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首页> 外文期刊>Genomics >The Mouse Laf4 Gene: Exon/Intron Organization, cDNA Sequence, Alternative Splicing, and Expression during Central Nervous System Development.
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The Mouse Laf4 Gene: Exon/Intron Organization, cDNA Sequence, Alternative Splicing, and Expression during Central Nervous System Development.

机译:小鼠Laf4基因:外显子/内含子组织,cDNA序列,可变剪接和中枢神经系统发育过程中的表达。

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The cerebral cortex is a tissue with a high degree of neuronal diversity. It consists of six cell layers with a unique set of neuronal subtypes. A crucial step in the process of cortical differentiation is the transition from a mitotically active neuroblast to a postmitotic young neuron. To identify genes involved in the control of this transition, we applied a novel method of cDNA subtraction based on mirror-orientation selection. One of the genes we have identified in our screening proved to be a mouse homolog of the human putative transcription factor LAF4. We identified alternatively spliced forms of mouse Laf4 that encode several forms of putative protein with potentially different transactivation functions. Two forms are expressed mainly during embryogenesis, whereas the other forms are expressed mainly in adults. We have found that Laf4 transcription becomes very quickly upregulated as soon as young cortical neurons leave the ventricular zone (VZ), the cortical-proliferative compartment. This coincides with the initial steps of cortical differentiation. Laf4 becomes downregulated in postnatal cortex, indicating its involvement in the transcriptional regulation of the early steps of cortical differentiation. We have also examined Laf4 expression in the brains of Sey and reeler mutants. Laf4 was downregulated in the lateroventral part of the cerebral cortex and completely lost in the piriform cortex of the Sey mutant embryos. We also compared its expression during central nervous system development with that of its closest homolog, Fmr2, a gene implicated in mental retardation in humans. (c)2002 Elsevier Science (USA).
机译:大脑皮层是具有高度神经元多样性的组织。它由六个具有独特的神经元亚型集的细胞层组成。皮质分化过程中的关键步骤是从有丝分裂活跃的神经母细胞过渡到有丝分裂后的年轻神经元。为了确定参与此过渡控制的基因,我们应用了基于镜像方向选择的cDNA减法新方法。我们在筛选中鉴定出的基因之一被证明是人类推定转录因子LAF4的小鼠同源物。我们确定了小鼠Laf4的可变剪接形式,其编码几种形式的推定蛋白质具有潜在的反式激活功能。两种形式主要在胚胎发生过程中表达,而其他形式主要在成年人中表达。我们已经发现,一旦年轻的皮质神经元离开心室区(VZ)(即皮质增殖区),Laf4转录就会迅速上调。这与皮层分化的初始步骤相吻合。 Laf4在产后皮质中被下调,表明其参与了皮质分化早期步骤的转录调控。我们还检查了Sey和reeler突变体大脑中的Laf4表达。 Laf4在大脑皮层的后腹部分被下调,并在Sey突变体胚胎的梨状皮层中完全消失。我们还比较了其在中枢神经系统发育过程中的表达与其最接近的同源基因Fmr2的表达,Fmr2是与人类智力发育迟缓有关的基因。 (c)2002 Elsevier Science(美国)。

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