Subarachnoid meloxicam does not inhibit the mechanical hypernociception on carrageenan test in rats

Moura, Lanucha Fidelis da Luz; Vidor, Silvana Bellini; Trindade, Anelise Bonilla; Mörschbächer, Priscilla Domingues; Oleskovicz, Nilson; Contesini, Emerson Antonio

doi:10.1016/j.bjane.2013.10.020

Abstracts

BACKGROUND AND OBJECTIVE:

Evaluate the antinociceptive effects of subarachnoid meloxicam on the mechanical hypernociception induced by carrageenan in rats.

METHODS:

Randomized controlled trial. Eighteen adult male Wistar rats underwent a cannula implantation into the subarachnoid space and were randomly divided into two groups: Group I received saline solution 5 µL, while Group II received meloxicam 30 mg. The mechanical hypernociception was induced by intraplantar injection of carrageenan and evaluated using a digital analgesy meter every 30 min during a 4-h period. The results were recorded as the Δ withdrawal threshold (in g), calculated by subtracting the measurement value after treatment from baseline.

RESULTS:

The Δ withdrawal threshold mean values were lower in the group of patients treated with meloxicam over all time points between 45 and 165 min, however, there was no statistical significance (p = 0.835) for this difference.

CONCLUSION:

Subarachnoid meloxicam at a dose of 30 µg animal^-1 did not suppress the mechanical hypernociception in a model of inflammatory pain induced by intraplantar administration of carrageenan in rats. The data suggest that other dosages should be investigated the drug effect is discarded.

NSAIDs; Carrageenan; Pain; Spinal cord

JUSTIFICATIVA E OBJETIVO:

Avaliar os efeitos antinociceptivos do meloxicam subaracnóideo sobre a hipernocicepção mecânica induzida pela carragenina em ratos.

MÉTODOS:

Estudo randômico e controlado. Dezoito ratos Wistar, machos adultos, foram submetidos à implantação de uma cânula subaracnóidea, e aleatoriamente distribuídos em dois grupos: o Grupo I (GI) recebeu 5 µL de solução salina, enquanto que ao Grupo II (GII) foram administrados 30 µg de meloxicam, ambos pela via subaracnóidea. A hipernocicepção mecânica foi induzida pela injeção intraplantar de carragenina e avaliada com o emprego de um analgesímetro digital a cada 30 minutos durante um período de 4 horas. Os resultados foram registrados como o Δ do limiar de retirada (g), calculado subtraindo-se o valor das mensurações após os tratamentos, do valor basal.

RESULTADOS:

Os valores médios do Δ do limiar de retirada foram menores no grupo tratado com meloxicam ao longo de todos os momentos de avaliação entre 45 e 165 minutos, contudo não foi demonstrada significância estatística (p = 0,835) para essa diferença.

CONCLUSÃO:

A administração subaracnóidea do meloxicam na dose de 30 µg.animal^-1 não foi capaz de suprimir a hipernocicepção mecânica em um modelo de dor inflamatória induzida pela administração intraplantar de carragenina em ratos. Os dados sugerem que outras doses sejam pesquisadas antes que o efeito do fármaco seja descartado.

AINE; Carragenina; Dor; Medula espinhal

JUSTIFICACIÓN Y OBJETIVO:

Evaluar los efectos antinociceptivos del meloxicam subaracnoideo sobre la hipernocicepción mecánica inducida por la carragenina en ratones.

MÉTODOS:

Estudio aleatorizado y controlado. Dieciocho ratones Wistar, machos adultos, fueron sometidos a la implantación de una cánula subaracnoidea y aleatoriamente distribuidos en 2 grupos: el grupo I recibió 5 µl de solución salina, mientras que al grupo II se le administró 30 µg de meloxicam, ambos por vía subaracnoidea. La hipernocicepción mecánica fue inducida mediante inyección intraplantar de carragenina y fue calculada con el uso de un analgesímetro digital cada 30 min durante un período de 4 h. Los resultados fueron registrados como el Δ del umbral de retirada (g), calculado restándose el valor de las medidas posteriormente a los tratamientos, del valor basal.

RESULTADOS:

Los valores medios del Δ del umbral de retirada fueron menores en el grupo tratado con meloxicam en todos los momentos de evaluación entre 45 y 165 min, sin embargo, no se demostró significación estadística (p = 0,835) para esa diferencia.

CONCLUSIÓN:

La administración subaracnoidea del meloxicam en la dosis de 30 µg/animal^-1 no fue capaz de suprimir la hipernocicepción mecánica en un modelo de dolor inflamatorio inducido por la administración intraplantar de carragenina en ratones. Los datos sugieren que deben investigarse otras dosis antes de descartar el efecto del fármaco.

AINE; Carragenina; Dolor; Médula espinal

Introduction

Evidence has shown that besides the known peripheral action nonsteroidal anti-inflammatory drugs (NSAIDs) have a powerful effect on experimental pain that is independent of its anti-inflammatory effects.¹1. Vinegar R, Truax JF, Selph JL, et al. Pathway to carrageenaninduced inflammation in the hind limb of the rat. Fed Proc. 1987;46:118-26. In addition to its peripheral inhibition of prostaglandin synthesis, a central action of NSAIDs has been suggested by experimental studies in which these drugs demonstrated greater potency by subarachnoid administration compared to systemic administration.²2. Malmberg AB, Yaksh TL. Antinociceptive actions of spinal nonsteroidal anti-inflammatory agents on the formalin test in the rat. J Pharmacol Exp Ther. 1992;263:136-46.^and³3. Malmberg AB, Yaksh TL. Hyperalgesia mediated by spinal glutamate or substance P receptor blocked by spinal cyclooxygenase inhibition. Science. 1992;257:1276-9. Studies have shown that both cyclooxygenase (COX) forms are constitutively expressed in the brain and spinal cord of rats,⁴4. Breder CD, Dewitt D, Kraig RP. Characterization of inducible cyclooxygenase in rat brain. J Comp Neurol. 1995;355:296-315. with COX-2 the predominant isoform in the spinal cord dorsal horn.⁵5. Burian M, Geisslinger G. COX-dependent mechanisms involved in the antinociceptive action of NSAIDs at central and peripheral sites. Pharmacol Ther. 2005;107:139-54. Spinal administration of anti-inflammatory drugs has shown to suppress the reflection of C fibers, inhibit neuronal sensitization in the spinal cord dorsal horn, and attenuate long-term inflammatory pain.²2. Malmberg AB, Yaksh TL. Antinociceptive actions of spinal nonsteroidal anti-inflammatory agents on the formalin test in the rat. J Pharmacol Exp Ther. 1992;263:136-46.^,⁶6. Beiche F, Scheuerer S, Brune K, et al. Up-regulation of cyclooxygenase-2 mRNA in the rat spinal cord following peripheral inflammation. FEBS Lett. 1996;390:165-9.^,⁷7. Bianchi M, Panerai AE. The dose-related effects of paracetamol on hyperalgesia and nociception in the rat. Br J Pharmacol. 1996;117:130-2.^,⁸8. Bustamante D, Paeile C, Willer JC, et al. Effects of intrathecal or intracerebroventricular administration of nonsteroidal antiinflammatory drugs on a C-fiber reflex in rats. J Pharmacol Exp Ther. 1997;281:1381-91.^,⁹9. Herrero JF, Parrado A, Cervero F. Central and peripheral actions of the NSAID ketoprofen on spinal cord nociceptive reflexes. Neuropharmacology. 1997;36:1425-31.^,¹⁰10. McCormack K. Non-steroidal anti-inflammatory drugs and spinal nociceptive processing. Pain. 1994;59:9-43.^and¹¹11. Willingale HL, Gardiner NJ, McLymont N, et al. Prostanoids synthesized by cyclo-oxygenase isoforms in rat spinal cord and their contribution to the development of neuronal hyperexcitability. Br J Pharmacol. 1997;122:1593-604.

Meloxicam is an analgesic and nonsteroidal anti-inflammatory drug, which belongs to the phenolic acid class and has a preference for COX-2 isoenzyme.¹²12. Leal LB, Silva MCT, Bedor DCG, et al. Desenvolvimento de teste de dissolução para o meloxicam utilizando o planejamento fatorial: estudo comparativo de produtos industrializados x produtos magistrais. Rev Bras Farm. 2008;89:160-3. Unlike many other NSAIDs, it has high oral bioavailability and a long half-life, although not free from side effects.¹³13. Turner PV, Chen HC, Taylor WM. Pharmacokinetics of meloxicam in rabbits after single and repeat oral dosing. Comp Med. 2006;56:63-7. Studies of meloxicam administered by spinal pathways are scarce¹⁴14. Pinardi G, Sierralta F, Miranda HF. Atropine reverses the antinociception of nonsteroidal anti-inflammatory drugs in the tail-flick test of mice. Pharmacol Biochem Behav. 2003;74:603-8.^,¹⁵15. Pinardi G, Prieto GC, Miranda HF. Analgesic synergism between intrathecal morphine and cyclooxygenase-2 inhibitors in mice. Pharmacol Biochem Behav. 2005;82:120-4.^,¹⁶16. Takeda K, Sawamura S, Tamai H, et al. Role for cyclooxygenase 2 in the development and maintenance of neuropathic pain and spinal glial activation. Anesthesiology. 2005;103:837-44.^and¹⁷17. Kimura S, Kontani H. Demonstration of antiallodynic effects of the cyclooxygenase-2 inhibitor meloxicam on established diabetic neuropathic pain in mice. J Pharmacol Sci. 2009;110:213-7. and do not assess its effects on acute inflammatory pain. The aim of this study was to evaluate the antinociceptive power of subarachnoid meloxicam on acute pain induced by carrageenan in rats.

Materials and methods

The experimental protocol was reviewed and approved by the Animal Experimentation Ethics Committee of the institution. Rats were individually housed under controlled temperature (21-24 °C) and light-dark cycle of 12 h, with food and water ad libitum offered for at least 14 days.

The animals were surgically prepared under anesthesia with intraperitoneal injections of ketamine and xylazine (100 and 10 mg kg^-1, respectively); then, a cannula was implanted in the subarachnoid space, according to a modification of the technique previously described in the literature.¹⁸18. Yaksh TL, Rudy T. Chronic catheterization of the spinal subarachnoid space. Physiol Behav. 1976;17:1031-6. Briefly, the animals were placed in prone position, with the fore and hind limbs fixed in abduction and the region of the head slightly elevated relative to the rest of the body. After skin antisepsis of atlantooccipital region, a vertical incision approximately 2 cm in length was made in the region midline, starting at the point between the ears and extending caudally. The subcutaneous tissue and biventer cervicis and rectus capitis dorsalis major muscles were removed by blunt dissection. With the muscular retraction, the dura and cisterna magna were seen, and after exposure of atlantooccipital membrane, an 18 G needle was used to puncture its central region, until cerebrospinal fluid is seen. A PE-10 polyethylene cannula (#BB31695-PE/1, Scientific Commodities, Lake Havasu City - AZ, USA) was then inserted through the hole and advanced caudally 8.5 cm into the subarachnoid space until it reaches the lumbar enlargement region. Measuring, cutting, and marking of cannulas with enamel paint were conducted prior to the experiment period, with this material individually packaged and sterilized with ethylene oxide. The cranial portion of the cannula was inserted through an 18 G needle, allowing its accommodation in the subcutaneous tissue, in order to emerge from the skin near the top of the head. Muscles and skin were sutured and the catheter external end was occluded with the insertion of a small fragment of dental needle (30 G × 21 mm). Finally, the outer portion of the cannula was fixed to the skin with sutures. During the period that followed the cannula implantation, the animals were kept in individual plastic boxes under the same conditions of the previous period. On the day following the cannula placement, the animals were assessed for neurological deficits. Those with neurological abnormalities were excluded from the study.

Eighteen Wistar rats, weighing 300-450 g were successfully prepared for the study and, one day after the cannula placement, they were tested for mechanical hypernociception induced by carrageenan. For this purpose, we used a digital analgesy meter (Insight Scientific Equipment Ltda, Ribeirão Preto - SP, Brazil), according to a previously described technique,¹⁹19. Vivancos GG, Verri WA Jr, Cunha TM, et al. An electronic pressure-meter nociception paw test for rats. Braz J Med Biol Res. 2004;37:401-7. in which a pressure transducer equipped with a 7 mm² polypropylene tip was applied perpendicular to the right plantar surface of the animals, with a linearly increasing pressure. The equipment recorded the force in grams (g) with a precision of 0.1 g. The animal limb stimulation was repeated until obtaining three similar measurements (the difference between the highest and the lowest value was less than 10 g). Thus, the nociceptive behavior was quantified by averaging the three values expressed in grams, which represents the paw withdrawal threshold to the mechanical stimulation at each time point. Limb withdrawal from contact with the tip or shaking and/or licking behavior at the time or immediately after stimulation (flinch) was considered positive response. Ambulation was considered an ambiguous response; therefore, when it occurred at the time of test application, the test was repeated.

About 30 min before starting the assessment, the rats were transferred to the testing place, consisting of acrylic boxes with malleable wire mesh floor, in a quiet room, allowing its acclimatization evidenced by cessation of the grooming and site exploration behavior. Throughout this period, approximately five stimulations of animal limbs were performed, in order to allow their familiarity with the stimulus applied. Subsequently, baseline values from each animal were established.

After registration of baseline values, the animals were manually restrained and the metal fragment the occluding the catheter was removed. Next, the animals were randomized into two groups. Animals in Group I (GI, n = 9) underwent subarachnoid administration of 5 µL saline solution, while animals in Group II (GII, n = 9) received meloxicam 30 µg diluted in saline to a final volume of 5 µL, by the same route. Solutions were administered with the aid of a Hamilton 10 µL microsyringe (701N, Hamilton Company, Reno - NV, USA) over a period of 30 s, after which, 10 µL sterile saline was injected to flush the catheter.

Immediately after substance administration into subarachnoid space, lambda-carrageenan (0.1 mL of 2.5% carrageenan) was injected into the intraplantar region of the right limb, following the technique previously described in the literature.²⁰20. Francischi JN, Chaves CT, Moura AC, et al. Selective inhibitors of cyclo-oxygenase-2 (COX-2) induce hypoalgesia in a rat paw model of inflammation. Br J Pharmacol. 2002;137:837-44. The carrageenan injection time was recorded as time-zero (T₀), and subsequent evaluations were performed every 30 min during the 4 h post-drug administration to obtain its temporal profile of action. All assessments were performed by an investigator who was blind to animal treatment. Because the animals were tested in the periods before and after the administration of drugs, the results were recorded as the Δ withdrawal threshold (g), calculated by subtracting the measurement value after treatments from the baseline value, and these values were compared.

Data are expressed as mean ± standard deviation. The Δ withdrawal values were compared using variance analysis with repeated measures and two factors, with GI or GII group as the fixed factor and the time (every 30 min) as the repetition factor. For analysis, an unstructured correlation matrix between time points was supposed. Analyses were performed with SAS software version 8.0 for Windows, and the level of significance was determined at p < 0.05.

Results

A mean increase of the Δ withdrawal threshold occurred over time, with statistically higher values in assessments at 210 and 240 min compared to other time points (p < 0.05). There were differences between other time points, always with a mean increase of Δ withdrawal threshold in the course of the experiment, as shown in Table 1.

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Table 1
Mean difference, standard error, and p-value of Δ withdrawal threshold (g) in rats from GI and GII at different time points of hypernociception induced by intraplantar injection of carrageenan.

The mean values of the Δ withdrawal threshold were lower in the group treated with meloxicam over all time points between 45 and 165 min, although not statistically significant (p = 0.835) for this difference ( Fig. 1). Mean differences in the Δ withdrawal threshold occurred between time points within each group (p < 0.001).

Figure 1
Mean values of Δ withdrawal threshold ± standard deviation (g) in different time points of mechanical hypernociception in rats after SA administration of saline solution (GI) or meloxicam (GII).

During antinociception evaluation, two rats, both from GI, showed clinically differentiated responses after induction of hyperalgesia. These animals presented with eye discharge, significant prostration, with vocalization at rest and reluctant to rest the limb subjected to carrageenan application, suggesting the presence of severe pain. The antinociceptive evaluation for these rats showed a high degree of difficulty compared to others, as the animals did not allow force to be exerted against the plantar surface during measurements. In these cases, the animals raised their affected limb, following the tip movement, not exerting pressure resistance. As a result, these animals showed high levels of withdrawal threshold, which were not consistent with what could be observed clinically.

Discussion

The effectiveness of conventional NSAIDs, COX-2 inhibitors, and monoclonal anti-prostaglandin E2 as anti-inflammatory agents in experimental models using carrageenan is well described in the literature.²⁰20. Francischi JN, Chaves CT, Moura AC, et al. Selective inhibitors of cyclo-oxygenase-2 (COX-2) induce hypoalgesia in a rat paw model of inflammation. Br J Pharmacol. 2002;137:837-44.^,²¹21. Zhang Y, Shaffer A, Portanova J, et al. Inhibition of cyclooxygenase-2 rapidly reverses inflammatory hyperalgesia and prostaglandin E2 production. J Pharmacol Exp Ther. 1997;283:1069-75.^and²²22. Riendeau D, Percival MD, Brideau C, et al. Etoricoxib (MK0663): preclinical profile and comparison with other agents that selectively inhibit cyclooxygenase-2. J Pharmacol Exp Ther. 2001;296:558-66. The actions were traditionally assigned to peripheral prostaglandin inhibition, which play an important role in nociceptor sensitization at the site of injury,²³23. Kelly DJ, Ahmad M, Brull SJ. Preemptive analgesia I: physiological pathways and pharmacological modalities. Can J Anaesth. 2001;48:1000-10. as carrageenan intraplantar injection induces a significant increase of COX-2 expression, as well as prostaglandin E2 production.²⁴24. Nantel F, Denis D, Gordon R, et al. Distribution and regulation of cycloocygenase-2 in carrageenan-induced inflammation. Br J Pharmacol. 1999;128:853-9. However, the relative amounts of each isoform expressed in different tissues vary and may be modulated in pathological conditions. Thus, in contrast to other organs, the rat's normal brain, as well as the spinal cord, expresses more COX-2 than COX-1,²⁵25. Martin F, Fletcher D, Chauvin M, et al. Constitutive cyclooxygenase-2 is involved in central nociceptive processes in humans. Anesthesiology. 2007;106:1013-8. and data confirm its role in the sensory processing of pain.²⁶26. Vanegas H, Schaible HG. Prostaglandins and cyclooxygenases in the spinal cord. Prog Neurobiol. 2001;64:327-63. Thus, a series of experimental evidence currently suggests that NSAIDs exert their analgesic action also by activity on the central nervous system, in addition to its well-known peripheral action.²⁵25. Martin F, Fletcher D, Chauvin M, et al. Constitutive cyclooxygenase-2 is involved in central nociceptive processes in humans. Anesthesiology. 2007;106:1013-8.

Several drugs have been administered by spinal route in an attempt to prove such a mechanism, and the lack of meloxicam consistent effects on spinal nociception induced in the experimental model used contradicts the findings of other authors who reported antinociceptive activity after spinal use of other NSAIDs.²2. Malmberg AB, Yaksh TL. Antinociceptive actions of spinal nonsteroidal anti-inflammatory agents on the formalin test in the rat. J Pharmacol Exp Ther. 1992;263:136-46.^,¹⁴14. Pinardi G, Sierralta F, Miranda HF. Atropine reverses the antinociception of nonsteroidal anti-inflammatory drugs in the tail-flick test of mice. Pharmacol Biochem Behav. 2003;74:603-8.^,¹⁵15. Pinardi G, Prieto GC, Miranda HF. Analgesic synergism between intrathecal morphine and cyclooxygenase-2 inhibitors in mice. Pharmacol Biochem Behav. 2005;82:120-4.^,²⁰20. Francischi JN, Chaves CT, Moura AC, et al. Selective inhibitors of cyclo-oxygenase-2 (COX-2) induce hypoalgesia in a rat paw model of inflammation. Br J Pharmacol. 2002;137:837-44.^,²⁷27. Wang BC, Hiller JM, Simon EJ, et al. Analgesia following subarachnoid sodium ibuprofen in rats. Anesthesiology. 1992;79:856.^,²⁸28. Wang BC, Li D, Hiller JM, et al. The antinociceptive effect of S-(+)-ibuprofen in rabbits: epidural versus intravenous administration. Anesth Analg. 1995;80:92-6.^,²⁹29. Parris WC, Janicki PK, Johnson B Jr, et al. Intrathecal ketorolac tromethamine produces analgesia after chronic constriction injury of sciatic nerve in rat. Can J Anesth. 1996;43: 867-70.^,³⁰30. Massue T, Dohi S, Asano T, et al. Spinal antinociceptive effect of epidural nonsteroidal antiinflammatory drugs on nitric oxide induced hyperalgesia in rats. Anesthesiology. 1999;91: 198-206.^,³¹31. Miranda HF, Pinardi G. Lack of effect of naltrexone on the spinal synergism between morphine and non steroidal antiinflammatory drugs. Pharmacol Rep. 2009;61:266-74.^and³²32. Eisenach JC, Curry R, Tong C, et al. Effects of intrathecal ketorolac on human experimental pain. Anesthesiology. 2010;112:1216-24. It is noteworthy, however, that although there are a variety of studies evaluating the antinociceptive power of COX-2 administered in the subarachnoid space, studies specifically investigating the effects of meloxicam are still scarce. These studies have found an inhibitory effect on the wind-up phenomenon in vitro,³³33. Lopeza-Garcia JA, Laird JM. Central antinociceptive effects of meloxicam on rat spinal cord in vitro. Neuroreport. 1998;9:647-51. as well as on nociception induced by capsaicin or formalin.³⁴34. Santos AR, Vedana EM, De Freitas GA. Antinociceptive effect of meloxicam, in neurogenic and inflammatory nociceptive models in mice. Inflamm Res. 1998;47:302-7. Additionally, a synergistic analgesic effect with morphine was found after its SA administration in animals with experimental visceral pain.¹⁵15. Pinardi G, Prieto GC, Miranda HF. Analgesic synergism between intrathecal morphine and cyclooxygenase-2 inhibitors in mice. Pharmacol Biochem Behav. 2005;82:120-4. In a previous study,¹⁷17. Kimura S, Kontani H. Demonstration of antiallodynic effects of the cyclooxygenase-2 inhibitor meloxicam on established diabetic neuropathic pain in mice. J Pharmacol Sci. 2009;110:213-7. a dose similar to the one used in the present study (30 µg animal^-1) was used to investigate the antiallodynic effects of SA meloxicam. The authors, however, used an experimental model of neuropathic pain in diabetic mice, differing from this study inflammatory pain model. However, the drug effects were demonstrated with the dose used, which did not occur in this study. Observing carefully the data shown in Fig. 1, one can see that the group receiving meloxicam showed mean values of Δ withdrawal threshold lower than those shown by the group receiving saline solution during all time points between 45 and 165 min.

The intraplantar carrageenan inflammation is characterized by a biphasic behavior with respect to swelling. The early phase (0-1 h) has been attributed to the release of histamine, 5-hydroxytryptamine, and bradykinin, so the effectiveness of NSAIDs in this period has been questioned. In the late phase (1-6 h), on the other hand, a high production of PGs has been verified.³⁵35. Di Rosa M, Sorrentino L. Some pharmacodynamic properties of carrageenin in the rat. Br J Pharmacol. 1970;38:214-20. However, hyperalgesia seems to develop in parallel with the increase of COX-2 spinal levels, and its peak only occurs within 4 h after carrageenan injection.³⁶36. Hilário MO, Terreri MT, Len CA. Nonsteroidal anti-inflammatory drugs: cyclooxygenase 2 inhibitors. J Pediatr. 2006;82:S206-12. Looking at Fig. 1, however, one can see that the effects of meloxicam on hyperalgesia occurred precisely in the period prior to the 4 h of assessment, with significantly higher values of Δ withdrawal threshold after 165 min of administration, which differs from such statements.

However, this response curve behavior has also been observed in studies using carrageenan model, which reported anti-hyperalgesic thermal effects with SA administration of SC58125 - a selective COX-2 inhibitor - only during the first 170 min of evaluation.³⁷37. Dirig DM, Isakson PC, Yaksh TL. Effect of COX-1 and COX-2 inhibition on induction and maintenance of carrageenanevoked thermal hyperalgesia in rats. J Pharmacol Exp Ther. 1998;285:1031-8. As thermal hyperalgesia has been shown to be similarly mediated by the action of spinal COX-2,³⁸38. Yamamoto T, Nozaki-Taguchi N. Role of spinal cyclooxygenase (COX)-2 on thermal hyperalgesia evoked by carageenan injection in the rat. Neuroreport. 1997;8:2179-82. studies that characterize the pattern of spinal COX-2 expression in carrageenan-induced inflammation, hitherto seemingly nonexistent, may help to elucidate such observations. A significant increase in the hypernociception intensity, characterized by increased Δ withdrawal threshold, especially in assessments at 210 and 240 min, was observed in both experimental groups. These findings may be explained by other authors who report that the repetition of mechanical stimulation can produce an increased sensitivity of the stimulated area.³⁹39. Le Bars D, Gozariu M, Cadden SW. Animal models of nociception. Pharmacol Rev. 2001;53:597-652. Thus, the administration of meloxicam also failed to prevent the increase of hypernociception over time.

Among the different factors that may have influenced this study outcomes, the establishment of an adequate dose has emerged as an essential need whose importance may have been decisive for the data presented here. Currently, few studies of subarachnoid meloxicam involve administration protocols distinct from that recommended in this study, such as continuous infusion techniques¹⁶16. Takeda K, Sawamura S, Tamai H, et al. Role for cyclooxygenase 2 in the development and maintenance of neuropathic pain and spinal glial activation. Anesthesiology. 2005;103:837-44. or its association with opioids.¹⁵15. Pinardi G, Prieto GC, Miranda HF. Analgesic synergism between intrathecal morphine and cyclooxygenase-2 inhibitors in mice. Pharmacol Biochem Behav. 2005;82:120-4. The need to determine a dose that shows consistent effects, or even the absence of such effects, was based on the extrapolation of results obtained in these studies and their suitability to the needs of this work. Thus, based on previous studies that showed satisfactory results using 30-µg animal^-1 of subarachnoid meloxicam on experimental neuropathic pain in diabetic animals,¹⁷17. Kimura S, Kontani H. Demonstration of antiallodynic effects of the cyclooxygenase-2 inhibitor meloxicam on established diabetic neuropathic pain in mice. J Pharmacol Sci. 2009;110:213-7. a similar dose was recommended in order to observe its effects on inflammatory hyperalgesia.

Neuropathic pain, however, is a complex syndrome involving inflammatory and immune theories yet to be understood, and whose hyperalgesia results from both neural and non-neural tissue involvement and is associated with Aβ and Ad fibers activation.⁴⁰40. Kraychete DC, Gozzani JL, Kraychete AC. Dor neuropática --aspectos neuroquímicos. Rev Bras Anestesiol. 2008;58:492-505. However, the nociceptive system complexity has shown that different sensory pathways are activated after minimal changes in the nature of a painful process,⁴¹41. Millan MJ. The induction of pain: an integrative review. Prog Neurobiol. 1999;66:1-164. leading to believe that different doses of the same drug may be required for suppression of pain of different origins. Such a possibility can be readily seen in the present study, as a dose capable of controlling neuropathic hyperalgesia did not achieve the same results as that of inflammatory origin, thus demonstrating the need for further studies with different doses of the drug.

Acknowledgments

The authors thank CNPq/CAPES for funding the research.

References

¹
Vinegar R, Truax JF, Selph JL, et al. Pathway to carrageenaninduced inflammation in the hind limb of the rat. Fed Proc. 1987;46:118-26.
²
Malmberg AB, Yaksh TL. Antinociceptive actions of spinal nonsteroidal anti-inflammatory agents on the formalin test in the rat. J Pharmacol Exp Ther. 1992;263:136-46.
³
Malmberg AB, Yaksh TL. Hyperalgesia mediated by spinal glutamate or substance P receptor blocked by spinal cyclooxygenase inhibition. Science. 1992;257:1276-9.
⁴
Breder CD, Dewitt D, Kraig RP. Characterization of inducible cyclooxygenase in rat brain. J Comp Neurol. 1995;355:296-315.
⁵
Burian M, Geisslinger G. COX-dependent mechanisms involved in the antinociceptive action of NSAIDs at central and peripheral sites. Pharmacol Ther. 2005;107:139-54.
⁶
Beiche F, Scheuerer S, Brune K, et al. Up-regulation of cyclooxygenase-2 mRNA in the rat spinal cord following peripheral inflammation. FEBS Lett. 1996;390:165-9.
⁷
Bianchi M, Panerai AE. The dose-related effects of paracetamol on hyperalgesia and nociception in the rat. Br J Pharmacol. 1996;117:130-2.
⁸
Bustamante D, Paeile C, Willer JC, et al. Effects of intrathecal or intracerebroventricular administration of nonsteroidal antiinflammatory drugs on a C-fiber reflex in rats. J Pharmacol Exp Ther. 1997;281:1381-91.
⁹
Herrero JF, Parrado A, Cervero F. Central and peripheral actions of the NSAID ketoprofen on spinal cord nociceptive reflexes. Neuropharmacology. 1997;36:1425-31.
¹⁰
McCormack K. Non-steroidal anti-inflammatory drugs and spinal nociceptive processing. Pain. 1994;59:9-43.
¹¹
Willingale HL, Gardiner NJ, McLymont N, et al. Prostanoids synthesized by cyclo-oxygenase isoforms in rat spinal cord and their contribution to the development of neuronal hyperexcitability. Br J Pharmacol. 1997;122:1593-604.
¹²
Leal LB, Silva MCT, Bedor DCG, et al. Desenvolvimento de teste de dissolução para o meloxicam utilizando o planejamento fatorial: estudo comparativo de produtos industrializados x produtos magistrais. Rev Bras Farm. 2008;89:160-3.
¹³
Turner PV, Chen HC, Taylor WM. Pharmacokinetics of meloxicam in rabbits after single and repeat oral dosing. Comp Med. 2006;56:63-7.
¹⁴
Pinardi G, Sierralta F, Miranda HF. Atropine reverses the antinociception of nonsteroidal anti-inflammatory drugs in the tail-flick test of mice. Pharmacol Biochem Behav. 2003;74:603-8.
¹⁵
Pinardi G, Prieto GC, Miranda HF. Analgesic synergism between intrathecal morphine and cyclooxygenase-2 inhibitors in mice. Pharmacol Biochem Behav. 2005;82:120-4.
¹⁶
Takeda K, Sawamura S, Tamai H, et al. Role for cyclooxygenase 2 in the development and maintenance of neuropathic pain and spinal glial activation. Anesthesiology. 2005;103:837-44.
¹⁷
Kimura S, Kontani H. Demonstration of antiallodynic effects of the cyclooxygenase-2 inhibitor meloxicam on established diabetic neuropathic pain in mice. J Pharmacol Sci. 2009;110:213-7.
¹⁸
Yaksh TL, Rudy T. Chronic catheterization of the spinal subarachnoid space. Physiol Behav. 1976;17:1031-6.
¹⁹
Vivancos GG, Verri WA Jr, Cunha TM, et al. An electronic pressure-meter nociception paw test for rats. Braz J Med Biol Res. 2004;37:401-7.
²⁰
Francischi JN, Chaves CT, Moura AC, et al. Selective inhibitors of cyclo-oxygenase-2 (COX-2) induce hypoalgesia in a rat paw model of inflammation. Br J Pharmacol. 2002;137:837-44.
²¹
Zhang Y, Shaffer A, Portanova J, et al. Inhibition of cyclooxygenase-2 rapidly reverses inflammatory hyperalgesia and prostaglandin E2 production. J Pharmacol Exp Ther. 1997;283:1069-75.
²²
Riendeau D, Percival MD, Brideau C, et al. Etoricoxib (MK0663): preclinical profile and comparison with other agents that selectively inhibit cyclooxygenase-2. J Pharmacol Exp Ther. 2001;296:558-66.
²³
Kelly DJ, Ahmad M, Brull SJ. Preemptive analgesia I: physiological pathways and pharmacological modalities. Can J Anaesth. 2001;48:1000-10.
²⁴
Nantel F, Denis D, Gordon R, et al. Distribution and regulation of cycloocygenase-2 in carrageenan-induced inflammation. Br J Pharmacol. 1999;128:853-9.
²⁵
Martin F, Fletcher D, Chauvin M, et al. Constitutive cyclooxygenase-2 is involved in central nociceptive processes in humans. Anesthesiology. 2007;106:1013-8.
²⁶
Vanegas H, Schaible HG. Prostaglandins and cyclooxygenases in the spinal cord. Prog Neurobiol. 2001;64:327-63.
²⁷
Wang BC, Hiller JM, Simon EJ, et al. Analgesia following subarachnoid sodium ibuprofen in rats. Anesthesiology. 1992;79:856.
²⁸
Wang BC, Li D, Hiller JM, et al. The antinociceptive effect of S-(+)-ibuprofen in rabbits: epidural versus intravenous administration. Anesth Analg. 1995;80:92-6.
²⁹
Parris WC, Janicki PK, Johnson B Jr, et al. Intrathecal ketorolac tromethamine produces analgesia after chronic constriction injury of sciatic nerve in rat. Can J Anesth. 1996;43: 867-70.
³⁰
Massue T, Dohi S, Asano T, et al. Spinal antinociceptive effect of epidural nonsteroidal antiinflammatory drugs on nitric oxide induced hyperalgesia in rats. Anesthesiology. 1999;91: 198-206.
³¹
Miranda HF, Pinardi G. Lack of effect of naltrexone on the spinal synergism between morphine and non steroidal antiinflammatory drugs. Pharmacol Rep. 2009;61:266-74.
³²
Eisenach JC, Curry R, Tong C, et al. Effects of intrathecal ketorolac on human experimental pain. Anesthesiology. 2010;112:1216-24.
³³
Lopeza-Garcia JA, Laird JM. Central antinociceptive effects of meloxicam on rat spinal cord in vitro. Neuroreport. 1998;9:647-51.
³⁴
Santos AR, Vedana EM, De Freitas GA. Antinociceptive effect of meloxicam, in neurogenic and inflammatory nociceptive models in mice. Inflamm Res. 1998;47:302-7.
³⁵
Di Rosa M, Sorrentino L. Some pharmacodynamic properties of carrageenin in the rat. Br J Pharmacol. 1970;38:214-20.
³⁶
Hilário MO, Terreri MT, Len CA. Nonsteroidal anti-inflammatory drugs: cyclooxygenase 2 inhibitors. J Pediatr. 2006;82:S206-12.
³⁷
Dirig DM, Isakson PC, Yaksh TL. Effect of COX-1 and COX-2 inhibition on induction and maintenance of carrageenanevoked thermal hyperalgesia in rats. J Pharmacol Exp Ther. 1998;285:1031-8.
³⁸
Yamamoto T, Nozaki-Taguchi N. Role of spinal cyclooxygenase (COX)-2 on thermal hyperalgesia evoked by carageenan injection in the rat. Neuroreport. 1997;8:2179-82.
³⁹
Le Bars D, Gozariu M, Cadden SW. Animal models of nociception. Pharmacol Rev. 2001;53:597-652.
⁴⁰
Kraychete DC, Gozzani JL, Kraychete AC. Dor neuropática --aspectos neuroquímicos. Rev Bras Anestesiol. 2008;58:492-505.
⁴¹
Millan MJ. The induction of pain: an integrative review. Prog Neurobiol. 1999;66:1-164.

☆
Work conducted at Hospital de Clínicas de Porto Alegre (HCPA), Porto Alegre, RS, Brazil.

Publication Dates

Publication in this collection
Mar-Apr 2015

History

Received
21 Aug 2013
Accepted
28 Oct 2013

This is an Open Access article distributed under the terms of the Creative Commons Attribution-Noncommercial No Derivative License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium provided the original work is properly cited and the work is not changed in any way.

[1] ¹
Vinegar R, Truax JF, Selph JL, et al. Pathway to carrageenaninduced inflammation in the hind limb of the rat. Fed Proc. 1987;46:118-26.

[2] ²
Malmberg AB, Yaksh TL. Antinociceptive actions of spinal nonsteroidal anti-inflammatory agents on the formalin test in the rat. J Pharmacol Exp Ther. 1992;263:136-46.

[3] ³
Malmberg AB, Yaksh TL. Hyperalgesia mediated by spinal glutamate or substance P receptor blocked by spinal cyclooxygenase inhibition. Science. 1992;257:1276-9.

[4] ⁴
Breder CD, Dewitt D, Kraig RP. Characterization of inducible cyclooxygenase in rat brain. J Comp Neurol. 1995;355:296-315.

[5] ⁵
Burian M, Geisslinger G. COX-dependent mechanisms involved in the antinociceptive action of NSAIDs at central and peripheral sites. Pharmacol Ther. 2005;107:139-54.

[6] ⁶
Beiche F, Scheuerer S, Brune K, et al. Up-regulation of cyclooxygenase-2 mRNA in the rat spinal cord following peripheral inflammation. FEBS Lett. 1996;390:165-9.

[7] ⁷
Bianchi M, Panerai AE. The dose-related effects of paracetamol on hyperalgesia and nociception in the rat. Br J Pharmacol. 1996;117:130-2.

[8] ⁸
Bustamante D, Paeile C, Willer JC, et al. Effects of intrathecal or intracerebroventricular administration of nonsteroidal antiinflammatory drugs on a C-fiber reflex in rats. J Pharmacol Exp Ther. 1997;281:1381-91.

[9] ⁹
Herrero JF, Parrado A, Cervero F. Central and peripheral actions of the NSAID ketoprofen on spinal cord nociceptive reflexes. Neuropharmacology. 1997;36:1425-31.

[10] ¹⁰
McCormack K. Non-steroidal anti-inflammatory drugs and spinal nociceptive processing. Pain. 1994;59:9-43.

[11] ¹¹
Willingale HL, Gardiner NJ, McLymont N, et al. Prostanoids synthesized by cyclo-oxygenase isoforms in rat spinal cord and their contribution to the development of neuronal hyperexcitability. Br J Pharmacol. 1997;122:1593-604.

[12] ¹²
Leal LB, Silva MCT, Bedor DCG, et al. Desenvolvimento de teste de dissolução para o meloxicam utilizando o planejamento fatorial: estudo comparativo de produtos industrializados x produtos magistrais. Rev Bras Farm. 2008;89:160-3.

[13] ¹³
Turner PV, Chen HC, Taylor WM. Pharmacokinetics of meloxicam in rabbits after single and repeat oral dosing. Comp Med. 2006;56:63-7.

[14] ¹⁴
Pinardi G, Sierralta F, Miranda HF. Atropine reverses the antinociception of nonsteroidal anti-inflammatory drugs in the tail-flick test of mice. Pharmacol Biochem Behav. 2003;74:603-8.

[15] ¹⁵
Pinardi G, Prieto GC, Miranda HF. Analgesic synergism between intrathecal morphine and cyclooxygenase-2 inhibitors in mice. Pharmacol Biochem Behav. 2005;82:120-4.

[16] ¹⁶
Takeda K, Sawamura S, Tamai H, et al. Role for cyclooxygenase 2 in the development and maintenance of neuropathic pain and spinal glial activation. Anesthesiology. 2005;103:837-44.

[17] ¹⁷
Kimura S, Kontani H. Demonstration of antiallodynic effects of the cyclooxygenase-2 inhibitor meloxicam on established diabetic neuropathic pain in mice. J Pharmacol Sci. 2009;110:213-7.

[18] ¹⁸
Yaksh TL, Rudy T. Chronic catheterization of the spinal subarachnoid space. Physiol Behav. 1976;17:1031-6.

[19] ¹⁹
Vivancos GG, Verri WA Jr, Cunha TM, et al. An electronic pressure-meter nociception paw test for rats. Braz J Med Biol Res. 2004;37:401-7.

[20] ²⁰
Francischi JN, Chaves CT, Moura AC, et al. Selective inhibitors of cyclo-oxygenase-2 (COX-2) induce hypoalgesia in a rat paw model of inflammation. Br J Pharmacol. 2002;137:837-44.

[21] ²¹
Zhang Y, Shaffer A, Portanova J, et al. Inhibition of cyclooxygenase-2 rapidly reverses inflammatory hyperalgesia and prostaglandin E2 production. J Pharmacol Exp Ther. 1997;283:1069-75.

[22] ²²
Riendeau D, Percival MD, Brideau C, et al. Etoricoxib (MK0663): preclinical profile and comparison with other agents that selectively inhibit cyclooxygenase-2. J Pharmacol Exp Ther. 2001;296:558-66.

[23] ²³
Kelly DJ, Ahmad M, Brull SJ. Preemptive analgesia I: physiological pathways and pharmacological modalities. Can J Anaesth. 2001;48:1000-10.

[24] ²⁴
Nantel F, Denis D, Gordon R, et al. Distribution and regulation of cycloocygenase-2 in carrageenan-induced inflammation. Br J Pharmacol. 1999;128:853-9.

[25] ²⁵
Martin F, Fletcher D, Chauvin M, et al. Constitutive cyclooxygenase-2 is involved in central nociceptive processes in humans. Anesthesiology. 2007;106:1013-8.

[26] ²⁶
Vanegas H, Schaible HG. Prostaglandins and cyclooxygenases in the spinal cord. Prog Neurobiol. 2001;64:327-63.

[27] ²⁷
Wang BC, Hiller JM, Simon EJ, et al. Analgesia following subarachnoid sodium ibuprofen in rats. Anesthesiology. 1992;79:856.

[28] ²⁸
Wang BC, Li D, Hiller JM, et al. The antinociceptive effect of S-(+)-ibuprofen in rabbits: epidural versus intravenous administration. Anesth Analg. 1995;80:92-6.

[29] ²⁹
Parris WC, Janicki PK, Johnson B Jr, et al. Intrathecal ketorolac tromethamine produces analgesia after chronic constriction injury of sciatic nerve in rat. Can J Anesth. 1996;43: 867-70.

[30] ³⁰
Massue T, Dohi S, Asano T, et al. Spinal antinociceptive effect of epidural nonsteroidal antiinflammatory drugs on nitric oxide induced hyperalgesia in rats. Anesthesiology. 1999;91: 198-206.

[31] ³¹
Miranda HF, Pinardi G. Lack of effect of naltrexone on the spinal synergism between morphine and non steroidal antiinflammatory drugs. Pharmacol Rep. 2009;61:266-74.

[32] ³²
Eisenach JC, Curry R, Tong C, et al. Effects of intrathecal ketorolac on human experimental pain. Anesthesiology. 2010;112:1216-24.

[33] ³³
Lopeza-Garcia JA, Laird JM. Central antinociceptive effects of meloxicam on rat spinal cord in vitro. Neuroreport. 1998;9:647-51.

[34] ³⁴
Santos AR, Vedana EM, De Freitas GA. Antinociceptive effect of meloxicam, in neurogenic and inflammatory nociceptive models in mice. Inflamm Res. 1998;47:302-7.

[35] ³⁵
Di Rosa M, Sorrentino L. Some pharmacodynamic properties of carrageenin in the rat. Br J Pharmacol. 1970;38:214-20.

[36] ³⁶
Hilário MO, Terreri MT, Len CA. Nonsteroidal anti-inflammatory drugs: cyclooxygenase 2 inhibitors. J Pediatr. 2006;82:S206-12.

[37] ³⁷
Dirig DM, Isakson PC, Yaksh TL. Effect of COX-1 and COX-2 inhibition on induction and maintenance of carrageenanevoked thermal hyperalgesia in rats. J Pharmacol Exp Ther. 1998;285:1031-8.

[38] ³⁸
Yamamoto T, Nozaki-Taguchi N. Role of spinal cyclooxygenase (COX)-2 on thermal hyperalgesia evoked by carageenan injection in the rat. Neuroreport. 1997;8:2179-82.

[39] ³⁹
Le Bars D, Gozariu M, Cadden SW. Animal models of nociception. Pharmacol Rev. 2001;53:597-652.

[40] ⁴⁰
Kraychete DC, Gozzani JL, Kraychete AC. Dor neuropática --aspectos neuroquímicos. Rev Bras Anestesiol. 2008;58:492-505.

[41] ⁴¹
Millan MJ. The induction of pain: an integrative review. Prog Neurobiol. 1999;66:1-164.

Time points	Estimated mean difference	Standard error	p
30–60 min	-4.13	3.38	0.914
30–90 min	-5.60	3.82	0.813
30–120 min	-7.59	2.96	0.234
30–150 min	-13.64	4.03	0.055
30–180 min	-15.30	4.24	0.036
30–210 min	-23.50	3.68	<0.001
30–240 min	-27.76	2.53	<0.001
60–90 min	-1.47	2.42	0.998
60–120 min	-3.46	2.58	0.872
60–150 min	-9.51	3.13	0.104
60–180 min	-11.16	3.67	0.104
60–210 min	-19.37	2.71	<0.001
60–240 min	-23.63	2.88	<0.001
90–120 min	-1.99	2.84	0.996
90–150 min	-8.04	2.67	0.111
90–180 min	-9.70	3.35	0.136
90–210 min	-17.90	2.71	<0.001
90–240 min	-22.16	2.99	<0.001
120–150 min	-6.06	2.41	0.254
120–180 min	-7.71	3.81	0.497
120–210 min	-15.92	2.22	<0.001
120–240 min	-20.18	2.80	<0.001
150–180 min	-1.65	3.37	1.000
150–210 min	-9.86	2.60	0.025
150–240 min	-14.12	3.02	0.004
180–210 min	-8.21	2.36	0.046
180–240 min	-12.47	3.03	0.013
210–240 min	-4.26	2.48	0.677

Brasil

Brasil

Subarachnoid meloxicam does not inhibit the mechanical hypernociception on carrageenan test in rats ^☆ ☆ Work conducted at Hospital de Clínicas de Porto Alegre (HCPA), Porto Alegre, RS, Brazil.

Abstracts

BACKGROUND AND OBJECTIVE:

METHODS:

RESULTS:

CONCLUSION:

JUSTIFICATIVA E OBJETIVO:

MÉTODOS:

RESULTADOS:

CONCLUSÃO:

JUSTIFICACIÓN Y OBJETIVO:

MÉTODOS:

RESULTADOS:

CONCLUSIÓN:

Introduction

Materials and methods

Results

Discussion

Acknowledgments

References

Publication Dates

History

Brasil

Brasil

Subarachnoid meloxicam does not inhibit the mechanical hypernociception on carrageenan test in rats ☆ ☆ Work conducted at Hospital de Clínicas de Porto Alegre (HCPA), Porto Alegre, RS, Brazil.

Abstracts

BACKGROUND AND OBJECTIVE:

METHODS:

RESULTS:

CONCLUSION:

JUSTIFICATIVA E OBJETIVO:

MÉTODOS:

RESULTADOS:

CONCLUSÃO:

JUSTIFICACIÓN Y OBJETIVO:

MÉTODOS:

RESULTADOS:

CONCLUSIÓN:

Introduction

Materials and methods

Results

Discussion

Acknowledgments

References

Publication Dates

History

Subarachnoid meloxicam does not inhibit the mechanical hypernociception on carrageenan test in rats ^☆ ☆ Work conducted at Hospital de Clínicas de Porto Alegre (HCPA), Porto Alegre, RS, Brazil.