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Recombineering-based dissection of flanking and paralogous Hox gene functions in mouse reproductive tracts

机译:基于重组的小鼠生殖道侧翼和旁系Hox基因功能的解剖

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摘要

Hox genes are key regulators of development. In mammals, the study of these genes is greatly confounded by their large number, overlapping functions and interspersed shared enhancers. Here, we describe the use of a novel recombineering strategy to introduce simultaneous frameshift mutations into the flanking Hoxa9, Hoxa10 and Hoxa11 genes, as well as their paralogs on the HoxD cluster. The resulting Hoxa9,10,11 mutant mice displayed dramatic synergistic homeotic transformations of the reproductive tracts, with the uterus anteriorized towards oviduct and the vas deferens anteriorized towards epididymis. The Hoxa9,10,11 mutant mice also provided a genetic setting that allowed the discovery of Hoxd9,10,11 redundant reproductive tract patterning function. Both shared and distinct Hox functions were defined. Hoxd9,10,11 play a crucial role in the regulation of uterine immune function. Non-coding nonpolyadenylated RNAs were among the key Hox targets, with dramatic downregulation in mutants. We observed Hox cross-regulation of transcription and splicing. In addition, we observed a surprising anti-dogmatic apparent posteriorization of the uterine epithelium. In caudal regions of the uterus, the normal simple columnar epithelium flanking the lumen was replaced by a pseudostratified transitional epithelium, normally found near the more posterior cervix. These results identify novel molecular functions of Hox genes in the development of the male and female reproductive tracts.
机译:Hox基因是发育的关键调节因子。在哺乳动物中,这些基因的研究因其数量众多,功能重叠和散布的共享增强子而大大混淆。在这里,我们描述了使用新的重组策略将同时移码突变引入侧翼Hoxa9,Hoxa10和Hoxa11基因,以及它们在HoxD簇上的旁系同源物。产生的Hoxa9,10,11突变小鼠表现出生殖道的显着协同顺同性转化,子宫向输卵管前移,输精管向附睾前移。 Hoxa9,10,11突变小鼠还提供了遗传背景,允许发现Hoxd9,10,11多余的生殖道构图功能。定义了共享的和不同的Hox函数。 Hoxd9,10,11在调节子宫免疫功能中起着至关重要的作用。非编码的非聚腺苷酸化的RNAs是关键的Hox靶标之一,突变体中的下调幅度很大。我们观察到转录和剪接的Hox交叉调节。此外,我们观察到了令人惊讶的子宫上皮的反教条性的明显后继性。在子宫的尾部区域,位于管腔两侧的正常简单柱状上皮被假复层状过渡上皮所取代,通常在子宫颈后部附近发现。这些结果确定了Hox基因在男性和女性生殖道发育中的新型分子功能。

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