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Arterial-venous network formation during brain vascularization involves hemodynamic regulation of chemokine signaling

机译:脑血管形成过程中的动静脉网络形成涉及趋化因子信号的血流动力学调节

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摘要

During angiogenic sprouting, newly forming blood vessels need to connect to the existing vasculature in order to establish a functional circulatory loop. Previous studies have implicated genetic pathways, such as VEGF and Notch signaling, in controlling angiogenesis. We show here that both pathways similarly act during vascularization of the zebrafish central nervous system. In addition, we find that chemokine signaling specifically controls arterial-venous network formation in the brain. Zebrafish mutants for the chemokine receptor cxcr4a or its ligand cxcl12b establish a decreased number of arterial-venous connections, leading to the formation of an unperfused and interconnected blood vessel network. We further find that expression of cxcr4a in newly forming brain capillaries is negatively regulated by blood flow. Accordingly, unperfused vessels continue to express cxcr4a, whereas connection of these vessels to the arterial circulation leads to rapid downregulation of cxcr4a expression and loss of angiogenic characteristics in endothelial cells, such as filopodia formation. Together, our findings indicate that hemodynamics, in addition to genetic pathways, influence vascular morphogenesis by regulating the expression of a proangiogenic factor that is necessary for the correct pathfinding of sprouting brain capillaries.
机译:在血管新生期间,新形成的血管需要连接到现有的脉管系统,以建立功能性循环环。先前的研究已牵涉到遗传途径,例如VEGF和Notch信号传导,来控制血管生成。我们在这里显示,这两种途径在斑马鱼中枢神经系统的血管形成过程中类似地起作用。此外,我们发现趋化因子信号传导专门控制大脑中的动静脉网络的形成。趋化因子受体cxcr4a或其配体cxcl12b的斑马鱼突变体建立的动静脉连接数量减少,导致形成未灌注和相互连接的血管网络。我们进一步发现,cxcr4a在新生脑毛细血管中的表达受到血流的负调节。因此,未灌注的血管继续表达cxcr4a,而这些血管与动脉循环的连接导致cxcr4a表达的快速下调和内皮细胞中血管生成特性的丧失,例如丝状伪足的形成。总之,我们的研究结果表明,除了遗传途径外,血液动力学还通过调节促血管新生因子的表达来影响血管形态发生,而促血管新生因子的表达对于正确寻找发芽的脑毛细血管是必需的。

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