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Inhibition of BRAF(V600E) Relieves IL-1– mediated T Cell Suppression

Forums Cutaneous Melanoma Community Inhibition of BRAF(V600E) Relieves IL-1– mediated T Cell Suppression

  • Post
    JerryfromFauq
    Participant

      Inhibition of BRAF(V600E) Relieves IL-1– mediated T Cell Suppression by
      Melanoma Tumor-associated Fibroblasts
      Jahan S. Khalili, Shujuan Liu, Tania G. Rodríguez-Cruz, Mayra Whittington, Seth Wardell, Chengwen
      Liu, Jieqing Chen, Minying Zhang, Yufeng Li, Richard W. Joseph, Suhendan Ekmekcioglu, Elizabeth
      Grimm, Laszlo G. Radvanyi, Michael A. Davies, Patrick Hwu and Gregory Lizée
      The BRAF oncogene demonstrates a characteristic mutation (V600E) in a significant fraction of
      cutaneous melanomas, leading to constitutive activation of the MAP kinase pathway. This genetic
      lesion endows tumor cells with proliferative and survival advantages, and metastatic melanoma patients
      treated with the BRAF(V600E)-specific inhibitor vemurafenib have shown dramatic clinical responses.
      Here, we show that BRAF(V600E) induces transcription of the IL-1α and IL-1β genes in both
      melanocytes and melanoma cell lines and that this upregulation is specifically abrogated by targeted
      BRAF(V600E) inhibitors. Furthermore, treatment of melanoma tumor-associated fibroblasts (TAFs) with
      IL-1α/β significantly enhanced the ability of TAFs to suppress the proliferation and function of
      melanoma antigen-specific cytotoxic T cells. IL-1α/β treatment of TAFs upregulated multiple
      immunosuppressive factors, including COX-2 and the PD-1 ligands PD-L1 and PD-L2. Specific
      BRAF(V600E) inhibitors largely abrogated the ability of melanoma cells to confer T cell-suppressive
      properties on TAFs. These results support a model in which BRAF(V600E) promotes immune
      suppression in the melanoma tumor environment through an IL-1-mediated mechanism involving
      resident stromal fibroblasts. Based on these findings, combination therapies involving targeted BRAF
      inhibition and T cell based immunotherapies are warranted.

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        boot2aboot
        Participant

          Interesting article…Moffitt reported that fibroblasts (regenerative cells) in tumor cells cause regenisis after braf drugs fail…hmmm…makes me wonder if i should work my way down the ras pathway or go another route…

          boot2aboot
          Participant

            Interesting article…Moffitt reported that fibroblasts (regenerative cells) in tumor cells cause regenisis after braf drugs fail…hmmm…makes me wonder if i should work my way down the ras pathway or go another route…

            boot2aboot
            Participant

              Interesting article…Moffitt reported that fibroblasts (regenerative cells) in tumor cells cause regenisis after braf drugs fail…hmmm…makes me wonder if i should work my way down the ras pathway or go another route…

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