Anti eotaxin-2 antibodies attenuate the initiation and progression of experimental atherosclerosis.docVIP

World Journal of Cardiovascular Diseases, 2013, 3, 339-346 WJCD /10.4236/wjcd.2013.34054 Published Online July 2013 (/journal/wjcd/) Anti eotaxin-2 antibodies attenuate the initiation and progression of experimental atherosclerosis* Adi Mor , Arnon Afek Michal Entin-Meer , Gad Keren , Jacob George 1# 1 2 2 1 1 2 ChemomAb Ltd., Tel Aviv, Israel The Department of Cardiology, Tel Aviv Sourasky Medical Center, Tel Aviv, Israel Email: adimor@ # Received 21 May 2013; revised 30 June 2013; accepted 10 July 2013 Copyright ? 2013 Adi Mor et al. This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited. ABSTRACT Inflammation; Eotaxin-2; Chemokines Background: The chemokine eotaxin-2 is a potent chemoattractant for inflammatory cells, the pre- dominants of which are eosinophils. Human and mur- ine atherosclerotic plaques are known to exhibit in- flammatory phenotypes where a complex interaction of cytokine and chemokines plays a role. We tested the hypothesis that eotaxin-2 (eo-2) plays a causative role in the initiation and progression of experimental atherosclerosis. Methods and Results: Sera collected from atherosclerotic ApoE knockout (KO) mice, ex- hibited significantly higher levels of eo-2 compared to sera collected from their background age matched C57BL/6 litters by ELISA. Moreover, levels of eo-2 were higher in old atherosclerotic ApoE KO mice than in young animals. Similarly, the expression level of the eo-2 receptor, CCR3, was increased in spleno- cytes of old ApoE compared to the young littermates. Administration of polyclonal blocking antibodies to eotaxin-2 resulted in a sig