Tetramer guided, cell sorter assisted production of clinical grade autologous NY-ESO-1 specific CD8+ T cells

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• 作者：Seth M Pollack (1) (2)
  Robin L Jones (1) (2)
  Erik A Farrar (1)
  Ivy P Lai (1) (8)
  Sylvia M Lee (1) (2)
  Jianhong Cao (1)
  Venu G Pillarisetty (1) (3)
  Benjamin L Hoch (4)
  Ashley Gullett (4)
  Marie Bleakley (1) (5)
  Ernest U Conrad III (6)
  Janet F Eary (7)
  Kendall C Shibuya (1)
  Edus H Warren (1) (2)
  Jason N Carstens (1)
  Shelly Heimfeld (1)
  Stanley R Riddell (1) (2) (8)
  Cassian Yee (1) (2) (9)
  
  1. Clinical Research Division ; D3-100 Fred Hutchinson Cancer Research Center ; 1100 Fairview Ave ; Seattle ; WA ; 98109 ; USA
  2. Department of Medicine ; University of Washington ; Seattle ; WA ; USA
  8. Institute for Advanced Study ; Technical University of Munich ; Munich ; Germany
  3. Department of Surgery ; University of Washington ; Seattle ; WA ; USA
  4. Department of Pathology ; University of Washington ; Seattle ; WA ; USA
  5. Department of Pediatrics ; University of Washington ; Seattle ; WA ; USA
  6. Department of Orthopedics ; University of Washington ; Seattle ; WA ; USA
  7. Department of Radiology ; University of Alabama ; Birmingham ; AL ; USA
  9. Department of Melanoma Medical Oncology ; UT MD Anderson Cancer Center ; 7455 Fannin St ; Unit 904 ; Houston ; TX ; 77054 ; USA
  
• 关键词：Adoptive T cell therapy ; NY ; ESO ; 1 ; Synovial sarcoma ; Myxoid ; Liposarcoma ; Immunotherapy ; Antigen specific T cells ; Tetramer ; Influx cell sorting
• 刊名：Journal for Immunotherapy of Cancer
• 出版年：2014
• 出版时间：December 2014
• 年：2014
• 卷：2
• 期：1
• 全文大小：910 KB
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• 刊物主题：Oncology;
• 出版者：BioMed Central
• ISSN：2051-1426

文摘

Background Adoptive T cell therapy represents an attractive modality for the treatment of patients with cancer. Peripheral blood mononuclear cells have been used as a source of antigen specific T cells but the very low frequency of T cells recognizing commonly expressed antigens such as NY-ESO-1 limit the applicability of this approach to other solid tumors. To overcome this, we tested a strategy combining IL-21 modulation during in vitro stimulation with first-in-class use of tetramer-guided cell sorting to generate NY-ESO-1 specific cytotoxic T lymphocytes (CTL). Methods CTL generation was evaluated in 6 patients with NY-ESO-1 positive sarcomas, under clinical manufacturing conditions and characterized for phenotypic and functional properties. Results Following in vitro stimulation, T cells stained with NY-ESO-1 tetramer were enriched from frequencies as low as 0.4% to >90% after single pass through a clinical grade sorter. NY-ESO-1 specific T cells were generated from all 6 patients. The final products expanded on average 1200-fold to a total of 36 billion cells, were oligoclonal and contained 67-97% CD8+, tetramer+ T cells with a memory phenotype that recognized endogenous NY-ESO-1. Conclusion This study represents the first series using tetramer-guided cell sorting to generate T cells for adoptive therapy. This approach, when used to target more broadly expressed tumor antigens such as WT-1 and additional Cancer-Testis antigens will enhance the scope and feasibility of adoptive T cell therapy.