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对定位Hoxd-11和Hoxd-10表达边界所需调控元件进行体内靶向诱变。

In vivo targeted mutagenesis of a regulatory element required for positioning the Hoxd-11 and Hoxd-10 expression boundaries.

作者信息

Gérard M, Chen J Y, Gronemeyer H, Chambon P, Duboule D, Zákány J

机构信息

Department of Zoology and Animal Biology, University of Geneva, Sciences III, Switzerland.

出版信息

Genes Dev. 1996 Sep 15;10(18):2326-34. doi: 10.1101/gad.10.18.2326.

Abstract

Vertebrate Hox genes are required for the proper organization of structures along the rostrocaudal axis. Hoxd-11 is expressed in the posterior part of the embryo, up to the level of prevertebra 27, and its expression boundary is reproduced by a Hoxd-11/lacZ transgene. Expression of this transgene anterior to prevertebra 27 is prevented by the silencing activity of a cis-acting element, region IX. Using transgenic mice, we show that Hoxd-11 repression by region IX is necessary to position the sacrum properly. This silencing activity depends on phylogenetically conserved sequences able to bind in vitro retinoic acid receptors and COUP-TFs. ES cells were used to generate mice carrying a subtle mutation that abolishes binding of nuclear receptors to region IX. Mutant mice display an anterior shift of their lumbosacral transition inherited as a codominant trait. In mutant embryos, expression of both Hoxd-11 and Hoxd-10 mRNAs in the prevertebral column is anteriorized. These results illustrate the sharing, in cis, of a single regulatory element in order to establish the expression boundaries of two neighboring Hoxd genes.

摘要

脊椎动物的Hox基因对于沿头尾轴正确组织结构是必需的。Hoxd - 11在胚胎后部表达,直至第27节椎骨水平,并且其表达边界可由Hoxd - 11 / lacZ转基因重现。该转基因在第27节椎骨前方的表达受到顺式作用元件IX区的沉默活性的抑制。利用转基因小鼠,我们发现IX区对Hoxd - 11的抑制作用对于正确定位骶骨是必要的。这种沉默活性依赖于能够在体外结合视黄酸受体和COUP - TF的系统发育保守序列。胚胎干细胞被用于生成携带微小突变的小鼠,该突变消除了核受体与IX区的结合。突变小鼠表现出腰骶移行的向前移位,这作为一种共显性性状遗传。在突变胚胎中,Hoxd - 11和Hoxd - 10 mRNA在椎骨前柱中的表达均向前移位。这些结果说明了为了建立两个相邻Hoxd基因的表达边界,在顺式作用中共享单个调控元件的情况。

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