Macrophages have a critical function in the recognition and engulfment of dead cells. In some settings, macrophages also actively signal programmed cell death. Here we show that during developmentally scheduled vascular regression, resident macrophages are an obligatory participant in a signaling switch that favors death over survival. This switch occurs when the signaling ligand angiopoietin 2 has the dual effect of suppressing survival signaling in vascular endothelial cells (VECs) and stimulating Wnt ligand production by macrophages. In response to the Wnt ligand, VECs enter the cell cycle and in the absence of survival signals, die from G1 phase of the cell cycle. We propose that this mechanism represents an adaptation to ensure that the macrophage and its disposal capability are on hand when cell death occurs.

译文

巨噬细胞在识别和吞噬死亡细胞方面具有关键功能。在某些情况下,巨噬细胞还主动发出程序性细胞死亡的信号。在这里,我们显示,在发育预定的血管消退期间,常驻巨噬细胞是信号转换的强制性参与者,该信号转换有利于死亡而不是生存。当信号配体血管生成素2具有抑制血管内皮细胞 (VECs) 中的存活信号和刺激巨噬细胞产生Wnt配体的双重作用时,就会发生这种切换。响应Wnt配体,VECs进入细胞周期,在没有存活信号的情况下,从细胞周期的G1期死亡。我们建议这种机制代表一种适应,以确保在发生细胞死亡时,巨噬细胞及其处置能力就在眼前。

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