Different Fgfs have distinct roles in regulating neurogenesis after spinal cord injury in zebrafish.

IF 4 3区生物学 Q1 DEVELOPMENTAL BIOLOGY

Neural Development Pub Date : 2018-11-17 DOI:10.1186/s13064-018-0122-9

Yona Goldshmit, Jean Kitty K Y Tang, Ashley L Siegel, Phong D Nguyen, Jan Kaslin, Peter D Currie, Patricia R Jusuf

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引用次数: 26

Abstract

Background: Despite conserved developmental processes and organization of the vertebrate central nervous system, only some vertebrates including zebrafish can efficiently regenerate neural damage including after spinal cord injury. The mammalian spinal cord shows very limited regeneration and neurogenesis, resulting in permanent life-long functional impairment. Therefore, there is an urgent need to identify the cellular and molecular mechanisms that can drive efficient vertebrate neurogenesis following injury. A key pathway implicated in zebrafish neurogenesis is fibroblast growth factor signaling.

Methods: In the present study we investigated the roles of distinct fibroblast growth factor members and their receptors in facilitating different aspects of neural development and regeneration at different timepoints following spinal cord injury. After spinal cord injury in adults and during larval development, loss and/or gain of Fgf signaling was combined with immunohistochemistry, in situ hybridization and transgenes marking motor neuron populations in in vivo zebrafish and in vitro mammalian PC12 cell culture models.

Results: Fgf3 drives neurogenesis of Islet1 expressing motor neuron subtypes and mediate axonogenesis in cMet expressing motor neuron subtypes. We also demonstrate that the role of Fgf members are not necessarily simple recapitulating development. During development Fgf2, Fgf3 and Fgf8 mediate neurogenesis of Islet1 expressing neurons and neuronal sprouting of both, Islet1 and cMet expressing motor neurons. Strikingly in mammalian PC12 cells, all three Fgfs increased cell proliferation, however, only Fgf2 and to some extent Fgf8, but not Fgf3 facilitated neurite outgrowth.

Conclusions: This study demonstrates differential Fgf member roles during neural development and adult regeneration, including in driving neural proliferation and neurite outgrowth of distinct spinal cord neuron populations, suggesting that factors including Fgf type, age of the organism, timing of expression, requirements for different neuronal populations could be tailored to best drive all of the required regenerative processes.

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不同的Fgfs在斑马鱼脊髓损伤后神经发生的调控中有不同的作用。

背景:尽管脊椎动物中枢神经系统的发育过程和组织是保守的，但只有斑马鱼等部分脊椎动物能够有效地再生神经损伤，包括脊髓损伤后的神经损伤。哺乳动物的脊髓显示出非常有限的再生和神经发生，导致永久性的终身功能损伤。因此，迫切需要确定脊椎动物损伤后神经发生的细胞和分子机制。斑马鱼神经发生的一个关键途径是成纤维细胞生长因子信号。方法:在本研究中，我们研究了不同的成纤维细胞生长因子成员及其受体在脊髓损伤后不同时间点促进神经发育和再生的不同方面的作用。在成年脊髓损伤后和幼虫发育过程中，将Fgf信号的丢失和/或获得与免疫组织化学、原位杂交和转基因相结合，在斑马鱼体内和哺乳动物体外PC12细胞培养模型中标记运动神经元群体。结果:Fgf3驱动Islet1表达运动神经元亚型的神经发生，介导cMet表达运动神经元亚型的轴突发生。我们还表明，论坛成员的作用不一定是简单地概括发展。在发育过程中，Fgf2、Fgf3和Fgf8介导表达Islet1的神经元的神经发生以及表达Islet1和cMet的运动神经元的神经元发芽。引人注目的是，在哺乳动物PC12细胞中，所有三种Fgfs都增加了细胞增殖，然而，只有Fgf2和Fgf8在一定程度上促进了神经突的生长，而Fgf3没有促进神经突的生长。结论:本研究证明了Fgf成员在神经发育和成体再生过程中的不同作用，包括驱动不同脊髓神经元群体的神经增殖和神经突生长，这表明Fgf类型、生物体年龄、表达时间、不同神经元群体的需求等因素可以被定制，以最好地驱动所有所需的再生过程。

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来源期刊

Neural Development 生物-发育生物学

CiteScore

6.60

自引率

0.00%

发文量

审稿时长

>12 weeks

期刊介绍： Neural Development is a peer-reviewed open access, online journal, which features studies that use molecular, cellular, physiological or behavioral methods to provide novel insights into the mechanisms that underlie the formation of the nervous system. Neural Development aims to discover how the nervous system arises and acquires the abilities to sense the world and control adaptive motor output. The field includes analysis of how progenitor cells form a nervous system during embryogenesis, and how the initially formed neural circuits are shaped by experience during early postnatal life. Some studies use well-established, genetically accessible model systems, but valuable insights are also obtained from less traditional models that provide behavioral or evolutionary insights.