斑马鱼 V0v 脊髓中间神经元的分子分析及这些细胞中 Evx1 和 Evx2 下游转录调控因子的鉴定。

Molecular analyses of zebrafish V0v spinal interneurons and identification of transcriptional regulators downstream of Evx1 and Evx2 in these cells.

机构信息

Biology Department, Syracuse University, Syracuse, NY, USA.

Physiology, Development and Neuroscience Department, Cambridge University, Cambridge, UK.

出版信息

Neural Dev. 2023 Nov 28;18(1):8. doi: 10.1186/s13064-023-00176-w.

DOI:10.1186/s13064-023-00176-w

PMID:38017520

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10683209/

Abstract

BACKGROUND

V0v spinal interneurons are highly conserved, glutamatergic, commissural neurons that function in locomotor circuits. We have previously shown that Evx1 and Evx2 are required to specify the neurotransmitter phenotype of these cells. However, we still know very little about the gene regulatory networks that act downstream of these transcription factors in V0v cells.

METHODS

To identify candidate members of V0v gene regulatory networks, we FAC-sorted wild-type and evx1;evx2 double mutant zebrafish V0v spinal interneurons and expression-profiled them using microarrays and single cell RNA-seq. We also used in situ hybridization to compare expression of a subset of candidate genes in evx1;evx2 double mutants and wild-type siblings.

RESULTS

Our data reveal two molecularly distinct subtypes of zebrafish V0v spinal interneurons at 48 h and suggest that, by this stage of development, evx1;evx2 double mutant cells transfate into either inhibitory spinal interneurons, or motoneurons. Our results also identify 25 transcriptional regulator genes that require Evx1/2 for their expression in V0v interneurons, plus a further 11 transcriptional regulator genes that are repressed in V0v interneurons by Evx1/2. Two of the latter genes are hmx2 and hmx3a. Intriguingly, we show that Hmx2/3a, repress dI2 interneuron expression of skor1a and nefma, two genes that require Evx1/2 for their expression in V0v interneurons. This suggests that Evx1/2 might regulate skor1a and nefma expression in V0v interneurons by repressing Hmx2/3a expression.

CONCLUSIONS

This study identifies two molecularly distinct subsets of zebrafish V0v spinal interneurons, as well as multiple transcriptional regulators that are strong candidates for acting downstream of Evx1/2 to specify the essential functional characteristics of these cells. Our data further suggest that in the absence of both Evx1 and Evx2, V0v spinal interneurons initially change their neurotransmitter phenotypes from excitatory to inhibitory and then, later, start to express markers of distinct types of inhibitory spinal interneurons, or motoneurons. Taken together, our findings significantly increase our knowledge of V0v and spinal development and move us closer towards the essential goal of identifying the complete gene regulatory networks that specify this crucial cell type.

摘要

背景

V0v 脊髓中间神经元是高度保守的谷氨酸能连合神经元，在运动回路中发挥作用。我们之前已经表明，Evx1 和 Evx2 对于这些细胞的神经递质表型的指定是必需的。然而，我们仍然对这些转录因子在 V0v 细胞中的下游的基因调控网络知之甚少。

方法

为了鉴定 V0v 基因调控网络的候选成员，我们使用 FAC 分选野生型和 evx1;evx2 双突变斑马鱼 V0v 脊髓中间神经元，并使用微阵列和单细胞 RNA-seq 对其进行表达谱分析。我们还使用原位杂交比较了候选基因的一部分在 evx1;evx2 双突变体和野生型同胞中的表达。

结果

我们的数据揭示了两种在 48 小时时有明显不同的斑马鱼 V0v 脊髓中间神经元亚型，并表明在这个发育阶段，evx1;evx2 双突变体细胞转变成抑制性脊髓中间神经元或运动神经元。我们的结果还鉴定了 25 个转录调节因子基因，它们的表达需要 Evx1/2 在 V0v 中间神经元中，另外还有 11 个转录调节因子基因在 Evx1/2 抑制 V0v 中间神经元的表达。其中两个基因是 hmx2 和 hmx3a。有趣的是，我们表明 Hmx2/3a 抑制了 dI2 中间神经元 skor1a 和 nefma 的表达，这两个基因的表达需要 Evx1/2 在 V0v 中间神经元中。这表明 Evx1/2 可能通过抑制 Hmx2/3a 的表达来调节 V0v 中间神经元中 skor1a 和 nefma 的表达。

结论

本研究鉴定了两种在分子上有明显区别的斑马鱼 V0v 脊髓中间神经元亚型，以及多个转录调节因子，它们是作为 Evx1/2 的下游因子，指定这些细胞的基本功能特征的有力候选者。我们的数据还表明，在缺乏 Evx1 和 Evx2 的情况下，V0v 脊髓中间神经元最初从兴奋性转变为抑制性，然后开始表达不同类型的抑制性脊髓中间神经元或运动神经元的标志物。总的来说，我们的发现显著增加了我们对 V0v 和脊髓发育的认识，并使我们更接近确定指定这种关键细胞类型的完整基因调控网络的重要目标。