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Analysis of Ellis van Creveld syndrome gene products: implications for cardiovascular development and disease

机译:Ellis van Creveld综合征基因产物的分析:对心血管发展和疾病的影响

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摘要

Mutations identified in a cohort of patients with atrioventricular septal defects as a part of Ellis van Creveld syndrome (EvC syndrome) led us to study the role of two non-homologous genes, EVC and LBN, in heart development and disease pathogenesis. To address the cause of locus heterogeneity resulting in an indistinguishable heart–hand phenotype, we carried out in situ hybridization and immunofluorescence and identified co-localization of Evc and Lbn mRNA and protein. In the heart, expression was identified to be strongest in the secondary heart field, including both the outflow tract and the dorsal mesenchymal protrusion, but was also found in mesenchymal structures of the atrial septum and the atrioventricular cushions. Finally, we studied the transcriptional hierarchy of EVC and LBN but did not find any evidence of direct transcriptional interregulation between the two. Due to the locus heterogeneity of human mutations predicted to result in a loss of protein function, a bidirectional genomic organization and overlapping expression patterns, we speculate that these proteins function coordinately in cardiac development and that loss of this coordinate function results in the characteristics of EvC syndrome.
机译:在一组房室间隔缺损患者中鉴定出的突变是Ellis van Creveld综合征(EvC综合征)的一部分,这使我们研究了两个非同源基因EVC和LBN在心脏发育和疾病发病机理中的作用。为了解决导致无法区分心手表型的基因座异质性的原因,我们进行了原位杂交和免疫荧光分析,并鉴定了Evc和Lbn mRNA和蛋白质的共定位。在心脏中,表达被确定为在次级心脏区域中最强,包括流出道和背侧间充质突出,但在房间隔和房室垫的间质结构中也发现。最后,我们研究了EVC和LBN的转录层次,但未发现两者之间直接转录互调控的任何证据。由于人类突变的基因座异质性预计会导致蛋白质功能丧失,双向基因组组织和重叠表达模式,因此我们推测这些蛋白质在心脏发育中具有协调功能,而这种协调功能的丧失导致EvC的特征综合症。

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