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首页> 外文期刊>Development >NKX2.1 specifies cortical interneuron fate by activating Lhx6.
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NKX2.1 specifies cortical interneuron fate by activating Lhx6.

机译:NKX2.1通过激活Lhx6来指定皮质神经元的命运。

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In the ventral telencephalon, the medial ganglionic eminence (MGE) is a major source of cortical interneurons. Expression of the transcription factor NKX2.1 in the MGE is required for the specification of two major subgroups of cortical interneurons - those that express parvalbumin (PV) or somatostatin (SST) - but direct targets of NKX2.1 remain to be established. We find that electroporation of Nkx2.1 cDNA into the ventral telencephalon of slice cultures from Nkx2.1-/- mouse embryos, followed by transplantation into neonatal cortex to permit postnatal analysis of their fate, rescues the loss of PV- and SST-expressing cells. The LIM-homeobox gene Lhx6 is induced by this rescue experiment, and gain- and loss-of-function studies suggest that Lhx6 is necessary and sufficient to rescue these and other interneuron phenotypes in cells transplanted from Nkx2.1-/- slices. Finally, NKX2.1 protein binds a highly conserved sequence in the Lhx6 promoter, and this sequence appears to mediate the direct activation of Lhx6 by NKX2.1. The slice transfection and transplantation methods employed here are beginning to uncover embryonic mechanisms for specifying neuronal fates that only become definable postnatally.
机译:在腹端脑中,神经节隆起(MGE)是皮层神经元的主要来源。规范两个主要的皮质中间神经元亚群-表达小白蛋白(PV)或生长抑素(SST)的两个亚群需要在MGE中表达转录因子NKX2.1-但仍需确定NKX2.1的直接靶标。我们发现,将Nkx2.1 cDNA电穿孔到Nkx2.1-/-小鼠胚胎切片培养的腹侧端脑中,然后移植到新生儿皮层中,以便对其命运进行产后分析,挽救了PV和SST表达的丧失细胞。 LIM-homeobox基因Lhx6是由该抢救实验诱导的,功能获得和功能丧失研究表明Lhx6对于抢救从Nkx2.1-/-切片移植的细胞中的这些和其他中间神经元表型是必要和充分的。最后,NKX2.1蛋白在Lhx6启动子中结合了高度保守的序列,该序列似乎介导了NKX2.1对Lhx6的直接激活。此处采用的切片转染和移植方法开始揭示特定于出生后才可确定的神经元命运的胚胎机制。

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