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Tbx18 function in epicardial development

机译:Tbx18在心外膜发育中的功能

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AimsThe embryonic epicardium is a source of smooth muscle cells and fibroblasts of the coronary vasculature and of the myocardium, but the molecular circuits that direct the temporal and spatial generation of these cell types from epicardium-derived cells are only partly known. We aimed to elucidate the functional significance of the conserved epicardial expression of the T-box transcription factor gene Tbx18 using transgenic technology in the mouse.Methods and resultsWe show by cellular and molecular analyses that in Tbx18-deficient mice the epicardium is formed normally and that epicardial cells undergo an epithelial-mesenchymal transition, differentiate into smooth muscle cells and fibroblasts, and form a normal coronary vasculature and fibrous skeleton. Prolonged expression of Tbx18 in epicardium-derived cells by a transgenic approach in vivo does not affect the differentiation and migratory behaviour of these cells. In contrast, epicardial misexpression of a transcriptional activator version of Tbx18, Tbx18VP16, results in premature smooth muscle differentiation of epicardial cells. Inhibition of Notch and transforming growth factor beta receptor signalling in Tbx18VP16 expressing epicardial cells in explant cultures reverts this phenotype.ConclusionTbx18 is dispensable for epicardial development, yet a repressive T-box function may be required to prevent premature smooth muscle cell differentiation by repressing transforming growth factor beta receptor and Notch signalling in the embryonic epicardium.
机译:目的胚胎心外膜是冠状血管和心肌的平滑肌细胞和成纤维细胞的来源,但是仅部分了解从心外膜衍生的细胞指导这些细胞类型的时空生成的分子回路。我们旨在通过转基因技术阐明小鼠T-box转录因子基因Tbx18保守心外膜表达的功能意义。方法和结果我们通过细胞和分子分析表明,在Tbx18缺陷小鼠中,心外膜正常形成,并且心外膜细胞经历上皮-间质转化,分化为平滑肌细胞和成纤维细胞,并形成正常的冠状脉管系统和纤维骨架。通过体内转基因方法,Tbx18在心外膜衍生细胞中的延长表达不会影响这些细胞的分化和迁移行为。相反,Tbx18,Tbx18VP16转录激活剂版本的心外膜错误表达会导致心外膜细胞过早的平滑肌分化。在外植体培养的心外膜表达Tbx18VP16的心外膜细胞中抑制Notch和转化生长因子β受体信号可逆转该表型。胚胎心外膜中的β因子受体和Notch信号传导。

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