Mutational activation of BRAF confers sensitivity to transforming growth factor beta inhibitors in human cancer cells

نویسندگان

  • Lindsay C. Spender
  • G. John Ferguson
  • Sijia Liu
  • Chao Cui
  • Maria Romina Girotti
  • Gary Sibbet
  • Ellen B. Higgs
  • Morven K. Shuttleworth
  • Tom Hamilton
  • Paul Lorigan
  • Michael Weller
  • David F. Vincent
  • Owen J. Sansom
  • Margaret Frame
  • Peter ten Dijke
  • Richard Marais
  • Gareth J. Inman
چکیده

Recent data implicate elevated transforming growth factor-β (TGFβ) signalling in BRAF inhibitor drug-resistance mechanisms, but the potential for targeting TGFβ signalling in cases of advanced melanoma has not been investigated. We show that mutant BRAFV600E confers an intrinsic dependence on TGFβ/TGFβ receptor 1 (TGFBR1) signalling for clonogenicity of murine melanocytes. Pharmacological inhibition of the TGFBR1 blocked the clonogenicity of human mutant BRAF melanoma cells through SMAD4-independent inhibition of mitosis, and also inhibited metastasis in xenografted zebrafish. When investigating the therapeutic potential of combining inhibitors of mutant BRAF and TGFBR1, we noted that unexpectedly, low-dose PLX-4720 (a vemurafenib analogue) promoted proliferation of drug-naïve melanoma cells. Pharmacological or pharmacogenetic inhibition of TGFBR1 blocked growth promotion and phosphorylation of SRC, which is frequently associated with vemurafenib-resistance mechanisms. Importantly, vemurafenib-resistant patient derived cells retained sensitivity to TGFBR1 inhibition, suggesting that TGFBR1 could be targeted therapeutically to combat the development of vemurafenib drug-resistance.

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عنوان ژورنال:

دوره 7  شماره 

صفحات  -

تاریخ انتشار 2016