A Purine-Sensitive Pathway Regulates Multiple Genes Involved in Axon Regeneration in Goldfish Retinal Ganglion Cells

Petrausch, Barbara; Tabibiazar, Raymond; Roser, Timo; Jing, Yun; Goldmann, Daniel; Stürmer, Claudia; Irwin, Nina; Benowitz, Larry I.

A Purine-Sensitive Pathway Regulates Multiple Genes Involved in Axon Regeneration in Goldfish Retinal Ganglion Cells

Files

A_purine_sensitive_pathway.pdf(866.11 KB)

Date

2000

Authors

Petrausch, Barbara

Tabibiazar, Raymond

Roser, Timo

Jing, Yun

Goldmann, Daniel

Stürmer, Claudia

Irwin, Nina

Benowitz, Larry I.

Publication type

Journal article

Published in

Journal of Neurobiology ; 20 (2000). - pp. 8031-8041

Abstract

In lower vertebrates, retinal ganglion cells (RGCs) can regenerate their axons and reestablish functional connections after optic nerve injury. We show here that in goldfish RGCs, the effects of several trophic factors converge on a purine-sensitive signaling mechanism that controls axonal outgrowth and the expression of multiple growth-associated proteins. In culture, goldfish RGCs regenerate their axons in response to two molecules secreted by optic nerve glia, axogenesis factor-1 (AF-1) and AF-2, along with ciliary neurotrophic factor. The purine analog 6-thioguanine (6-TG) blocked outgrowth induced by each of these factors. Previous studies in PC12 cells have shown that the effects of 6-TG on neurite outgrowth may be mediated via inhibition of a 47 kDa protein kinase. Growth factor-induced axogenesis in RGCs was accompanied by many of the molecular changes that characterize regenerative growth in vivo, e.g., increased expression of GAP-43 and certain cell surface glycoproteins. 6-TG inhibited all of these changes but not those associated with axotomy per se, e.g., induction of jun family transcription factors, nor did it affect cell survival. Additional studies using RGCs from transgenic zebrafish showed that expression of Ta-1 tubulin is likewise stimulated by AF-1 and blocked by 6-TG. The purine nucleoside inosine had effects opposite to those of 6-TG. Inosine stimulated outgrowth and the characteristic pattern of molecular changes in RGCs and competitively reversed the inhibitory effects of 6-TG. We conclude that axon regeneration and the underlying program of gene expression in goldfish RGCs are mediated via a common, purine-sensitive pathway.

Subject (DDC)

570 Biosciences, Biology

Keywords

regeneration,axon,retinal ganglion cell,GAP-43,E587 antigen,L1,neurolin,DM-GRASP,reggie-2,inosine,optic nerve,zebrafisch

Cite This

ISO 690

PETRAUSCH, Barbara, Raymond TABIBIAZAR, Timo ROSER, Yun JING, Daniel GOLDMANN, Claudia STÜRMER, Nina IRWIN, Larry I. BENOWITZ, 2000. A Purine-Sensitive Pathway Regulates Multiple Genes Involved in Axon Regeneration in Goldfish Retinal Ganglion Cells. In: Journal of Neurobiology. 20, pp. 8031-8041

BibTex

@article{Petrausch2000Purin-8502,
  year={2000},
  title={A Purine-Sensitive Pathway Regulates Multiple Genes Involved in Axon Regeneration in Goldfish Retinal Ganglion Cells},
  volume={20},
  journal={Journal of Neurobiology},
  pages={8031--8041},
  author={Petrausch, Barbara and Tabibiazar, Raymond and Roser, Timo and Jing, Yun and Goldmann, Daniel and Stürmer, Claudia and Irwin, Nina and Benowitz, Larry I.}
}

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Bibliography of Konstanz

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