CCR5 Blockade Modulates Inflammation and Alloimmunity in Primates

Overview

Journal J Immunol

Specialty Allergy & Immunology

Date 2007 Aug 7

PMID 17675490

Citations 24

Authors

Carsten Schroder

Richard N Pierson 3rd

Bao-Ngoc H Nguyen

Douglas W Kawka

Laurence B Peterson

Guosheng Wu

Tianshu Zhang

Martin S Springer

Sal J Siciliano

Susan Iliff

Julia M Ayala

Min Lu

John S Mudgett

Kathy Lyons

Sander G Mills

Geraldine G Miller

Irwin I Singer

Agnes M Azimzadeh

Julie A Demartino

Affiliations

Soon will be listed here.

Abstract

Pharmacologic antagonism of CCR5, a chemokine receptor expressed on macrophages and activated T cells, is an effective antiviral therapy in patients with macrophage-tropic HIV infection, but its efficacy in modulating inflammation and immunity is only just beginning to be investigated. In this regard, the recruitment of CCR5-bearing cells into clinical allografts is a hallmark of acute rejection and may anticipate chronic rejection, whereas conventionally immunosuppressed renal transplant patients homozygous for a nonfunctional Delta32 CCR5 receptor rarely exhibit late graft loss. Therefore, we explored the effects of a potent, highly selective CCR5 antagonist, Merck's compound 167 (CMPD 167), in an established cynomolgus monkey cardiac allograft model. Although perioperative stress responses (fever, diminished activity) and the recruitment of CCR5-bearing leukocytes into the graft were markedly attenuated, anti-CCR5 monotherapy only marginally prolonged allograft survival. In contrast, relative to cyclosporine A monotherapy, CMPD 167 with cyclosporine A delayed alloantibody production, suppressed cardiac allograft vasculopathy, and tended to further prolong graft survival. CCR5 therefore represents an attractive therapeutic target for attenuating postsurgical stress responses and favorably modulating pathogenic alloimmunity in primates, including man.

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