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受体蛋白酪氨酸磷酸酶调节非洲爪蟾视觉系统发育过程中视网膜神经节细胞轴突的生长。

Receptor protein tyrosine phosphatases regulate retinal ganglion cell axon outgrowth in the developing Xenopus visual system.

作者信息

Johnson K G, McKinnell I W, Stoker A W, Holt C E

机构信息

Department of Anatomy, University of Cambridge, Downing Street, Cambridge CB2 3DY, United Kingdom.

出版信息

J Neurobiol. 2001 Nov 5;49(2):99-117. doi: 10.1002/neu.1068.

Abstract

Receptor protein tyrosine phosphatases (RPTPs) are regulators of axon outgrowth and guidance in a variety of different vertebrate and invertebrate systems. Three RPTPs, CRYP-alpha, PTP-delta, and LAR, are expressed in overlapping but distinct patterns in the developing Xenopus retina, including expression in retinal ganglion cells (RGCs) as they send axons to the tectum (Johnson KG, Holt CE. 2000. Expression of CRYP-alpha, LAR, PTP-delta, and PTP-rho in the developing Xenopus visual system. Mech Dev 92:291-294). In order to examine the role of these RPTPs in visual system development, putative dominant negative RPTP mutants (CS-CRYP-alpha, CS-PTP-delta, and CS-LAR) were expressed either singly or in combination in retinal cells. No effect was found on either retinal cell fate determination or on gross RGC axon guidance to the tectum. However, expression of these CS-RPTP constructs differentially affected the rate of RGC axon outgrowth. In vivo, expression of all three CS-RPTPs or CS-PTP-delta alone inhibited RGC axon outgrowth, while CS-LAR and CS-CRYP-alpha had no significant effect. In vitro, expression of CS-CRYP-alpha enhanced neurite outgrowth, while CS-PTP-delta inhibited neurite outgrowth in a substrate-dependent manner. This study provides the first in vivo evidence that RPTPs regulate retinal axon outgrowth.

摘要

受体蛋白酪氨酸磷酸酶(RPTPs)是多种不同脊椎动物和无脊椎动物系统中轴突生长和导向的调节因子。三种RPTPs,即CRYP-α、PTP-δ和LAR,在非洲爪蟾发育中的视网膜中以重叠但不同的模式表达,包括在视网膜神经节细胞(RGCs)中将轴突发送到顶盖时的表达(Johnson KG,Holt CE. 2000.非洲爪蟾视觉系统发育过程中CRYP-α、LAR、PTP-δ和PTP-ρ的表达。《机制与发育》92:291-294)。为了研究这些RPTPs在视觉系统发育中的作用,将推定的显性负性RPTP突变体(CS-CRYP-α、CS-PTP-δ和CS-LAR)单独或组合在视网膜细胞中表达。未发现对视网膜细胞命运决定或RGC轴突向顶盖的总体导向有任何影响。然而,这些CS-RPTP构建体的表达对RGC轴突生长速率有不同影响。在体内,所有三种CS-RPTPs或单独的CS-PTP-δ的表达均抑制RGC轴突生长,而CS-LAR和CS-CRYP-α没有显著影响。在体外,CS-CRYP-α的表达增强了神经突生长,而CS-PTP-δ以底物依赖的方式抑制神经突生长。这项研究提供了第一个体内证据,证明RPTPs调节视网膜轴突生长。

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