Migration of cytotoxic T lymphocytes toward melanoma cells in three‐dimensional organotypic culture is dependent on CCL2 and CCR4

Zhang, Tianqian; Somasundaram, Rajasekharan; Berencsi, Klára; Caputo, Laura; Gimotty, Phyllis A.; Rani, Pyapalli; Guerry, DuPont; Swoboda, Rolf; Herlyn, Dorothee

doi:10.1002/eji.200526208

Cited by 81 publications

(68 citation statements)

References 39 publications

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“…Recently, Metelitsa et al (40) have shown that 53% of primary neuroblastomas from patients with metastatic disease (stage 4) secrete MCP-1, suggesting that there is heterogeneity of MCP-1 expression even within a certain type of tumor. This may help explain the fact that our studies with the human melanoma A2058 cells are in direct contrast to the recent report by Zhang et al (33), where it was found that human T cell migration toward autologous melanoma cells in culture was dependent on MCP-1/CCL2. Furthermore, our studies do not preclude the necessity of future studies aimed at identifying chemokines other than MCP-1 that mediate T cell tumor tropism, especially because the chemotactic capacity of SW480 cells appeared to be independent of MCP-1 (and IL-8).…”

Section: Discussioncontrasting

confidence: 83%

“…tumor xenografts in response to the tumor-derived chemokine MCP-1. Although our data suggest that this chemotaxis may be mediated through CCR2, future studies will better define the receptors involved in the observed MCP-1-mediated homing of T cells to tumors, since others have found that MCP-1 directed migration can be dependent on CCR4 (32,33).…”

Section: Discussionmentioning

confidence: 68%

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Tumor-Derived Chemokine MCP-1/CCL2 Is Sufficient for Mediating Tumor Tropism of Adoptively Transferred T Cells

Brown¹,

Vishwanath²,

Aguilar³

et al. 2007

The Journal of Immunology

127

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To exert a therapeutic effect, adoptively transferred tumor-specific CTLs must traffic to sites of tumor burden, exit the circulation, and infiltrate the tumor microenvironment. In this study, we examine the ability of adoptively transferred human CTL to traffic to tumors with disparate chemokine secretion profiles independent of tumor Ag recognition. Using a combination of in vivo tumor tropism studies and in vitro biophotonic chemotaxis assays, we observed that cell lines derived from glioma, medulloblastoma, and renal cell carcinoma efficiently chemoattracted ex vivo-expanded primary human T cells. We compared the chemokines secreted by tumor cell lines with high chemotactic activity with those that failed to elicit T cell chemotaxis (Daudi lymphoma, 10HTB neuroblastoma, and A2058 melanoma cells) and found a correlation between tumor-derived production of MCP-1/CCL2 (≥10 ng/ml) and T cell chemotaxis. Chemokine immunodepletion studies confirmed that tumor-derived MCP-1 elicits effector T cell chemotaxis. Moreover, MCP-1 is sufficient for in vivo T cell tumor tropism as evidenced by the selective accumulation of i.v. administered firefly luciferase-expressing T cells in intracerebral xenografts of tumor transfectants secreting MCP-1. These studies suggest that the capacity of adoptively transferred T cells to home to tumors may be, in part, dictated by the species and amounts of tumor-derived chemokines, in particular MCP-1.

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Section: Discussioncontrasting

confidence: 83%

Section: Discussionmentioning

confidence: 68%

Tumor-Derived Chemokine MCP-1/CCL2 Is Sufficient for Mediating Tumor Tropism of Adoptively Transferred T Cells

Brown¹,

Vishwanath²,

Aguilar³

et al. 2007

The Journal of Immunology

127

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“…Analysis in two different in vitro culture systems showed that migration is dependent on CXCL12 produced by tumor cells and CXCR4 expressed by T cells, consistent with the previous demonstration of chemokine dependency of human CTL migration toward tumor cells. 7,8 The reconstruct culture system which consists of a bottom layer of collagen type I with fibroblasts, superimposed by a tumor cell layer, collagen/fibroblast separating layer and finally a top layer of collagen, fibroblasts and T cells, has several advantages over the Transwell plate cultures usually used to study chemotaxis of T cells: (i) the cultures include growing tumor cells whereas Transwell does not; (ii) chemokines are produced by the growing tumor cells in physiological concentrations as compared to the artificially high chemokine concentrations used in Transwell; (iii) collagen and fibroblasts, missing from Transwell, provide stromal components important for T-cell migration and activation; 29 (iv) T-cell migration can be determined over 6-9 days as compared to a few hours for Transwell; and (v) T cells migrate through a distance of at least 500 µm, as compared to about 10 µm using Transwell. In the reconstruct, human melanoma is recapitulated in vitro using a mixture of collagen and fibroblasts (lattices or matrices).…”

Section: Discussionmentioning

confidence: 99%

“…We recently showed that migration of CTL derived from two melanoma patients toward autologous tumor cells is dependent on CXCR4 or CCR4 expressed by the CTL and on CXCL12 or CCL2 produced by the melanoma cells. 7,8 Here, we have examined chemokine and chemokine receptor usage for T cell migration in one additional patient and chemokine/chemokine receptor expression in 12 additional melanoma patients, since involvement of the same chemokine in the migration toward autologous melanoma cells of CTL derived from different patients would underscore the potential usefulness of this chemokine in immunotherapy of melanoma.…”

Section: Introductionmentioning

confidence: 99%

Preferential involvement of CX chemokine receptor 4 and CX chemokine ligand 12 in T-Cell migration toward melanoma cells

Zhang

Somasundaram²,

Berking³

et al. 2006

Cancer Biology & Therapy

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Our previous analysis of the role of chemokines in T lymphocyte trafficking toward human tumor cells revealed the migration of a melanoma patient's cytotoxic T lymphocytes (CTL) toward autologous tumor cells, resulting in tumor cell apoptosis, in an organotypic melanoma culture. CTL migration was mediated by CX chemokine receptor (CXCR) 4 expressed by the CTL and CX chemokine ligand (CXCL) 12 secreted by the tumor cells, as evidenced by blockage of CTL migration by antibodies to CXCL12 or CXCR4, high concentrations of CXCL12 or small molecule CXCR4 antagonist. Here, we present the results of T cell migration in one additional melanoma patient and T cell and tumor cell analyses for CXCR4 and CXCL12 expression, respectively, in 12 additional melanoma patients, indicating the preferential role of CXCR4 and CXCL12 in CTL migration toward melanoma cells. These studies add to the increasing body of evidence suggesting that CXCL12 is a potent chemoattractant for T cells.

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“…It allows CTL migration and killing of specific tumor cells and better reflects the cell-to-cell and cellto-matrix interactions occurring in an in vivo tumor microenvironment (19,21). The three-dimensional construct consisted of a collagen matrix containing autologous tumor, endothelial, and CD8 ϩ CTLs.…”

Section: The Lysis Of M4e Ecs By the Tumor-specific Clone Requires Thmentioning

confidence: 99%

Gap Junction Communication between Autologous Endothelial and Tumor Cells Induce Cross-Recognition and Elimination by Specific CTL

Benlalam

Jalil

Hasmim

et al. 2009

The Journal of Immunology

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International audienceCellular interactions in the tumor stroma play a major role in cancer progression but can also induce tumor rejection. To explore the role of endothelial cells in these interactions, we used an in vitro three-dimensional collagen matrix model containing a cytotoxic T lymphocyte CTL clone (M4.48), autologous tumor cells (M4T), and an endothelial cell (M4E) line that are A derived from the same tumor. We demonstrate in this study that specific killing of the endothelial cells by the CTL clone required the autologous tumor cells and involved Ag cross-presentation. The formation of gap junctions between endothelial and tumor cells is required for antigenic peptide transfer to endothelial cells that are then recognized and eliminated by CTL. Our results indicate that gap junctions facilitate an effective CTL-mediated destruction of endothelial cells from the tumor microenvironment that may contribute to the control of tumor progression

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Migration of cytotoxic T lymphocytes toward melanoma cells in three‐dimensional organotypic culture is dependent on CCL2 and CCR4

Cited by 81 publications

References 39 publications

Tumor-Derived Chemokine MCP-1/CCL2 Is Sufficient for Mediating Tumor Tropism of Adoptively Transferred T Cells

Tumor-Derived Chemokine MCP-1/CCL2 Is Sufficient for Mediating Tumor Tropism of Adoptively Transferred T Cells

Preferential involvement of CX chemokine receptor 4 and CX chemokine ligand 12 in T-Cell migration toward melanoma cells

Gap Junction Communication between Autologous Endothelial and Tumor Cells Induce Cross-Recognition and Elimination by Specific CTL

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