Institute of Neuroanatomy, Hannover Medical School, Hannover, Germany.
PLoS One. 2011;6(8):e23564. doi: 10.1371/journal.pone.0023564. Epub 2011 Aug 18.
Secreted proteins of the fibroblast growth factor (FGF) family play important roles during development of various organ systems. A detailed knowledge of their temporal and spatial expression profiles, especially of closely related FGF family members, are essential to further identification of specific functions in distinct tissues. In the central nervous system dopaminergic neurons of the substantia nigra and their axonal projections into the striatum progressively degenerate in Parkinson's disease. In contrast, FGF-2 deficient mice display increased numbers of dopaminergic neurons. In this study, we determined the expression profiles of all 22 FGF-ligands and 10 FGF-receptor isoforms, in order to clarify, if FGF-2 deficiency leads to compensatory up-regulation of other FGFs in the nigrostriatal system. Three tissues, ventral mesencephalon (VM), striatum (STR) and as reference tissue spinal cord (SC) of wild-type and FGF-2 deficient mice at four developmental stages E14.5, P0, P28, and adult were comparatively analyzed by quantitative RT-PCR. As no differences between the genotypes were observed, a compensatory up-regulation can be excluded. Moreover, this analysis revealed that the majority of FGF-ligands (18/22) and FGF-receptors (9/10) are expressed during normal development of the nigrostriatal system and identified dynamic changes for some family members. By comparing relative expression level changes to SC reference tissue, general alterations in all 3 tissues, such as increased expression of FGF-1, -2, -22, FgfR-2c, -3c and decreased expression of FGF-13 during postnatal development were identified. Further, specific changes affecting only one tissue, such as increased FGF-16 (STR) or decreased FGF-17 (VM) expression, or two tissues, such as decreased expression of FGF-8 (VM, STR) and FGF-15 (SC, VM) were found. Moreover, 3 developmentally down-regulated FGFs (FGF-8b, FGF-15, FGF-17a) were functionally characterized by plasmid-based over-expression in dissociated E11.5 VM cell cultures, however, such a continuous exposure had no influence on the yield of dopaminergic neurons in vitro.
成纤维细胞生长因子(FGF)家族的分泌蛋白在各种器官系统的发育过程中发挥着重要作用。详细了解它们的时空表达谱,尤其是密切相关的 FGF 家族成员的表达谱,对于进一步确定特定组织中的特定功能至关重要。在中枢神经系统中,黑质中的多巴胺能神经元及其轴突投射到纹状体中逐渐退化,而在帕金森病中。相比之下,FGF-2 缺陷小鼠显示出多巴胺能神经元数量增加。在这项研究中,我们确定了所有 22 种 FGF 配体和 10 种 FGF 受体同工型的表达谱,以阐明 FGF-2 缺乏是否会导致黑质纹状体系统中其他 FGFs 的代偿性上调。在四个发育阶段 E14.5、P0、P28 和成年期,通过定量 RT-PCR 比较分析了野生型和 FGF-2 缺陷型小鼠的腹侧中脑(VM)、纹状体(STR)和作为参考组织脊髓(SC)三种组织。由于基因型之间没有差异,因此可以排除代偿性上调。此外,这项分析表明,大多数 FGF 配体(18/22)和 FGF 受体(9/10)在黑质纹状体系统的正常发育过程中表达,并确定了一些家族成员的动态变化。通过将相对表达水平变化与 SC 参考组织进行比较,鉴定了所有 3 种组织的一般变化,例如 FGF-1、-2、-22、FgfR-2c、-3c 的表达增加,以及 FGF-13 在出生后的发育过程中的表达减少。此外,仅影响一种组织的特定变化,例如 FGF-16(STR)或 FGF-17(VM)表达减少,或两种组织,例如 FGF-8(VM、STR)和 FGF-15(SC、VM)表达减少,也被发现。此外,3 种发育下调的 FGFs(FGF-8b、FGF-15、FGF-17a)通过基于质粒的过表达在 E11.5 VM 细胞培养物中进行功能表征,然而,这种持续暴露对体外多巴胺能神经元的产量没有影响。
Zotero 插件