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  4. Electroporation-Mediated Pain-Killer Gene Therapy for Mononeuropathic Rats
 
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Electroporation-Mediated Pain-Killer Gene Therapy for Mononeuropathic Rats

Resource
GENE THERAPY v.9 n.18 pp.1247-1253
Journal
GENE THERAPY
Journal Volume
v.9
Journal Issue
n.18
Pages
1247-1253
Date Issued
2002
Date
2002
Author(s)
SUN, WEI-ZEN
URI
http://ntur.lib.ntu.edu.tw//handle/246246/99212
Abstract
The relatively low expression levels achieved from transferred genes have limited the application of nonviral vectors for gene transfer into the spinal cord in vivo. Thus , the aim of this study was to evaluate the efficacy of electroporation-mediated pro-opiomelanocortin (POMC) gene therapy for neuropathic pain using an animal model of chronic constrictive injury (M). Firstly, the optimal pulse characteristics (voltage, pulse duration, number of shocks) were investigated for in vivo electroporation- mediated gene transfer into the spinal cord. The electroporation process makes use of plasmid DNA, which expresses the POMC gene. Expression levels were evaluated in this study by Western blot. We conclude that the optimal conditions for electroporation are a pulse voltage of 200 V, 75-ms duration , 925-ms interval, for five iterations. Secondly, electroporation treatment for neuropathic pain was attempted on CCl rats using plasmid DNA that expresses the POMC gene. Intrathecal administrations of the POMC vector elevated spinal beta-endorphin levels, as manifested in a significantly elevated pain threshold for the CCl limbs . This result suggests that gene therapy for neuropathic pain using this novel technique is very efficacious, and thus shows promise for further clinical trials.
Subjects
pro-opiomelanocortin
gene transfer
electroporation
spinal cord
Western blot neuropathic pain

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