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短散在重复序列可能参与哺乳动物特有的脑形成过程。

Possible involvement of SINEs in mammalian-specific brain formation.

作者信息

Sasaki Takeshi, Nishihara Hidenori, Hirakawa Mika, Fujimura Koji, Tanaka Mikiko, Kokubo Nobuhiro, Kimura-Yoshida Chiharu, Matsuo Isao, Sumiyama Kenta, Saitou Naruya, Shimogori Tomomi, Okada Norihiro

机构信息

Graduate School of Bioscience and Biotechnology, Tokyo Institute of Technology, 4259-B-21 Nagatsuta-cho, Midori-ku, Yokohama, Kanagawa 226-8501, Japan.

出版信息

Proc Natl Acad Sci U S A. 2008 Mar 18;105(11):4220-5. doi: 10.1073/pnas.0709398105. Epub 2008 Mar 11.

Abstract

Retroposons, such as short interspersed elements (SINEs) and long interspersed elements (LINEs), are the major constituents of higher vertebrate genomes. Although there are many examples of retroposons' acquiring function, none has been implicated in the morphological innovations specific to a certain taxonomic group. We previously characterized a SINE family, AmnSINE1, members of which constitute a part of conserved noncoding elements (CNEs) in mammalian genomes. We proposed that this family acquired genomic functionality or was exapted after retropositioning in a mammalian ancestor. Here we identified 53 new AmnSINE1 loci and refined 124 total loci, two of which were further analyzed. Using a mouse enhancer assay, we demonstrate that one SINE locus, AS071, 178 kbp from the gene FGF8 (fibroblast growth factor 8), is an enhancer that recapitulates FGF8 expression in two regions of the developing forebrain, namely the diencephalon and the hypothalamus. Our gain-of-function analysis revealed that FGF8 expression in the diencephalon controls patterning of thalamic nuclei, which act as a relay center of the neocortex, suggesting a role for FGF8 in mammalian-specific forebrain patterning. Furthermore, we demonstrated that the locus, AS021, 392 kbp from the gene SATB2, controls gene expression in the lateral telencephalon, which is thought to be a signaling center during development. These results suggest important roles for SINEs in the development of the mammalian neuronal network, a part of which was initiated with the exaptation of AmnSINE1 in a common mammalian ancestor.

摘要

逆转座子,如短散在元件(SINEs)和长散在元件(LINEs),是高等脊椎动物基因组的主要组成部分。尽管有许多逆转座子获得功能的例子,但尚无一个与特定分类群特有的形态创新有关。我们之前鉴定了一个SINE家族,即AmnSINE1,其成员构成了哺乳动物基因组中保守非编码元件(CNEs)的一部分。我们提出,这个家族在哺乳动物祖先中逆转座后获得了基因组功能或被适应性利用。在这里,我们鉴定了53个新的AmnSINE1位点,并完善了总共124个位点,其中两个位点进行了进一步分析。使用小鼠增强子检测法,我们证明一个SINE位点AS071,距离基因FGF8(成纤维细胞生长因子8)178千碱基对,是一个增强子,它在发育中的前脑的两个区域,即间脑和下丘脑,重现FGF8的表达。我们的功能获得分析表明,间脑中FGF8的表达控制着丘脑核的模式形成,丘脑核作为新皮层的中继中心,这表明FGF8在哺乳动物特有的前脑模式形成中发挥作用。此外,我们证明了距离基因SATB2 392千碱基对的位点AS021控制着端脑外侧的基因表达,端脑外侧在发育过程中被认为是一个信号中心。这些结果表明SINEs在哺乳动物神经网络发育中起着重要作用,其中一部分始于AmnSINE1在共同的哺乳动物祖先中的适应性利用。

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