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Mechanisms of BRAF Inhibitor Resistance in Metastatic Melanoma

Forums General Melanoma Community Mechanisms of BRAF Inhibitor Resistance in Metastatic Melanoma

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    lou2
    Participant

      Mechanisms of BRAF Inhibitor Resistance in Metastatic Melanoma

       

      Clin. Cancer Res 2014 Jan 24;[EPub Ahead of Print], H Rizos, AM Menzies, GM Pupo, MS Carlino, C Fung, J Hyman, LE Haydu, B Mijatov, TM Becker, SC Boyd, J Howle, S Robyn, JF Thompson, RF Kefford, RA Scolyer, GV Long

      Research · February 06, 2014
       
       
       

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      ABSTRACT


      Clinical Cancer Research

      BRAF Inhibitor Resistance Mechanisms in Metastatic Melanoma; Spectrum and Clinical Impact

      Clin. Cancer Res 2014 Jan 24;[EPub Ahead of Print], H Rizos, AM Menzies, GM Pupo, MS Carlino, C Fung, J Hyman, LE Haydu, B Mijatov, TM Becker, SC Boyd, J Howle, S Robyn, JF Thompson, RF Kefford, RA Scolyer, GV Long

       

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        NYKaren
        Participant

          Please help me understand this. Are they saying that people who progress after BRAF/MEK therapy have a lesser chance of responding to targeted therapy?  I.e PD1?

          thanks, 

          karen

          NYKaren
          Participant

            Please help me understand this. Are they saying that people who progress after BRAF/MEK therapy have a lesser chance of responding to targeted therapy?  I.e PD1?

            thanks, 

            karen

            NYKaren
            Participant

              Please help me understand this. Are they saying that people who progress after BRAF/MEK therapy have a lesser chance of responding to targeted therapy?  I.e PD1?

              thanks, 

              karen

                POW
                Participant

                  It is my understanding that  now-a-days the term "targeted" therapy refers to chemical drugs like vemurafenib and trametinib that are deliberately designed to bind to and inhibit a "target" molecule. The BRAF and MEK inhibitors fall into this category. The term "immunotherapy" is now used to refer to general (usually naturally-occuring)  immune system regulators like IL-2 and interferon. The term "check point therapy" is now used to refer to treatments (usually monocloncal antibodies) that stimulate or block very specific T-cell subpopulations like helper T cells and cytotoxic T cells. Ipi, anti-PD1 and anti-PDL1 are all check point therapies; this article is not talking about them.  

                  POW
                  Participant

                    It is my understanding that  now-a-days the term "targeted" therapy refers to chemical drugs like vemurafenib and trametinib that are deliberately designed to bind to and inhibit a "target" molecule. The BRAF and MEK inhibitors fall into this category. The term "immunotherapy" is now used to refer to general (usually naturally-occuring)  immune system regulators like IL-2 and interferon. The term "check point therapy" is now used to refer to treatments (usually monocloncal antibodies) that stimulate or block very specific T-cell subpopulations like helper T cells and cytotoxic T cells. Ipi, anti-PD1 and anti-PDL1 are all check point therapies; this article is not talking about them.  

                    POW
                    Participant

                      It is my understanding that  now-a-days the term "targeted" therapy refers to chemical drugs like vemurafenib and trametinib that are deliberately designed to bind to and inhibit a "target" molecule. The BRAF and MEK inhibitors fall into this category. The term "immunotherapy" is now used to refer to general (usually naturally-occuring)  immune system regulators like IL-2 and interferon. The term "check point therapy" is now used to refer to treatments (usually monocloncal antibodies) that stimulate or block very specific T-cell subpopulations like helper T cells and cytotoxic T cells. Ipi, anti-PD1 and anti-PDL1 are all check point therapies; this article is not talking about them.  

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