Combination Immunotherapy after ASCT for Multiple Myeloma Using MAGE-A3/Poly-ICLC Immunizations Followed by Adoptive Transfer of Vaccine-Primed and Costimulated Autologous T Cells

Aaron P. Rapoport(University of Maryland, Baltimore), Nicole A. Aqui(University of Maryland, Baltimore), Edward A. Stadtmauer(University of Maryland, Baltimore), Dan T. Vogl(University of Maryland, Baltimore), Yin Xu(University of Maryland, Baltimore), Michael Kalos(University of Maryland, Baltimore), Ling Cai(University of Maryland, Baltimore), Hong‐Bin Fang(University of Maryland, Baltimore), Brendan M. Weiss(University of Maryland, Baltimore), Ashraf Badros(University of Maryland, Baltimore), Saul Yanovich(University of Maryland, Baltimore), Görgün Akpek(University of Maryland, Baltimore), Patricia Tsao(University of Maryland, Baltimore), Alan S. Cross(University of Maryland, Baltimore), Dean L. Mann(University of Maryland, Baltimore), Sunita Philip(University of Maryland, Baltimore), Naseem Kerr(University of Maryland, Baltimore), Andrea Brennan(University of Maryland, Baltimore), Zhaohui Zheng(University of Maryland, Baltimore), Kathleen Ruehle(University of Maryland, Baltimore), Todd Milliron(University of Maryland, Baltimore), Scott E. Strome(University of Maryland, Baltimore), Andres Μ. Salazar(University of Maryland, Baltimore), Bruce L. Levine(University of Maryland, Baltimore), Carl H. June(University of Maryland, Baltimore)
Clinical Cancer Research
February 11, 2014
10.1158/1078-0432.ccr-13-2817
Cited by 123

Abstract

PURPOSE: Myeloma-directed cellular immune responses after autologous stem cell transplantation (ASCT) may reduce relapse rates. We studied whether coinjecting the TLR-3 agonist and vaccine adjuvant Poly-ICLC with a MAGE-A3 peptide vaccine was safe and would elicit a high frequency of vaccine-directed immune responses when combined with vaccine-primed and costimulated autologous T cells. EXPERIMENTAL DESIGN: In a phase II clinical trial (NCT01245673), we evaluated the safety and activity of ex vivo expanded autologous T cells primed in vivo using a MAGE-A3 multipeptide vaccine (compound GL-0817) combined with Poly-ICLC (Hiltonol), granulocyte macrophage colony-stimulating factor (GM-CSF) ± montanide. Twenty-seven patients with active and/or high-risk myeloma received autografts followed by anti-CD3/anti-CD28-costimulated autologous T cells, accompanied by MAGE-A3 peptide immunizations before T-cell collection and five times after ASCT. Immune responses to the vaccine were evaluated by cytokine production (all patients), dextramer binding to CD8(+) T cells, and ELISA performed serially after transplant. RESULTS: T-cell infusions were well tolerated, whereas vaccine injection site reactions occurred in >90% of patients. Two of nine patients who received montanide developed sterile abscesses; however, this did not occur in the 18 patients who did not receive montanide. Dextramer staining demonstrated MAGE-A3-specific CD8 T cells in 7 of 8 evaluable HLA-A2(+) patients (88%), whereas vaccine-specific cytokine-producing T cells were generated in 19 of 25 patients (76%). Antibody responses developed in 7 of 9 patients (78%) who received montanide and only weakly in 2 of 18 patients (11%) who did not. The 2-year overall survival was 74% [95% confidence interval (CI), 54%-100%] and 2-year event-free survival was 56% (95% CI, 37%-85%). CONCLUSIONS: A high frequency of vaccine-specific T-cell responses were generated after transplant by combining costimulated autologous T cells with a Poly-ICLC/GM-CSF-primed MAGE-A3 vaccine.

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