Regression of Extensive Pulmonary Metastases in Mice by Adoptive Transfer of Antigen-Specific CD8+ CTL Reactive Against Tumor Cells Expressing a Naturally Occurring Rejection Epitope

Ryan, Mary H.; Bristol, J. Andrew; McDuffie, Elwood; Abrams, Scott I.

doi:10.4049/jimmunol.167.8.4286

Cited by 43 publications

(50 citation statements)

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“…administration. CMS4-reactive CTL lines can be produced in mice (9) using an anti-CTLA4 mAb-based strategy (11,12). In vivo, we showed that the adoptive transfer of these CTL resulted in nearly complete regression of 3-day established experimental lung metastases, with half-maximal antitumor activity observed between 3-10 ϫ 10 4 CTL/mouse.…”

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confidence: 86%

“…Furthermore, the potential relevance of the animal model would be further enriched if it were based on immune recognition of malignant cells naturally expressing tumor rejection Ag, as it would better mirror what occurs in human neoplasia. To that end, we have developed a syngeneic mouse model of CTL adoptive immunotherapy against experimental pulmonary metastases in both minimal (i.e., day 3 tumor-bearing mice) and extensive (day 10 tumor-bearing mice) disease settings (9). The model consisted of the CMS4 sarcoma, a solid tumor of BALB/c (H-2 d ) origin (10) that grows aggressively in naive, syngeneic hosts (9) either as an s.c. tumor or as a metastasis in the lung following i.v.…”

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confidence: 99%

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The Fas/Fas Ligand Pathway Is Important for Optimal Tumor Regression in a Mouse Model of CTL Adoptive Immunotherapy of Experimental CMS4 Lung Metastases

Caldwell

Ryan

McDuffie

et al. 2003

The Journal of Immunology

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The mechanisms of CTL-mediated tumor regression in vivo remain to be fully understood. If CTL do mediate tumor regression in vivo by direct cytotoxicity, this may occur via two major effector mechanisms involving the secretion of perforin/granzymes and/or engagement of Fas by Fas ligand (FasL) expressed by the activated CTL. Although the perforin pathway has been considered the dominant player, it is unclear whether Fas-mediated cytotoxicity is additionally required for optimal tumor rejection. Previously, we produced H-2Ld-restricted CTL reactive against the CMS4 sarcoma, which expresses a naturally occurring rejection Ag recognized by these CTL and harbors a cytokine (IFN-γ plus TNF)-inducible, Fas-responsive phenotype. The adoptive transfer of these CTL to syngeneic BALB/c mice with minimal (day 3 established) or extensive (day 10 established) experimental pulmonary metastases resulted in strong antitumor responses. Here we investigated whether a FasL-dependent CTL effector mechanism was important for optimal tumor regression in this adoptive immunotherapy model. The approach taken was to compare the therapeutic efficacy of wild-type to FasL-deficient (gld) CTL clones by adoptive transfer. In comparison with wild-type CTL, gld-CTL efficiently mediated tumor cytolysis and produced comparable amounts of IFN-γ, after tumor-specific stimulation, as in vitro assessments of Ag recognition. Moreover, gld-CTL mediated comparably potent antitumor effects in a minimal disease setting, but were significantly less effective under conditions of an extensive tumor burden. Overall, under conditions of extensive lung metastases, these data revealed for the first time an important role for a FasL-dependent CTL effector mechanism in optimal tumor regression.

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confidence: 86%

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confidence: 99%

The Fas/Fas Ligand Pathway Is Important for Optimal Tumor Regression in a Mouse Model of CTL Adoptive Immunotherapy of Experimental CMS4 Lung Metastases

Caldwell

Ryan

McDuffie

et al. 2003

The Journal of Immunology

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“…26,27 Several vaccine strategies using HLA-A2-binding Her-2/neu CTL epitope peptide were reported to be safe and effective in eliciting CTL responses even in Her-2/neu-expressing cancer patients. 28,29 However, it is difficult to directly measure CTL activity in nonhuman primates, because little information is available on MHC class I-binding epitope peptide.…”

Section: Non-human Primate Study Against Human Her-2/neu H-j Ko Et Almentioning

confidence: 99%

Immunogenicity and safety profiles of genetic vaccines against human Her-2/neu in cynomolgus monkeys

Kim

et al. 2008

Gene Ther

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“…Cells adhered within the first 5 min reached a maximum at 60 min [tumor vs. normal 20 (12)(13)(14)(15)(16)(17)(18)(19)(20)(21)(22)(23)(24) vs. 1 (1-2)] and were elevated for the duration of the study period. Neither population adhered to the endothelium of the normal microcirculation.…”

Section: Adherent Cellsmentioning

confidence: 99%

“…3,[17][18][19] The effector cells used in adoptive cellular therapy range from ex vivo tumor-draining lymph node cells specifically or nonspecifically activated 20 to antigen-specific CTLs reactive to tumor cells naturally expressing appropriate peptide epitopes via MHC molecules. 21 CTLs mediating MHC-restricted tumor cell killing are particularly attractive as effector cells for adoptive therapy, with the therapeutic potency being governed by their binding affinity, number and specificity.…”

Section: Rolling and Flying Cellsmentioning

confidence: 99%

Trafficking of tumor peptide‐specific cytotoxic T lymphocytes into the tumor microcirculation

Ali¹,

Ahmad²,

Lynam³

et al. 2004

Intl Journal of Cancer

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The major histocompatibility complex class I-restricted CD8 ؉ cytotoxic T-lymphocyte (CTL) effector arm of the adaptive immune response can specifically recognize and destroy tumor cells expressing peptide antigens. Although adoptive T-cell therapy has been successfully used for the treatment of viral and malignant diseases, little is known of the trafficking and fate of adoptively transferred antigenspecific T cells. In the present study, splenocytes derived from mice that rejected their tumors (CT26 or CT26-clone 25 tumors) in response to direct intratumor injection of disabled infectious single-cycle herpes simplex virus (DISC-HSV) encoding murine GM-CSF were restimulated with peptide in vitro. CTLs specific for the AH-1 and ␤-gal peptides expressed by CT26 and CT26-clone 25 tumor cells, respectively, were generated and used for adoptive cellular therapy and trafficking studies. Intravenous administration of AH-1-specific CTLs 3 days following i.v. injection of CT26 cells resulted in significant tumor growth inhibition, whereas administration of control CTLs generated against a bacterial ␤-gal peptide did not inhibit the growth of tumors. Trafficking of AH-1-specific lymphocytes and their interaction with the CT26 tumor microcirculation was analyzed using realtime in vivo microscopy (IVM). AH-1-specific but not ␤-galspecific CTLs adhered and localized in the CT26 tumor microvasculature, but neither population adhered to the endothelium of the normal microcirculation. This study provides direct visual evidence suggesting that AH-1-specific CTLs that mediate a therapeutic response traffic to and localize within the tumor microenvironment. © 2004 Wiley-Liss, Inc. Key words: cytotoxic T lymphocytes; adoptive transfer; traffickingThe immune system consists of a complex network of cells that mediate innate and antigen-specific responses to invading microbes and tumors. Processing and presentation of antigen by antigen-presenting cells (dendritic cells) via peptide antigens bound to cell surface major histocompatibility complex (MHC) antigens is a prerequisite for the stimulation of T-cell responses (cytotoxic and helper T cells). 1,2 Tumor-specific cytotoxic T lymphocytes (CTLs) play an important role against cancer; this has been demonstrated using a number of experimental approaches, including the adoptive transfer of tumor-specific CTLs in animal models and clinical trials. 3,4 Beneficial antitumor effects have been reported using adoptive cellular therapy with lymphokine-activated killer (LAK) cells, autolymphocyte therapy (ALT) and in vitro expanded tumor-infiltrating lymphocytes. [5][6][7] The efficacy of adoptive cellular immunotherapy with cultured lymphocytes activated toward tumor antigens requires effector cells to migrate into tumor tissue and, once resident at the tumor site, to mediate an antitumor rejection response either by direct killing of tumor cells and/or indirectly through cytokine release and recruitment of other cells. Using the A2/K b transgenic mouse model, Sutmuller et al. 3 have shown t...

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Regression of Extensive Pulmonary Metastases in Mice by Adoptive Transfer of Antigen-Specific CD8+ CTL Reactive Against Tumor Cells Expressing a Naturally Occurring Rejection Epitope

Cited by 43 publications

References 20 publications

The Fas/Fas Ligand Pathway Is Important for Optimal Tumor Regression in a Mouse Model of CTL Adoptive Immunotherapy of Experimental CMS4 Lung Metastases

The Fas/Fas Ligand Pathway Is Important for Optimal Tumor Regression in a Mouse Model of CTL Adoptive Immunotherapy of Experimental CMS4 Lung Metastases

Immunogenicity and safety profiles of genetic vaccines against human Her-2/neu in cynomolgus monkeys

Trafficking of tumor peptide‐specific cytotoxic T lymphocytes into the tumor microcirculation

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