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Arid3b对于第二心脏区域细胞的部署和心脏模式形成至关重要。

Arid3b is essential for second heart field cell deployment and heart patterning.

作者信息

Uribe Verónica, Badía-Careaga Claudio, Casanova Jesús C, Domínguez Jorge N, de la Pompa José Luis, Sanz-Ezquerro Juan José

机构信息

Departamento de Desarrollo y Reparación Cardiovascular, Centro Nacional de Investigaciones Cardiovasculares (CNIC), Melchor Fernández Almagro, 3, Madrid 28029, Spain.

Departamento de Biología Experimental, Facultad de Ciencias Experimentales, Universidad de Jaén, CU Las Lagunillas, Jáen 23071, Spain.

出版信息

Development. 2014 Nov;141(21):4168-81. doi: 10.1242/dev.109918.

Abstract

Arid3b, a member of the conserved ARID family of transcription factors, is essential for mouse embryonic development but its precise roles are poorly understood. Here, we show that Arid3b is expressed in the myocardium of the tubular heart and in second heart field progenitors. Arid3b-deficient embryos show cardiac abnormalities, including a notable shortening of the poles, absence of myocardial differentiation and altered patterning of the atrioventricular canal, which also lacks epithelial-to-mesenchymal transition. Proliferation and death of progenitors as well as early patterning of the heart appear normal. However, DiI labelling of second heart field progenitors revealed a defect in the addition of cells to the heart. RNA microarray analysis uncovered a set of differentially expressed genes in Arid3b-deficient tissues, including Bhlhb2, a regulator of cardiomyocyte differentiation, and Lims2, a gene involved in cell migration. Arid3b is thus required for heart development by regulating the motility and differentiation of heart progenitors. These findings identify Arid3b as a candidate gene involved in the aetiology of human congenital malformations.

摘要

Arid3b是保守的ARID转录因子家族成员,对小鼠胚胎发育至关重要,但其确切作用尚不清楚。在此,我们表明Arid3b在管状心脏的心肌和第二心脏场祖细胞中表达。Arid3b缺陷型胚胎表现出心脏异常,包括两极明显缩短、心肌分化缺失以及房室管模式改变,房室管也缺乏上皮-间充质转化。祖细胞的增殖和死亡以及心脏的早期模式看起来正常。然而,对第二心脏场祖细胞的DiI标记显示心脏在添加细胞方面存在缺陷。RNA微阵列分析揭示了Arid3b缺陷组织中一组差异表达基因,包括心肌细胞分化调节因子Bhlhb2和参与细胞迁移的基因Lims2。因此,Arid3b通过调节心脏祖细胞的运动性和分化来促进心脏发育。这些发现确定Arid3b是参与人类先天性畸形病因学的候选基因。

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