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首页> 外文期刊>BMC Genomics >Hif1α down-regulation is associated with transposition of great arteries in mice treated with a retinoic acid antagonist
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Hif1α down-regulation is associated with transposition of great arteries in mice treated with a retinoic acid antagonist

机译:Hif1α下调与视黄酸拮抗剂治疗的小鼠大动脉转位有关

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Background Congenital heart defect (CHD) account for 25% of all human congenital abnormalities. However, very few CHD-causing genes have been identified so far. A promising approach for the identification of essential cardiac regulators whose mutations may be linked to human CHD, is the molecular and genetic analysis of heart development. With the use of a triple retinoic acid competitive antagonist (BMS189453) we previously developed a mouse model of congenital heart defects (81%), thymic abnormalities (98%) and neural tube defects (20%). D-TGA (D-transposition of great arteries) was the most prevalent cardiac defect observed (61%). Recently we were able to partially rescue this abnormal phenotype (CHD were reduced to 64.8%, p = 0.05), by oral administration of folic acid (FA). Now we have performed a microarray analysis in our mouse models to discover genes/transcripts potentially implicated in the pathogenesis of this CHD. Results We analysed mouse embryos (8.5 dpc) treated with BMS189453 alone and with BMS189453 plus folic acid (FA) by microarray and qRT-PCR. By selecting a fold change (FC) ≥ ± 1.5, we detected 447 genes that were differentially expressed in BMS-treated embryos vs. untreated control embryos, while 239 genes were differentially expressed in BMS-treated embryos whose mothers had also received FA supplementation vs. BMS-treated embryos. On the basis of microarray and qRT-PCR results, we further analysed the Hif1α gene. In fact Hif1α is down-regulated in BMS-treated embryos vs. untreated controls (FCmicro = -1.79; FCqRT-PCR = -1.76; p = 0.005) and its expression level is increased in BMS+FA-treated embryos compared to BMS-treated embryos (FCmicro = +1.17; FCqRT-PCR = +1.28: p = 0.005). Immunofluorescence experiments confirmed the under-expression of Hif1α protein in BMS-treated embryos compared to untreated and BMS+FA-treated embryos and, moreover, we demonstrated that at 8.5 dpc, Hif1α is mainly expressed in the embryo heart region. Conclusions We propose that Hif1α down-regulation in response to blocking retinoic acid binding may contribute to the development of cardiac defects in mouse newborns. In line with our hypothesis, when Hif1α expression level is restored (by supplementation of folic acid), a decrement of CHD is found. To the best of our knowledge, this is the first report that links retinoic acid metabolism to Hif1α regulation and the development of D-TGA.
机译:背景先天性心脏缺陷(CHD)占所有人类先天性异常的25%。但是,到目前为止,几乎没有发现引起冠心病的基因。鉴定可能与人类冠心病相关的突变的基本心脏调节剂的一种有前途的方法是心脏发育的分子和遗传分析。通过使用三视黄酸竞争性拮抗剂(BMS189453),我们先前开发了先天性心脏缺陷(81%),胸腺异常(98%)和神经管缺陷(20%)的小鼠模型。 D-TGA(大动脉的D-移位)是观察到的最普遍的心脏缺陷(61%)。最近,我们能够通过口服叶酸(FA)来部分挽救这种异常表型(CHD降至64.8%,p = 0.05)。现在,我们已经在小鼠模型中进行了微阵列分析,以发现可能与该冠心病发病机制有关的基因/转录本。结果我们通过微阵列和qRT-PCR分析了单独用BMS189453和用BMS189453加叶酸(FA)处理的小鼠胚胎(8.5 dpc)。通过选择倍数变化(FC)≥±1.5,我们检测到447个在BMS处理的胚胎与未处理的对照胚胎中差异表达的基因,而239个基因在BMS处理的胚胎中,其母亲也接受了FA补充的基因差异表达。 BMS处理过的胚胎基于芯片和qRT-PCR结果,我们进一步分析了Hif1α基因。实际上,Hif1α在BMS处理的胚胎与未处理的对照中被下调(FC micro = -1.79; FC qRT-PCR = -1.76; p = 0.005)和与BMS处理过的胚胎相比,其在BMS + FA处理过的胚胎中的表达水平有所提高(FC micro = +1.17; FC qRT-PCR = +1.28:p = 0.005 )。免疫荧光实验证实,与未处理和BMS + FA处理的胚胎相比,BMS处理的胚胎中的Hif1α蛋白表达不足,此外,我们证明了8.5 dpc时,Hif1α主要在胚胎心脏区域表达。结论我们建议响应阻滞视黄酸结合而下调Hif1α可能有助于小鼠新生儿心脏缺陷的发展。根据我们的假设,当Hif1α表达水平恢复(通过补充叶酸)时,发现CHD减少。据我们所知,这是第一个将视黄酸代谢与Hif1α调节和D-TGA的发展联系起来的报告。

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