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该未实现的基因是果蝇蘑菇体神经原发育所必需的。

The unfulfilled gene is required for the development of mushroom body neuropil in Drosophila.

机构信息

Department of Zoology, University of Hawaii, Honolulu, HI 96822, USA.

出版信息

Neural Dev. 2010 Feb 1;5:4. doi: 10.1186/1749-8104-5-4.

Abstract

BACKGROUND

The mushroom bodies (MBs) of Drosophila are required for complex behaviors and consist of three types of neurons, gamma, alpha'/beta' and alpha/beta. Previously, roles for transcription factors in MB neuronal differentiation have only been described for a subset of MB neurons. We are investigating the roles of unfulfilled (unf; HR51, CG16801) in MB development. unf encodes a nuclear receptor that is orthologous to the nuclear receptors fasciculation of axons defective 1 (FAX-1) of the nematode and photoreceptor specific nuclear receptor (PNR) of mammals. Based on our previous observations that unf transcripts accumulate in MB neurons at all developmental stages and the presence of axon pathfinding defects in fax-1 mutants, we hypothesized that unf regulates MB axon growth and pathfinding.

RESULTS

We show that unf mutants exhibit a range of highly penetrant axon stalling phenotypes affecting all neurons of the larval and adult MBs. Phenotypic analysis of unfX1 mutants revealed that alpha'/beta' and alpha/beta neurons initially project axons but stall prior to the formation of medial or dorsal MB lobes. unfZ0001 mutants form medial lobes, although these axons fail to branch, which results in a failure to form the alpha or alpha' dorsal lobes. In either mutant background, gamma neurons fail to develop larval-specific dorsal projections. These mutant gamma neurons undergo normal pruning, but fail to re-extend axons medially during pupal development. unfRNAi animals displayed phenotypes similar to those seen in unfZ0001 mutants. Unique asymmetrical phenotypes were observed in unfX1/unfZ0001 compound heterozygotes. Expression of UAS-unf transgenes in MB neurons rescues the larval and adult unf mutant phenotypes.

CONCLUSIONS

These data support the hypothesis that unf plays a common role in the development of all types of MB neurons. Our data indicate that unf is necessary for MB axon extension and branching and that the formation of dorsal collaterals is more sensitive to the loss of unf function than medial projections. The asymmetrical phenotypes observed in compound heterozygotes support the hypothesis that the earliest MB axons may serve as pioneers for the later-born MB neurons, providing evidence for pioneer MB axon guidance in post-embryonic development.

摘要

背景

果蝇的蘑菇体(MBs)对于复杂行为是必需的,它由三种类型的神经元组成,γ、α'/β'和α/β。以前,转录因子在 MB 神经元分化中的作用只被描述为 MB 神经元的一个亚群。我们正在研究未满足的(unf; HR51,CG16801)在 MB 发育中的作用。unf 编码一种核受体,与线虫的轴突聚集缺陷 1(FAX-1)和哺乳动物的光受体特异性核受体(PNR)同源。基于我们之前的观察结果,即 unf 转录本在所有发育阶段都在 MB 神经元中积累,以及在 fax-1 突变体中存在轴突寻路缺陷,我们假设 unf 调节 MB 轴突生长和寻路。

结果

我们表明 unf 突变体表现出一系列高 penetrant 的轴突停滞表型,影响幼虫和成年 MB 的所有神经元。unfX1 突变体的表型分析表明,α'/β'和α/β神经元最初投射轴突,但在形成中脑或背侧 MB 叶之前停滞。unfZ0001 突变体形成中脑叶,尽管这些轴突不能分支,导致不能形成α或α'背侧叶。在任何突变体背景下,γ神经元都不能发育出幼虫特异性的背侧投射。这些突变体γ神经元经历正常的修剪,但在蛹期发育过程中不能向内侧重新延伸轴突。unfRNAi 动物表现出与 unfZ0001 突变体相似的表型。在 unfX1/unfZ0001 杂合突变体中观察到独特的不对称表型。MB 神经元中 UAS-unf 转基因的表达挽救了幼虫和成年 unf 突变体的表型。

结论

这些数据支持 unf 在所有类型的 MB 神经元发育中发挥共同作用的假设。我们的数据表明,unf 对于 MB 轴突延伸和分支是必需的,并且背侧分支的形成比内侧投射对 unf 功能的丧失更为敏感。在杂合突变体中观察到的不对称表型支持了这样的假设,即最早的 MB 轴突可能作为后来出生的 MB 神经元的先驱,为胚胎后发育中的先驱 MB 轴突导向提供了证据。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/21b2/2829026/d1d854c96837/1749-8104-5-4-1.jpg

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