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Regulatory analysis of the mouse Hoxb3 gene: Multiple elements work inconcert to direct temporal and spatial patterns of expression

机译:小鼠Hoxb3基因的调控分析:多种因素无法协调一致地指导表达的时空分布

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The expression pattern of the mouse Hoxb3 gene is exceptionally complex and dynamic compared with that of other members of the Herb cluster. There are multiple types of transcripts for Hoxb3 gene, and the anterior boundaries of its expression vary at different stages of development. Two enhancers nanking Hoxb3 on the 3' and 5' sides regulate Hoxb2 and Hoxb4, respectively, and these control regions define the two ends of a 28-kb interval in and around the Hoxb3 locus. To assay the regulatory potential of DNA fragments in this interval we have used transgenic analysis with a lacZ reporter gene to locate cis-elements for directing the dynamic patterns of Hoxb3 expression. Our detailed analysis has identified four new and widely spaced cis-acting regulatory regions that can together account for major aspects of the Hoxb3 expression pattern. Elements Ib, IIIa, and IVb control gene expression in neural and mesodermal tissues; element Va controls mesoderm-specific gene expression. The most anterior neural expression domain of Hoxb3 is controlled by an r5 enhancer (element Na); element IIIa directs reporter expression in the anterior spinal cord and hindbrain up to rb, and the region A enhancer tin element I) mediates posterior neural expression. Hence, the regulation of segmental expression of Hoxb3 in the hindbrain is different from that of Hoxa3, as two separate enhancer elements contribute to expression in r5 and r6,. The mesoderm-specific element (Va) directs reporter expression to prevertebra C1 at 12.5 dpc, which is the anterior limit of paraxial mesoderm expression for Hoxb3. When tested in combinations, these cis-elements appear to work as modules in an additive manner to recapitulate the major endogenous expression patterns of Hoxb3 during embryogenesis. Together our study shows that multiple control elements direct reporter gene expression in diverse tissue-, temporal-, and spatially restricted subset of the endogenous Hoxb3 expression domains and work in concert to control the neural and mesodermal patterns of expression,
机译:与Herb簇的其他成员相比,小鼠Hoxb3基因的表达模式异常复杂且动态。 Hoxb3基因的转录物有多种类型,其表达的前边界在发育的不同阶段会有所不同。位于3'和5'侧的Hoxb3的两个增强子分别调节Hoxb2和Hoxb4,这些控制区域在Hoxb3基因座内和周围定义了一个28kb区间的两端。为了测定此区间内DNA片段的调控潜力,我们使用了带有lacZ报告基因的转基因分析来定位顺式元件,以指导Hoxb3表达的动态模式。我们的详细分析已确定了四个新的且相距较远的顺式作用调控区,它们可以共同构成Hoxb3表达模式的主要方面。元素Ib,IIIa和IVb控制神经和中胚层组织中的基因表达;元素Va控制中胚层特异性基因表达。 Hoxb3的最前神经表达域是由r5增强子(Na元素)控制的。元素IIIa指导记者在前脊髓和后脑中的表达直至rb,而区域A增强子锡元素I)介导后神经表达。因此,Hoxb3在后脑中的节段性表达调控与Hoxa3的调控不同,因为两个独立的增强子元件在r5和r6中表达。中胚层特异性元件(Va)在12.5 dpc时将报告基因的表达导向椎体C1,这是Hoxb3的近轴中胚层表达的前极限。当组合测试时,这些顺式元件似乎以加性方式作为模块起作用,以概括胚胎发生过程中Hoxb3的主要内源表达模式。我们的共同研究表明,多种控制元件指导内源性Hoxb3表达域在不同组织,时间和空间上受限制的子集中的报告基因表达,并协同控制神经和中胚层表达模式,

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