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EMX2通过直接指定皮质祖细胞来调节新皮质中主要感觉和运动区域的大小和位置。

EMX2 regulates sizes and positioning of the primary sensory and motor areas in neocortex by direct specification of cortical progenitors.

作者信息

Hamasaki Tadashi, Leingärtner Axel, Ringstedt Thomas, O'Leary Dennis D M

机构信息

Molecular Neurobiology Laboratory, The Salk Institute, 10010 North Torrey Pines Road, La Jolla, CA 92037, USA.

出版信息

Neuron. 2004 Aug 5;43(3):359-72. doi: 10.1016/j.neuron.2004.07.016.

Abstract

Genetic studies of neocortical area patterning are limited, because mice deficient for candidate regulatory genes die before areas emerge and have other complicating issues. To define roles for the homeodomain transcription factor EMX2, we engineered nestin-Emx2 transgenic mice that overexpress Emx2 in cortical progenitors coincident with expression of endogenous Emx2 and survive postnatally. Cortical size, lamination, thalamus, and thalamocortical pathfinding are normal in homozygous nestin-Emx2 mice. However, primary sensory and motor areas are disproportionately altered in size and shift rostrolaterally. Heterozygous transgenics have similar but smaller changes. Opposite changes are found in heterozygous Emx2 knockout mice. Fgf8 expression in the commissural plate of nestin-Emx2 mice is indistinguishable from wild-type, but Pax6 expression is downregulated in rostral cortical progenitors, suggesting that EMX2 repression of PAX6 specification of rostral identities contributes to reduced rostral areas. We conclude that EMX2 levels in cortical progenitors disproportionately specify sizes and positions of primary cortical areas.

摘要

新皮质区域模式形成的遗传学研究受到限制,因为候选调控基因缺陷的小鼠在区域形成之前就死亡了,并且存在其他复杂问题。为了确定同源结构域转录因子EMX2的作用,我们构建了巢蛋白-Emx2转基因小鼠,其在皮质祖细胞中与内源性Emx2的表达同时过表达Emx2,并能在出生后存活。纯合巢蛋白-Emx2小鼠的皮质大小、分层、丘脑和丘脑皮质路径寻找均正常。然而,主要感觉和运动区域的大小发生了不成比例的改变,并向 rostrolaterally 移位。杂合转基因小鼠有类似但较小的变化。在杂合Emx2基因敲除小鼠中发现了相反的变化。巢蛋白-Emx2小鼠连合板中的Fgf8表达与野生型无差异,但Pax6在 Rostral 皮质祖细胞中的表达下调,提示EMX2对 Rostral 身份的PAX6特化的抑制作用导致 Rostral 区域减少。我们得出结论,皮质祖细胞中的EMX2水平不成比例地决定了主要皮质区域的大小和位置。

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