Reduced Tumorigenicity and Augmented Leukocyte Infiltration After Monocyte Chemotactic Protein-3 (MCP-3) Gene Transfer: Perivascular Accumulation of Dendritic Cells in Peritumoral Tissue and Neutrophil Recruitment Within the Tumor

Author:

Fioretti Francesca1,Fradelizi Didier2,Stoppacciaro Antonella3,Ramponi Simona1,Ruco Luigi3,Minty Adrian4,Sozzani Silvano1,Garlanda Cecilia1,Vecchi Annunciata1,Mantovani Alberto15

Affiliation:

1. *Istituto Ricerche Farmacologiche Mario Negri, Milan, Italy;

2. †Hôpital Cochin, Institut National de la Santé et de la Recherche Médicale (INSERM) U283, Paris, France;

3. ‡Dipartimento Medicina Sperimentale e Patologia, Università La Sapienza, Rome, Italy;

4. §Sanofi Recherches, Labège, France; and

5. ¶Dipartimento Biotecnologie, Univ. Brescia, Brescia, Italy

Abstract

AbstractMonocyte chemotactic protein-3 (MCP-3) is a C-C chemokine that interacts with the CCR1, CCR2, and CCR3 receptors and has a spectrum of action encompassing T cells, NK cells, eosinophils, and dendritic cells (DC), in addition to mononuclear phagocytes. This broad spectrum of action prompted the present study aimed at assessing the antitumor activity of MCP-3 in a gene transfer approach and at providing information as to the actual in vivo leukocyte recruiting capacity of MCP-3. P815 mastocytoma cells transfected with the gene coding MCP-3 (P815/MCP-3) grew in syngeneic hosts and underwent rejection. Rejection was associated with profound alterations of leukocyte infiltration and resistance to subsequent challenge with P815 cells. Tumor-associated macrophages, already present in copious numbers, T cells, eosinophils, and neutrophils, increased in tumor tissues after gene transfer. DC, identified as DEC205+, high MHC class II+, CD11c+ cells, did not increase substantially in the tumor mass. However, in peritumoral tissues, DC accumulated in perivascular areas. P815/MCP-3-transfected tumor cells grew normally in nude mice. Increased accumulation of macrophages and polymorphonuclear neutrophils was evident also in nude mice. mAb against CD4, CD8, and IFN-γ, but not against IL-4, inhibited rejection of MCP-3-producing cells. An anti-polymorphonuclear mAb caused only a retardation of MCP-3-elicited tumor rejection. Thus, MCP-3 gene transfer elicits tumor rejection by activating type I T cell-dependent immunity. It is tempting to speculate that altered trafficking of APCs, which express receptors and respond to MCP-3, together with recruitment of activated T cells, underlies activation of specific immunity by MCP-3-transfected cells.

Publisher

The American Association of Immunologists

Subject

Immunology,Immunology and Allergy

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