Role of the endocannabinoid system on the antihyperalgesic action of gabapentin in animal model of neuropathic pain induced by partial sciatic nerve ligation

BUFFON, ALEXANDRE C.; JAVORNIK, MARCELO A.; HEYMANNS, ANA C.; SALM, DAIANA C.; HOREWICZ, VERÔNICA V.; MARTINS, DANIEL F.; PIOVEZAN, ANNA P.

doi:10.1590/0001-3765202020191155

Abstract

Gabapentin has antihyperalgesic action, decreasing central sensitization in neuropathic pain models; this effect depends on the mobilization of endogenous pain control pathways. This study aims to investigate the contribution of the endocannabinoid system to the antihyperalgesic action of gabapentin. Mus musculus Swiss, male, were submitted to PSL. On the 7th and 14th days post PSL, different groups were treated with CB1 receptor antagonist, AM281 via i.t. (2 μg/5 μl) or i.pl. (10 μg/20 μl) or CB2, AM630 via i.t. (5 μL i.t.) or (20 μL i.p.) and 15 min after gabapentin (30 mg / kg orally). Mechanical hyperalgesia was measured by the frequency of paw removal by the von Frey monofilament. Gabapentin demonstrated antihypernociceptive action, which was attenuated in animals pretreated with AM281 in both the i.t. and i.pl routes on the 7th and 14th days, differently from animals pretreated with AM630 that did not achieve a significant reduction with administration i.t. only on the 14th day with administration i.pl. The results show that endocannabinoid system contributes to the antihyperalgesic action of gabapetin in neuropathic pain by PSL, suggesting participation in the medullary and peripheral levels of CB1 receptors, and the peripheral performance of CB2 receptors.

Key words
Endocannabinoid; gabapentin; hyperalgesia; nerve ligation

INTRODUCTION

Hypersensitivity to noxious stimuli is a common symptom in patients suffering from peripheral neuropathic pain in diverse conditions (Bannister et al. 2017BANNISTER K, QU C, NAVRATILOVA E, OYARZO J, XIE JY, KING T, DICKENSON AH & PORRECA F. 2017. Multiple sites and actions of gabapentin-induced relief of ongoing experimental neuropathic pain. Pain 158: 2386-2395.) and, for a better understanding of all these phenomena, studies have been carried out at various scales, but mostly using animal models, which are validated to mimic diverse etiologies of neuropathies (Munro et al. 2017MUNRO G, JANSEN-OLESEN I & OLESEN J. 2017. Animal models of pain and migraine in drug discovery. Drug Discov Today 22: 1103-1111.).

Gabapentin is a common first or second line treatment in such conditions, promoting antihyperalgesic action through a mechanism that mainly involves its action on the α_2δ subunit of the voltage-dependent Ca²⁺ channels (Lozovaya et al. 2009LOZOVAYA N, MIN R, TSINTSADZE V & BURNASHEV N. 2009. Dual modulation of CNS voltage-gated calcium channels by cannabinoids: Focus on CB1 receptor-independent effects. Cell Calcium 46: 154-162.), decreasing the central sensitization (Colloca et al. 2017COLLOCA L ET AL. 2017. Neuropathic pain. Nat Rev Dis Primers 3: 17002.) by reducing the release of excitatory neurotransmitters such as glutamate (GLU) and substance P (Moulin et al. 2014MOULIN D ET AL. 2014. Pharmacological management of chronic neuropathic pain: revised consensus statement from the Canadian Pain Society. Pain Res Manag 19: 328-335.). Other mechanisms recorded for its action in cases of pain concern its performance in 9-N-methyl-D-aspartate (NMDA) receptors, in transient receptor potential (TRP) channels, protein kinase-C (PKC), inflammatory cytokines and others (Kukkar et al. 2013KUKKAR A, BALI A, SINGH N & JAGGI AS. 2013. Implications and mechanism of action of gabapentin in neuropathic pain. Arch Pharm Res 36: 237-351.). However, this effect still needs to be better elucidated, and the contribution of the endocannabinoid system to the antihyperalgesic activity of gabapentin can be speculated since gabapentin is used to manage cannabis-use disorders (Lile et al. 2016LILE JA, WESLEY MJ, KELLY TH & HAYS LR. 2016. Separate and combined effects of gabapentin and Δ9-THC in humans discriminating Δ9-THC. Behav Pharmacol 27: 215-224.).

The endocannabinoid system is constituted of endogenous lipid-based retrograde neurotransmitters, being the most important the anandamide and 2-arachidonoylglycerol which are degraded, respectively, by the metabolizing enzymes fatty acid amide hydrolase (FAAH), which cleaves anandamide into arachidonic acid and ethanolamine or monoacylglycerol lipase (MAGL), and 2-AG into arachidonic acid and glycerol. Besides of this, after neurotransmitter release, endocannabinoids bind to two main cannabinoid receptors proteins, named CB₁ and CB₂; while the first type is predominantly found in the CNS and peripheral, the second type is mainly found in the immune system and, to a lesser extent scale in the CNS (Burston & Woodhams 2014BURSTON JJ & WOODHAMS SG. 2014. Endocannabinoid system and pain: an introduction. Proc Nutr Soc 73: 106-117.). CB₁ receptors are widely spread and distributed in the brain, with effects including the control of motor activity, hypothermia, increased hunger and disturbances in memory consolidation, besides psychotropic effects (Dogrul et al. 2012DOGRUL A, SEYREK M, YALCIN B & ULUGOL A. 2012. Involvement of descending serotonergic and noradrenergic pathways in CB1 receptor-mediated antinociception. Prog Neuropsychopharmacol Biol Psychiatry 38: 97-105.). Meanwhile, the expression of CB₂ receptors was observed in astroglia and microglial cells in the CNS (Burston & Woodhams 2014BURSTON JJ & WOODHAMS SG. 2014. Endocannabinoid system and pain: an introduction. Proc Nutr Soc 73: 106-117.).

In view of the above mentioned facts: 1) the high prevalence/incidence of neuropathic pain in patients around the world, 2) the need of better understanding endogenous mechanisms for analgesia promoted by gabapentin in painful conditions, 3) the fact that gabapentin is used to manage cannabis-use disorders, as well as that endocannabinoids modulate glutamate release, which is involved in the effects of gabapentin, the present study aims to investigate the participation of the endocannabinoid system in the antihyperalgesic effect of gabapentin in the model of partial sciatic nerve ligation in mice.

MATERIALS AND METHODS

Animals

Mus musculus Swiss mice, weighing between 25-35g were used. The animals were housed at a temperature of 22 ± 2 °C, under a cyclic regime of 12 h of light and 12 h of darkness (lights on at 6:00 p.m. and off at 6:00 p.m. by a timer) and with free access to food and water. The animals were acclimatized to the laboratory for at least 1 h before the behavioral tests, which were carried out between 8:00 a.m. and 12:00 a.m. The number of animals per group was calculated in n= 8, using the formula for comparison of two means, among independent samples, considering the power of the test of 80%, the significance level of 5%, the standard deviation of 12.5% for the hyperalgesic response from previous study records in our laboratory (Martins et al. 2015aMARTINS DF, PRADO MRB, DARUGE-NETO E, BATISTI AP, EMER AA, MAZZARDO-MARTINS L, SANTOS ARS & PIOVEZAN AP. 2015a. Caffeine prevents antihyperalgesic effect of gabapentin in an animal model of CRPS-I: evidence for the involvement of spinal adenosine A1 receptor. J Peripher Nerv Syst 20: 403-409.) and the difference value to be detected equal to 18%. The animals were used once during the experiment and animal care and experiments were carried out in accordance with the provisions of National Institutes of Animal Health Care (NIH publications 80-23), after approval by the CEUA-UNISUL Animal Ethics Committee under protocol number 16.027.5.01.IV. The number of animals and the intensity of the noxious stimulus used were the minimum necessary to demonstrate the consistency of the treatments.

Induction of neuropathic pain

To assess the neuropathic pain behavior, the procedure used was similar to that described in a previous study (Martins et al. 2015aMARTINS DF, PRADO MRB, DARUGE-NETO E, BATISTI AP, EMER AA, MAZZARDO-MARTINS L, SANTOS ARS & PIOVEZAN AP. 2015a. Caffeine prevents antihyperalgesic effect of gabapentin in an animal model of CRPS-I: evidence for the involvement of spinal adenosine A1 receptor. J Peripher Nerv Syst 20: 403-409.). Briefly, the mice were anesthetized with 2% isoflurane in 100% oxygen, with surgery performed by 1/3-1/2 ligation of the medial portion of the sciatic nerve with 8-0 silk thread. In the control group, the nerve was exposed but not ligated.

Influence of gabapentin on the hyperalgesia observed in the partial sciatic nerve ligation model (PSL)

To confirm the antihyperalgesic effect of gabapentin, different animals were submitted to the PSL procedure as described above and treated on days 7 and 14 after the PSL procedure with intraperitoneal (i.p.) vehicle administration (saline, 10 ml/kg) or gabapentin at the dose of 30 mg/kg, which is the dose that induced the most efficacious antihyperalgesic effect in the previous study model performed in our laboratory, and these periods of observation were chosen considering the minimum time required for the installation of the neuropathic process in the model, also according to an earlier study (Martins et al. 2015aMARTINS DF, PRADO MRB, DARUGE-NETO E, BATISTI AP, EMER AA, MAZZARDO-MARTINS L, SANTOS ARS & PIOVEZAN AP. 2015a. Caffeine prevents antihyperalgesic effect of gabapentin in an animal model of CRPS-I: evidence for the involvement of spinal adenosine A1 receptor. J Peripher Nerv Syst 20: 403-409.). During these days, the animals were evaluated in relation to mechanical hyperalgesia at different time points after administration (0.5 to 4 h after), in order to select the best treatment time with this drug.

Influence of intrathecal (I.T.) or intraplantar (I.PL.) treatment with CB₁ receptor antagonists on the antineuropathic effect of gabapentin

To evaluate the contribution of CB₁ receptors at central or peripheral level on the effect of gabapentin, the mice were submitted to the PSL procedure and, on the 14^th day after, they were treated with AM281 by i.t. (2 μg/5 μl) or i.pl. (10 μg/20 μl) and 15 min later they were given oral gabapentin (30 mg/kg). After 1 h of this last treatment, the animals were evaluated for mechanical hyperalgesia. These doses of antagonists were selected from the study by Martins et al. 2013MARTINS DF, MAZZARDO-MARTINS L, CIDRAL-FILHO FJ, GADOTTI VM & SANTOS AR. 2013. Peripheral and spinal activation of cannabinoid receptors by joint mobilization alleviates postoperative pain in mice. Neurosci 255: 110-121..

Influence of treatment by i.t. or i.pl. with CB₂ receptor antagonists on the antineuropathic effect of gabapentin

To evaluate the contribution of CB₂ receptors at the central or peripheral level on the effect of gabapentin, the mice were submitted to the PSL procedure and after the 14^th day, they were treated by i.t. (5 µL) or i.pl. (20 µL) with AM630 and 15 min later they received oral gabapentin (30 mg/kg). After 1 h of this last treatment, the animals were evaluated for mechanical hyperalgesia. These doses of antagonists were selected from the study by Martins et al. 2013MARTINS DF, MAZZARDO-MARTINS L, CIDRAL-FILHO FJ, GADOTTI VM & SANTOS AR. 2013. Peripheral and spinal activation of cannabinoid receptors by joint mobilization alleviates postoperative pain in mice. Neurosci 255: 110-121..

Response to von Frey filament-induced hind paw removal

For the evaluation of mechanical hyperalgesia, the mice were individually placed in transparent acrylic boxes (9 X 7 X 11 cm) on a wire mesh screen, elevated 30 cm from the stand, to allow access to the ventral surface of the right hind paw. The hyperalgesic response was recorded as the frequency of paw removal for 10 applications of the von Frey 10 filament. Data were presented as a percentage of each animal’s response to 10 stimulus applications. A significant increase in the number of this response in the animals with PSL in relation to the animals of the sham group, in the different time periods mentioned previously, was interpreted as a response of mechanical hyperalgesia.

Statistical analysis

Results are expressed as media ± standard mean (S.M.) and a p< 0.05 value was considered statistically significant. The comparison between and within groups were assessed using one-way or two-way ANOVA, when appropriated, followed by Bonferroni’s test. The GraphPad InStat® software was used for data analysis.

RESULTS

Contribution of peripheral and spinal CB₁ receptors to the antihyperalgesic effect of gabapentin

In the present study we reproduced data from previous registers of our laboratory (Martins et al. 2015aMARTINS DF, PRADO MRB, DARUGE-NETO E, BATISTI AP, EMER AA, MAZZARDO-MARTINS L, SANTOS ARS & PIOVEZAN AP. 2015a. Caffeine prevents antihyperalgesic effect of gabapentin in an animal model of CRPS-I: evidence for the involvement of spinal adenosine A1 receptor. J Peripher Nerv Syst 20: 403-409.) demonstrating the efficacy of the PSL model to cause a state-dependent effect, since operated animals presented higher frequency of response to mechanical stimulus when compared to sham animals (Figure 1).

Figure 1
Efficacy of the PSL model to cause a neurophatic pain state. Hyperalgesia to mechanical stimulus was assessed in non-operated (sham) animals or in animals submitted to the PSL induction on days 7 and 14 after procedure. Data are expressed as the mean ± standard error of the mean (S.M.), n= 8 animals. (*) represents the comparison with the sham group. One-way ANOVA followed by Bonferroni, p< 0.05.

The results presented in Figure 2a demonstrate that CB₁ peripheral receptors are important for the antihyperalgesic activity of gabapentin, since the treatment by i.pl. with the antagonist of these receptors, AM281 (10 μg/20 μl, 15 min before) partially reversed this effect of the drug on the mechanical hyperalgesia promoted by PSL. Although this effect was not observed on the 7^th day after the nerve injury procedure, when this route of administration was used, AM281, which have no isolated effect (92.5 ± 3.7% response) on hyperalgesia due to PSL (85.0 ± 5.0% response), it reversed the antihyperalgesic effect for gabapentin (75.0 ± 11.8% response) on the 14^th day after this procedure (47.5 ± 10.6% response). Important to note still that, at the dose of 30 mg/kg, gabapentin did not influence animals’ locomotor activity in the Rota Rod test, demonstrating the specificity of its antyhiperalgesic action (Martins et al. 2015aMARTINS DF, PRADO MRB, DARUGE-NETO E, BATISTI AP, EMER AA, MAZZARDO-MARTINS L, SANTOS ARS & PIOVEZAN AP. 2015a. Caffeine prevents antihyperalgesic effect of gabapentin in an animal model of CRPS-I: evidence for the involvement of spinal adenosine A1 receptor. J Peripher Nerv Syst 20: 403-409.).

Figure 2
Influence of the CB₁ antagonist, via i.pl. (panel A) or i.t. (panel B), on the antihyperalgesic effect of gabapentin on the 7^th day and on the 14^th day after nerve injury induction in the PSL model in mice. Data are expressed as the mean ± standard error of the mean (SEM), n= 8 animals. (*) represents the comparison with the saline-saline group; (#) denotes the comparison with the salt-gabapentin group. Two-way ANOVA followed by Bonferroni, p< 0.05.

Detailed information from the statistical analyses of these data are following described. From 7^th day: for pre-treatment factor F= 35.58/ DF= 1/ p= < 0.0001; for treatment factor F= 0.02905/ DF= 1/ p= 0.8659 and for interaction F= 0.2614/ DF= 1/ p= 0.6132. From 14^th day: for pre-treatment factor F= 9.358/ DF= 1/ p= 0.0051; for treatment factor F= 10.09/ DF= 1/ p= 0.0038 and for interaction F= 3.810/ DF= 1/ p= 0.0618.

Unlike what happened with the i.pl. treatment, the results presented in Figure 2b show that CB₁ spinal receptors have already contributed to the antihyperalgesic activity of gabapentin since the first observation period of this study. The i.t. treatment with the antagonist of these receptors, AM281 (2 μg/5 μl, 15 min before) partially reversed the antihyperalgesic effect of gabapentin on the mechanical hyperalgesia promoted by PSL on the 7th day after PSL (saline-gabapentin: 35.0 ± 8.2% response; AM281-gabapentin: 70.0 ± 5.3% response), and this participation continued to be observed on the 14^th day after this procedure (saline-gabapentin: 47.5 ± 10.6% response; AM281-gabapentin: 82.5 ± 5.9% response). Once more, when administered under the same conditions by this route, the antagonist did not have an effect on PSL hyperalgesia alone nor on the 7^th, nor on the 14^th day after the nerve injury. Detailed information from the statistical analyses of these data are following described. From 7^th day: for pre-treatment factor F= 16.77/ DF= 1/ p= 0.0003; for treatment factor F= 4.990/ DF= 1/ p= 0.0337 and for interaction F= 8.871/ DF= 1/ p= 0.0059. From 14^th day: for pre-treatment factor F= 10.98/ DF= 1/ p= 0.0026; for treatment factor F= 9.449/ DF= 1/ p= 0.0072 and for interaction F= 2.842/ DF= 1/ p= 0.1033.

Contribution of peripheral and spinal CB₂ receptors to the antihyperalgesic effect of gabapentin

Results similar to that observed for CB₁ receptors were observed for CB₂ receptors assessed peripherally. The data presented in Figure 3a show that the i.pl. treatment with the antagonist of these receptors, AM630 (4 μg/20 μl, 15 min before), only on the 14^th day after the PSL partially reversed this effect of gabapentin (67.5 ± 5.3% response) on the mechanical hyperalgesia promoted by the procedure (40.0 ± 5.3% response). Furthermore, AM630 also had no effect in isolation (95.0 ± 3.3% response) on hyperalgesia due to PSL (88.7 ± 4.4% response). Detailed information from the statistical analyses of these data are following described. From 7^th day: for pre-treatment factor F= 26.20/ DF= 1/ p< 0.0001; for treatment factor F= 0.3772/ DF= 1/ p= 0.5440 and for interaction F= 0.3772/ DF= 1/ p= 0.5440. From 14^th day: for pre-treatment factor F= 67.30/ DF= 1/ p= <0.0001; for treatment factor F= 13.19/ DF= 1/ p= 0.0011 and for interaction F= 5.227/ DF= 1/ p= 0.0300.

Figure 3
Influence of the CB₂ antagonist, via i.pl. (panel A) or i.t. (panel B), on the antihyperalgesic effect of gabapentin on the 7^th day and on the 14^th day after nerve injury induction in the PSL model in mice. Data are expressed as the mean ± standard error of the mean (SEM), n= 8 animals. (*) represents the comparison with the saline-saline group; (#) denotes the comparison with the salt-gabapentin group. Two-way ANOVA followed by Bonferroni, p< 0.05.

Unlike what happened with the peripheral pathway treatment, the results presented in Figure 3b demonstrate that the spinal CB₂ receptors have not contributed to the antihyperalgesic activity of gabapentin in any of the observation periods evaluated in this study. The i.t. treatment with the antagonist of these receptors, AM630 (2 μg/5 μl, 15 min before), did not reverse the antihyperalgesic effect of gabapentin on the mechanical hyperalgesia promoted by PSL on the 7^th day after PSL (saline-gabapentin: 35.0 ± 8.2% response; AM281-gabapentin: 45.7 ± 7.2% response), and this absence of influence was also observed on the 14^th day after this procedure (saline-gabapentin: 47.5 ± 10.6% response; AM281-gabapentin: 82.5 ± 5.9% response). Here again, when administered under the same conditions by this route, the antagonist has not had an effect either alone on hyperalgesia resulting from PSL nor on the 7^th day, nor on the 14^th day after the nerve injury. Detailed information from the statistical analyses of these data are following described. From 7^th day: for pre-treatment factor F= 30.71/ DF= 1/ p< 0.0001; for treatment factor F= 0.1595/ DF= 1/ p= 0.6927 and for interaction F= 1.206/ DF= 1/ p= 0.2817. From 14^th day: for pre-treatment factor F= 50.11/ DF= 1/ p= <0.0001; for treatment factor F= 0.04682/ DF= 1/ p= 0.8304 and for interaction F= 1.308/ DF= 1/ p= 0.2631.

DISCUSSION

A large number of preclinical studies have demonstrated the beneficial role of gabapentin in different models of neuropathic pain. These studies demonstrate the action of gabapentin on the reduction of pain behaviors in several models, via i.p. or i.t (Kukkar et al. 2013KUKKAR A, BALI A, SINGH N & JAGGI AS. 2013. Implications and mechanism of action of gabapentin in neuropathic pain. Arch Pharm Res 36: 237-351.). In this same sense, a previous study carried out in our laboratory demonstrated the antineuropathic activity of gabapentin, at a dose of 30 mg/kg orally, in the model of partial sciatic ligation (PSL); moreover, the participation of the adenosinergic system for this action of gabapentin (Martins et al. 2015aMARTINS DF, PRADO MRB, DARUGE-NETO E, BATISTI AP, EMER AA, MAZZARDO-MARTINS L, SANTOS ARS & PIOVEZAN AP. 2015a. Caffeine prevents antihyperalgesic effect of gabapentin in an animal model of CRPS-I: evidence for the involvement of spinal adenosine A1 receptor. J Peripher Nerv Syst 20: 403-409.) was recorded. The present study expands these findings by noting that the endocannabinoid system also contributes to this action of gabapentin in the same model, both at the central (spinal, i.t.) and peripheral (i.pl) levels.

In the present study, the CB₁ receptor antagonist (AM281) when administered i.pl or i.t. partially reversed the effect promoted by gabapentin on mechanical hyperalgesia at days 7 and 14 after PSL. This data shows that antagonising CB₁ receptors can reverse the loss of hypersensitivity induced by gabapentin, from what we could suggest that this subtype of receptors contribute to the anihyperalgesic activity of the gabapentinoid; this point, however, only could be clarified by the use of a convincing method to demonstrate an interaction between the drugs, such as an isobologram analysis using different drug gradients.

Besides this is a limitation of the present study, suggestions on the contribution of this receptor in the medullary and peripheral level for a specific antihyperalgesic effect are found in other studies in literature, strengthening this idea. Recently, evaluating the antineuropathic effect of spinal electrical stimulation in rats following PSL-induced neuropathy, Sun et al. (2017)SUN L, TAI L, QIU Q, MITCHELL R, FLEETWOOD-WALKER S, JOOSTEN EA & CHEUNG CW. 2017. Endocannabinoid activation of CB1 receptors contributes to long-lasting reversal of neuropathic pain by repetitive spinal cord stimulation. Eur J Pain 21: 804-814. demonstrated that the antihyperalgesic effect (mechanical hyperalgesia) induced by therapeutic approach is amplified by the administration of the endocannabinoid receptor inhibitor, LY2183240, and the systemic administration of the CB₁ antagonist, AM251, reverses this amplification. In the publication of Hama et al. (2014)HAMA AT, PEARSON JP & SAGEN J. 2014. Effects of repeated dosing with mechanistically distinct antinociceptive ligands in a rat model of neuropathic spinal cord injury pain. Pharmacol Res Perspect 2(2): e00034., the model of neuropathy induced by spinal cord injury in rats was used to evaluate the possible acute or chronic effect of different classes of drugs on mechanical hyperalgesia. The authors reported that a previous systemic treatment of animals with a specific CB₁ receptor antagonist, rimonabant, blocked the antinociceptive effect of CP 55,940, an analog of the non- selective endocannabinoid receptor agonist. Similar effects were also observed after central or systemic administration of the CB₁ or CB₂ receptor antagonists (Yang et al. 2016YANG F ET AL. 2016. Activation of cannabinoid CB1 receptor contributes to suppression of spinal nociceptive transmission and inhibition of mechanical hypersensitivity by Aβ-fiber stimulation. Pain 157: 2582-2593., Munawar et al. 2017MUNAWAR N, ORIOWO MA & MASOCHA W. 2017. Antihyperalgesic activities of endocannabinoids in a mouse model of antiretroviral-induced neuropathic pain. Front Pharmacol 8: 136.). Another approach to investigate contribution of CB₁ or CB₂ receptors in the peripheral antinociceptive action of ANA and 2-AG was the use of knock out animals. Knocking out for one or both receptors affected the antihyperalgesic effect of peripheral administration of ANA, 2-AG, URB597 and URB602 (Desroches et al. 2014DESROCHES J, CHARRON S, BOUCHARD JF & BEAULIEU P. 2014. Endocannabinoids decrease neuropathic pain-related behavior in mice through the activation of one or both peripheral CB1 and CB2 receptors. Neuropharmacology 77: 441-452.).

Still reinforcing the data of the present study for the CB₂ receptor antagonist, Martins et al. (2015b)MARTINS DF, BRITO RN, STRAMOSK J, BATISTI AP, MADEIRA F, TURNES BL, MAZZARDO- MARTINS L, SANTOS AR & PIOVEZAN AP. 2015b. Peripheral neurobiologic mechanisms of antiallodynic effect of warm water immersion therapy on persistent inflammatory pain. J Neurosci Res 93: 157-166. shows that the antihyperalgesic effect (mechanical hyperalgesia) promoted by immersion of the paw of mice in heated water in the model of pain induced by i.pl. of CFA (Complete Freund’s Adjuvant) was antagonized by i.pl. of AM630, a CB₂ receptor antagonist. On the other hand, despite this peripheral action, CB₂ spinal receptors did not influenced the reversion of mechanical hyperalgesia promoted by gabapentin in the present study. In contrast to the present results, however, Fu & Taylor (2015)FU W & TAYLOR BK. 2015. Activation of cannabinoid CB2 receptors reduces hyperalgesia in an experimental autoimmune encephalomyelitis mouse model of multiple sclerosis. Neurosci Lett 595: 1-6. reported that i.t. administration of JWH-133, a specific CB₂ receptor agonist, dose-dependently reduced mechanical and thermal hyperalgesia observed in an experimental model of autoimmune encephalomyelitis, this effect being reversed by the same CB₂ receptor antagonist employed in the present study at similar doses and also via i.t., AM630.

Our results regarding that CB₁ antagonist reverted the loss of hypersensitivity induced by gabapentin at the central level are consistent with findings that show the expression of these receptors physiologically at the central (dorsal horn and dorsal root ganglion) and peripheral (Fu & Taylor 2015FU W & TAYLOR BK. 2015. Activation of cannabinoid CB2 receptors reduces hyperalgesia in an experimental autoimmune encephalomyelitis mouse model of multiple sclerosis. Neurosci Lett 595: 1-6.) levels, which may have their expression increased after nerve injury (Maldonado et al. 2016MALDONADO R, BANOS JE & CABANERO D. 2016. The endocannabinoid system and neuropathic pain. Pain 157: S23-32.). On the other hand, the fact that this same effect for the CB₂ antagonist has been observed peripherally can be explained since in the periphery, besides being present in nerve endings this receptor also occurs in immune cells and in keratinocytes, from which they may reduce the release of nociceptive agents (Maldonado et al. 2016MALDONADO R, BANOS JE & CABANERO D. 2016. The endocannabinoid system and neuropathic pain. Pain 157: S23-32.). Furthermore, since receptor expression is a time dependent process, this could explain why in our study the AM630 antagonist had effect only on the 14^th day after the PSL. Despite this, other authors have suggested the participation of this receptor in the spinal cord and dorsal root ganglion levels in the antihyperalgesic action after sciatic nerve injury (Hsieh et al. 2011HSIEH GC ET AL. 2011. Central and peripheral sites of action for CB2 receptor mediated analgesic activity in chronic inflammatory and neuropathic pain models in rats. Br J Pharmacol 162: 428-440.). Such differences may be justified by factors such as 1) the sensory modality evaluated, which means that different results could be acquired for thermal hyperalgesia, for example, 2) the level of endocannabinoid produced by the injury, 3) the species and genus of animals used in the studies, among others.

Regarding the mechanisms for the reversion of the antihyperalgesic effect induced by gabapentin observed in the present study for the CB₁ antagonist at the spinal level, it could involve a potentiating effect of inhibition of the nociceptive ascending pathway or in retrograde inhibitory modulation of GLU release with consequent depression of presynaptic activity (Alger et al. 2012ALGER BE. 2012. Endocannabinoids at the synapse a decade after the dies mirabilis (29 March 2001): what we still do not know. J Physiol 590: 2203-2212.). From this on, it can be hypothesized that the contribution of EC, acting on CB₁ receptors in the dorsal horn of the spinal cord, to the action of gabapentin in the PSL model (mechanical stimulus), could result from a potentiation of the latter’s action to inhibit the nociceptive stimulus ascension through the ascending nociceptive pathway by activating the pain inhibitory descending pathway.

In addition, regarding the effect found in the present study for i.pl. of the CB₂ antagonist, one could think of a summation effect between the central action of gabapentin with the action of endocannabinoid on neuronal cells (CB₁, as discussed above) and immune ones at the periphery. This is because it is known that CB₂ receptors located in immune cells and keratinocytes reduce the release of pronociceptive agents or even increase the release of antinociceptive agents (opioids), according to a recent review by Maldonado et al. (2016)MALDONADO R, BANOS JE & CABANERO D. 2016. The endocannabinoid system and neuropathic pain. Pain 157: S23-32..

In conclusion, the present study demonstrated the participation of the endocannabinoid system in the effect of gabapentin reducing mechanical hyperalgesic in the model of partial sciatic nerve ligation in mice, through participation of CB₁ and CB₂ receptors. These results suggest that agonists of these receptors could be better investigated as potential target in the adjuvant treatment of neuropathic pain in humans.

ACKNOWLEGMENTS

This work was supported by grants from FAPESC/Brazil (Fundação de Amparo à Pesquisa e Inovação do Estado de Santa Catarina), Call 09/2015). DCS was scholarship FAPESC/Brazil and ACH was financed by the Coordenação de Aperfeiçoamento de Pessoal de Nível Superior - Brazil (CAPES) - Finance Code 001.

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DOGRUL A, SEYREK M, YALCIN B & ULUGOL A. 2012. Involvement of descending serotonergic and noradrenergic pathways in CB1 receptor-mediated antinociception. Prog Neuropsychopharmacol Biol Psychiatry 38: 97-105.
FU W & TAYLOR BK. 2015. Activation of cannabinoid CB2 receptors reduces hyperalgesia in an experimental autoimmune encephalomyelitis mouse model of multiple sclerosis. Neurosci Lett 595: 1-6.
HAMA AT, PEARSON JP & SAGEN J. 2014. Effects of repeated dosing with mechanistically distinct antinociceptive ligands in a rat model of neuropathic spinal cord injury pain. Pharmacol Res Perspect 2(2): e00034.
HSIEH GC ET AL. 2011. Central and peripheral sites of action for CB2 receptor mediated analgesic activity in chronic inflammatory and neuropathic pain models in rats. Br J Pharmacol 162: 428-440.
KUKKAR A, BALI A, SINGH N & JAGGI AS. 2013. Implications and mechanism of action of gabapentin in neuropathic pain. Arch Pharm Res 36: 237-351.
LILE JA, WESLEY MJ, KELLY TH & HAYS LR. 2016. Separate and combined effects of gabapentin and Δ9-THC in humans discriminating Δ9-THC. Behav Pharmacol 27: 215-224.
LOZOVAYA N, MIN R, TSINTSADZE V & BURNASHEV N. 2009. Dual modulation of CNS voltage-gated calcium channels by cannabinoids: Focus on CB1 receptor-independent effects. Cell Calcium 46: 154-162.
MALDONADO R, BANOS JE & CABANERO D. 2016. The endocannabinoid system and neuropathic pain. Pain 157: S23-32.
MARTINS DF, MAZZARDO-MARTINS L, CIDRAL-FILHO FJ, GADOTTI VM & SANTOS AR. 2013. Peripheral and spinal activation of cannabinoid receptors by joint mobilization alleviates postoperative pain in mice. Neurosci 255: 110-121.
MARTINS DF, PRADO MRB, DARUGE-NETO E, BATISTI AP, EMER AA, MAZZARDO-MARTINS L, SANTOS ARS & PIOVEZAN AP. 2015a. Caffeine prevents antihyperalgesic effect of gabapentin in an animal model of CRPS-I: evidence for the involvement of spinal adenosine A1 receptor. J Peripher Nerv Syst 20: 403-409.
MARTINS DF, BRITO RN, STRAMOSK J, BATISTI AP, MADEIRA F, TURNES BL, MAZZARDO- MARTINS L, SANTOS AR & PIOVEZAN AP. 2015b. Peripheral neurobiologic mechanisms of antiallodynic effect of warm water immersion therapy on persistent inflammatory pain. J Neurosci Res 93: 157-166.
MOULIN D ET AL. 2014. Pharmacological management of chronic neuropathic pain: revised consensus statement from the Canadian Pain Society. Pain Res Manag 19: 328-335.
MUNAWAR N, ORIOWO MA & MASOCHA W. 2017. Antihyperalgesic activities of endocannabinoids in a mouse model of antiretroviral-induced neuropathic pain. Front Pharmacol 8: 136.
MUNRO G, JANSEN-OLESEN I & OLESEN J. 2017. Animal models of pain and migraine in drug discovery. Drug Discov Today 22: 1103-1111.
SUN L, TAI L, QIU Q, MITCHELL R, FLEETWOOD-WALKER S, JOOSTEN EA & CHEUNG CW. 2017. Endocannabinoid activation of CB1 receptors contributes to long-lasting reversal of neuropathic pain by repetitive spinal cord stimulation. Eur J Pain 21: 804-814.
YANG F ET AL. 2016. Activation of cannabinoid CB1 receptor contributes to suppression of spinal nociceptive transmission and inhibition of mechanical hypersensitivity by Aβ-fiber stimulation. Pain 157: 2582-2593.

Publication Dates

Publication in this collection
14 Dec 2020
Date of issue
2020

History

Received
25 Sept 2019
Accepted
20 Aug 2020

This is an open-access article distributed under the terms of the Creative Commons Attribution License

[1] ALGER BE. 2012. Endocannabinoids at the synapse a decade after the dies mirabilis (29 March 2001): what we still do not know. J Physiol 590: 2203-2212.

[2] BANNISTER K, QU C, NAVRATILOVA E, OYARZO J, XIE JY, KING T, DICKENSON AH & PORRECA F. 2017. Multiple sites and actions of gabapentin-induced relief of ongoing experimental neuropathic pain. Pain 158: 2386-2395.

[3] BURSTON JJ & WOODHAMS SG. 2014. Endocannabinoid system and pain: an introduction. Proc Nutr Soc 73: 106-117.

[4] COLLOCA L ET AL. 2017. Neuropathic pain. Nat Rev Dis Primers 3: 17002.

[5] DESROCHES J, CHARRON S, BOUCHARD JF & BEAULIEU P. 2014. Endocannabinoids decrease neuropathic pain-related behavior in mice through the activation of one or both peripheral CB1 and CB2 receptors. Neuropharmacology 77: 441-452.

[6] DOGRUL A, SEYREK M, YALCIN B & ULUGOL A. 2012. Involvement of descending serotonergic and noradrenergic pathways in CB1 receptor-mediated antinociception. Prog Neuropsychopharmacol Biol Psychiatry 38: 97-105.

[7] FU W & TAYLOR BK. 2015. Activation of cannabinoid CB2 receptors reduces hyperalgesia in an experimental autoimmune encephalomyelitis mouse model of multiple sclerosis. Neurosci Lett 595: 1-6.

[8] HAMA AT, PEARSON JP & SAGEN J. 2014. Effects of repeated dosing with mechanistically distinct antinociceptive ligands in a rat model of neuropathic spinal cord injury pain. Pharmacol Res Perspect 2(2): e00034.

[9] HSIEH GC ET AL. 2011. Central and peripheral sites of action for CB2 receptor mediated analgesic activity in chronic inflammatory and neuropathic pain models in rats. Br J Pharmacol 162: 428-440.

[10] KUKKAR A, BALI A, SINGH N & JAGGI AS. 2013. Implications and mechanism of action of gabapentin in neuropathic pain. Arch Pharm Res 36: 237-351.

[11] LILE JA, WESLEY MJ, KELLY TH & HAYS LR. 2016. Separate and combined effects of gabapentin and Δ9-THC in humans discriminating Δ9-THC. Behav Pharmacol 27: 215-224.

[12] LOZOVAYA N, MIN R, TSINTSADZE V & BURNASHEV N. 2009. Dual modulation of CNS voltage-gated calcium channels by cannabinoids: Focus on CB1 receptor-independent effects. Cell Calcium 46: 154-162.

[13] MALDONADO R, BANOS JE & CABANERO D. 2016. The endocannabinoid system and neuropathic pain. Pain 157: S23-32.

[14] MARTINS DF, MAZZARDO-MARTINS L, CIDRAL-FILHO FJ, GADOTTI VM & SANTOS AR. 2013. Peripheral and spinal activation of cannabinoid receptors by joint mobilization alleviates postoperative pain in mice. Neurosci 255: 110-121.

[15] MARTINS DF, PRADO MRB, DARUGE-NETO E, BATISTI AP, EMER AA, MAZZARDO-MARTINS L, SANTOS ARS & PIOVEZAN AP. 2015a. Caffeine prevents antihyperalgesic effect of gabapentin in an animal model of CRPS-I: evidence for the involvement of spinal adenosine A1 receptor. J Peripher Nerv Syst 20: 403-409.

[16] MARTINS DF, BRITO RN, STRAMOSK J, BATISTI AP, MADEIRA F, TURNES BL, MAZZARDO- MARTINS L, SANTOS AR & PIOVEZAN AP. 2015b. Peripheral neurobiologic mechanisms of antiallodynic effect of warm water immersion therapy on persistent inflammatory pain. J Neurosci Res 93: 157-166.

[17] MOULIN D ET AL. 2014. Pharmacological management of chronic neuropathic pain: revised consensus statement from the Canadian Pain Society. Pain Res Manag 19: 328-335.

[18] MUNAWAR N, ORIOWO MA & MASOCHA W. 2017. Antihyperalgesic activities of endocannabinoids in a mouse model of antiretroviral-induced neuropathic pain. Front Pharmacol 8: 136.

[19] MUNRO G, JANSEN-OLESEN I & OLESEN J. 2017. Animal models of pain and migraine in drug discovery. Drug Discov Today 22: 1103-1111.

[20] SUN L, TAI L, QIU Q, MITCHELL R, FLEETWOOD-WALKER S, JOOSTEN EA & CHEUNG CW. 2017. Endocannabinoid activation of CB1 receptors contributes to long-lasting reversal of neuropathic pain by repetitive spinal cord stimulation. Eur J Pain 21: 804-814.

[21] YANG F ET AL. 2016. Activation of cannabinoid CB1 receptor contributes to suppression of spinal nociceptive transmission and inhibition of mechanical hypersensitivity by Aβ-fiber stimulation. Pain 157: 2582-2593.

Brasil

Brasil

Role of the endocannabinoid system on the antihyperalgesic action of gabapentin in animal model of neuropathic pain induced by partial sciatic nerve ligation

Abstract

INTRODUCTION

MATERIALS AND METHODS

Animals

Induction of neuropathic pain

Influence of gabapentin on the hyperalgesia observed in the partial sciatic nerve ligation model (PSL)

Influence of intrathecal (I.T.) or intraplantar (I.PL.) treatment with CB₁ receptor antagonists on the antineuropathic effect of gabapentin

Influence of treatment by i.t. or i.pl. with CB₂ receptor antagonists on the antineuropathic effect of gabapentin

Response to von Frey filament-induced hind paw removal

Statistical analysis

RESULTS

Contribution of peripheral and spinal CB₁ receptors to the antihyperalgesic effect of gabapentin

Contribution of peripheral and spinal CB₂ receptors to the antihyperalgesic effect of gabapentin

DISCUSSION

ACKNOWLEGMENTS

REFERENCES

Publication Dates

History

Brasil

Brasil

Role of the endocannabinoid system on the antihyperalgesic action of gabapentin in animal model of neuropathic pain induced by partial sciatic nerve ligation

Abstract

INTRODUCTION

MATERIALS AND METHODS

Animals

Induction of neuropathic pain

Influence of gabapentin on the hyperalgesia observed in the partial sciatic nerve ligation model (PSL)

Influence of intrathecal (I.T.) or intraplantar (I.PL.) treatment with CB1 receptor antagonists on the antineuropathic effect of gabapentin

Influence of treatment by i.t. or i.pl. with CB2 receptor antagonists on the antineuropathic effect of gabapentin

Response to von Frey filament-induced hind paw removal

Statistical analysis

RESULTS

Contribution of peripheral and spinal CB1 receptors to the antihyperalgesic effect of gabapentin

Contribution of peripheral and spinal CB2 receptors to the antihyperalgesic effect of gabapentin

DISCUSSION

ACKNOWLEGMENTS

REFERENCES

Publication Dates

History

Influence of intrathecal (I.T.) or intraplantar (I.PL.) treatment with CB₁ receptor antagonists on the antineuropathic effect of gabapentin

Influence of treatment by i.t. or i.pl. with CB₂ receptor antagonists on the antineuropathic effect of gabapentin

Contribution of peripheral and spinal CB₁ receptors to the antihyperalgesic effect of gabapentin

Contribution of peripheral and spinal CB₂ receptors to the antihyperalgesic effect of gabapentin