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对于En-2转基因的早期胚胎脑表达而言,需要两个Pax结合位点。

Two Pax-binding sites are required for early embryonic brain expression of an Engrailed-2 transgene.

作者信息

Song D L, Chalepakis G, Gruss P, Joyner A L

机构信息

Department of Molecular and Medical Genetics, University of Toronto, Canada.

出版信息

Development. 1996 Feb;122(2):627-35. doi: 10.1242/dev.122.2.627.

Abstract

The temporally and spatially restricted expression of the mouse Engrailed (En) genes is essential for development of the midbrain and cerebellum. The regulation of En-2 expression was studied using in vitro protein-DNA binding assays and in vivo expression analysis in transgenic mice to gain insight into the genetic events that lead to regionalization of the developing brain. A minimum En-2 1.0 kb enhancer fragment was defined and found to contain multiple positive and negative regulatory elements that function in concert to establish the early embryonic mid-hindbrain expression. Furthermore, the mid-hindbrain regulatory sequences were shown to be structurally and functionally conserved in humans. The mouse paired-box-containing genes Pax-2, Pax-5 and Pax-8 show overlapping expression with the En genes in the developing brain. Significantly, two DNA-binding sites for Pax-2, Pax-5 and Pax-8 proteins were identified in the 1.0 kb En-2 regulatory sequences, and mutation of the binding sites disrupted initiation and maintenance of expression in transgenic mice. These results present strong molecular evidence that the Pax genes are direct upstream regulators of En-2 in the genetic cascade controlling mid-hindbrain development. These mouse studies, taken together with others in Drosophila and zebrafish on the role of Pax genes in controlling expression of En family members, indicate that a Pax-En genetic pathway has been conserved during evolution.

摘要

小鼠Engrailed(En)基因在时间和空间上的受限表达对于中脑和小脑的发育至关重要。利用体外蛋白质-DNA结合试验和转基因小鼠体内表达分析对En-2表达的调控进行了研究,以深入了解导致发育中脑区域化的遗传事件。确定了一个最小的En-2 1.0 kb增强子片段,发现其含有多个正负调控元件,这些元件协同作用以建立早期胚胎中后脑表达。此外,中后脑调控序列在结构和功能上在人类中是保守的。小鼠含配对盒基因Pax-2、Pax-5和Pax-8在发育中的脑中与En基因表现出重叠表达。重要的是,在1.0 kb En-2调控序列中鉴定出两个Pax-2、Pax-5和Pax-8蛋白的DNA结合位点,结合位点的突变破坏了转基因小鼠中表达的起始和维持。这些结果提供了强有力的分子证据,表明在控制中后脑发育的遗传级联中,Pax基因是En-2的直接上游调节因子。这些小鼠研究,连同果蝇和斑马鱼中关于Pax基因在控制En家族成员表达中的作用的其他研究,表明Pax-En遗传途径在进化过程中是保守的。

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