Broad-Spectrum CC-Chemokine Blockade by Gene Transfer Inhibits Macrophage Recruitment and Atherosclerotic Plaque Formation in Apolipoprotein E-Knockout Mice

doi:10.1161/01.CIR.0000145122.58420.CO

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Circulation. 2004;110:2460-2466
Published online before print October 11, 2004, doi: 10.1161/01.CIR.0000145122.58420.CO

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(Circulation. 2004;110:2460-2466.)
© 2004 American Heart Association, Inc.

Molecular Cardiology

Broad-Spectrum CC-Chemokine Blockade by Gene Transfer Inhibits Macrophage Recruitment and Atherosclerotic Plaque Formation in Apolipoprotein E–Knockout Mice

Christina A. Bursill, PhD; Robin P. Choudhury, MD; Ziad Ali, MD; David R. Greaves, PhD; Keith M. Channon, MD, FRCP

From the Department of Cardiovascular Medicine (C.A.B., R.P.C., Z.A., K.M.C.), University of Oxford, John Radcliffe Hospital, and the Sir William Dunn School of Pathology (C.A.B., D.R.G.), University of Oxford, Oxford, England.

Correspondence to Prof Keith Channon, Department of Cardiovascular Medicine, John Radcliffe Hospital, University of Oxford, Oxford OX3 9DU, UK. E-mail keith.channon{at}cardiov.ox.ac.uk

Received June 18, 2004; revision received July 24, 2004; accepted July 29, 2004.

Background— The CC-chemokines (CKs) recruit monocytes/macrophagesto sites of inflammation; several different CC-CKs play a rolein the pathogenesis of atherosclerosis. The vaccinia virus expressesa 35-kDa soluble protein (35K) that binds to and inactivatesnearly all of the CC-CKs, providing a potentially useful therapeuticstrategy for broad-spectrum CC-CK inhibition in atherosclerosis.A recombinant adenovirus encoding soluble 35K (Ad35K) was generatedto investigate the effect of 35K gene transfer on atherosclerosisin Western diet–fed apolipoprotein E–knockout (ApoEKO) mice.

Methods and Results— ApoE KO mice received tail-vein injectionsof phosphate-buffered saline, Ad35K, or control adenovirus AdGFPencoding green fluorescence protein. Two weeks after Ad35K genetransfer, atherosclerotic lesion area was significantly reducedin aortic roots by 55% compared with PBS or AdGFP control mice(P<0.05). Furthermore, 35K gene transfer strikingly reducedthe macrophage content in aortic root lesions by 85% (P<0.01)and reduced lipid deposition in descending aortas by more thanhalf (P<0.05). By an in vitro chemotaxis assay, plasma andaortic homogenates from 35K gene transfer mice promoted significantlyless CC-CK–induced cell migration than did PBS or AdGFPcontrols.

Conclusions— These findings show that a single intravenousinjection of a recombinant adenovirus encoding the broad-spectrumCC-CK inhibitor 35K can reduce atherosclerosis by inhibitingCC-CK–induced macrophage recruitment in atheroscleroticApoE KO mice. These experiments suggest that CC-CKs play animportant role in atherogenesis and are a rational target fortherapeutic intervention.

Key Words: gene therapy • inflammation • atherosclerosis • plaque • aorta

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