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Predictors of ACT response

Forums General Melanoma Community Predictors of ACT response

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    JerryfromFauq
    Participant

      Specific Lymphocyte Subsets Predict Response to Adoptive Cell Therapy using Expanded
      Autologous Tumor-infiltrating Lymphocytes in Metastatic Melanoma Patients
      Chantale Bernatchez1, Rahmatu Mansaray3, Orenthial J. Fulbright3, Christopher Toth3, Renjith
      Ramachandran3, Seth Wardell3, Minying Zhang1, Jessica Chacon1, Richard Wu1, Priscilla Miller1, Sandy
      Mahoney1, Gladys Alvarado1, Michelle Glass1, Peter Thall2, Patricia Fox2, Roland Bassett2, John D.
      McMannis3, Elizabeth Shpall3, Victor Prieto4, Nicholas Papadopoulos1, Kevin Kim1, Jade Homsi1, Agop

      Specific Lymphocyte Subsets Predict Response to Adoptive Cell Therapy using Expanded
      Autologous Tumor-infiltrating Lymphocytes in Metastatic Melanoma Patients
      Chantale Bernatchez1, Rahmatu Mansaray3, Orenthial J. Fulbright3, Christopher Toth3, Renjith
      Ramachandran3, Seth Wardell3, Minying Zhang1, Jessica Chacon1, Richard Wu1, Priscilla Miller1, Sandy
      Mahoney1, Gladys Alvarado1, Michelle Glass1, Peter Thall2, Patricia Fox2, Roland Bassett2, John D.
      McMannis3, Elizabeth Shpall3, Victor Prieto4, Nicholas Papadopoulos1, Kevin Kim1, Jade Homsi1, Agop
      Bedikian1, Wen-Jen Hwu1, Sapna Patel1, Merrick I. Ross5, Jeffrey E. Lee5, Jeffrey E. Gershenwald5,
      Anthony Lucci5, Richard Royal5, Janice Cormier5, Gregory Lizee1 Patrick Hwu1,* and Laszlo G.
      Radvanyi1,*
      Adoptive cell therapy (ACT) using autologous tumor-infiltrating lymphocytes (TIL) is a promising
      treatment for metastatic melanoma that is unresponsive to conventional therapies. Here, we report on
      the results of a Phase II clinical trial testing the efficacy of ACT using TIL in metastatic melanoma
      patients. Transiently lymphodepleted patients received their expanded TIL followed by two cycles of
      high-dose (HD) IL-2 therapy. Altogether, 31 patients were treated with expanded TIL ranging from 8-
      150 billion cells. Overall, 15/31 (48.4%) patients had an objective clinical response with one patient
      having a complete response. The responses have been durable, with relapse-free survival of >10
      months for the majority (10/15) of the responding patients and all responding patients being alive one
      year after TIL ACT. Factors associated with objective tumor regression included a higher number of
      TIL infused, a higher proportion of CD8+ TIL in the infusion product (P=0.0011), a more differentiated
      effector phenotype of the CD8+ population and, unexpectedly, a higher frequency of CD8+ TIL coexpressing
      the negative costimulation molecule “B- and T-lymphocyte attenuator” (BTLA) (P=0.0006).
      Tumor regression was also associated with the persistence of dominant TIL TCR Vβ clonotypes in vivo
      for at least 3 months. No significant difference in telomere lengths of TIL between responders versus
      non-responders was evident. These results indicate that immunotherapy with expanded autologous
      TIL is capable of achieving high durable clinical responses in metastatic melanoma patients and that
      CD8+ T cells, particularly differentiated effectors and cells expressing BTLA+, may be critical in
      mediating tumor regression.

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