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碱性成纤维细胞生长因子促进周围神经再生轴突的延伸。使用雪旺细胞基膜管模型的体内实验。

Basic fibroblast growth factor promotes extension of regenerating axons of peripheral nerve. In vivo experiments using a Schwann cell basal lamina tube model.

作者信息

Fujimoto E, Mizoguchi A, Hanada K, Yajima M, Ide C

机构信息

Department of Anatomy, Kobe University School of Medicine, Japan.

出版信息

J Neurocytol. 1997 Aug;26(8):511-28. doi: 10.1023/a:1015410023132.

Abstract

Schwann cell basal lamina tubes serve as attractive conduits for regeneration of peripheral nerve axons. In the present study, by using basal lamina tubes prepared by in situ freeze-treatment of rat saphenous nerve, the effects of exogenously applied basic fibroblast growth factor (bFGF) on peripheral nerve regeneration was examined 2 and 5 days after bFGF administration. Regenerating axons were observed by light and electron microscopy using PGP9.5-immunohistochemistry for specific staining of axons. In addition, the localizations of bFGF and its receptor (FGF receptor-1) were examined by immunohistochemistry using anti-bFGF antibody and anti-FGF receptor-1 antibody, respectively. Regenerating axons extended further in the bFGF-administered segment than in the bFGF-untreated control segment. Electron microscopy showed that regenerating axons grew out unaccompanied by Schwann cells. Findings concerning angiogenesis and Schwann cell migration were very similar between the bFGF treated and control nerve segment. bFGF-immunoreactivity was not detected in the control nerve segment. In contrast, bFGF-immunoreactivity was detected on the basal lamina tubes as well as on the plasmalemma of regenerating axons facing the basal lamina in the bFGF treated nerve segment up to 5 days after administration, suggesting that exogenous bFGF can be retained in the basal lamina for several days after administration. FGF receptor was detected on the plasma membrane of regenerating axons where they abutted the basal lamina. These results indicate that bFGF could promote the extension of early regenerating axons by directly influencing the axons, but not via Schwann cells or angiogenesis.

摘要

施万细胞基膜管是周围神经轴突再生的有吸引力的通道。在本研究中,通过使用对大鼠隐神经进行原位冷冻处理制备的基膜管,在给予碱性成纤维细胞生长因子(bFGF)后2天和5天,检测外源性应用bFGF对周围神经再生的影响。使用PGP9.5免疫组织化学对轴突进行特异性染色,通过光学显微镜和电子显微镜观察再生轴突。此外,分别使用抗bFGF抗体和抗FGF受体-1抗体,通过免疫组织化学检测bFGF及其受体(FGF受体-1)的定位。与未处理bFGF的对照段相比,在给予bFGF的段中再生轴突延伸得更远。电子显微镜显示再生轴突在没有施万细胞伴随的情况下生长出来。在bFGF处理的神经段和对照神经段之间,关于血管生成和施万细胞迁移的发现非常相似。在对照神经段中未检测到bFGF免疫反应性。相反,在给予bFGF后长达5天的时间里,在bFGF处理的神经段的基膜管以及面对基膜的再生轴突的质膜上检测到bFGF免疫反应性,这表明外源性bFGF在给药后可在基膜中保留数天。在再生轴突与基膜邻接的质膜上检测到FGF受体。这些结果表明,bFGF可通过直接影响轴突而非通过施万细胞或血管生成来促进早期再生轴突的延伸。

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