Genomic profiling of ER+ breast cancers after short-term estrogen suppression reveals alterations associated with endocrine resistance.

نویسندگان

  • Jennifer M Giltnane
  • Katherine E Hutchinson
  • Thomas P Stricker
  • Luigi Formisano
  • Christian D Young
  • Monica V Estrada
  • Mellissa J Nixon
  • Liping Du
  • Violeta Sanchez
  • Paula Gonzalez Ericsson
  • Maria G Kuba
  • Melinda E Sanders
  • Xinmeng J Mu
  • Eliezer M Van Allen
  • Nikhil Wagle
  • Ingrid A Mayer
  • Vandana Abramson
  • Henry Gόmez
  • Monica Rizzo
  • Weiyi Toy
  • Sarat Chandarlapaty
  • Erica L Mayer
  • Jason Christiansen
  • Danielle Murphy
  • Kerry Fitzgerald
  • Kai Wang
  • Jeffrey S Ross
  • Vincent A Miller
  • Phillip J Stephens
  • Roman Yelensky
  • Levi Garraway
  • Yu Shyr
  • Ingrid Meszoely
  • Justin M Balko
  • Carlos L Arteaga
چکیده

Inhibition of proliferation in estrogen receptor-positive (ER+) breast cancers after short-term antiestrogen therapy correlates with long-term patient outcome. We profiled 155 ER+/human epidermal growth factor receptor 2-negative (HER2-) early breast cancers from 143 patients treated with the aromatase inhibitor letrozole for 10 to 21 days before surgery. Twenty-one percent of tumors remained highly proliferative, suggesting that these tumors harbor alterations associated with intrinsic endocrine therapy resistance. Whole-exome sequencing revealed a correlation between 8p11-12 and 11q13 gene amplifications, including FGFR1 and CCND1, respectively, and high Ki67. We corroborated these findings in a separate cohort of serial pretreatment, postneoadjuvant chemotherapy, and recurrent ER+ tumors. Combined inhibition of FGFR1 and CDK4/6 reversed antiestrogen resistance in ER+FGFR1/CCND1 coamplified CAMA1 breast cancer cells. RNA sequencing of letrozole-treated tumors revealed the existence of intrachromosomal ESR1 fusion transcripts and increased expression of gene signatures indicative of enhanced E2F-mediated transcription and cell cycle processes in cancers with high Ki67. These data suggest that short-term preoperative estrogen deprivation followed by genomic profiling can be used to identify druggable alterations that may cause intrinsic endocrine therapy resistance.

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عنوان ژورنال:
  • Science translational medicine

دوره 9 402  شماره 

صفحات  -

تاریخ انتشار 2017