Aortic intimal resident macrophages are essential for maintenance of the non-thrombogenic intravascular state

主动脉内膜驻留巨噬细胞对于维持非血栓形成血管内状态至关重要

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作者:Gloria E Hernandez, Feiyang Ma, Guadalupe Martinez, Nadia B Firozabadi, Jocelynda Salvador, Lih Jiin Juang, Jerry Leung, Peng Zhao, Diego A López, Reza Ardehali, Anna E Beaudin, Christian J Kastrup, Matteo Pellegrini, Matthew J Flick, M Luisa Iruela-Arispe

Abstract

Leukocytes and endothelial cells frequently cooperate to resolve inflammatory events. In most cases, these interactions are transient in nature and triggered by immunological insults. Here, we report that in areas of disturbed blood flow, aortic endothelial cells permanently and intimately associate with a population of specialized macrophages that are recruited at birth from the closing ductus arteriosus and share the luminal surface with the endothelium becoming interwoven in the tunica intima. Anatomical changes that affect hemodynamics, like in patent ductus arteriosus, alter macrophage seeding to coincide with regions of disturbed flow. Aortic resident macrophages expand in situ via direct cell renewal. Induced-depletion of intimal macrophages led to thrombin-mediated endothelial cell contraction, progressive fibrin accumulation and formation of microthrombi that, once dislodged, caused blockade of vessels in several organs. Together the findings revealed that intravascular resident macrophages are essential to regulate thrombin activity and clear fibrin deposits in regions of disturbed blood flow.

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