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双性同源基因 Dmrt5 对于哺乳动物尾侧脑皮质的发育是必需的。

The doublesex homolog Dmrt5 is required for the development of the caudomedial cerebral cortex in mammals.

机构信息

Laboratoire de Génétique du Développement, Université Libre de Bruxelles, Institut de Biologie et de Médecine Moléculaires (IBMM), Gosselies, Belgium.

出版信息

Cereb Cortex. 2013 Nov;23(11):2552-67. doi: 10.1093/cercor/bhs234. Epub 2012 Aug 23.

Abstract

Regional patterning of the cerebral cortex is initiated by morphogens secreted by patterning centers that establish graded expression of transcription factors within cortical progenitors. Here, we show that Dmrt5 is expressed in cortical progenitors in a high-caudomedial to low-rostrolateral gradient. In its absence, the cortex is strongly reduced and exhibits severe abnormalities, including agenesis of the hippocampus and choroid plexus and defects in commissural and thalamocortical tracts. Loss of Dmrt5 results in decreased Wnt and Bmp in one of the major telencephalic patterning centers, the dorsomedial telencephalon, and in a reduction of Cajal-Retzius cells. Expression of the dorsal midline signaling center-dependent transcription factors is downregulated, including Emx2, which promotes caudomedial fates, while the rostral determinant Pax6, which is inhibited by midline signals, is upregulated. Consistently, Dmrt5(-/-) brains exhibit patterning defects with a dramatic reduction of the caudomedial cortex. Dmrt5 is increased upon the activation of Wnt signaling and downregulated in Gli3(xt/xt) mutants. We conclude that Dmrt5 is a novel Wnt-dependent transcription factor required for early cortical development and that it may regulate initial cortical patterning by promoting dorsal midline signaling center formation and thereby helping to establish the graded expression of the other transcription regulators of cortical identity.

摘要

大脑皮层的区域性模式是由模式中心分泌的形态发生素来启动的,这些形态发生素在皮质祖细胞内建立转录因子的梯度表达。在这里,我们表明 Dmrt5 在皮质祖细胞中以高尾侧至低额侧的梯度表达。在其缺失的情况下,皮层强烈减小并表现出严重的异常,包括海马体和脉络丛的发育不全以及连合和丘脑皮质束的缺陷。Dmrt5 的缺失导致主要的端脑模式中心之一背内侧端脑的 Wnt 和 Bmp 减少,并且 Cajal-Retzius 细胞减少。背中线信号中心依赖性转录因子的表达下调,包括促进尾侧命运的 Emx2,而中线信号抑制的头侧决定因素 Pax6 上调。一致地,Dmrt5(-/-) 大脑表现出模式缺陷,尾侧皮层显著减少。Wnt 信号的激活会增加 Dmrt5 的表达,而 Gli3(xt/xt) 突变体会下调其表达。我们得出结论,Dmrt5 是一种新型的 Wnt 依赖性转录因子,对于早期皮层发育是必需的,它可能通过促进背中线信号中心的形成来调节初始皮层模式,从而有助于建立皮层身份的其他转录调节剂的梯度表达。

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