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The Journal of Neurophysiology Vol. 86 No. 2 August 2001, pp. 986-996
Copyright ©2001 by the American Physiological Society
1Department of Preventive Science, 2Department of Oral Science, and 3Department of Psychiatry, Schools of Dentistry and Medicine, University of Minnesota, Minneapolis, Minnesota 55455
Khasabov, Sergey G.,
David M. Cain,
Dinh Thong,
Patrick W. Mantyh, and
Donald A. Simone.
Enhanced Responses of Spinal Dorsal Horn Neurons to Heat and Cold
Stimuli Following Mild Freeze Injury to the Skin. J. Neurophysiol. 86: 986-996, 2001. The effects
of a mild freeze injury to the skin on responses of nociceptive dorsal
horn neurons to cold and heat stimuli were examined in anesthetized
rats. Electrophysiological recordings were obtained from 72 nociceptive
spinal neurons located in the superficial and deep dorsal horn. All
neurons had receptive fields (RFs) on the glabrous skin of the hindpaw,
and neurons were functionally divided into wide dynamic range (WDR) and
high-threshold (HT) neurons. Forty-four neurons (61%) were classified
as WDR and responded to both innocuous and noxious mechanical stimuli
(mean mechanical threshold of 12.8 ± 1.6 mN). Twenty-eight
neurons (39%) were classified as HT and were excited only by noxious
mechanical stimuli (mean mechanical threshold of 154.2 ± 18.3 mN). Neurons were characterized for their sensitivity heat (35 to
51°C) and cold (28 to
12°C) stimuli applied to their RF. Among
WDR neurons, 86% were excited by both noxious heat and cold stimuli,
while 14% responded only to heat. For HT neurons, 61% responded to
heat and cold stimuli, 32% responded only to noxious heat, and 7%
responded only to noxious cold. Effects of a mild freeze injury
(
15°C applied to the RF for 20 s) on responses to heat and
cold stimuli were examined in 30 WDR and 22 HT neurons. Skin freezing
was verified as an abrupt increase in skin temperature at the site of
injury due to the exothermic reaction associated with crystallization.
Freezing produced a decrease in response thresholds to heat and cold
stimuli in most WDR and HT neurons. WDR and HT neurons exhibited a mean decrease in response threshold for cold of 9.0 ± 1.3°C and
10.0 ± 1.6°C, respectively. Mean response thresholds for heat
decreased 4.0 ± 0.4°C and 4.3 ± 1.3°C in WDR and HT
neurons, respectively. In addition, responses to suprathreshold cold
and heat stimuli increased. WDR and HT neurons exhibited an 89% and a
192% increase in response across all cold stimuli, and a 93 and 92%
increase in responses evoked across all heat stimuli, respectively. Our results demonstrate that many spinal neurons encode intensity of
noxious cold as well as noxious heat over a broad range of stimulus
temperatures. Enhanced responses of WDR and HT neurons to cold and heat
stimuli after a mild freeze injury is likely to contribute to thermal
hyperalgesia following a similar freeze injury in humans.
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