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首页> 外文期刊>Circulation journal >Transcription profiles of the ductus arteriosus in Brown-Norway rats with irregular elastic fiber formation
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Transcription profiles of the ductus arteriosus in Brown-Norway rats with irregular elastic fiber formation

机译:具有不规则弹性纤维形成的棕挪威大鼠导管动脉术的转录谱

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摘要

Background: Patent ductus arteriosus (PDA) is one of the most common congenital cardiovascular defects in children. The Brown-Norway (BN) inbred rat presents a higher frequency of PDA. A previous study reported that 2 different quantitative trait loci on chromosomes 8 and 9 were significantly linked to PDA in this strain. Nevertheless, the genetic or molecular mechanisms underlying PDA phenotypes in BN rats have not been fully investigated yet. Methods and Results: It was found that the elastic fibers were abundant in the subendothelial area but scarce in the media even in the closed ductus arteriosus (DA) of full-term BN neonates. DNA microarray analysis identified 52 upregulated genes (fold difference >2.5) and 23 downregulated genes (fold difference <0.4) when compared with those of F344 control neonates. Among these genes, 8 (Tbx20, Scn3b, Stac, Sphkap, Trpm8, Rup2, Slc37a2, and RGD1561216) are located in chromosomes 8 and 9. Interestingly, it was also suggested that the significant decrease in the expression levels of the PGE2-specfic receptor, EP4, plays a critical role in elastogenesis in the DA. Conclusions: BN rats exhibited dysregulation of elastogenesis in the DA. DNA microarray analysis identified the candidate genes including EP4 involved in the DNA phenotype. Further investigation of these newly identified genes will hopefully clarify the molecular mechanisms underlying the irregular formation of elastic fibers in PDA.
机译:背景:专利导管(PDA)是儿童中最常见的先天性心血管缺陷之一。棕挪威(BN)近交大鼠呈现较高的PDA频率。先前的研究报告说,在该菌株中,染色体8和9上的2个不同的定量性状基因座与PDA显着连接。然而,BN大鼠PDA表型下面的遗传或分子机制尚未得到完全研究。方法和结果:发现弹性纤维在潜水区域中丰富,但甚至在全术BN新生儿的闭合导管(DA)中均匀的介质中稀缺。与F344控制新生儿相比,DNA微阵列分析鉴定了52个上调基因(折叠差> 2.5)和23个下调基因(折叠差<0.4)。在这些基因中,8(TBX20,SCN3B,StAC,SPHKAP,TRPM8,RUP2,SLC37A2和RGD1561216)位于染色体8和9中。有趣的是,还表明PGE2-SPECFIC的表达水平显着降低受体,EP4,在DA中的弹性发生中起着关键作用。结论:BN大鼠在DA中表现出弹性发生的诱导。 DNA微阵列分析鉴定候选基因,包括EP4参与DNA表型。进一步调查这些新发现基因的进一步调查将阐明PDA中弹性纤维不规则形成的分子机制。

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