.1016/j.celrep.2019.12.056 | DOI Listing |
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