Flow-Dependent Remodeling in the Carotid Artery of Fibroblast Growth Factor-2 Knockout Mice

C. Sullivan, J. Hoying
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引用次数: 67

Abstract

Objective—Fibroblast growth factor-2 (FGF2) has been implicated as a mediator in the structural remodeling of arteries. Chronic changes in blood flow are known to cause reorganization of the vessel wall, resulting in permanent changes in artery size (flow-dependent remodeling). Using FGF2 knockout (Fgf2−/−) mice, we tested the hypothesis that FGF2 is required during flow-dependent remodeling of the carotid arteries. Methods and Results—All branches originating from the left common carotid artery (LCCA), except for the left thyroid artery, were ligated to reduce flow in the LCCA and increase flow in the contralateral right common carotid artery (RCCA). Age- and sex-matched control animals did not undergo ligation of the LCCA branches. Morphometric analysis showed that by day 7, vessel diameter was significantly greater in the high-flow RCCA of FGF2 wild-type (Fgf2+/+) and Fgf2−/− mice versus the respective control RCCA, demonstrating outward remodeling. In contrast, vessel diameter was decreased by day 7 in the low-flow LCCA of both genotypes compared with the control LCCA, showing inward remodeling. No differences were observed between Fgf2+/+ and Fgf2−/− mice in either high-flow or low-flow remodeling. Conclusions—Given these results, we demonstrate that FGF2 is not essential for flow-dependent remodeling of the carotid arteries.
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成纤维细胞生长因子-2敲除小鼠颈动脉血流依赖性重构
目的:成纤维细胞生长因子-2 (FGF2)被认为是动脉结构重塑的中介。众所周知,血流的慢性变化会引起血管壁的重组,从而导致动脉大小的永久性变化(血流依赖性重塑)。使用FGF2敲除(FGF2−/−)小鼠,我们验证了颈动脉血流依赖性重塑过程中需要FGF2的假设。方法与结果:结扎左颈总动脉(LCCA)除左甲状腺动脉外的所有分支,减少LCCA流量,增加对侧右颈总动脉(RCCA)流量。年龄和性别匹配的对照动物没有进行LCCA分支的结扎。形态计量学分析显示,到第7天,FGF2野生型(FGF2 +/+)和FGF2−/−小鼠的高流量RCCA血管直径明显大于各自的对照RCCA,表现出向外重构。相比之下,与对照LCCA相比,两种基因型低流量LCCA的血管直径在第7天减小,表现出向内重构。Fgf2+/+和Fgf2 - / -小鼠在高流量或低流量重塑方面均无差异。结论-鉴于这些结果,我们证明FGF2对于颈动脉血流依赖性重构不是必需的。
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