Academic Department of Vascular Surgery, Cardiovascular Division, BHF Centre of Research Excellence, King's College London, St Thomas' Hospital, London, England, UK.
Department of Ultrasonic Angiology, Guy's and St Thomas' NHS Foundation Trust, London, England, UK.
J Exp Med. 2017 Aug 7;214(8):2437-2452. doi: 10.1084/jem.20160875.
Venous valves (VVs) prevent venous hypertension and ulceration. We report that FOXC2 and GJC2 mutations are associated with reduced VV number and length. In mice, early VV formation is marked by elongation and reorientation ("organization") of Prox1hi endothelial cells by postnatal day 0. The expression of the transcription factors Foxc2 and Nfatc1 and the gap junction proteins Gjc2, Gja1, and Gja4 were temporospatially regulated during this process. Foxc2 and Nfatc1 were coexpressed at P0, and combined Foxc2 deletion with calcineurin-Nfat inhibition disrupted early Prox1hi endothelial organization, suggesting cooperative Foxc2-Nfatc1 patterning of these events. Genetic deletion of Gjc2, Gja4, or Gja1 also disrupted early VV Prox1hi endothelial organization at postnatal day 0, and this likely underlies the VV defects seen in patients with GJC2 mutations. Knockout of Gja4 or Gjc2 resulted in reduced proliferation of Prox1hi valve-forming cells. At later stages of blood flow, Foxc2 and calcineurin-Nfat signaling are each required for growth of the valve leaflets, whereas Foxc2 is not required for VV maintenance.
静脉瓣膜 (VVs) 可防止静脉高压和溃疡。我们报告称,FOXC2 和 GJC2 突变与静脉瓣膜数量和长度减少有关。在小鼠中,早期静脉瓣膜形成的标志是 Prox1hi 内皮细胞在出生后第 0 天的伸长和重新定向(“组织化”)。转录因子 Foxc2 和 Nfatc1 的表达以及间隙连接蛋白 Gjc2、Gja1 和 Gja4 在这个过程中时空调节。Foxc2 和 Nfatc1 在 P0 时共表达,并且联合 Foxc2 缺失和钙调神经磷酸酶-Nfat 抑制破坏了早期 Prox1hi 内皮组织,表明 Foxc2-Nfatc1 共同对这些事件进行模式化。Gjc2、Gja4 或 Gja1 的基因缺失也破坏了出生后第 0 天的早期静脉瓣膜 Prox1hi 内皮组织,这可能是 GJC2 突变患者中观察到的静脉瓣膜缺陷的基础。Gja4 或 Gjc2 的敲除导致形成瓣膜的 Prox1hi 细胞增殖减少。在血流的后期阶段,Foxc2 和钙调神经磷酸酶-Nfat 信号对于瓣膜小叶的生长都是必需的,而 Foxc2 对于静脉瓣膜的维持不是必需的。
Zotero 插件
