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与血小板衍生生长因子受体α、少突胶质细胞转录因子2和蛋白脂蛋白/dm20相比,成纤维细胞生长因子受体1、2、3在胚胎期和出生后小鼠大脑中的表达:对少突胶质细胞发育的影响

Expression of FGF receptors 1, 2, 3 in the embryonic and postnatal mouse brain compared with Pdgfralpha, Olig2 and Plp/dm20: implications for oligodendrocyte development.

作者信息

Bansal Rashmi, Lakhina Vanisha, Remedios Ryan, Tole Shubha

机构信息

Department of Neuroscience, University of Connecticut Medical School, Farmington, Conn 06030-3401, USA.

出版信息

Dev Neurosci. 2003 Mar-Aug;25(2-4):83-95. doi: 10.1159/000072258.

Abstract

Fibroblast growth factors (FGF) receptors FgfR1, FgfR2 and FgfR3 are differentially regulated during oligodendrocyte (OL) maturation in vitro: FgfR3 is expressed by OL progenitors whereas FgfR2 is expressed by differentiated OLs [Mol Cell Neurosci 1996;7:263-275], and we have recently shown that FgfR3 is required for the timely differentiation of OLs in vivo [J Neurosci 2003;23:883-894]. Here we have used in situ hybridization to investigate the expression patterns of FgfR1-3 and compare them to the putative OL progenitor markers Olig2, Pdgfralpha and Plp/dm20 as a function of development in vivo, in particular at sites of OL specification, migration or differentiation in the mouse forebrain and cerebellum. We show that at early stages FgfR1-3 expression overlaps with that of Olig2 in the embryonic ventricular zone of the lateral and medial ganglionic eminences. Further, a scattered population of cells expressing FgfR3 (but not FgfR1 or FgfR2) in the ventral telencephalon appear to arise from the ventricular zone, and at later stages are found more dorsally in the cortex, in an overall pattern similar to Olig2 and/or Pdgfralpha. Postnatal expression of FgfR2 increases with age, more prominently in specific regions, including the cortical and cerebellar white matter and optic nerve. Thus, the differential expression pattern of FgfR2 and FgfR3 observed in vivo suggests that their expression is developmentally regulated in a manner consistent with the pattern of their expression in culture. These data provide further insights into role of FgfRs in OL development, and they emphasize that these receptors are positioned both spatially and temporally to impact OL generation in vivo.

摘要

成纤维细胞生长因子(FGF)受体FgfR1、FgfR2和FgfR3在体外少突胶质细胞(OL)成熟过程中受到不同调控:FgfR3由OL祖细胞表达,而FgfR2由分化的OL表达[《分子与细胞神经科学》1996年;7:263 - 275],并且我们最近表明FgfR3是体内OL及时分化所必需的[《神经科学杂志》2003年;23:883 - 894]。在此,我们利用原位杂交来研究FgfR1 - 3的表达模式,并将它们与假定的OL祖细胞标志物Olig2、Pdgfralpha和Plp/dm20进行比较,作为体内发育的一个函数,特别是在小鼠前脑和小脑中OL特化、迁移或分化的部位。我们发现,在早期阶段,FgfR1 - 3的表达与外侧和内侧神经节隆起的胚胎脑室区中Olig2的表达重叠。此外,在腹侧端脑中,一群分散的表达FgfR3(但不表达FgfR1或FgfR2)的细胞似乎起源于脑室区,并且在后期阶段在皮质中更靠背侧被发现,其总体模式类似于Olig2和/或Pdgfralpha。FgfR2的出生后表达随年龄增加,在特定区域更明显,包括皮质和小脑白质以及视神经。因此,在体内观察到FgfR2和FgfR3的差异表达模式表明它们的表达在发育过程中受到调控,其方式与它们在培养物中的表达模式一致。这些数据进一步深入了解了FgfR在OL发育中的作用,并且它们强调这些受体在空间和时间上的定位都会影响体内OL的生成。

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