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一个 GATA/同源结构域转录码通过 Unc-5 受体调节轴突导向。

A GATA/homeodomain transcriptional code regulates axon guidance through the Unc-5 receptor.

机构信息

Smurfit Institute of Genetics, Institute of Neuroscience, Trinity College Dublin, Dublin 2, Ireland.

出版信息

Development. 2012 May;139(10):1798-805. doi: 10.1242/dev.070656. Epub 2012 Mar 29.

DOI:10.1242/dev.070656
PMID:22461564
Abstract

Transcription factor codes play an essential role in neuronal specification and axonal guidance in both vertebrate and invertebrate organisms. However, how transcription codes regulate axon pathfinding remains poorly understood. One such code defined by the homeodomain transcription factor Even-skipped (Eve) and by the GATA 2/3 homologue Grain (Grn) is specifically required for motor axon projection towards dorsal muscles in Drosophila. Using different mutant combinations, we present genetic evidence that both Grn and Eve are in the same pathway as Unc-5 in dorsal motoneurons (dMNs). In grn mutants, in which dMNs fail to reach their muscle targets, dMNs show significantly reduced levels of unc-5 mRNA expression and this phenotype can be partially rescued by the reintroduction of unc-5. We also show that both eve and grn are required independently to induce expression of unc-5 in dMNs. Reconstitution of the eve-grn transcriptional code of a dMN in dMP2 neurons, which do not project to lateral muscles in Drosophila, is able to reprogramme those cells accordingly; they robustly express unc-5 and project towards the muscle field as dMNs. Each transcription factor can independently induce unc-5 expression but unc-5 expression is more robust when both factors are expressed together. Furthermore, dMP2 exit is dependent on the level of unc-5 induced by eve and grn. Taken together, our data strongly suggests that the eve-grn transcriptional code controls axon guidance, in part, by regulating the level of unc-5 expression.

摘要

转录因子代码在脊椎动物和无脊椎动物的神经元特化和轴突导向中发挥着重要作用。然而,转录代码如何调节轴突寻迹仍知之甚少。在家域转录因子 Even-skipped(Eve)和 GATA2/3 同源物 Grain(Grn)定义的一个这样的代码,对于果蝇中运动轴突向背侧肌肉的投射是必需的。使用不同的突变体组合,我们提供了遗传证据,表明 Grn 和 Eve 与 Unc-5 一样,在背侧运动神经元(dMNs)中处于同一途径。在 grn 突变体中,dMNs 无法到达其肌肉靶标,dMNs 中 unc-5 mRNA 的表达水平显著降低,这种表型可以部分通过引入 unc-5 来挽救。我们还表明,Grn 和 Eve 都需要独立地在 dMNs 中诱导 unc-5 的表达。在 dMP2 神经元中重建 dMN 的 eve-grn 转录代码,dMP2 神经元在果蝇中不投射到侧肌,能够相应地重新编程这些细胞;它们强烈表达 unc-5 并像 dMNs 一样投射到肌肉区域。每个转录因子都可以独立地诱导 unc-5 的表达,但当两个因子一起表达时,unc-5 的表达更加强烈。此外,dMP2 的退出依赖于 eve 和 grn 诱导的 unc-5 水平。总之,我们的数据强烈表明,eve-grn 转录代码通过调节 unc-5 表达水平来控制轴突导向。

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