Targeting HSP90-HDAC6 Regulating Network Implicates Precision Treatment of Breast Cancer

نویسندگان

  • Shiyi Yu
  • Xiuxiu Cai
  • Chenxi Wu
  • Yan Liu
  • Jun Zhang
  • Xue Gong
  • Xin Wang
  • Xiaoli Wu
  • Tao Zhu
  • Lin Mo
  • Jun Gu
  • Zhenghong Yu
  • Jinfei Chen
  • Jean Paul Thiery
  • Renjie Chai
  • Liming Chen
چکیده

Breast cancer is the leading cause of women death. Heat shock protein 90 (HSP90) and Histone deacetylase 6 (HDAC6) are promising anti-cancer drug targets. However, it's still unclear the applicability of anti-HSP90 and anti-HDAC6 strategies in precision treatment of breast cancer. In current study, we found that triple negative breast cancer (TNBC) cells, compared to T47D, an ERα+ breast cancer cell line, exhibited 7~40 times lower IC50 values, stronger cell cycle perturbation, increased cell apoptosis and stronger inhibition of cell migration upon 17-DMAG treatment, while T47D, compared to TNBC cells, expressed higher HDAC6 and showed stronger anti-cancer response upon treatment of Tubacin. Mechanically, 17-DMAG treatment inhibited a complex network consists at least ERK, AKT, and Hippo pathway in TNBC cells, and higher expression of HDAC6 inhibited HSP90 activity via deacetylating HSP90. Furthermore, we found higher HDAC6 expression level in tamoxifen-resistance T47D than that in T47D, and Tubacin treatment suppressed the growth of tamoxifen-resistant cells in vivo. Our data suggested that anti-HSP90 and anti-HDAC6 are promising strategies to treat TNBC and ERα+ breast cancers respectively, and anti-HDAC6 can be considered during treatment of tamoxifen-resistance breast cancers.

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عنوان ژورنال:

دوره 13  شماره 

صفحات  -

تاریخ انتشار 2017