作者
Florian Leuschner, Partha Dutta, Rostic Gorbatov, Tatiana I Novobrantseva, Jessica S Donahoe, Gabriel Courties, Kang Mi Lee, James I Kim, James F Markmann, Brett Marinelli, Peter Panizzi, Won Woo Lee, Yoshiko Iwamoto, Stuart Milstein, Hila Epstein-Barash, William Cantley, Jamie Wong, Virna Cortez-Retamozo, Andita Newton, Kevin Love, Peter Libby, Mikael J Pittet, Filip K Swirski, Victor Koteliansky, Robert Langer, Ralph Weissleder, Daniel G Anderson, Matthias Nahrendorf
发表日期
2011/11
期刊
Nature biotechnology
卷号
29
期号
11
页码范围
1005-1010
出版商
Nature Publishing Group US
简介
Excessive and prolonged activity of inflammatory monocytes is a hallmark of many diseases with an inflammatory component. In such conditions, precise targeting of these cells could be therapeutically beneficial while sparing many essential functions of the innate immune system, thus limiting unwanted effects. Inflammatory monocytes—but not the noninflammatory subset—depend on the chemokine receptor CCR2 for localization to injured tissue. Here we present an optimized lipid nanoparticle and a CCR2-silencing short interfering RNA that, when administered systemically in mice, show rapid blood clearance, accumulate in spleen and bone marrow, and localize to monocytes. Efficient degradation of CCR2 mRNA in monocytes prevents their accumulation in sites of inflammation. Specifically, the treatment attenuates their number in atherosclerotic plaques, reduces infarct size after coronary artery occlusion …
学术搜索中的文章
F Leuschner, P Dutta, R Gorbatov, TI Novobrantseva… - Nature biotechnology, 2011