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Physical and genetic interactions between Alx4 and Cart1.

机译:Alx4和Cart1之间的物理和遗传相互作用。

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Alx4 and Cart1 are closely related members of the family of transcription factors that contain the paired-type homeodomain. In contrast to other types of homeodomains, the paired-type homeodomain has been shown to mediate high-affinity sequence-specific DNA binding to palindromic elements as either homodimers or as heterodimers with other family members. Alx4 and Cart1 are co-expressed at several sites during development, including the craniofacial mesenchyme, the mesenchymal derivatives of neural crest cells in the first branchial arch and the limb bud mesenchyme. Because of the molecular similarity and overlapping expression pattern, we have analyzed the functional and genetic relationships between Alx4 and Cart1. The two proteins have similar DNA-binding activity in vitro and can form DNA-binding heterodimers; furthermore, they activate transcription of reporter genes that contain high-affinity DNA-binding sites in cell culture in a similar manner. Therefore, at least by these criteria, the two proteins are functionally redundant. Analysis of double mutant animals reveals several genetic interactions. First, mutation of Cart1 exacerbates Alx4-dependent polydactyly in a manner that is dependent on gene dosage. Second, there are complex genetic interactions in the craniofacial region that reveal a role for both genes in the fusion of the nasal cartilages and proper patterning of the mandible, as well as other craniofacial structures. Third, double mutant mice show a split sternum that is not detected in mice with any other genotype. Interpreted in the context of the biochemical characterization, the genetic analysis suggests that Alx4 and Cart1 are indeed functionally redundant, and reveal both unique and redundant functions for these genes in development.
机译:Alx4和Cart1是包含配对型同源域的转录因子家族的密切相关成员。与其他类型的同源域相反,成对类型的同源域已显示出以同二聚体或与其他家族成员异二聚体的形式与回文元素介导高亲和力序列特异性DNA结合。 Alx4和Cart1在发育过程中在多个位点共表达,包括颅面间充质,第一arch弓中神经the细胞的间充质衍生物和肢芽间充质。由于分子的相似性和重叠的表达模式,我们已经分析了Alx4和Cart1之间的功能和遗传关系。这两种蛋白质在体外具有相似的DNA结合活性,可以形成DNA结合异二聚体。此外,它们以类似方式激活细胞培养物中含有高亲和力DNA结合位点的报告基因的转录。因此,至少根据这些标准,这两种蛋白质在功能上是多余的。对双突变动物的分析揭示了几种遗传相互作用。首先,Cart1的突变以依赖于基因剂量的方式加剧了Alx4依赖性。其次,颅面区域存在复杂的遗传相互作用,揭示了这两个基因在鼻软骨融合和下颌骨以及其他颅面结构的正确模式中的作用。第三,双突变小鼠显示胸骨分裂,而其他任何基因型的小鼠均未检测到。在生化特征的背景下解释,遗传分析表明Alx4和Cart1确实在功能上是多余的,并揭示了这些基因在发育中的独特和冗余功能。

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