Melatonin enhances the in vitro and in vivo repair of severed rat sciatic axons.

Neurosci Lett

Section of Neurobiology, The University of Texas at Austin, 1 University Station 0C0920, Austin, TX, 78712-0248, USA.

Published: March 2005

AI Article Synopsis

  • This study explores the impact of various experimental compounds (melatonin, cyclosporin A, glial-derived neurotrophic factor, methylprednisolone) on the repair of crushed sciatic axons using polyethylene glycol-induced fusion.
  • Results show that melatonin significantly enhances the repair rate of these axons in vitro, achieving 75% success compared to just 20% in controls.
  • Additionally, melatonin also shows improved conduction of nerve signals (higher amplitude of compound action potentials) and enhances repair success in vivo when compared to control conditions.

Article Abstract

This study examines the effects of several experimental compounds [melatonin (MEL), cyclosporin A (CsA), glial-derived neurotrophic factor (GDNF), and methylprednisolone (MP)] on polyethylene glycol (PEG)-induced repair in vitro and/or in vivo by plasmalemmal fusion (PEG-fusion) of sciatic axons severed by crushing. As measured by conduction of compound action potentials (CAPs) through the lesion site, a significantly (p<0.025) higher percentage (75%) of crushed rat sciatic axons can be repaired in vitro by PEG-fusion following exposure to MEL compared to PEG-fusion of severed sciatic axons in control Krebs saline that contains calcium (CTL=20%). In contrast, no other experimental compound (GDNF: 45%; MP: 42%; CsA: 24%) produces a significant improvement in PEG-fusion success compared to CTL. Further, MEL produces significantly (p<0.001) larger peak CAP amplitudes conducted through the lesion site following PEG-fusion compared to CTL or any other experimental compound in vitro. Additionally, MEL significantly (p<0.025) increases the ability to PEG-fuse sciatic axons in vivo, compared to CTL. Finally, PEG-fusion success in vivo is significantly (p<0.01) greater in calcium-free CTL (CTL-Ca) compared to CTL.

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Source
http://dx.doi.org/10.1016/j.neulet.2004.11.033DOI Listing

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