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J Neurophysiol (February 1, 2003). 10.1152/jn.00568.2002
Submitted on Submitted 16 July 2002; accepted in final form 16 October 2002
1Department of Anatomy and Neurosciences, Marine Biomedical Institute, and 2Division of Neurosurgery, Department of Surgery, The University of Texas Medical Branch, Texas 77555-1069
Lin, Qing,
Xiaoju Zou,
Li Fang, and
William D. Willis.
Sympathetic Modulation of Acute Cutaneous Flare Induced by
Intradermal Injection of Capsaicin in Anesthetized Rats. J. Neurophysiol. 89: 853-861, 2003. Much of the acute
cutaneous neurogenic inflammation after intradermal injection of
capsaicin (CAP) in rats is mediated by dorsal root reflexes (DRRs),
which cause the release of inflammatory agents from primary afferent
terminals. Sympathetic efferents modulate neurogenic inflammation by
interaction with primary afferent terminals. In this study, we examined
if DRR-mediated flare after CAP injection is subject to sympathetic
modulation. Changes in cutaneous blood flow on the plantar surface of
the foot were measured using a laser Doppler flow meter. After CAP
injection, cutaneous flare spread more than 20 mm away from the site of
CAP injection. However, this CAP-induced flare was significantly
reduced after surgical sympathectomy. Decentralization of
postganglionic neurons did not affect the flare induced by CAP
injection. If the foot of sympathectomized rats was pretreated with an
1-adrenoceptor agonist (phenylephrine) by
intra-arterial injection, the spread of flare induced by CAP injection
could be restored. However, if the spinal cord was pretreated with a
GABAA receptor antagonist, bicuculline, to
prevent DRRs, phenylephrine no longer restored the CAP-evoked flare. An
2-adrenoceptor agonist (UK14,304) did not
affect the CAP-evoked flare in sympathectomized rats. In
sympathetically intact rats, blockade of peripheral
1-adrenoceptors with terazosin profoundly
reduced the flare induced by CAP injection, whereas blockade of
peripheral 2-adrenoceptors by yohimbine did
not obviously affect the flare. Therefore the pathogenesis of acute
neurogenic inflammation in the intradermal CAP injection model depends
in part on intact sympathetic efferents and
1-adrenoceptors. Peripheral 1-adrenoceptors thus modulate the ability of
capsaicin sensitive afferents to evoke the release of inflammatory
agents from primary afferents by DRRs.
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