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The Journal of Neuroscience, October 1, 2002, 22(19):8352-8356
BRIEF COMMUNICATION
Deficits in Visceral Pain and Referred Hyperalgesia in Nav1.8 (SNS/PN3)-Null MiceJennifer M. A. Laird1, Veronika Souslova2, John N. Wood2, and Fernando Cervero1 1 Department of Physiology, University of Alcalá, Alcalá de Henares, E-28871 Madrid, Spain, and 2 Department of Biology, University College London, London WC1E 6BT, United Kingdom
ABSTRACT
TOP
ABSTRACT
INTRODUCTION
The tetrodotoxin-resistant sodium channel
subunit Nav1.8 is expressed exclusively in primary sensory neurons and is proposed to play an important role in sensitization of nociceptors. Here we compared visceral pain and referred hyperalgesia in Nav1.8-null mice and their wild-type littermates in five tests that differ in the degree to which behavior depends on spontaneous, ongoing firing in sensitized nociceptors. Nav1.8-null mice showed normal nociceptive behavior provoked by acute noxious stimulation of abdominal viscera (intracolonic saline or intraperitoneal acetylcholine). However, Nav1.8-null mutants showed weak pain and no referred hyperalgesia to intracolonic capsaicin, a model in which behavior is sustained by ongoing activity in nociceptors sensitized by the initial application. Nav1.8-null mice also showed blunted pain and hyperalgesia to intracolonic mustard oil, which sensitizes nociceptors but also provokes tissue damage. To distinguish between a possible role for Nav1.8 in ongoing activity per se and ongoing activity after sensitization in the absence of additional stimuli, we tried a visceral model of tonic noxious chemical stimulation, cyclophosphamide cystitis. Cyclophosphamide produces cystitis by gradual accumulation of toxic metabolites in the bladder. In this model, Nav1.8-null mice showed normal responses. There were no differences between null mutants and their normal littermates in tissue damage and inflammation evoked by any of the stimuli tested, suggesting that the behavioral differences are not secondary to impairment of inflammatory responses. We conclude that there is an essential role for Nav1.8 in mediating spontaneous activity in sensitized nociceptors.
Key words: viscera; referred hyperalgesia; tetrodotoxin resistant sodium channels; colitis; cystitis; cyclophosphamide; inflammation; knock-out mice
INTRODUCTION
Tissue damage or inflammation provokes an increase in sensitivity and spontaneous firing of action potentials in primary afferent nociceptors. This process, known as sensitization, gives rise to primary hyperalgesia (hypersensitivity at the site of injury) and ongoing pain. The ongoing nociceptor firing is also essential to establish and maintain secondary hyperalgesia (touch-evoked pain in undamaged tissue). The molecular mechanisms underlying nociceptor sensitization are not fully understood, but there is evidence for the involvement of voltage-gated sodium currents, particularly those that are resistant to tetrodotoxin (TTX). When primary afferent cell bodies in culture are exposed to inflammatory mediators known to produce sensitization of nociceptor terminals, TTX-resistant (TTX-r) sodium currents are enhanced (England et al., 1996
; Gold et al., 1996
Two sodium channel
Sensitization of primary afferent nociceptors plays a key role in many forms of visceral pain. TTX-r currents are present in the majority of visceral afferents (Yoshimura et al., 1996
MATERIALS AND METHODS
Adult male mice were used. Mice homozygous for the disrupted allele (
/
30 min before the test started. After testing, the mice were humanely killed. European Union and State legislation regulating animal experiments were followed. Statistical analyses were performed using ANOVA with post hoc tests or Mann-Whitney U or Student's t tests, as appropriate. The level of statistical significance was set at p < 0.05.
Behavioral responses to intraperitoneal injections of acetylcholine. The mice were placed individually in plastic boxes (20 × 27 × 15 cm). Behaviors counted were: (1) licking of the abdomen, (2) stretching, and (3) squashing of the abdomen against the floor. A volume of 0.3 ml of acetylcholine (0.3 mg/ml) was given intraperitoneally, and the behavior of the mice was observed for 10 min (n = 6-7/group).
Behavioral responses to stimulation of the colon. The methods used were as we have described previously (Laird et al., 2001
Cyclophosphamide cystitis. Behavioral experiments examining the effect of cyclophosphamide over 4 hr postinjection were performed in +/+ and
After behavioral testing, the animals were killed, and the bladder was removed, opened, and pinned out. Digital photographs of the mucosal side of the entire bladder were taken at 10× magnification. The degree of damage to the mucosa was assessed from the stored digital images.
Plasma extravasation in the viscera evoked by chemical stimulation. Evan's Blue (50 mg/kg, i.v.) was administered 18 hr before behavioral testing to allow subsequent quantification of plasma extravasation in the bladder or colon. The affected viscus was removed postmortem for determination of Evan's Blue content. The tissue was dried and weighed, the dye was extracted in formamide (60°C for 24 hr), and the absorbance was measured with a spectrophotometer (
= 620 nm).
RESULTS
Nav1.8-null mice showed no overt differences from wild-type littermates in general behavior or locomotor skills, as reported previously (Akopian et al., 1999
Nav1.8-null mice show normal responses to acute noxious visceral stimuli
The response to intracolonic instillation of 0.1 ml of isotonic saline was tested in +/+ and
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Figure 1. Spontaneous visceral pain-related behavior in wild-type (+/+) and Nav1.8-null (
Nav1.8-null mice show blunted responses to sensitizing visceral stimuli
Capsaicin produces activation of nociceptors followed by prolonged ongoing activity (because of sensitization) in the absence of additional stimulation (for discussion, see Laird et al., 2001
We subsequently tried the effect of intracolonic 1% mustard oil, because this stimulus activates and sensitizes a mixed population of afferents and also produces tissue damage, in contrast to intracolonic capsaicin, which activates only afferents expressing transient receptor potential V1 (TrpV1 or V1) and produces a pure neurogenic inflammation (Laird et al., 2000
Nav1.8-null mutants show no referred hyperalgesia after intracolonic capsaicin and weak hyperalgesia after intracolonic mustard oil
Tests of mechanical sensitivity of the abdomen and hindpaw 20 min after intracolonic capsaicin in +/+ mice revealed a marked shift of the stimulus response function to the left compared with baseline, evidence of referred hyperalgesia. Significant referred hyperalgesia was seen in both the abdomen (data not shown) and the hindpaws (Fig. 2A). In contrast,
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Figure 2. Referred visceral hyperalgesia in wild-type (+/+) and Nav1.8-null (
Nav1.8-null mice showed blunted pain responses to intracolonic capsaicin or mustard oil. In these models, pain and hyperalgesia, once initiated, are likely maintained by ongoing activity in sensitized nociceptors in the absence of additional stimuli (Laird et al., 2000
Nav1.8-null mice show normal pain responses to cyclophosphamide-induced cystitis
The systemic administration of cyclophosphamide in +/+ mice (n = 6) produced a gradually increasing display of visceral nociceptive behaviors that were scored every 30 min. The behavioral response was clearly established 90-120 min after cyclophosphamide treatment and continued increasing for the remainder of the 4 hr observation period. Nav1.8-null mice (n = 6) showed a very similar behavioral response to systemic cyclophosphamide, such that the number and time course of behaviors were not significantly different (Fig. 1C). Both +/+ and
Nav1.8-null mice show normal inflammatory responses to noxious visceral stimuli
At the end of the behavioral experiment, the affected viscus (descending colon or urinary bladder) was removed postmortem, and plasma extravasation was assessed by measuring Evan's Blue content. There were no significant differences between +/+ and
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Table 1. Plasma extravasation evoked by inflammation of the colon or bladder In normal animals, cyclophosphamide treatment produces mucosal erosion and hemorrhage of the bladder in addition to edema (Fraiser et al., 1991
DISCUSSION
In the present study, we found that Nav1.8-null mice showed blunted responses and no referred hyperalgesia in response to intracolonic capsaicin. After application of an acute tissue-damaging inflammatory stimulus, intracolonic mustard oil, Nav1.8-null mice also showed attenuated visceral pain and hyperalgesia. However, Nav1.8-null mice showed no deficits in pain behavior provoked by acute noxious mechanical or mixed mechanical/chemical stimulation of the abdominal viscera or in pain and hyperalgesia evoked by cyclophosphamide cystitis. In all cases, tissue damage and inflammation were no different in Nav1.8-null mice compared with their wild-type littermates.
Nav1.8 is not required for visceral neurogenic or non-neurogenic inflammation
In the present study, Nav1.8-null mice showed no differences from wild type in inflammatory responses to intracolonic capsaicin or to cyclophosphamide, which provokes visceral inflammation wholly or partly via neurogenic mechanisms (Maggi et al., 1992
Nav1.8 is not required for responses to acute, noxious visceral stimuli
Intracolonic isotonic saline, which produces a brief distension, and intraperitoneal acetylcholine are acute noxious stimuli that do not provoke sensitization of nociceptors or evidence of referred hyperalgesia. Nav1.8-null mice responded normally to these stimuli. We also found that responses to phasic mechanical stimuli applied to the skin were intact in Nav1.8-null mice when testing responses to von Frey hairs applied to the abdomen and paws, as described previously by Akopian et al. (1999)
Nav1.8 is required for the expression of normal visceral pain and hyperalgesia to intracolonic capsaicin or mustard oil
Nav1.8-null mice showed markedly reduced pain responses and no referred hyperalgesia in response to intracolonic capsaicin. After intracolonic mustard oil, Nav1.8-null mice showed attenuated visceral pain and hyperalgesia, but the reduction was less pronounced than after capsaicin. The difference between the responses to these stimuli may be ascribed to the different populations of afferents excited. Capsaicin selectively activates afferent endings expressing VR1 receptors, probably all of which are nociceptors (Caterina and Julius, 2001
Mustard oil excites all classes of unmyelinated afferents, because it is a nonspecific pore-forming substance, and also sensitizes nociceptors (Kress and Reeh, 1996
Role for Nav1.8 in responses that depend on ongoing activity in sensitized visceral nociceptors
The blunted pain and hyperalgesia to chemical stimuli (intracolonic capsaicin or mustard oil) in Nav1.8-null mice could be attributable to participation of Nav1.8 in sustained spontaneous activity in sensitized nociceptors in the absence of additional stimuli or to an involvement of Nav1.8 in sustained activity per se. The sustained pain and hyperalgesia after capsaicin rely on ongoing activity in nociceptors sensitized by the initial application. As well as sensitizing nociceptors, mustard oil provokes tissue damage, thus providing an additional source of ongoing input that may account for the less pronounced deficit in mustard oil-evoked behavior in Nav1.8-null mice.
A role for Nav1.8 in sustained firing and in control of the firing threshold has been proposed on the basis of the kinetic properties of the channel (McCleskey and Gold, 1999
To distinguish between the two possibilities discussed above, we tested the responses of Nav1.8-null mice to intraperitoneal cyclophosphamide. Cyclophosphamide administration produces cystitis as a result of the accumulation in the bladder of a toxic metabolite, acrolein, excreted in urine (Cox, 1979
We conclude that the complete lack of referred hyperalgesia and a greatly attenuated pain response after capsaicin observed in Nav1.8-null mice support the idea that Nav1.8 has an essential role in mediating sustained spontaneous activity in sensitized nociceptors. The attenuated response to intracolonic mustard oil in Nav1.8
FOOTNOTES Received May 8, 2002; revised July 9, 2002; accepted July 12, 2002.
This work was supported by the Madrid Regional Government (Contrato Programa), the Ministry of Science and Technology, Spain (SAF-2000-0199), the Medical Research Council, and the Wellcome Trust, UK. J.M.A.L. was a Ramón y Cajal Investigator (Ministry of Science and Technology, Spain). We thank María-José García for expert technical assistance and Fleur Geoghegan for help with genotyping.
Correspondence should be addressed to Dr. J. M. A. Laird, Department of Bioscience, AstraZeneca R&D Montreal, 7171 Frederick-Banting, St. Laurent, Quebec H4S 1Z9, Canada. E-mail: jennifer.laird{at}astrazeneca.com.
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