Stimulation of Deep Somatic Tissue with Capsaicin Produces Long-Lasting Mechanical Allodynia and Heat Hypoalgesia that Depends on Early Activation of the cAMP Pathway

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The Journal of Neuroscience, July 1, 2002, 22(13):5687-5693

Stimulation of Deep Somatic Tissue with Capsaicin Produces Long-Lasting Mechanical Allodynia and Heat Hypoalgesia that Depends on Early Activation of the cAMP Pathway
K. A. Sluka
Graduate Program in Physical Therapy and Rehabilitation Science, Neuroscience Graduate Program, Pain Research Program, University of Iowa, Iowa City, Iowa 52242

  ABSTRACT

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Pain and hyperalgesia from deep somatic tissue (i.e., muscle and joint) are processed differently from that from skin. Thisstudy examined differences between deep and cutaneous tissue allodyniaand the role of cAMP in associated behavioral changes. Capsaicinwas injected into the plantar aspect of the skin, plantar musclesof the paw, or ankle joint, and responses to mechanical and heatstimuli were assessed until allodynia resolved. Capsaicin injectedinto skin resulted in a secondary mechanical allodynia and heathypoalgesia lasting ~3 hr. In contrast, capsaicin injection intomuscle or joint resulted in a long-lasting bilateral (1-4 weeks)mechanical allodynia with a simultaneous unilateral heat hypoalgesia.The pattern and degree of inflammation were similar when capsaicinwas injected into skin, muscle, or joint, with peak increases24 hr after injection. Heat hypoalgesia that occurs after injectioninto deep tissue was reversed by spinal blockade of adenylatecyclase or protein kinase A (PKA). Interestingly, mechanical allodyniawas reversed if adenylate cyclase or PKA inhibitors were administeredspinally 24 hr, but not 1 week, after injection of capsaicin.Spinally administered 8-bromo-cAMP resulted in a similar pattern,with heat hypoalgesia and mechanical allodynia occurring simultaneously.Thus, injection of capsaicin into deep tissues results in a longer-lastingmechanical allodynia and heat hypoalgesia compared with injectionof capsaicin into skin. The mechanical allodynia depends on earlyactivation of the cAMP pathway during the first 24 hr but is independentof the cAMP pathway by 1 week after injection ofcapsaicin.

Key words: pain; analgesia; protein kinase A; adenylate cyclase; muscle; joint

  INTRODUCTION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Pain and hyperalgesia from deep somatic tissue, muscle, and joint are processed differently from that from skin (for review,see Mense, 1993; Schaible and Grubb, 1993). Pain from deep tissuesis diffuse, dull, aching, and difficult to localize, whereas thatfrom cutaneous tissues is typically sharp and easy to localize(Kellgren, 1938; Ochoa and Torebjork, 1989; Simone et al., 1994;Marchettini et al., 1996). Furthermore, deep tissue pain is typicallyreferred to superficial structures, whereas cutaneous pain isnot usually referred (Ochoa and Torebjork, 1983; Marchettini etal., 1990). Longer-lasting enhancement of the ventral root reflexoccurs after C-fiber stimulation of a muscle nerve compared withC-fiber stimulation of a cutaneous nerve (Wall and Woolf, 1984).Afferent innervation of the spinal cord by skin and deep tissuesis significantly different. Cutaneous nociceptors send dense projectionsto laminas I and II (Willis and Coggeshall, 1991). In contrast,joint and muscle afferents innervate laminas I and V, and thereare no projections to lamina II (Craig et al., 1988; Mense andCraig, 1988). Furthermore, different biochemicals are observedin DRG that innervate the skin, muscle, and joint (O'Brien etal., 1989; Plenderleith and Snow, 1993). Thus, the same stimuluspresented to muscle or joint would be expected behaviorally toresult in a different patterned response than when injected intoskin.

Capsaicin is a chemical irritant that causes a local neurogenic inflammation when injected into the skin. It produces primaryheat and mechanical hyperalgesia and secondary mechanical hyperalgesiain humans and rats that resolves within hours (Simone et al.,1989; Lamotte et al., 1991; Sluka, 1997). There are also reportsthat capsaicin produces hypoalgesia in the area surrounding theinjection site (Raja et al., 1984). Preliminary data show thatinjection of capsaicin into joint or muscle produces secondarymechanical allodynia and heat hypoalgesia (Sluka, 2000).

After intradermal capsaicin injection, spinothalamic tract cells show increased sensitivity to innocuous and noxious mechanicalstimuli both at and distant from the site of injection (Simoneet al., 1991; Sluka et al., 1997; Dougherty et al., 1998). However,the responsiveness of spinothalamic tract cells to heat is decreasedafter intradermal capsaicin injection (Sluka et al., 1997; Doughertyet al., 1998). Interestingly, the decreased responsiveness toheat of spinothalamic tract cells induced by intradermal capsaicininjection is reversed by inhibition of protein kinase A (PKA)(Sluka et al., 1997). Furthermore, sensitization of spinothalamictract cells to mechanical stimuli (Sluka et al., 1997) and mechanicalhyperalgesia (Sluka, 1997; Sluka and Willis, 1997) produced byintradermal injection of capsaicin are reversed by blockade ofPKA or adenylatecyclase.

Thus, these experiments were undertaken to examine (1) differences in mechanical and heat sensitivity in response to capsaicininjection in the skin, muscle, and joint and (2) the role of thecAMP pathway in the behavioral responses to capsaicin injection.I hypothesized that capsaicin injection into muscle or joint wouldresult in a longer-lasting allodynia than when injected into skin.I also hypothesized that heat hypoalgesia and mechanical allodyniainduced by capsaicin injection would be reduced by spinal blockadeof the cAMPpathway.

  MATERIALS AND METHODS

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

All experiments were approved by the Animal Care and Use Committee at the University of Iowa and were in accordance with theNational Institutes of Health and the International Associationfor the Study of Pain policies on use of laboratoryanimals.

Capsaicin injection. Male Sprague Dawley rats (250-350 gm; n = 173; Harlan Sprague Dawley, Indianapolis, IN) were used forthese experiments. Capsaicin (0.2%; 50 µl; Fluka Chemical Corporation,Milwaukee, WI) was injected (1) intradermally into the rostralaspect of the plantar surface of the paw, (2) intra-articularlyinto the ankle joint, or (3) intramuscularly into the plantarmuscles of the foot. These tissues were chosen because they areall supplied by branches of the tibial nerve and they are in closeproximity to each other (Greene, 1963). Capsaicin was dissolvedin 10% Tween 80, 10% ethanol, and sterilesaline.

Myeloperoxidase assay. Myeloperoxidase is a neutrophil-specific marker used to assess the infiltration of neutrophils intoan area of inflammation. To measure myeloperoxidase, a variationof the method described by Desser (1971) was used in which anenzyme unit is defined as the amount of enzyme necessary to producean increase of 1 absorbance unit in 1 min. Rats were deeply anesthetizedwith sodium pentobarbital (Abbott Laboratories, North Chicago,IL) and guillotined, and tissues were removed promptly. The anklejoint, plantar muscles of the foot, or plantar surface of theskin was removed on both the ipsilateral and contralateral sidesat 2 hr (n = 4), 24 hr (n = 4), and 1 week (n = 4) after capsaicininjection and in normal rats (n = 3). The specimens were homogenizedin 0.5% hexadecyltrimethylammonium bromide (Sigma, St. Louis,MO) to temporarily neutralize enzyme activity. The samples subsequentlyunderwent three cycles of freezing and thawing, followed by centrifugationto remove debris. A Spectramax 190 (Molecular Devices, Sunnyvale,CA) plate reader at a wavelength of 450 nm was used to read thechanges in absorbance over time. Samples were reacted with hydrogenperoxide and o-dianisidine dihydrochloride at ambient temperature.Absorbance was measured every minute for up to 10 min. V_max wasused to determine the units of myeloperoxidase per gram of tissuefrom the standard curve. Samples were prepared in triplicate andaveraged. Myeloperoxidase obtained from humans (Sigma) was usedas a standard. The assay showed a 3% coefficient of variance betweendays and a limit of quantification of 0.07 U/gmtissue.

Behavioral testing. Animals were tested for withdrawal thresholds to mechanical stimuli (von Frey filaments) applied to thedistal portion of the plantar aspect of the hindpaw (Sluka, 1997;Gopalkrishnan and Sluka, 2000). von Frey filaments with bendingforces from 7 to 360 mN were applied in a progressively increasingmanner until the hindpaw was withdrawn or 360 mN was reached.Each filament was applied twice. The filament of lowest bendingforce from which the animal withdrew was considered the mechanicalwithdrawal threshold of the hindpaw. After a response, the filamentsabove and below were tested to confirm the withdrawal threshold.The test-retest reliability of this method has been establishedpreviously (Gopalkrishnan and Sluka, 2000).

Animals were also tested for response to radiant heat applied to the plantar surface of the paw as described previously (Hargreaveset al., 1988). Briefly, animals were placed in clear plastic cubicleson an elevated glass plate and allowed to acclimate for 10-20min before testing. The latency to withdrawal of the paw fromradiant heat was measured. Five trials per time were averagedto give one number per animal. The test-retest reliability ofthis method has been established previously (Sluka et al., 1999).

Both mechanical withdrawal thresholds and response to radiant heat were applied to the caudal portion of the paw, which wasoutside the site of capsaicin injection in the skin, muscle, orjoint. Thus, behavioral tests are interpreted as a measure ofsecondary hyperalgesia or allodynia (Sluka, 1997; Sluka and Willis,1997).

Motor testing. Because 100 nmol of PKA inhibitor (PKI) produced significant motor effects in five animals, rats administeredthe 60 nmol dose of PKI (n = 4) were tested for motor effectswith a Rota-Rod treadmill test and placing reflex test. Specifically,they were placed on a Rota-Rod treadmill (Ugo Basile Rota-Rod;Stoelting, Wood Dale, IL) rotating at a gradually increasing speedfrom 1 to 18 rpm for 120 sec and maintained for another 30 secat 18 rpm (Sluka et al., 2001). For stable Rota-Rod treadmillresults, the rats were trained for 2 d before injection of drug.Three sessions of three trials each were performed at an intersessioninterval of >2 hr and an intertrial interval of >5 min. Performancetime in minutes was recorded until the rat failed to stay on theRota-Rod or reached 150 sec. The placing reflex was also evaluatedafter drug administration (Coderre and Van Empel, 1994; Zahn andBrennan, 1998). This test is performed by drawing the dorsum ofthe hindpaw across the edge of a table. The animal responds bylifting the paw onto the surface of the table. This was scoredas 2, normal; 1, delay of 1-2 sec; and 0, >2 sec. Motor functionwas assessed at baseline and 15, 30, 45, and 60 min after administrationofdrug.

Intrathecal catheterization. Intrathecal catheters (n = 142; 32 gauge polyurethane; 10 cm length; Recathco, Allison Park,PA) were placed 5-6 d before the first intramuscular injectionof saline (Storkson et al., 1996; Pogatzki et al., 2000). In brief,animals were anesthetized with halothane (2-5%), and a 23 gaugehypodermic needle was inserted into the intervertebral space betweenL5 and L6. A 32 gauge polyurethane catheter was inserted throughthe needle and advanced cranially until 3.5-4.0 cm of the catheterwas under the skin. The external portion of the catheter was securedto the muscle and fascia. The free end was subsequently insertedinto polyethylene-10 tubing and tunneled to the cervicalregion.

Experimental design. In the first set of experiments, capsaicin was injected into the skin (n = 6), muscle (n = 13), or joint(n = 12). Behavioral tests were performed before the injectionand hourly through 4, 8, 24, and 48 hr and 1 week and then weeklyuntil the allodynia resolved. Responses to heat and mechanicalstimuli were assessed at each timeperiod.

The second series of experiments was designed to test the role of the cAMP pathway in the maintenance of the mechanical allodyniaand heat hypoalgesia observed in the first experiment after injectionof capsaicin into the muscle or joint. Behavioral tests were performed24 hr or 1 week after injection of capsaicin into the muscle orjoint, and then 9-(tetrahydro-2'-furyl)adenine (SQ22536; blocksadenylate cyclase; 0.07-0.7 nmol/5 µl; n = 51; Biomol ResearchLaboratories Inc, Plymouth Meeting, PA), myristoylated PKI (14-22)amide (blocks PKA; 10-100 nmol/5 µl; n = 45; Biomol Research LaboratoriesInc), or vehicle (n = 21) was injected intrathecally. Each dosewas given to only one animal, and each group consisted of threeto eight animals. Heat testing began 10 min after administrationof drug and was subsequently performed at 5 min intervals for30 min. After the heat testing, 40-45 min after injection of drug,the mechanical withdrawal threshold was tested. We demonstratedpreviously that spinal application of either SQ22536 or PKI hasno effect on normal behavioral responses (Sluka, 1997).

In the last series of experiments, the effects of spinal activation of the cAMP pathway on mechanical and heat sensitivitywere assessed. 8-Bromo-cAMP (3-30 nmol/5 µl; n = 16) was injectedintrathecally, and withdrawal latency to heat was measured for30-45 min after injection, followed by withdrawal threshold tomechanical stimulation at ~35-45 min after injection. A higherdose of 8-bromo-cAMP, 100 nmol/5 µl, was tested in three animalsbut produced agitation, making it difficult to test the animals,and thus was not tested further. The effect of pretreatment withPKI (60 nmol/5 µl) on the effects of 30 nmol/5 µl 8-bromo-cAMPwas also tested (n =4).

Statistical analysis. Differences between groups and across time for paw withdrawal latency to heat were analyzed with a one-wayANOVA. Post hoc testing was done as appropriate with a Tukey'stest. Because there was no difference between normal tissue andthe contralateral side, side-to-side differences were calculatedfor myeloperoxidase activity, and a one-way ANOVA was used toanalyze differences between groups. Post hoc testing was doneas appropriate with a Tukey's test. Kruskal-Wallis ANOVA was usedto analyze differences in withdrawal threshold to mechanical stimulibetween groups. Post hoc testing was done as appropriate witha sign test. Data were reported as the mean ± SEM for paw withdrawallatency to heat and myeloperoxidase assay and as the median ±25th and 75th percentiles for mechanical withdrawalthreshold.

  RESULTS

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Behavioral effects of capsaicin

As reported previously (Sluka, 1997), intradermal injection of capsaicin resulted in a decrease in the withdrawal thresholdto mechanical stimuli by 30 min that lasted ~3 hr after injection(Fig. 1). The withdrawal threshold to mechanical stimuli returnedto baseline threshold values by 4 hr after injection. Similarly,the withdrawal threshold to mechanical stimuli decreased by 30min after injection into the plantar muscles of the paw (Fig.1). However, it remained decreased through 1 week and resolvedby 2 weeks after injection of capsaicin into the muscle. Furthermore,the mechanical withdrawal threshold decreased contralaterally24 hr after capsaicin injection into the muscle and remained decreasedthrough 1 week, returning to baseline by 2 weeks (Fig. 2). Incontrast, capsaicin injection into the ankle joint showed a longertime to onset, with allodynia developing by 2 hr. This decreasein withdrawal threshold spread to the contralateral side after24 hr and lasted through 4 weeks (Fig. 2). Minimal limb guardingoccurred within the first few hours after injection of capsaicininto the skin, muscle, or joint, and by 24 hr, no differencesbetween ipsilateral and contralateral sides were observed.

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Figure 1. The paw withdrawal latency to heat (top) and withdrawal threshold to mechanical stimulation (bottom) are shown before and for 4 hr after injection of capsaicin into the skin (squares), muscle (triangles), or joint (circles) for the ipsilateral (closed symbols) or the contralateral (open symbols) side. Significant increases in withdrawal latency to heat ipsilaterally occur after injection of capsaicin into the skin, muscle, or joint. No changes are observed for the contralateral paw. *p < 0.05, significantly different from before capsaicin injection.

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Figure 2. Responses to mechanical and heat stimuli after injection of capsaicin into the ankle joint or plantar muscles of the foot for the ipsilateral (closed circles) and contralateral (open circles) paws. Significant bilateral decreases in withdrawal threshold to mechanical stimuli are evident through 6 weeks after injection into the ankle joint and 1 week after injection into the plantar muscles. The response to heat is elevated ipsilaterally for 6 weeks after injection into the ankle joint and 2 weeks after injection into the plantar muscles. *p < 0.05, significantly different from baseline.

The response to heat stimuli was surprising. Specifically, injection of capsaicin into the skin, plantar muscles, or anklejoint resulted in a significant increase in the latency to heatstimulation (Fig. 1). The increase after injection into the deeptissues, muscle, or joint was long lasting. This increase occurredonly on the side that had received an injection and lasted through2 weeks for injection into the muscles and 5 weeks for injectioninto the ankle joint. The contralateral side remained at baselinethroughout the testingperiod.

Assessment of inflammation

Of the three tissues tested, the joint tissue had the highest baseline levels of myeloperoxidase activity. There were no significantdifferences between normal tissue and the contralateral side.For this reason, differences between the side injected with capsaicinand the contralateral side were analyzed. Capsaicin injected intothe muscle or joint resulted in significant increases in myeloperoxidaseactivity 2 and 24 hr after injection compared with tissue fromanimals without inflammation (Table 1). Significant increasesin myeloperoxidase activity also occurred after capsaicin injectioninto the skin 24 hr after injection but not at 2 hr or 1 week.There was no difference between tissue types 2 hr, 24 hr, or 1week after inflammation, suggesting that a similar degree of inflammationwas produced by a single injection of 0.2% capsaicin.


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Table 1. Myeloperoxidase activity

Inhibition of adenylate cyclase

SQ22536 was injected intrathecally into the spinal cord to assess the role of adenylate cyclase in the mechanical allodyniaand heat hypoalgesia associated with capsaicin injection intothe muscle or joint. Twenty-four hours and 1 week after injectionof capsaicin, a bilateral decrease in withdrawal threshold tomechanical stimulation and an ipsilateral increase in withdrawallatency to heat stimulation occurred. Intrathecal injection ofSQ22536, administered 24 hr or 1 week after capsaicin injection,reversed the increased paw withdrawal latency significantly ina dose-dependent manner compared with vehicle controls (Fig. 3).Furthermore, intrathecal injection of SQ22536 significantly reversedthe decreased mechanical withdrawal threshold when administered24 hr after injection of capsaicin. Surprisingly, intrathecallyadministered SQ22536 had no effect on the decreased withdrawalthreshold to mechanical stimuli induced by capsaicin when administered1 week after injection of capsaicin into the joint (Fig. 4).

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Figure 3. Withdrawal latency to heat ipsilaterally after spinal blockade with SQ22536 or PKI at 24 hr (top) or 1 week (bottom). A dose-dependent reduction in the capsaicin-induced increased withdrawal latency to heat is observed after spinal blockade of adenylate cyclase with SQ22536 or PKA with PKI. *p < 0.05, significantly different from vehicle control.

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Figure 4. Withdrawal threshold to mechanical stimuli bilaterally 24 hr and 1 week after injection of capsaicin. After spinal blockade with SQ22536 or PKI at 24 hr (top), there is a dose-dependent inhibition of the capsaicin-induced decrease in the withdrawal threshold to mechanical stimuli for animals injected with capsaicin into the muscle (squares) or joint (circles). No effect of SQ22536 or PKI occurred when they were administered 1 week after injection of capsaicin for either the ipsilateral or contralateral paw (bottom). The contralateral side is depicted with open symbols, and the ipsilateral side is depicted with closed symbols. *p < 0.05, significantly different from vehicle control.

Inhibition of PKA

Intrathecal blockade of PKA with PKI resulted in a pattern similar to that observed by blockade of adenylate cyclase withSQ22536. Specifically, PKI dose-dependently reversed the increasedlatency to radiant heat when administered either 24 hr or 1 weekafter injection of capsaicin (Fig. 3). The decreased withdrawalthreshold to mechanical stimuli associated with capsaicin injectioninto the muscle or ankle joint was reversed when PKI was administered24 hr after injection of capsaicin but not when it was administered1 week after injection of capsaicin (Fig. 4). Unexpectedly, the100 nmol dose of PKI resulted in significant motor deficits infive animals, and they were removed from the study. Motor testingof the 60 nmol dose of PKI had no effect on the Rota-Rod treadmilltest for up to 1 hr after administration of drug, with rats stayingon the treadmill for the full 150 sec. The placing reflex wasnormal in all four animals for up to 1 hr after administrationof 60 nmol ofPKI.

Activation of cAMP

Intrathecal injection of 8-bromo-cAMP resulted in a dose-dependent increase in the withdrawal latency to radiant heat anda simultaneous decrease in the withdrawal threshold to mechanicalstimuli (Fig. 5). The increase in withdrawal latency to heat anddecrease in withdrawal threshold to mechanical stimuli were preventedby previous treatment with an intrathecal injection of 60 nmolof PKI.

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Figure 5. Intrathecal administration of 8-bromo-cAMP resulted in a simultaneous increase in the withdrawal latency to heat and a decrease in the withdrawal threshold to mechanical stimuli compared with baseline. Pretreatment with 60 nmol of PKI prevented the increase in withdrawal latency to heat and the decrease in withdrawal threshold to mechanical stimuli produced by 30 nmol of 8-bromo-cAMP. *p < 0.05, significantly different from baseline; ⁺p < 0.05, significantly different from 30 nmol of 8-bromo-cAMP.

  DISCUSSION

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

Differences between skin, muscle, and joint

The present data show that intra-articular or intramuscular injection of capsaicin results in a long-lasting mechanical allodyniaand heat hypoalgesia of the skin. Furthermore, the mechanicalallodynia spreads to the contralateral paw ~24 hr after capsaicininjection into muscle or joint. The allodynia resolves more quicklyif injected into the muscle compared with the ankle joint. Althoughthe ankle joint, plantar muscle, and plantar aspect of the skinare supplied by branches of the tibial nerve (Greene, 1963), differentcentral anatomic pathways and/or different biochemical mediatorscould result in a different pattern of response. Dorsal root ganglianeurons innervating muscle and joint have less isolectin B4 andsomatostatin and more calcitonin gene-related peptide and substanceP than dorsal root ganglia neurons innervating cutaneous tissue(O'Brien et al., 1989; Plenderleith and Snow, 1993). The centralprojections from neurons innervating muscle and joint are predominatelyto lamina I and deeper dorsal horn, whereas those from cutaneoustissue have a dense projection to lamina II (Craig et al., 1988;Mense and Craig, 1988; Mense, 1993; Schaible and Grubb, 1993).Formalin injected into skin increases c-Fos expression throughoutlaminas I-V, but when it is injected into muscle, there is nolabeling in lamina II (Ohtori et al., 2000). Furthermore, C-fiberstimulation of a muscle nerve produces a longer-lasting increasein the flexion reflex compared with C-fiber stimulation of a cutaneousnerve (Wall and Woolf, 1984). In human subjects, painful intramuscularstimulation is rated as more unpleasant than painful cutaneousstimulation (Svensson et al., 1997). Capsaicin injected into muscleof human subjects produces longer-lasting pain, and referred painis more frequent (Witting et al., 2000). Thus, biochemical, anatomic,and physiological differences support the hypothesis that injuryto muscle and joint results in distinctly different behavioralresponses compared withskin.

Alternatively, capsaicin injection into muscle or joint may produce a more severe neurogenic inflammation than injection intoskin. However, assessment of neutrophilic activity after capsaicininjection shows that the amount of inflammation is similar betweenmuscle, skin, and joint tissues. Peak activity occurs 24 hr afterinjection for all three tissues, a time in which there was noallodynia from injection into skin. These data support differentialprocessing of nociceptive information from muscle and joint comparedwith skin. Measurement of myeloperoxidase activity as a measureof neutrophil infiltration is used extensively to measure acuteinflammation for periods up to 1 week after induction of inflammationin several animal models (Recio et al., 2000; Reifen et al., 2001).It should also be noted that, although it was our intention toinject capsaicin into the muscle tissue of the paw, it could alsohave affected tendons that course through the muscle layers inthe foot and ligaments that surround the small joints of the foot.However, visually, the muscle of the paw was inflamed and theskin was not red, suggesting that the injection into the plantarmuscles did affect predominantly deep and not cutaneoustissues.

Finally, repeated behavioral testing could result in a learning paradigm that caused the animals to withdraw at a lower bendingforce or with a faster latency to heat, and it would thus appearthat the animals were hyperalgesic to mechanical stimuli and/orheat stimuli. Previous data show that the responses of the animalsdid not change with repeated testing to mechanical and heat stimuliover a 6 week time course (Sluka et al., 2001). Furthermore, theincrease in heat response, with a simultaneous decrease in mechanicalresponse and different time course of behavioral changes afterinjection into muscle or joint tissue, argues against a learnedbehavior.

Activation of the cAMP pathway and mechanical allodynia

A time-dependent effect on mechanical allodynia was observed in the present study such that when adenylate cyclase or PKAis inhibited 24 hr after capsaicin injection, allodynia is reversed,but when it is inhibited 1 week after capsaicin injection, thereis no effect. Similarly, mice lacking the type I regulatory subunitof PKA showed attenuated nocifensive behaviors to the short-lastingstimuli formalin and prostaglandin E₂ but still developed hyperalgesiato a more chronic injury, neuropathic pain (Malmberg et al., 1997a).Alternatively, mice lacking PKC $gamma$ show a deficit in hyperalgesiaassociated with neuropathic pain but no deficit associated withthe first phase of the formalin test, which is thought to representacute pain (Malmberg et al., 1997b). However, the second phaseof the formalin test was reduced in mice lacking PKC $gamma$ (Malmberget al., 1997b). The later stages of mechanical allodynia inducedby intramuscular or intra-articular injection of capsaicin couldthus be maintained byPKC.

Previous studies show that the mechanical allodynia that occurs after intradermal injection of capsaicin is reversed by spinaladministration of the same inhibitors of PKA and adenylate cyclase(Sluka, 1997; Sluka and Willis, 1997). Furthermore, the presentstudy shows that 8-bromo-cAMP produces mechanical allodynia ina dose-dependent manner and agrees with other studies (Sluka,1997; Sluka and Willis, 1997; Dolan and Nolan, 2001). However,a low dose of 8-bromo-cAMP produces mechanical hypoalgesia insheep, but increasing the dose produces mechanical hyperalgesia(Dolan and Nolan, 2001).

Activation of adenylate cyclases in neurons can occur through neurotransmitter-receptor interactions that are linked to stimulatoryG-proteins. Alternatively, three (of nine) adenylate cyclase isoforms(AC1, AC3, and AC8) are calcium-calmodulin regulated (Xia andStorm, 1997). Activation of adenylate cyclase then converts ATPto cAMP, which results in activation of PKA. Activation of proteinkinases can result in neuroplasticity through phosphorylationof a variety of substrates including ion channels, neurotransmitterreceptors, and transcription factors. PKA phosphorylates calciumchannels, glutamate receptors, and the cAMP response element-bindingprotein (Dash et al., 1991; Blackstone et al., 1995; Hell et al.,1995). Indeed, phosphorylation of the PKA site of the NR1 subunitof NMDA glutamate receptors is increased after intradermal injectionof capsaicin (Zou et al., 2000). Injection of PKA enhances dorsalhorn neuron responsiveness to glutamate (Cerne et al., 1992, 1993),whereas blockade of PKA reduces capsaicin-induced sensitizationof spinothalamic tract cells (Sluka et al., 1997). Phosphorylationof the cAMP response element-binding protein enhances gene transcriptionof cell proteins (Dash et al., 1991; Shaywitz and Greenberg, 1999)and increases after carrageenan inflammation (Messersmith et al.,1996), formalin injection (Ji and Rupp, 1997; Anderson and Seybold,2000), sciatic nerve stimulation at C-fiber strength (Ji et al.,2000), and neuropathic pain (Ma and Quirion, 2001).

The role of the cAMP pathway in neuroplasticity has been studied extensively with respect to long-term potentiation (LTP)and learning in the hippocampus and parallels the time-dependentactivation of the cAMP pathway observed in the present study.Specifically, PKA activity increases in the early phases of spatiallearning tasks (Vazquez et al., 2000). PKC appears to be importantin the maintenance as well as the initiation of LTP and learning(Sweatt, 1999; Vazquez et al., 2000). In learning and memory behavioraltasks, mice deficient in the calcium-dependent adenylate cyclasesAC1 and AC8 show a selective deficit in hippocampus-dependentlearning and LTP (Wong et al., 1999). Thus, the mechanical allodyniaobserved in the present study shows an activation pattern of thecAMP pathway similar to that observed in LTP and memory. Specifically,activation of the cAMP second messenger pathway is necessary duringthe early phase of development but not in the later maintenancephase. Furthermore, on the basis of these similarities and previousdata with PKC $gamma$ knock-out mice (Malmberg et al., 1997a), it ispossible that PKC is important in the maintenance phase of mechanicalallodynia.

Activation of the cAMP pathway and heat hypoalgesia

The heat hypoalgesia that occurs after capsaicin injection could be related to damage to peripheral nerves, changes in peripheralnociceptors, or changes in the CNS. The reversal of heat hypoalgesiaby spinal blockade of adenylate cyclase or PKA suggests that thishypoalgesia is mediated by plastic changes in the CNS rather thanby damage to peripheral nerves. The effects may be related tochanges in spinothalamic tract neurons and not to modulation ofneurotransmitter release. Previous studies show a decreased responsivenessof spinothalamic tract cells to heat stimuli after intradermalinjection of capsaicin (Sluka et al., 1997; Dougherty et al.,1998) that is reversed by spinal blockade of PKA (Sluka et al.,1997). PKA has no effect on increased excitatory amino acid releasethat occurs after capsaicin injection (Sluka and Willis, 1998).More recently, Liu et al. (2001) demonstrated that capsaicin desensitizesprimary afferent nociceptors by inhibiting sodium channel conductanceand that this inhibition is mediated by cAMP. Vanilloid 1 receptorsare activated by capsaicin, are thought to be heat sensors, arefound on nociceptors, and desensitize after capsaicin injection.It is possible that this desensitization also occurs on centralterminals of primary afferents and that the effects of spinalinhibition of adenylate cyclase and PKA are to reverse cAMP-mediateddesensitization.

Summary

In summary, this study showed that activation of the cAMP pathway in the spinal cord results in divergent behavioral signsdepending on the modality of stimulus tested (i.e., mechanicalor heat), suggesting that processing of mechanical and heat responsivenessto tissue injury involves unique processes. Furthermore, activationof the cAMP pathway is time-dependent with respect to maintenanceof mechanical allodynia and appears to be necessary in the earlyphases of central sensitization but not in later phases. Finally,deep tissue injury results in longer-lasting allodynia comparedwith the same stimulus applied to the skin, supporting the theorythat nociceptive processing from deep tissue injury is distinctfrom nociceptive processing from cutaneous tissueinjury.

  FOOTNOTES

Received Jan. 24, 2002; revised March 8, 2002; accepted April 4, 2002.

This study was supported by National Institutes of Health Grants R01-NS-39734 and K02-AR-02201. I thank Tammy Lisi and CharlesCibula for excellent technicalassistance.

Correspondence should be addressed to K. A. Sluka, Graduate Program in Physical Therapy and Rehabilitation Science, Universityof Iowa, Iowa City, IA 52242. E-mail: ksluka{at}blue.weeg.uiowa.edu.

  REFERENCES

TOP
ABSTRACT
INTRODUCTION
MATERIALS AND METHODS
RESULTS
DISCUSSION
REFERENCES

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