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首页> 外文期刊>Genesis: the journal of genetics and development >A unique mouse strain expressing Cre recombinase for tissue-specific analysis of gene function in palate and kidney development.
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A unique mouse strain expressing Cre recombinase for tissue-specific analysis of gene function in palate and kidney development.

机译:表达Cre重组酶的独特小鼠品系,用于组织特异性分析pa和肾脏发育中的基因功能。

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摘要

Mammalian palate development is a multistep process, involving initial bilateral downward outgrowth of the palatal shelves from the oral side of the maxillary processes, followed by stage-specific palatal shelf elevation to the horizontal position above the developing tongue and subsequent fusion of the bilateral palatal shelves at the midline to form the intact roof of the oral cavity. While mutations in many genes have been associated with cleft palate pathogenesis, the molecular mechanisms regulating palatal shelf growth, patterning, and elevation are not well understood. Genetic studies of the molecular mechanisms controlling palate development in mutant mouse models are often complicated by early embryonic lethality or gross craniofacial malformation. We report here the development of a mouse strain for tissue-specific analysis of gene function in palate development. We inserted an IresCre bicistronic expression cassette into the 3' untranslated region of the mouse Osr2 gene through gene targeting. We show, upon crossing to the R26R reporter mice, that Cre expression from the Osr2(IresCre) knockin allele activated beta-galactosidase expression specifically throughout the developing palatal mesenchyme from the onset of palatal shelf outgrowth. In addition, the Osr2(IresCre) mice display exclusive Cre-mediated recombination in the glomeruli tissues derived from the metanephric mesenchyme and complete absence of Cre activity in other epithelial and mesenchymal tissues in the developing metanephric kidney. These data indicate that the Osr2(IresCre) knockin mice provide a unique tool for tissue-specific studies of the molecular mechanisms regulating palate and kidney development.
机译:哺乳动物的development骨发育是一个多步骤的过程,涉及从上颌骨的口腔一侧开始shelves骨支架的双向向下生长,然后是特定阶段的pa骨支架升高到发育舌上方的水平位置,随后融合双侧lat骨支架在中线形成完整的口腔顶部。尽管许多基因的突变与c裂的发病机理有关,但调节regulating架生长,构图和升高的分子机制尚不清楚。早期胚胎致死率或严重颅面畸形常常使在突变小鼠模型中控制pa发育的分子机制的遗传研究复杂化。我们在这里报告了小鼠品系的发展,用于组织特异性分析pa发育中的基因功能。我们通过基因靶向将IresCre双顺反子表达盒插入小鼠Osr2基因的3'非翻译区。我们显示,与R26R报告基因小鼠杂交后,从Osr2(IresCre)敲入等位基因的Cre表达激活了β-半乳糖苷酶的表达,特别是从pa架生长开始就贯穿整个pa间充质。此外,Osr2(IresCre)小鼠在衍生自后肾间充质的肾小球组织中显示出独家的Cre介导重组,而在发育中的后肾中其他上皮和间充质组织中完全没有Cre活性。这些数据表明,Osr2(IresCre)敲入小鼠为调节pa和肾脏发育的分子机制提供了组织特异性研究的独特工具。

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