Tumor-Specific CTL Kill Murine Renal Cancer Cells Using Both Perforin and Fas Ligand-Mediated Lysis In Vitro, But Cause Tumor Regression In Vivo in the Absence of Perforin

Seki, Naoko; Brooks, Alan D.; Carter, Clive R. D.; Back, Timothy C.; Parsoneault, Erin M.; Smyth, Mark J.; Wiltrout, Robert H.; Sayers, Thomas J.

doi:10.4049/jimmunol.168.7.3484

Cited by 118 publications

(95 citation statements)

References 42 publications

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“…Besides the two main killing pathways, it has been reported that other killing mechanisms, for example the proinflammatory cytokines gIFN and TNFa, have important roles in rejection of pulmonary metastasis of tumor cells. 38 In the study of Poehlein et al, 31 adoptive transfer of effector T cells, which are taken from perforin and gIFN double knockout mice (PKO/GKO), mediated complete tumor regression and cured wild-type animals with established pulmonary metastasis of melanoma cells by a TNF-a mediated killing mechanism. In addition, Smyth et al 39 have reported that, using the Renca carcinoma tumor model, TRAIL expression on NK and NKT cells has effective antimetastatic functions in vivo mediated by a gIFNdependent immune mechanism.…”

Section: Discussionmentioning

confidence: 99%

In vivo rejection of tumor cells dependent on CD8 cells that kill independently of perforin and FasL

et al. 2004

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Perforin/granzyme B-and Fas/FasL-mediated killing pathways are the main effector mechanisms of CTL and NK cells in antitumor immune responses. In this study, we investigated the relative role of these two lytic mechanisms in protection of the host from tumor progression, as well as spontaneous metastasis, using the D122 Lewis lung carcinoma and its gene-modified cells. Utilizing perforin knockout mice (B6-PKO) and Fas and FasL mutant (B6-MRL and B6-Smn) mice, we found that perforin expression in the host plays a crucial function in the prevention of metastasis. However, local tumor rejection of an H-2K b and B7-1 transfectant, 39.5-B7 cells, was not dependent either on perforin or Fas/FasL expression in vivo. In addition, CTL lysis of 39.5-B7 cells was independent of perforin and Fas/FasL interactions in 18-hour in vitro assays. We also confirmed that CD8 T-cells were responsible for rejecting 39.5-B7 local tumors, yet cytokines, TNF-a and gIFN were not involved in tumor rejection in vivo. Furthermore, blocking assays using caspase inhibitors (zVAD-fmk, zIETD-fmk and zLEHD-fmk) showed that, whereas caspase activation was partially required to induce 39.5-B7 lysis mediated by the perforin-dependent pathway, 39.5-B7 lysis by CTLs through the perforin-independent mechanism required caspase activation. Thus, these results suggested that perforin, Fas/FasL, gIFN and TNF-a independent lytic mechanisms, mediated by CD8 T cells, have a crucial role in rejection of 39.5-B7 cells in vivo. Caspase activation is a pre requisite for apoptosis of targets by CTLs

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Section: Discussionmentioning

confidence: 99%

In vivo rejection of tumor cells dependent on CD8 cells that kill independently of perforin and FasL

et al. 2004

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“…The relative importance of granule exocytosis versus FAS/FASL-mediated lytic activities for tumour control in vivo is controversial. While many studies point to a dominance of the granule exocytosis mechanism, other studies using perforin-knockout mice (Seki et al, 2002) suggest that FAS-dependent apoptosis may constitute a more prominent pathway in vivo. Therefore, it is of concern that most tumour cells, including RCC, are intrinsically resistant to FASmediated killing (Frost et al, 2003).…”

Section: Discussionmentioning

confidence: 99%

GPI-anchored TIMP-1 treatment renders renal cell carcinoma sensitive to FAS-meditated killing

Djafarzadeh

Noeßner²,

Engelmann

et al. 2005

Oncogene

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The resistance of tumours to immune-mediated lysis has been linked to the biology of matrix metalloproteinases (MMPs), and specifically to the cell surface expression of MMPs by the tumour cell. The endogenous tissue inhibitors of metalloproteinases (TIMPs) exhibit diverse physiological/biological functions including the moderation of tumour growth, metastasis and apoptosis. These biologic activities are mediated in part by the stoichiometry of TIMP/MMP/cell surface protein interactions. A glycosylphosphatidylinositol (GPI) anchor was fused to TIMP-1 to focus defined concentrations of this inhibitory protein on the surface of three renal cell carcinoma (RCC) cell lines (RCC-26, RCC-53 and A498) independently of cell surface protein-protein interactions. Exogenously added TIMP-1-GPI efficiently inserted into the RCC cell membrane and dramatically altered the association of MMPs with the cell surface. TIMP-1-GPI treatment inhibited RCC proliferation and rendered the normally FAS-resistant RCC cells sensitive to FAS-induced apoptosis but did not alter perforin-mediated lysis by cytotoxic effector cells. The increased sensitivity to FAS-mediated apoptosis correlated with an alteration in the balance of pro-and antiapoptotic BCL-2-family proteins. By interfering with the proliferative capacity and inducing sensitivity to immune effector mechanisms GPI-anchored TIMP-1 may represent a more effective version of the TIMP-1 protein for therapeutic strategies.

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“…Subcutaneous injections of NK-stimulating doses of IL-2 or administration of preactivated NK cells (adoptive transfer of LAK cells) showed a 15-30% positive effect in patients with advanced renal cell carcinoma (RCC) or melanoma (MEL) (42). However, both MEL and RCC show a variable susceptibility to apoptosis induced by TNF ligand members (46 -48), and the clearance of murine renal cancer cells in vivo often does not even require the perforin-mediated pathway (49). Thus, antitumor response following IL-2 treatment also involves the NKR-independent pathways of NK (and T) cell cytotoxicity.…”

Section: Nk Cell-based Immunotherapeutic Strategies Against Cancermentioning

confidence: 99%

NK Cells and Cancer

Zamai

Ponti

Mirandola

et al. 2007

The Journal of Immunology

260

199

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In this review, we overview the main features and functions of NK cells, focusing on their role in cell-mediated immune response to tumor cells. In parallel, we discuss the information available in the field of NK cell receptors and offer a wide general overview of functional aspects of cell targeting and killing, focusing on the recent acknowledgments on the efficacy of NK cells after cytokine and mAb administration in cancer therapy. Since efficacy of NK cell-based immunotherapy has been proven in KIR-mismatch regimens or in TRAIL-dependent apoptosis, the ability to manipulate the balance of activating and inhibitory receptors on NK cells and of their cognate ligands, as well as the sensitivity of tumor cells to apoptosis, opens new perspectives for NK cell-based immunotherapy.

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Tumor-Specific CTL Kill Murine Renal Cancer Cells Using Both Perforin and Fas Ligand-Mediated Lysis In Vitro, But Cause Tumor Regression In Vivo in the Absence of Perforin

Cited by 118 publications

References 42 publications

In vivo rejection of tumor cells dependent on CD8 cells that kill independently of perforin and FasL

In vivo rejection of tumor cells dependent on CD8 cells that kill independently of perforin and FasL

GPI-anchored TIMP-1 treatment renders renal cell carcinoma sensitive to FAS-meditated killing

NK Cells and Cancer

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