Host Absence of CCR5 Potentiates Dendritic Cell Vaccination

Overview

Journal J Immunol

Specialty Allergy & Immunology

Date 2003 Apr 12

PMID 12682253

Citations 14

Authors

Judith Ng-Cashin

Jennifer J Kuhns

Susan E Burkett

John D Powderly

Robin R Craven

Hank W van Deventer

Suzanne L Kirby

Jonathan S Serody

Affiliations

Soon will be listed here.

Abstract

Previous work has shown that dendritic cells (DCs) express specific chemokine receptors that allow for coordinated movement in vivo. To test the in vivo relevance of this, we used a murine melanoma system and knockout mice to investigate the function of the chemokine receptor CCR5 and its ligands, CCR ligand (CCL)3 and CCL5. We found that the lack of CCR5 in the host mouse resulted in delayed tumor growth, but this effect was overcome at a higher tumor load. With the administration of tumor charged DCs, CCR5(-/-) mice that had previously been injected with tumor were completely protected from tumor. This effect was dependent on the dose of tumor cells and the expression of CCR5 on the DC and its absence in the host. In contrast, the loss of the CCR5 ligand, CCL3, led to an early delay in tumor growth that did not persist, while the absence of the CCR5 ligand, CCL5, had no effect. Blocking the activity of CCR5 in the host may represent a new strategy for enhancing the activity of a therapeutic melanoma DC vaccine.

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