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Misexpression of Polycomb-Group Proteins in Xenopus Alters Anterior Neural Development and Represses Neural Target Genes

机译:在非洲爪蟾中的多梳子组蛋白的过表达改变前神经发育并抑制神经靶基因。

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In Drosophila, the Polycomb-group constitutes a set of structurally diverse proteins that act together to silence target genes. Many mammalian Polycomb-group proteins have also been identified and show functional similarities with their invertebrate counterparts. To begin to analyze the function of Polycomb-group proteins in Xenopus development, we have cloned a Xenopus homology of Drosophila Polycomblike, XPcl1. XPcl1 mRNA is present both maternally and zygotically, with prominent zygotic expression in the anterior central nervous system. Misexpression of Pcl1 by RNA injection into embryos produces defects in the anterior central nervous system. The forebrain and midbrain contain excess neural tissue at the expense of the ventricle and include greatly thickened floor and roof plates. The eye fields are present but Rx2A, an eye-specific marker, is completely repressed. Overexpression of Pcl1 in Xenopus embryos alters two hindbrain markers, repressing En-2 and shifting it and Krox-20 in a posterior direction. Similar neural phenotypes and effects on the En-2 expression pattern were produced by overexpression of three other structurally unrelated Polycomb-group proteins: M33, XBmi-1, and mPh2. These observations indicate an important role for the Polycomb-group in regulating gene expression in the developing anterior central nervous system.
机译:在果蝇中,Polycomb-基团构成了一组结构多样的蛋白质,这些蛋白质共同作用以使靶基因沉默。许多哺乳动物的Polycomb-group蛋白也已被鉴定出来,并与它们的无脊椎动物对应蛋白显示出功能相似性。为了开始分析Polycomb-group蛋白在非洲爪蟾发育中的功能,我们克隆了果蝇Polycomblike XPcl1的非洲爪蟾同源性。 XPcl1 mRNA既存在于母体中又存在于合子中,在中枢神经系统前部具有突出的合子表达。通过将RNA注入胚胎而导致Pcl1的错误表达在中枢神经系统中产生缺陷。前脑和中脑包含过多的神经组织,但以脑室为代价,并且包括大大增厚的地板和顶板。存在眼场,但完全抑制了眼睛特异性标记Rx2A。非洲爪蟾胚胎中Pcl1的过表达改变了两个后脑标志物,抑制了En-2并将其和Krox-20向后移动。类似的神经表型和对En-2表达模式的影响是通过三种其他与结构无关的Polycomb-group蛋白(M33,XBmi-1和mPh2)的过表达产生的。这些观察表明,Polycomb-基团在调节发育中的前中枢神经系统中的基因表达中具有重要作用。

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