Breast Cancer Research (Mar 2023)

Lineage plasticity enables low-ER luminal tumors to evolve and gain basal-like traits

  • Gadisti Aisha Mohamed,
  • Sundis Mahmood,
  • Nevena B. Ognjenovic,
  • Min Kyung Lee,
  • Owen M. Wilkins,
  • Brock C. Christensen,
  • Kristen E. Muller,
  • Diwakar R. Pattabiraman

DOI
https://doi.org/10.1186/s13058-023-01621-8
Journal volume & issue
Vol. 25, no. 1
pp. 1 – 21

Abstract

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Abstract Stratifying breast cancer into specific molecular or histologic subtypes aids in therapeutic decision-making and predicting outcomes; however, these subtypes may not be as distinct as previously thought. Patients with luminal-like, estrogen receptor (ER)-expressing tumors have better prognosis than patients with more aggressive, triple-negative or basal-like tumors. There is, however, a subset of luminal-like tumors that express lower levels of ER, which exhibit more basal-like features. We have found that breast tumors expressing lower levels of ER, traditionally considered to be luminal-like, represent a distinct subset of breast cancer characterized by the emergence of basal-like features. Lineage tracing of low-ER tumors in the MMTV-PyMT mouse mammary tumor model revealed that basal marker-expressing cells arose from normal luminal epithelial cells, suggesting that luminal-to-basal plasticity is responsible for the evolution and emergence of basal-like characteristics. This plasticity allows tumor cells to gain a new lumino-basal phenotype, thus leading to intratumoral lumino-basal heterogeneity. Single-cell RNA sequencing revealed SOX10 as a potential driver for this plasticity, which is known among breast tumors to be almost exclusively expressed in triple-negative breast cancer (TNBC) and was also found to be highly expressed in low-ER tumors. These findings suggest that basal-like tumors may result from the evolutionary progression of luminal tumors with low ER expression.

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