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首页> 外文期刊>European Heart Journal: The Journal of the European Society of Cardiology >A cell-autonomous role of Cited2 in controlling myocardial and coronary vascular development
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A cell-autonomous role of Cited2 in controlling myocardial and coronary vascular development

机译:Cited2在控制心肌和冠状血管发育中的细胞自主作用

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AimsMyocardial development is dependent on concomitant growth of cardiomyocytes and a supporting vascular network. The coupling of myocardial and coronary vascular development is partly mediated by vascular endothelial growth factor (VEGFA) signalling and additional unknown mechanisms. We examined the cardiomyocyte specific role of the transcriptional co-activator Cited2 on myocardial microstructure and vessel growth, in relation to Vegfa expression.Methods and resultsA cardiomyocyte-specific knockout of mouse Cited2 (Cited2Nkx) was analysed using magnetic resonance imaging and histology. Ventricular septal defects and significant compact layer thinning (P 0.02 at right ventricular apex, P 0.009 at the left ventricular apex in Cited2Nkx vs. controls, n= 11 vs. n= 7, respectively) were found. This was associated with a significant decrease in the number of capillaries to larger vessels (ratio 1.56 ± 0.56 vs. 3.25 ± 1.63, P= 2.7 × 10-6 Cited2Nkx vs. controls, n= 11 vs. n= 7, respectively) concomitant with a 1.5-fold reduction in Vegfa expression (P 0.02, Cited2Nkx vs. controls, n= 12 vs. n= 12, respectively). CITED2 was subsequently found at the Vegfa promoter in mouse embryonic hearts using chromatin immunoprecipitation, and moreover found to stimulate human VEGFA promoter activity in cooperation with TFAP2 transcription factors in transient transfection assays. There was no change in the myocardial expression of the left-right patterning gene Pitx2c, a previously known target of CITED2.ConclusionsThis study delineates a novel cell-autonomous role of Cited2 in regulating VEGFA transcription and the development of myocardium and coronary vasculature in the mouse. We suggest that coupling of myocardial and coronary growth in the developing heart may occur in part through a Cited2→Vegfa pathway.
机译:目的心肌的发育取决于心肌细胞的伴随生长和支持性血管网络。心肌和冠状血管发育的耦合部分由血管内皮生长因子(VEGFA)信号传导和其他未知机制介导。我们检查了转录共激活因子Cited2在心肌微结构和血管生长方面与Vegfa表达有关的心肌特异性作用。发现室间隔缺损和显着的致密层变薄(在Cited2Nkx与对照组相比,右心室顶点的P <0.02,左心室顶点的P <0.009,分别为n = 11 vs. n = 7)。这与较大血管的毛细血管数目显着减少有关(比率分别为1.56±0.56与3.25±1.63,P = 2.7×10-6 Cited2Nkx与对照组,n = 11与n = 7)。 Vegfa表达降低1.5倍(P <0.02,Cited2Nkx与对照组相比,n = 12与n = 12)。随后,使用染色质免疫沉淀法在小鼠胚胎心脏的Vegfa启动子处发现了CITED2,并且在瞬时转染测定中发现与TFAP2转录因子协同刺激人VEGFA启动子活性。左右模式基因Pitx2c(先前已知的CITED2靶标)的心肌表达没有变化。 。我们建议在发育中的心脏中,心肌和冠状动脉生长的耦合可能部分通过Cited2→Vegfa途径发生。

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