Transferred melanoma-specific CD8+ T cells persist, mediate tumor regression, and acquire central memory phenotype

Adoptively transferred tumor-specific T cells offer the potential for non–cross-resistant therapy and long-term immunoprotection. Strategies to enhance in vivo persistence of transferred T cells can lead to improved antitumor efficacy. However, the extrinsic (patient conditioning) and intrinsic (eff...

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Published in:Proceedings of the National Academy of Sciences - PNAS 2012-03, Vol.109 (12), p.4592-4597
Main Authors: Chapuis, Aude G, Thompson, John A, Margolin, Kim A, Rodmyre, Rebecca, Lai, Ivy P, Dowdy, Kaye, Farrar, Erik A, Bhatia, Shailender, Sabath, Daniel E, Cao, Jianhong, Li, Yongqing, Yee, Cassian
Format: Article
Language:English
Subjects:
Adoptive transfer
Adult
Aged
Animals
Antigens
Autoimmunity
Biological Sciences
Blood
CD8-Positive T-Lymphocytes - metabolism
CD8-Positive T-Lymphocytes - pathology
Cell Proliferation
clones
Cloning
cyclophosphamide
cytotoxic T-lymphocytes
Disease remission
Exanthema
Female
Genotype & phenotype
Humans
Immunologic Memory
Immunotherapy - methods
Interleukin-1 - metabolism
interleukin-2
Lymph nodes
Lymphocytes
Male
Melanoma
Melanoma - immunology
Melanoma - therapy
Memory
metastasis
Mice
Middle Aged
Neoplasms - pathology
Neoplasms - therapy
patients
Phenotype
Phenotypes
remission
T cell receptors
T lymphocytes
T-Lymphocytes, Cytotoxic - cytology
therapeutics
Toxicity
Tumors
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Summary:Adoptively transferred tumor-specific T cells offer the potential for non–cross-resistant therapy and long-term immunoprotection. Strategies to enhance in vivo persistence of transferred T cells can lead to improved antitumor efficacy. However, the extrinsic (patient conditioning) and intrinsic (effector cell) factors contributing to long-term in vivo persistence are not well-defined. As a means to enhance persistence of infused T cells in vivo and limit toxicity, 11 patients with refractory, progressive metastatic melanoma received cyclophosphamide alone as conditioning before the infusion of peripheral blood mononuclear cell-derived, antigen-specific, CD8+ cytotoxic T-lymphocyte (CTL) clones followed by low-dose or high-dose IL-2. No life-threatening toxicities occurred with low-dose IL-2. Five of 10 evaluable patients had stable disease at 8 wk, and 1 of 11 had a complete remission that continued for longer than 3 y. On-target autoimmune events with the early appearance of skin rashes were observed in patients with stable disease or complete remission at 4 wk or longer. In vivo tracking revealed that the conditioning regimen provided a favorable milieu that enabled CTL proliferation early after transfer and localization to nonvascular compartments, such as skin and lymph nodes. CTL clones, on infusion, were characterized by an effector memory phenotype, and CTL that persisted long term acquired phenotypic and/or functional qualities of central memory type CTLs in vivo. The use of a T-cell product composed of a clonal population of antigen-specific CTLs afforded the opportunity to demonstrate phenotypic and/or functional conversion to a central memory type with the potential for sustained clinical benefit.
ISSN:0027-8424
1091-6490
DOI:10.1073/pnas.1113748109