Altered nociceptive C fibre input to primary somatosensory cortex in an animal model of hyperalgesia.

Jensen, Tanja; Granmo, Marcus; Schouenborg, Jens

Altered nociceptive C fibre input to primary somatosensory cortex in an animal model of hyperalgesia.

Mark

Jensen, Tanja ^LU ; Granmo, Marcus ^LU and Schouenborg, Jens ^LU

(2011) In European Journal of Pain 15(4). p.368-375

Abstract: Evaluating potentially analgesic effects of drugs and various treatments is critically dependent on valid animal models of pain. Since primary somatosensory (SI) cortex is likely to play an important role in processing sensory aspects of pain, we here assess whether monitoring SI cortex nociceptive C fibre evoked potentials can provide useful information about central changes related to hyperalgesia in rats. Recordings of tactile and CO(2)-laser C fibre evoked potentials (LCEPs) in forelimb and hind limb SI cortex were made 20-24h after UV-B irradiation of the heel at a dose that produced behavioural signs of hyperalgesia. LCEPs from irradiated skin increased significantly in duration but showed no significant change in magnitude, measured... (More); Evaluating potentially analgesic effects of drugs and various treatments is critically dependent on valid animal models of pain. Since primary somatosensory (SI) cortex is likely to play an important role in processing sensory aspects of pain, we here assess whether monitoring SI cortex nociceptive C fibre evoked potentials can provide useful information about central changes related to hyperalgesia in rats. Recordings of tactile and CO(2)-laser C fibre evoked potentials (LCEPs) in forelimb and hind limb SI cortex were made 20-24h after UV-B irradiation of the heel at a dose that produced behavioural signs of hyperalgesia. LCEPs from irradiated skin increased significantly in duration but showed no significant change in magnitude, measured as area under curve (AUC). By contrast, LCEPs in hind limb SI cortex from skin sites nearby the irradiated skin showed no increase in duration or onset latency but increased significantly in magnitude after UV-B irradiation. The LCEPs in forelimb or hind limb SI cortex elicited from forelimb skin did not change in magnitude, but were significantly delayed in hind limb SI cortex. Tramadol, a centrally acting analgesic known to reduce hyperalgesia, induced changes that counteracted the changes produced by UV-B irradiation on transmission to SI cortex from the hind paw, but had no significant effect on time course of LCEPs from forelimb skin. Tactile evoked potentials were not affected by UV-B irradiation or tramadol. We conclude that altered sensory processing related to hyperalgesia is reflected in altered LCEPs in SI cortex. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/1711145

author

Jensen, Tanja ^LU ; Granmo, Marcus ^LU and Schouenborg, Jens ^LU

organization

publishing date

2011

type

Contribution to journal

publication status

published

subject

Neurosciences

in

European Journal of Pain

volume

15

issue

4

pages

368 - 375

publisher

Elsevier

external identifiers

wos:000289280200005
pmid:20947398
scopus:79954420208
pmid:20947398

ISSN

1090-3801

DOI

10.1016/j.ejpain.2010.09.009

language

English

LU publication?

yes

id

9af4f11d-f0bf-490d-a5fc-8fc1a66afc1c (old id 1711145)

alternative location

http://www.ncbi.nlm.nih.gov/pubmed/20947398?dopt=Abstract

date added to LUP

2016-04-01 10:39:23

date last changed

2024-01-06 21:54:41

@article{9af4f11d-f0bf-490d-a5fc-8fc1a66afc1c,
  abstract     = {{Evaluating potentially analgesic effects of drugs and various treatments is critically dependent on valid animal models of pain. Since primary somatosensory (SI) cortex is likely to play an important role in processing sensory aspects of pain, we here assess whether monitoring SI cortex nociceptive C fibre evoked potentials can provide useful information about central changes related to hyperalgesia in rats. Recordings of tactile and CO(2)-laser C fibre evoked potentials (LCEPs) in forelimb and hind limb SI cortex were made 20-24h after UV-B irradiation of the heel at a dose that produced behavioural signs of hyperalgesia. LCEPs from irradiated skin increased significantly in duration but showed no significant change in magnitude, measured as area under curve (AUC). By contrast, LCEPs in hind limb SI cortex from skin sites nearby the irradiated skin showed no increase in duration or onset latency but increased significantly in magnitude after UV-B irradiation. The LCEPs in forelimb or hind limb SI cortex elicited from forelimb skin did not change in magnitude, but were significantly delayed in hind limb SI cortex. Tramadol, a centrally acting analgesic known to reduce hyperalgesia, induced changes that counteracted the changes produced by UV-B irradiation on transmission to SI cortex from the hind paw, but had no significant effect on time course of LCEPs from forelimb skin. Tactile evoked potentials were not affected by UV-B irradiation or tramadol. We conclude that altered sensory processing related to hyperalgesia is reflected in altered LCEPs in SI cortex.}},
  author       = {{Jensen, Tanja and Granmo, Marcus and Schouenborg, Jens}},
  issn         = {{1090-3801}},
  language     = {{eng}},
  number       = {{4}},
  pages        = {{368--375}},
  publisher    = {{Elsevier}},
  series       = {{European Journal of Pain}},
  title        = {{Altered nociceptive C fibre input to primary somatosensory cortex in an animal model of hyperalgesia.}},
  url          = {{https://lup.lub.lu.se/search/files/2027065/1897742.pdf}},
  doi          = {{10.1016/j.ejpain.2010.09.009}},
  volume       = {{15}},
  year         = {{2011}},
}

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Altered nociceptive C fibre input to primary somatosensory cortex in an animal model of hyperalgesia.