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Journal ArticleDOI

Characterisation of ultraviolet-B-induced inflammation as a model of hyperalgesia in the rat.

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TLDR
It is concluded that UVB inflammation produces a dose‐dependent hyperalgesic state sensitive to established analgesics, which suggests thatUVB inflammation in the rat may represent a useful translational tool in the study of pain and the testing of analgesic agents.
Abstract
In humans, the acute inflammatory reaction caused by ultraviolet (UV) radiation is well studied and the sensory changes that are found have been used as a model of cutaneous hyperalgesia. Similar paradigms are now emerging as rodent models of inflammatory pain. Using a narrowband UVB source, we irradiated the plantar surface of rat hind paws. This produced the classical feature of inflammation, erythema, and a significant dose-dependent reduction in both thermal and mechanical paw withdrawal thresholds. These sensory changes peaked 48 h after irradiation. At this time there is a graded facilitation of noxious heat evoked (but not basal) c-fos-like immunoreactivity in the L4/5 segments of the spinal cord. We also studied the effects of established analgesic compounds on the UVB-induced hyperalgesia. Systemic as well as topical application of ibuprofen significantly reduced both thermal and mechanical hyperalgesia. Systemic morphine produced a dose-dependent and naloxone sensitive reversal of sensory changes. Similarly, the peripherally restricted opioid loperamide also had a dose-dependent anti-hyperalgesic effect, again reversed by naloxone methiodide. Sequestration of NGF, starting at the time of UVB irradiation, significantly reduced sensory changes. We conclude that UVB inflammation produces a dose-dependent hyperalgesic state sensitive to established analgesics. This suggests that UVB inflammation in the rat may represent a useful translational tool in the study of pain and the testing of analgesic agents.

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Citations
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Journal ArticleDOI

Burn Pain: A Systematic and Critical Review of Epidemiology, Pathophysiology, and Treatment.

TL;DR: The pathophysiology of burn pain is poorly understood, with limited clinical trials available to assess the effectiveness of analgesics in burn patients and further studies are needed to identify new pharmacological targets and treatments for the effective management of burn injury pain.
Journal ArticleDOI

Ultraviolet-B-induced mechanical hyperalgesia: A role for peripheral sensitisation

TL;DR: It is concluded that UVB‐induced mechanical hyperalgesia may be explained by a net shift in peripheral nociceptor response properties and alteration in mechanical responses of A&dgr;‐ and heat‐insensitive C‐nocicePTors were particular to stronger stimuli.
Journal ArticleDOI

Predicting therapeutic efficacy — Experimental pain in human subjects

TL;DR: The application and potential of cortical EEG studies are discussed as an objective alternative to more conventional pain assessment tools with specific examples of how this technique has been applied to the study of NSAID and opiate-based therapeutics.
Journal ArticleDOI

Nanostructured lipid carriers (NLCs) versus solid lipid nanoparticles (SLNs) for topical delivery of meloxicam.

TL;DR: It can be concluded that lipid nanoparticles represent promising particulate carriers for topical application as shown in the results of this study.
Journal ArticleDOI

Translating nociceptive processing into human pain models

TL;DR: Current human pain models cannot replace patient studies for testing efficacy of analgesic compounds, but if the experimental models include sensitization of the peripheral or central pain processing they may indeed mimic certain aspects of chronic pain conditions.
References
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Journal ArticleDOI

Ethical guidelines for investigations of experimental pain in conscious animals.

Manfred Zimmermann
- 01 Jun 1983 - 
TL;DR: The Committee for Research and Ethical Issues of the International Association for the Study of Pain (IASP®) is concerned with the ethical aspects of studies producing experimental pain and any suffering it may cause in animals.
Journal ArticleDOI

A new and sensitive method for measuring thermal nociception in cutaneous hyperalgesia.

TL;DR: Both the thermal method and the Randall‐Selitto mechanical method detected dose‐related hyperalgesia and its blockade by either morphine or indomethacin, but the Thermal method showed greater bioassay sensitivity and allowed for the measurement of other behavioral parameters in addition to the nociceptive threshold.
Journal ArticleDOI

Textbook of pain

Patrick D. Wall, +1 more
- 01 Mar 1990 - 
TL;DR: Part 1 Basic aspects: peripheral - peripheral neural mechnaisms of nociception, the course and termination of primary afferent fibres, teh pathophysiology of damaged peripheral nerves, functional chemistry ofPrimary afferent neurons central - the dorsal horn.
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