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High expression of SLC20A1 is less effective for endocrine therapy and predicts late recurrence in ER-positive breast cancer

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  • Chotaro Onaga
  • Shoma Tamori
  • Izumi Matsuoka
  • Ayaka Ozaki
  • Hitomi Motomura
  • Yuka Nagashima
  • Tsugumichi Sato
  • Keiko Sato
  • Yuyun Xiong
  • Kazunori Sasaki
  • Shigeo Ohno
  • Kazunori Akimoto

Abstract

Estrogen receptor-positive (ER+) breast cancer intrinsically confers satisfactory clinical outcomes in response to endocrine therapy. However, a significant proportion of patients with ER+ breast cancer do not respond well to this treatment. Therefore, to evaluate the effects of endocrine therapy, there is a need for identification of novel markers that can be used at the time of diagnosis for predicting clinical outcomes, especially for early-stage and late recurrence. Solute carrier family 20 member 1 (SLC20A1) is a sodium/inorganic phosphate symporter that has been proposed to be a viable prognostic marker for the luminal A and luminal B types of ER+ breast cancer. In the present study, we examined the possible association of SLC20A1 expression with tumor staging, endocrine therapy and chemotherapy in the luminal A and luminal B subtypes of breast cancer. In addition, we analyzed the relationship between SLC20A1 expression and late recurrence in patients with luminal A and luminal B breast cancer following endocrine therapy. We showed that patients with higher levels of SLC20A1 expression (SLC20A1high) exhibited poorer clinical outcomes in those with tumor stage I luminal A breast cancer. In addition, this SLC20A1high subgroup of patients exhibited less responses to endocrine therapy, specifically in those with the luminal A and luminal B subtypes of breast cancer. However, patients with SLC20A1high showed good clinical outcomes following chemotherapy. Patients tested to be in the SLC20A1high group at the time of diagnosis also showed a higher incidence of recurrence compared with those with lower expression levels of SLC20A1, at >15 years for luminal A breast cancer and at 10–15 years for luminal B breast cancer. Therefore, we conclude that SLC20A1high can be used as a prognostic biomarker for predicting the efficacy of endocrine therapy and late recurrence for ER+ breast cancer.

Suggested Citation

  • Chotaro Onaga & Shoma Tamori & Izumi Matsuoka & Ayaka Ozaki & Hitomi Motomura & Yuka Nagashima & Tsugumichi Sato & Keiko Sato & Yuyun Xiong & Kazunori Sasaki & Shigeo Ohno & Kazunori Akimoto, 2022. "High expression of SLC20A1 is less effective for endocrine therapy and predicts late recurrence in ER-positive breast cancer," PLOS ONE, Public Library of Science, vol. 17(5), pages 1-22, May.
    • Handle: RePEc:plo:pone00:0268799
    DOI: 10.1371/journal.pone.0268799
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    1. Bernard Pereira & Suet-Feung Chin & Oscar M. Rueda & Hans-Kristian Moen Vollan & Elena Provenzano & Helen A. Bardwell & Michelle Pugh & Linda Jones & Roslin Russell & Stephen-John Sammut & Dana W. Y. , 2016. "The somatic mutation profiles of 2,433 breast cancers refine their genomic and transcriptomic landscapes," Nature Communications, Nature, vol. 7(1), pages 1-16, September.
    2. Bernard Pereira & Suet-Feung Chin & Oscar M. Rueda & Hans-Kristian Moen Vollan & Elena Provenzano & Helen A. Bardwell & Michelle Pugh & Linda Jones & Roslin Russell & Stephen-John Sammut & Dana W. Y. , 2016. "Erratum: The somatic mutation profiles of 2,433 breast cancers refine their genomic and transcriptomic landscapes," Nature Communications, Nature, vol. 7(1), pages 1-1, September.
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