1. Systemic and local immunity following adoptive transfer of NY-ESO-1 SPEAR T cells in synovial sarcoma
- Author
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Ramachandran, Indu, Lowther, Daniel E, Dryer-Minnerly, Rebecca, Wang, Ruoxi, Fayngerts, Svetlana, Nunez, Daniel, Betts, Gareth, Bath, Natalie, Tipping, Alex J, Melchiori, Luca, Navenot, Jean-Marc, Glod, John, Mackall, Crystal L, D’Angelo, Sandra P, Araujo, Dejka M, Chow, Warren A, Demetri, George D, Druta, Mihaela, Van Tine, Brian A, Grupp, Stephan A, Abdul Razak, Albiruni R, Wilky, Breelyn, Iyengar, Malini, Trivedi, Trupti, Winkle, Erin Van, Chagin, Karen, Amado, Rafael, Binder, Gwendolyn K, and Basu, Samik
- Subjects
Vaccine Related ,Biotechnology ,Immunization ,Cancer ,Clinical Research ,2.1 Biological and endogenous factors ,Aetiology ,Antigens ,Neoplasm ,Biomarkers ,Clinical Trials ,Phase I as Topic ,Clinical Trials ,Phase II as Topic ,Cytokines ,Cytotoxicity ,Immunologic ,HLA-A Antigens ,Humans ,Immunohistochemistry ,Immunotherapy ,Adoptive ,Lymphocytes ,Tumor-Infiltrating ,Membrane Proteins ,Receptors ,Antigen ,T-Cell ,Receptors ,Chimeric Antigen ,Sarcoma ,Synovial ,T-Cell Antigen Receptor Specificity ,T-Lymphocytes ,Treatment Outcome ,Tumor Microenvironment ,Adoptive immunotherapy ,Synovial sarcoma ,NY-ESO-1 ,Fludarabine ,Cyclophosphamide ,T cell ,TCR ,IL-15 ,Cytokine ,Antigen loss ,Checkpoint therapy ,Engineered cell therapy - Abstract
BackgroundGene-modified autologous T cells expressing NY-ESO-1c259, an affinity-enhanced T-cell receptor (TCR) reactive against the NY-ESO-1-specific HLA-A*02-restricted peptide SLLMWITQC (NY-ESO-1 SPEAR T-cells; GSK 794), have demonstrated clinical activity in patients with advanced synovial sarcoma (SS). The factors contributing to gene-modified T-cell expansion and the changes within the tumor microenvironment (TME) following T-cell infusion remain unclear. These studies address the immunological mechanisms of response and resistance in patients with SS treated with NY-ESO-1 SPEAR T-cells.MethodsFour cohorts were included to evaluate antigen expression and preconditioning on efficacy. Clinical responses were assessed by RECIST v1.1. Engineered T-cell persistence was determined by qPCR. Serum cytokines were evaluated by immunoassay. Transcriptomic analyses and immunohistochemistry were performed on tumor biopsies from patients before and after T-cell infusion. Gene-modified T-cells were detected within the TME via an RNAish assay.ResultsResponses across cohorts were affected by preconditioning and intra-tumoral NY-ESO-1 expression. Of the 42 patients reported (data cut-off 4June2018), 1 patient had a complete response, 14 patients had partial responses, 24 patients had stable disease, and 3 patients had progressive disease. The magnitude of gene-modified T-cell expansion shortly after infusion was associated with response in patients with high intra-tumoral NY-ESO-1 expression. Patients receiving a fludarabine-containing conditioning regimen experienced increases in serum IL-7 and IL-15. Prior to infusion, the TME exhibited minimal leukocyte infiltration; CD163+ tumor-associated macrophages (TAMs) were the dominant population. Modest increases in intra-tumoral leukocytes (≤5%) were observed in a subset of subjects at approximately 8 weeks. Beyond 8 weeks post infusion, the TME was minimally infiltrated with a TAM-dominant leukocyte infiltrate. Tumor-associated antigens and antigen presentation did not significantly change within the tumor post-T-cell infusion. Finally, NY-ESO-1 SPEAR T cells trafficked to the TME and maintained cytotoxicity in a subset of patients.ConclusionsOur studies elucidate some factors that underpin response and resistance to NY-ESO-1 SPEAR T-cell therapy. From these data, we conclude that a lymphodepletion regimen containing high doses of fludarabine and cyclophosphamide is necessary for SPEAR T-cell persistence and efficacy. Furthermore, these data demonstrate that non-T-cell inflamed tumors, which are resistant to PD-1/PD-L1 inhibitors, can be treated with adoptive T-cell based immunotherapy.Trial registrationClinicalTrials.gov, NCT01343043 , Registered 27 April 2011.
- Published
- 2019