前列腺素 E2 通过 EP4 受体控制动脉导管平滑肌基因表达模式,对于出生时的重塑至关重要。
PGE2 through the EP4 receptor controls smooth muscle gene expression patterns in the ductus arteriosus critical for remodeling at birth.
机构信息
Department of Genetics, University of North Carolina at Chapel Hill, Chapel Hill, NC 27599-7248, USA.
出版信息
Prostaglandins Other Lipid Mediat. 2012 Mar;97(3-4):109-19. doi: 10.1016/j.prostaglandins.2012.02.001. Epub 2012 Feb 11.
Abstract
The ductus arteriosus (DA) is a fetal shunt that directs right ventricular outflow away from pulmonary circulation and into the aorta. Critical roles for prostaglandin E(2) (PGE(2)) and the EP4 receptor (EP4) have been established in maintaining both the patency of the vessel in utero and in its closure at birth. Here we have generated mice in which loss of EP4 expression is limited to either the smooth muscle (SMC) or endothelial cells and demonstrated that SMC, but not endothelial cell expression of EP4 is required for DA closure. The genome wide expression analysis of full term wild type and EP4(-/-) DA indicates that PGE(2)/EP4 signaling modulates expression of a number of unique pathways, including those involved in SMC proliferation, cell migration, and vascular tone. Together this supports a mechanism by which maturation and increased contractility of the vessel is coupled to the potent smooth muscle dilatory actions of PGE(2).
摘要
动脉导管(DA)是一种胎儿分流,将右心室流出道从肺循环引导至主动脉。前列腺素 E2(PGE2)和 EP4 受体(EP4)在维持血管在子宫内的通畅和出生时的关闭方面发挥着重要作用。在这里,我们生成了 EP4 表达仅限于平滑肌(SMC)或内皮细胞的小鼠,并证明了 DA 关闭需要 SMC 而不是内皮细胞表达 EP4。对足月野生型和 EP4(-/-)DA 的全基因组表达分析表明,PGE2/EP4 信号转导调节许多独特途径的表达,包括涉及 SMC 增殖、细胞迁移和血管张力的途径。综上所述,这支持了一种机制,即血管的成熟和收缩性增加与 PGE2 对平滑肌的强烈扩张作用相偶联。
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