Molecular Pain (Feb 2005)

Controlling neuropathic pain by adeno-associated virus driven production of the anti-inflammatory cytokine, interleukin-10

  • Flotte Terence R,
  • Maier Steven F,
  • Hammack Sayamwong E,
  • Wieseler-Frank Julie,
  • Spataro Leah,
  • Chacur Marucia,
  • Cruz Pedro E,
  • Langer Stephen J,
  • Sloane Evan M,
  • Milligan Erin D,
  • Forsayeth John R,
  • Leinwand Leslie A,
  • Chavez Raymond,
  • Watkins Linda R

DOI
https://doi.org/10.1186/1744-8069-1-9
Journal volume & issue
Vol. 1, no. 1
p. 9

Abstract

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Abstract Despite many decades of drug development, effective therapies for neuropathic pain remain elusive. The recent recognition of spinal cord glia and glial pro-inflammatory cytokines as important contributors to neuropathic pain suggests an alternative therapeutic strategy; that is, targeting glial activation or its downstream consequences. While several glial-selective drugs have been successful in controlling neuropathic pain in animal models, none are optimal for human use. Thus the aim of the present studies was to explore a novel approach for controlling neuropathic pain. Here, an adeno-associated viral (serotype II; AAV2) vector was created that encodes the anti-inflammatory cytokine, interleukin-10 (IL-10). This anti-inflammatory cytokine is known to suppress the production of pro-inflammatory cytokines. Upon intrathecal administration, this novel AAV2-IL-10 vector was successful in transiently preventing and reversing neuropathic pain. Intrathecal administration of an AAV2 vector encoding beta-galactosidase revealed that AAV2 preferentially infects meningeal cells surrounding the CSF space. Taken together, these data provide initial support that intrathecal gene therapy to drive the production of IL-10 may prove to be an efficacious treatment for neuropathic pain.