Your search keyword '"antinociception"' showing total 67 results

1. BNT12, a novel hybrid peptide of opioid and neurotensin pharmacophores, produces potent central antinociception with limited side effects.

Author

Wang SY, Zhang YZ, Liu XH, Guo XC, Wang XF, Wang JR, Liu BJ, Han FT, Zhang Y, and Wang CL

Subjects

Animals, Male, Mice, Analgesics pharmacology, Analgesics chemistry, Analgesics administration & dosage, Analgesics, Opioid pharmacology, Analgesics, Opioid administration & dosage, Drug Tolerance, Pain drug therapy, Neurotensin analogs & derivatives, Neurotensin pharmacology, Neurotensin chemistry, Receptors, Neurotensin metabolism, Receptors, Neurotensin agonists

Abstract

The development of multitarget opioid drugs has emerged as an attractive approach for innovative pain management with reduced side effects. In the present study, a novel hybrid peptide BNT12 containing the opioid and neurotensin (NT)-like fragments was synthesized and pharmacologically characterized. In acute radiant heat paw withdrawal test, intracerebroventricular (i.c.v.) administration of BNT12 produced potent antinociception in mice. The central antinociceptive activity of BNT12 was mainly mediated by μ-, δ-opioid receptor, neurotensin receptor type 1 (NTSR1) and 2 (NTSR2), supporting a multifunctional agonism of BNT12 in the functional assays. BNT12 also exhibited significant antinociceptive effects in spared nerve injury (SNI)-neuropathic pain, complete Freund's adjuvant (CFA)-induced inflammatory pain, acetic acid-induced visceral and formalin-induced pain after i.c.v. administration. Furthermore, BNT12 exhibited substantial reduction of acute antinociceptive tolerance, shifted the dose-response curve to the right by only 1.3-fold. It is noteworthy that BNT12 showed insignificant chronic antinociceptive tolerance at the supraspinal level. In addition, BNT12 exhibited reduced or no opioid-like side effects on conditioned place preference (CPP) response, naloxone-precipitated withdrawal response, acute hyperlocomotion, motor coordination, gastrointestinal transit, and cardiovascular responses. The present investigation demonstrated that the novel hybrid peptide BNT12 might serve as a promising analgesic candidate with limited opioid-like side effects., Competing Interests: Declaration of competing interest The authors have no conflicts of interest to declare., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

2. Melatonin promotes orofacial antinociception in adult zebrafish by modulating TRP channels.

Author

Sampaio GMMS, Vieira-Neto AE, Leite GO, and Campos AR

Subjects

Animals, Zebrafish, Analgesics pharmacology, Analgesics therapeutic use, Capsaicin pharmacology, TRPV Cation Channels, Molecular Docking Simulation, TRPA1 Cation Channel, Melatonin pharmacology, TRPM Cation Channels

Abstract

Melatonin is an endogenous hormone, known as the sleep hormone, which has already demonstrated its antinociceptive effect. This study aimed to evaluate the participation of TRP's channels in the orofacial antinociceptive effect of melatonin (MT) in adult zebrafish. Initially, the open field test was performed to evaluate the effect of MT on the locomotor activity of adult zebrafish. Then, the animals were pre-treated with MT (0.1, 0.3 or 1 mg/mL; gavage) and acute orofacial nociception was induced by the application of capsaicin (TRPV1 agonist), cinnamaldehyde (TRPA1 agonist) or menthol (TRPM8 agonist) applied into the animal's lip. Naive groups were included. MT, per se, did not alter the locomotor activity of the animals. MT reduced the nociceptive behavior induced by the three agonists; however, the most significant effect was obtained with the lowest concentration tested (0.1 mg/mL) in the capsaicin test. The orofacial antinociceptive effect of melatonin was prevented by capsazepine (TRPV1 antagonist), but not by HC-030031 (TRPA1 antagonist). The molecular docking study indicated interaction between MT and the TRPV1, TRPA1 and TRPM8 channels and, in line with the in vivo results, there was greater affinity between MT and the TRPV1 channel. The results confirm the pharmacological relevance of melatonin as an inhibitor of orofacial nociception and this effect seems to be related to the modulation of TRP's channels., Competing Interests: Declaration of Competing Interest The authors declare that there is no conflict of interest., (Copyright © 2023 Elsevier Inc. All rights reserved.)

Published

2023

3. MMG22 Potently Blocks Hyperalgesia in Cisplatin-treated Mice.

Author

Cataldo G, Lunzer MM, Akgün E, Wong HL, Portoghese PS, and Simone DA

Subjects

Mice, Male, Animals, Cisplatin, Morphine pharmacology, Inflammation, Disease Models, Animal, Hyperalgesia drug therapy, Neuralgia chemically induced, Neuralgia drug therapy

Abstract

MMG22 is a bivalent ligand containing MOR agonist and mGluR5 antagonist pharmacophores connected by a 22-atom linker. Intrathecal (i.t.) administration of MMG22 to inflamed mice has been reported to produce fmol-range antinociception in the reversal of LPS-induced hyperalgesia. MMG22 reduced hyperalgesia in the spared nerve injury (SNI) model of neuropathic pain at 10 days after injury but not at 30 days after injury, perhaps related to the inflammation that occurs early after injury but subsequently subsides. The present study determined the efficacy of MMG22 in cisplatin-treated male mice in order to provide data relating to the efficacy of MMG22 in the treatment of neuropathic pain that is associated with inflammation. Groups of eight mice each received daily intraperitoneal (i.p.) injections of cisplatin for seven days to produce robust mechanical allodynia defined by the decrease in withdrawal threshold using an electronic von Frey applied to the plantar surface of the hind paw. Intrathecal administration of MMG22 potently reduced mechanical hyperalgesia (ED 50 0.04 fmol/mouse) without tolerance, whereas MMG10 was essentially inactive. Morphine was less potent than MMG22 by >5-orders of magnitude and displayed tolerance. Subcutaneous MMG22 was effective (ED 50  = 2.41 mg/kg) and devoid of chronic tolerance. We propose that MMG22 induces the formation of a MOR-mGluR5 heteromer through selective interaction with the upregulated NR2B subunit of activated NMDAR, in view of the 4600-fold reduction of i.t. MMG22 antinociception by the selective NR2B antagonist, Ro25-6981. A possible explanation for the substantially reduced potency for MMG22 in the SNI model is discussed., (Copyright © 2023 IBRO. Published by Elsevier Ltd. All rights reserved.)

Published

2023

4. Nicotine suppresses central post-stroke pain via facilitation of descending noradrenergic neuron through activation of orexinergic neuron.

Author

Nakamoto K, Matsuura W, and Tokuyama S

Subjects

Mice, Animals, Orexins pharmacology, Nicotine pharmacology, Hyperalgesia drug therapy, Hyperalgesia etiology, Orexin Receptors, Adrenergic Neurons, Neuralgia

Abstract

Central post-stroke pain (CPSP) is a type of central neuropathic pain, whose underlying mechanisms remain unknown. We previously reported that bilateral carotid artery occlusion (BCAO)-induced CPSP model mice showed mechanical hypersensitivity and decreased mRNA levels of preproorexin, an orexin precursor, in the hypothalamus. Recently, nicotine was shown to regulate the neuronal activity of orexin in the lateral hypothalamus (LH) and suppress inflammatory and neuropathic pain. In this study, we evaluated whether nicotine could suppress BCAO-induced mechanical allodynia through the activation of orexinergic neurons. Mice were subjected to BCAO for 30 min. Mechanical hypersensitivity was assessed by the von Frey test. BCAO mice showed hypersensitivity to mechanical stimuli three days after BCAO surgery. The intracerebroventricular injection of nicotine suppressed BCAO-induced mechanical hypersensitivity in a dose-dependent manner. These effects were inhibited by α7 or α4β2-nicotinic receptor antagonists. After nicotine injection, the level of c-fos, a neuronal activity marker, increased in the LH and locus coeruleus (LC) of Sham and BCAO mice. Increased number of c-Fos-positive cells partly colocalized with orexin A-positive cells in the LH, as well as tyrosine hydroxylase-positive cells in the LC. Orexinergic neurons project to the LC area. Nicotine-induced antinociception tended to cancel by the pretreatment of SB334867, an orexin receptor1 antagonist into the LC. Intra-LH microinjection of nicotine attenuated BCAO-induced mechanical hypersensitivity. Nicotine-induced antinociception was inhibited by intrathecal pre-treatment with yohimbine, an α2 adrenergic receptor antagonist. These results indicated that nicotine may suppress BCAO-induced mechanical hypersensitivity through the activation of the descending pain control system via orexin neurons., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023 Elsevier B.V. All rights reserved.)

Published

2023

5. Analgesia and pain: Dual effect of dopamine on the peripheral nociceptive system is dependent on D 2 -or D 1 -like receptor activation.

Author

Queiroz BFG, Fonseca FCS, Ferreira RCM, Romero TRL, Perez AC, and Duarte IDG

Subjects

Analgesics adverse effects, Animals, Dopamine Antagonists pharmacology, Hyperalgesia drug therapy, Male, Mice, Nociception, Pain chemically induced, Pain drug therapy, Receptors, Dopamine D1, Remoxipride adverse effects, Analgesia, Dopamine

Abstract

In this study, a pharmacological approach, together with the paw pressure test, was used to investigate the role of dopamine and its receptors in the peripheral processing of the nociceptive response in mice. Initially, the administration of dopamine (5, 20, and 80 ng/paw) in the hind paw of male Swiss mice (30-40 g) promoted antinociceptive effects in a dose-dependent manner. This was considered a peripheral effect, as it did not produce changes in the nociceptive threshold of the contralateral paw. The D 2 , D 3 , and D 4 dopamine receptor antagonists remoxipride (4 μg/paw), U99194 (16 μg/paw), and L-745,870 (16 μg/paw), respectively, reversed the dopamine-mediated antinociception in mice with PGE 2 -induced hyperalgesia. The D 1 and D 5 dopamine receptor antagonists SKF 83566 (2 μg/paw) and SCH 23390 (1.6 μg/paw), respectively, did not alter dopamine antinociception. In contrast, dopamine at higher doses (0.1, 1, and 10 μg/paw) caused hyperalgesia in the animals, and the D 1 and D 5 receptor antagonists reversed this pronociceptive effect (10 μg/paw), whereas the D 2 receptor antagonist remoxipride did not. Our data suggest that dopamine has a dual effect that depends on the dose, as it causes peripheral antinociceptive effects at small doses via the activation of D 2 -like receptors and nociceptive effects at higher doses via the activation of D 1 -like receptors., (Copyright © 2022 Elsevier B.V. All rights reserved.)

Published

2022

6. Bradykinin induces peripheral antinociception in PGE 2 -induced hyperalgesia in mice.

Author

Ferreira RCM, de Sousa Fonseca FC, de Almeida DL, Freitas ACN, Peigneur S, Romero TRL, Amaral FA, and Duarte IDG

Subjects

Analgesics pharmacology, Analgesics therapeutic use, Animals, Dinoprostone, Male, Mice, Mice, Inbred C57BL, Receptors, Bradykinin, Bradykinin pharmacology, Hyperalgesia chemically induced, Hyperalgesia drug therapy

Abstract

Background: Bradykinin (BK) is an endogenous peptide involved in vascular permeability and inflammation. It has opposite effects (inducing hyperalgesia or antinociception) when administered directly in the central nervous system. The aim of this study was to evaluate whether BK may also present this dual effect when injected peripherally in a PGE 2 -induced nociceptive pain model, as well as to investigate the possible mechanisms of action involved in this event in mice., Methods: Male Swiss and C57BL/6 knockout mice for B 1 or B 2 bradykinin receptors were submitted to a mechanical paw pressure test and hyperalgesia was induced by intraplantar prostaglandin E 2 (2 µg/paw) injection., Results: Bradykinin (20, 40 and 80 ng/paw) produced dose-dependent peripheral antinociception against PGE 2 -induced hyperalgesia. This effect was antagonized by bradyzide (8, 16 and 32 μg/paw), naloxone (12.5, 25 and 50 μg/paw), nor-binaltorphimine (50, 100 and 200 μg/paw) and AM251 (20, 40 and 80 μg/paw). Bestatin (400 µg/paw), MAFP (0.5 µg/paw) and VDM11 (2.5 µg/paw) potentiated the antinociception of a lower 20 ng BK dose. The knockout of B 1 or B 2 bradykinin receptors partially abolished the antinociceptive action of BK (80 ng/paw), bremazocine (1 μg/paw) and anandamide (40 ng/paw) when compared with wild-type animals, which show complete antinociception with the same dose of each drug., Conclusion: The present study is the first to demonstrate BK-induced antinociception in peripheral tissues against PGE 2 -induced nociception in mice and the involvement of κ-opioid and CB 1 cannabinoid receptors in this effect., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published

2022

7. Nitric oxide modulates tapentadol antinociceptive tolerance and physical dependence.

Author

Wolińska R, Kleczkowska P, de Cordé-Skurska A, Poznański P, Sacharczuk M, Mika J, and Bujalska-Zadrożny M

Abstract

Tapentadol, an analgesic with a dual mechanism of action, involving both μ-opioid receptor agonism and noradrenaline reuptake inhibition (MOP-NRI), was designed for the treatment of moderate to severe pain. However, the widely acknowledged risk of analgesic tolerance and development of physical dependence following sustained opioid use may hinder their effectiveness. One of the possible mechanisms behind these phenomena are alterations in nitric oxide synthase (NOS) system activity. The aim of the study was to investigate the tolerance and dependence potential of tapentadol in rodent models and to evaluate the possible role of nitric oxide (NO) in these processes. Our study showed that chronic tapentadol treatment resulted in tolerance to its antinociceptive effects to an extent similar to tramadol, but much less than morphine. A single injection of a non-selective NOS inhibitor, N G -nitro-L-arginine (L-NOArg), reversed the tapentadol tolerance. In dependence studies, repeated administration of L-NOArg attenuated naloxone-precipitated withdrawal in tapentadol-treated mice, whereas a single injection of L-NOArg was ineffective. Biochemical analysis revealed that tapentadol decreased nNOS protein levels in the dorsal root ganglia of rats following 31 days of treatment, while no significant changes were found in iNOS and eNOS protein expression. Moreover, pre-treatment with L-NOArg augmented tapentadol antinociception in an opioid- and α 2 -adrenoceptor-dependent manner. In conclusion, our data suggest that the NOS system plays an important role in the attenuation of tapentadol-induced tolerance and withdrawal. Thus, inhibition of NOS activity can serve as a promising treatment option for long-term tapentadol use by extending its effectiveness and improving the side-effects profile., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

8. Role of β-arrestin-2 in short- and long-term opioid tolerance in the dorsal root ganglia.

Author

Muchhala KH, Jacob JC, Dewey WL, and Akbarali HI

Subjects

Animals, Behavior, Animal drug effects, Cells, Cultured, Disease Models, Animal, Female, Ganglia, Spinal metabolism, Ganglia, Spinal physiopathology, Male, Mice, Knockout, Neurons metabolism, Nociceptive Pain genetics, Nociceptive Pain metabolism, Nociceptive Pain physiopathology, Pain Threshold drug effects, Receptors, Opioid, mu metabolism, Time Factors, beta-Arrestin 2 deficiency, beta-Arrestin 2 genetics, Mice, Analgesics, Opioid pharmacology, Drug Tolerance, Ganglia, Spinal drug effects, Morphine pharmacology, Neurons drug effects, Nociceptive Pain prevention & control, Receptors, Opioid, mu agonists, Spiro Compounds pharmacology, Thiophenes pharmacology, beta-Arrestin 2 metabolism

Abstract

G-protein-biased agonists with reduced β-arrestin-2 activation are being investigated as safer alternatives to clinically-used opioids. β-arrestin-2 has been implicated in the mechanism of opioid-induced antinociceptive tolerance. Opioid-induced analgesic tolerance is classically considered as centrally-mediated, but recent reports implicate nociceptive dorsal root ganglia neurons as critical mediators in this process. Here, we investigated the role of β-arrestin-2 in the mechanism of opioid tolerance in dorsal root ganglia nociceptive neurons using β-arrestin-2 knockout mice and the G-protein-biased μ-opioid receptor agonist, TRV130. Whole-cell current-clamp electrophysiology experiments revealed that 15-18-h overnight exposure to 10 μM morphine in vitro induced acute tolerance in β-arrestin-2 wild-type but not knockout neurons. Furthermore, in wild-type neurons circumventing β-arrestin-2 activation by overnight treatment with 200 nM TRV130 attenuated tolerance. Similarly, acute morphine tolerance in vivo in β-arrestin-2 knockout mice was prevented in the warm-water tail-withdrawal assay. Treatment with 30 mg/kg TRV130 s.c. also inhibited acute antinociceptive tolerance in vivo in wild-type mice. Alternately, in β-arrestin-2 knockout neurons tolerance induced by 7-day in vivo exposure to 50 mg morphine pellet was conserved. Likewise, β-arrestin-2 deletion did not mitigate in vivo antinociceptive tolerance induced by 7-day exposure to 25 mg or 50 mg morphine pellet in both female or male mice, respectively. Consequently, these results indicated that β-arrestin-2 mediates acute but not chronic opioid tolerance in dorsal root ganglia neurons and to antinociception in vivo. This suggests that opioid-induced antinociceptive tolerance may develop even in the absence of β-arrestin-2 activation, and thus significantly affect the clinical utility of biased agonists., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

9. Antinociceptive effect of intrathecal P7C3 via GABA in a rat model of inflammatory pain.

Author

Ryu SW, Kim YO, Kim HB, Oh SB, Choi JI, and Yoon MH

Subjects

Animals, Calcium Signaling, Disease Models, Animal, Formaldehyde, Glutamate Decarboxylase metabolism, Inflammation chemically induced, Injections, Spinal, Male, Nociceptive Pain etiology, Nociceptive Pain metabolism, Nociceptive Pain physiopathology, Rats, Sprague-Dawley, Spinal Cord metabolism, Spinal Cord physiopathology, Rats, Analgesics administration & dosage, Carbazoles administration & dosage, Nociceptive Pain drug therapy, Pain Threshold drug effects, Spinal Cord drug effects, gamma-Aminobutyric Acid metabolism

Abstract

The recently identified molecule P7C3 has been highlighted in the field of pain research. We examined the effect of intrathecal P7C3 in tissue injury pain evoked by formalin injection and determined the role of the GABA system in the activity of P7C3 at the spinal level. Male Sprague-Dawley rats with intrathecal catheters implanted for experimental drug delivery were studied. The effects of intrathecal P7C3 and nicotinamide phosphoribosyltransferase (NAMPT) administered 10 min before the formalin injection were examined. Animals were pretreated with bicuculline, a GABA-A receptor antagonist; saclofen, a GABA-B receptor antagonist; L-allylglycine, a glutamic acid decarboxylase (GAD) blocker; and CHS 828, an NAMPT inhibitor; to observe involvement in the effects of P7C3. The effects of P7C3 alone and the mixture of P7C3 with GABA receptor antagonists on KCl-induced calcium transients were examined in rat dorsal root ganglion (DRG) neurons. The expression of GAD and the concentration of GABA in the spinal cord were evaluated. Intrathecal P7C3 and NAMPT produced an antinociceptive effect in the formalin test. Intrathecal bicuculline, saclofen, L-allylglycine, and CHS 828 reversed the antinociception of P7C3 in both phases. P7C3 decreased the KCl-induced calcium transients in DRG neurons. Both bicuculline and saclofen reversed the blocking effect of P7C3. The levels of GAD expression and GABA concentration decreased after formalin injection and were increased by P7C3. These results suggest that P7C3 increases GAD activity and then increases the GABA concentration in the spinal cord, which in turn may act on GABA receptors causing the antinociceptive effect against pain evoked by formalin injection., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

10. The synergistic effects of opioid and neuropeptide B/W in rat acute inflammatory and neuropathic pain models.

Author

Xing Y, Liu Y, Deng M, Wang HP, Abdul M, Zhang FF, Zhang Z, and Cao JL

Subjects

Animals, Behavior, Animal drug effects, Disease Models, Animal, Drug Synergism, Drug Therapy, Combination, Formaldehyde, HEK293 Cells, Humans, Male, Mitogen-Activated Protein Kinases metabolism, Neuropeptides chemical synthesis, Neuropeptides therapeutic use, Nociceptive Pain chemically induced, Nociceptive Pain metabolism, Nociceptive Pain physiopathology, Phosphorylation, Rats, Sprague-Dawley, Receptors, G-Protein-Coupled agonists, Receptors, G-Protein-Coupled genetics, Receptors, G-Protein-Coupled metabolism, Receptors, Neuropeptide agonists, Receptors, Neuropeptide genetics, Receptors, Neuropeptide metabolism, Receptors, Opioid, mu agonists, Receptors, Opioid, mu genetics, Receptors, Opioid, mu metabolism, Sciatica metabolism, Sciatica physiopathology, Spinal Cord Dorsal Horn metabolism, Spinal Cord Dorsal Horn physiopathology, Rats, Analgesics, Opioid pharmacology, Neuropeptides pharmacology, Nociceptive Pain prevention & control, Pain Threshold drug effects, Sciatica prevention & control, Spinal Cord Dorsal Horn drug effects

Abstract

The use of morphine is controversial due to the incidence of rewarding behavior, respiratory depression, and tolerance, leading to increased drug dose requirements, advancing to morphine addiction. To overcome these barriers, strategies have been taken to combine morphine with other analgesics. Neuropeptide B23 and neuropeptide W23 (NPB23 and NPW23) are commonly used to relieve inflammatory pain and neuropathic pain. As NPB23 and NPW23 system shares similar anatomical basis with opioid system at least in the spinal cord we hypothesized that NPB23 or NPW23 and morphine may synergistically relieve inflammatory pain and neuropathic pain. To test this hypothesis, we demonstrated that μ opioid receptor and NPBW1 receptor (receptor of NPB23 and NPW23) are colocalized in the superficial dorsal horn of the spinal cord. Secondly, co-administration of morphine witheitherNPB23 or NPW23 synergistically attenuated inflammatory and neuropathic pain. Furthermore, either NPB23 or NPW23 significantly reduced morphine-induced conditioned place preference (CPP) and constipation. We also found that phosphorylation of extracellular-regulated protein kinase (ERK1/2) following morphine was profoundly potentiated by the application of NPB23 or NPW23. Hence, combination of morphine with either NPB23 or NPW23 reduced dose of morphine required for pain relief in inflammatory and neuropathic pain, while effectively prevented some side-effects of morphine., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

11. TNF-α, CXCL-1 and IL-1 β as activators of the opioid system involved in peripheral analgesic control in mice.

Author

Dias Quintão JL, Reis Gonzaga AC, Galdino G, Lima Romero TR, Silva J, Lemos V, Campolina-Silva GH, Aparecida de Oliveira C, Bohórquez Mahecha G, and Gama Duarte I

Subjects

Animals, Carrageenan, Dinoprostone, Disease Models, Animal, Hyperalgesia metabolism, Hyperalgesia physiopathology, Hyperalgesia prevention & control, Male, Mice, Narcotic Antagonists pharmacology, Nociceptive Pain metabolism, Nociceptive Pain physiopathology, Nociceptive Pain prevention & control, Norepinephrine, Receptors, Opioid drug effects, Signal Transduction, Chemokine CXCL1, Hyperalgesia chemically induced, Interleukin-1beta, Nociception drug effects, Nociceptive Pain chemically induced, Opioid Peptides metabolism, Receptors, Opioid metabolism, Tumor Necrosis Factor-alpha

Abstract

Tissue injury results in the release of inflammatory mediators, including a cascade of nociceptive substances, which contribute to development of hyperalgesia. In addition, during this process endogenous analgesic substances are also peripherally released with the aim of controlling the hyperalgesia. Thus, the present study aimed to investigate whether inflammatory mediators TNF-α, IL-1β, CXCL1, norepinephrine (NE) and prostaglandin E2 (PGE2) may be involved in the deflagration of peripheral endogenous modulation of inflammatory pain by activation of the opioid system. Thus, male Swiss mice and the paw withdrawal test were used. All substances were injected by the intraplantar route. Carrageenan, TNF-α, CXCL-1, IL1-β, NE and PGE2 induced hyperalgesia. Selectives μ (clocinamox), δ (naltrindole) and κ (norbinaltorphimine, nor-BNI) and non-selective (naloxone) opioid receptor antagonists potentiated the hyperalgesia induced by carrageenan, TNF-α, CXCL-1 and IL1-β. In contrast, when the enzyme N-aminopeptidase involved in the degradation of endogenous opioid peptides was inhibited by bestatin, the hyperalgesia was significantly reduced. In addition, the western blotting assay indicated that the expression of the opioid δ receptor was increased after intraplantar injection of carrageenan. The data obtained in this work corroborate the hypothesis that TNF-α, CXCL-1 and IL-β cause, in addition to hyperalgesia, the release of endogenous substances such as opioid peptides, which in turn exert endogenous control over peripheral inflammatory pain., (Copyright © 2021 Elsevier B.V. All rights reserved.)

Published

2021

12. Morphine-Conditioned Placebo Analgesia in Female and Male Rats with Chronic Neuropathic Pain: c-Fos Expression in the Rostral Ventromedial Medulla.

Author

Boorman DC and Keay KA

Subjects

Animals, Female, Male, Medulla Oblongata, Morphine pharmacology, Rats, Rats, Sprague-Dawley, Analgesia, Neuralgia drug therapy

Abstract

Placebo analgesia has great potential to overcome the inadequacies of current drug therapies to treat conditions of chronic pain. The rostral ventromedial medulla (RVM) has been implicated as a critical relay in the antinociceptive pathway underpinning placebo analgesia in humans. We developed a model of opiate-conditioned placebo analgesia in rats with neuropathic injury to identify medullary nuclei active during placebo analgesia. Using female and male rats the degree of thermal allodynia was first determined following nerve injury, and a pharmacological conditioning procedure, pairing contextual cues with the experience of morphine-induced analgesia, was used to elicit placebo analgesic reactions. This protocol revealed clear subpopulations of placebo reactors (36% of males, 25% of females) and non-reactors in proportions similar to those reported in human studies. We detected injury-specific c-Fos expression in the gracile nucleus and morphine-specific c-Fos expression in the serotonergic midline raphe nuclei and the caudal nuclei of the solitary tract. However, c-Fos expression did not differ between placebo reactors and non-reactors in either serotonergic or non-serotonergic neurons of the RVM. Despite a subpopulation of rats demonstrating placebo reactions, we found no evidence for enhanced activity in the nuclei from which the classical RVM → spinal cord descending analgesic pathways emerge., (Crown Copyright © 2020. Published by Elsevier Ltd. All rights reserved.)

Published

2021

13. Haloperidol potentiates antinociceptive effects of morphine and disrupt opioid tolerance.

Author

Mena-Valdés LC, Blanco-Hernández Y, Espinosa-Juárez JV, and López-Muñoz FJ

Subjects

Analgesics, Opioid toxicity, Animals, Disease Models, Animal, Dose-Response Relationship, Drug, Drug Synergism, Drug Therapy, Combination, Male, Morphine toxicity, Neuralgia metabolism, Neuralgia physiopathology, Rats, Wistar, Receptors, sigma metabolism, Signal Transduction, Time Factors, Sigma-1 Receptor, Rats, Analgesics, Opioid pharmacology, Drug Tolerance, Haloperidol pharmacology, Morphine pharmacology, Neuralgia drug therapy, Nociception drug effects, Receptors, sigma antagonists & inhibitors

Abstract

Haloperidol is an antipsychotic agent recently described as an antinociceptive drug able to mediate the antagonism of sigma-1 receptors while morphine is an opioid used in the treatment of neuropathic pain. The objectives of this work were to determine the type of interaction generated by the combination of morphine and haloperidol in neuropathic pain induced by chronic constriction injury and to evaluate morphine tolerance and side effects. The antiallodynic and anti-hyperalgesic effects of morphine (0.01-3.16 mg/kg, s.c.) and haloperidol (0.0178-0.1778 mg/kg, s.c.) were determined after single-doses, in monotherapy and combined, using the acetone and von Frey tests, respectively. Evaluations were performed until 10-days postsurgery. Data were processed using "Surface of Synergic Interaction analysis". The rotarod test was used to evaluate motor coordination, and the constipation test was performed using 5% charcoal. The effects of haloperidol and BD-1063, sigma-1 receptor antagonists, naloxone and PRE-084 (sigma-1 agonist) were determined using the morphine-tolerance model. Morphine (0.0316 mg/kg)+haloperidol (0.0178 mg/kg) was determined to be the optimal combination. Morphine-tolerance was observed on day 5 after 11 administrations, although in animals that received the combination, tolerance was delayed until day 8. PRE-084 and naloxone administered on day 5 in animals treated with the combination resulted in a blockade of its antiallodynic effects. Adverse effects of constipation or motor incoordination were not shown in animals treated with morphine + haloperidol. In conclusion, haloperidol enhances the antinociceptive effects of morphine without significant adverse effects, as it is able to disrupt or delay the morphine-tolerance in neuropathic pain., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2021

14. Antinociceptive effects of rotigotine-loaded microspheres and its synergistic interactions with analgesics in inflammatory pain in rats.

Author

Li T, Wang T, Wang L, Liu R, Zhang L, Zhai R, and Fu F

Subjects

Analgesics chemistry, Analgesics pharmacokinetics, Animals, Behavior, Animal drug effects, Carrageenan, Delayed-Action Preparations, Disease Models, Animal, Drug Compounding, Drug Synergism, Drug Therapy, Combination, Hyperalgesia chemically induced, Hyperalgesia physiopathology, Locomotion drug effects, Male, Microspheres, Nociceptive Pain chemically induced, Nociceptive Pain physiopathology, Open Field Test drug effects, Rats, Sprague-Dawley, Tetrahydronaphthalenes chemistry, Tetrahydronaphthalenes pharmacokinetics, Thiophenes chemistry, Thiophenes pharmacokinetics, Rats, Acetaminophen pharmacology, Analgesics pharmacology, Hyperalgesia prevention & control, Nociceptive Pain prevention & control, Pain Threshold drug effects, Tetrahydronaphthalenes pharmacology, Thiophenes pharmacology, Tramadol pharmacology

Abstract

Rotigotine-loaded microspheres (RoMS) are sustained-release formulations with prolonged anti-Parkinson's effects. Given that pain is a non-motor symptom of Parkinson's disease, this study investigated the antinociceptive effects of RoMS and their synergistic effects with analgesics on inflammatory pain. A model of inflammatory pain was prepared by intraplantarly injecting male Sprague-Dawley rats with carrageenan. The antinociceptive effects of RoMS, acetaminophen, and tramadol, both alone and in combination, were evaluated using the hind paw withdrawal latency in the hot plate test and Randall-Selitto test. The rotigotine concentrations in serum and tissues were assayed using ultra-performance liquid chromatography-tandem mass spectrometry. Isobolographic analysis was performed to evaluate the nature of the interactions of RoMS with acetaminophen or tramadol. The results showed that hind paw withdrawal latency to thermal and mechanical stimuli was significantly increased on day 3 and 7 after administered RoMS. Rotigotine could be detected in serum and tissues 3 and 7 days after an intramuscular injection of RoMS. However, the rotigotine concentration fell the detection limit of the assay on day 14 after administration. RoMS produced synergistic antinociceptive effects in the inflammatory pain model when RoMS is combined with acetaminophen or tramadol. These findings suggest that RoMS can relieve inflammatory pain in rats. Furthermore, the combination of RoMS with acetaminophen or tramadol produces synergistic antinociception, which may be clinically worthy because combination therapies may reduce the drug doses required for antinociception., (Copyright © 2020. Published by Elsevier B.V.)

Published

2021

15. Thermal Hyperalgesia and Mechanical Allodynia Elicited by Histamine and Non-histaminergic Itch Mediators: Respective Involvement of TRPV1 and TRPA1.

Author

Tsagareli MG, Nozadze I, Tsiklauri N, Carstens MI, Gurtskaia G, and Carstens E

Subjects

Animals, Male, Mice, Receptors, G-Protein-Coupled metabolism, TRPA1 Cation Channel, TRPV Cation Channels, Histamine pharmacology, Hyperalgesia, Pruritus chemically induced, Pruritus drug therapy, Transient Receptor Potential Channels

Abstract

Acute itch is elicited by histamine, as well as non-histaminergic itch mediators including chloroquine, BAM8-22 and Ser-Leu-Ile-Gly-Arg-Leu (SLIGRL). When injected intradermally, histamine binds to histamine H1 and H4 receptors that activate transient receptor potential vanilloid 1 (TRPV1) to depolarize pruriceptors. Chloroquine, BAM8-22, and SLIGRL, respectively, bind to Mas-related G-protein-coupled receptors MrgprA3, MrgprC11, and MrgprC11/PAR2 that in turn activate transient receptor potential ankyrin 1 (TRPA1). In this study we tested if histamine, chloroquine, BAM8-22 and SLIGRL elicit thermal hyperalgesia and mechanical allodynia in adult male mice. We measured the latency of hindpaw withdrawal from a noxious heat stimulus, and the threshold for hindpaw withdrawal from a von Frey mechanical stimulus. Intraplantar injection of histamine resulted in significant thermal hyperalgesia (p < 0.001) and mechanical allodynia (p < 0.001) ipsilaterally that persisted for 1 h. Pretreatment with the TRPV1 antagonist AMG-517 (10 or 20 μg), but not the TRPA1 antagonist HC-030031 (50 or 100 μg), significantly attenuated the magnitude and time course of thermal hyperalgesia and mechanical allodynia elicited by histamine (p < 0.001 for both), indicating that these effects are mediated by TRPV1. In contrast, pretreatment with the TRPA1 antagonist significantly reduced thermal hyperalgesia and mechanical allodynia elicited by chloroquine (p < 0.001 for both ), BAM-822 (p < 0.01, p < 0.001, respectively) and SLGRL (p < 0.05, p < 0.001, respectively), indicating that effects elicited by these non-histaminergic itch mediators require TRPA1. TRPV1 and TRPA1 channel inhibitors thus may have potential use in reducing hyperalgesia and allodynia associated with histaminergic and non-histaminergic itch, respectively., (Copyright © 2020 IBRO. Published by Elsevier Ltd. All rights reserved.)

Published

2020

16. Pain relief devoid of opioid side effects following central action of a silylated neurotensin analog.

Author

Tétreault P, Besserer-Offroy É, Brouillette RL, René A, Murza A, Fanelli R, Kirby K, Parent AJ, Dubuc I, Beaudet N, Côté J, Longpré JM, Martinez J, Cavelier F, and Sarret P

Subjects

Analgesics pharmacology, Animals, Blood Pressure drug effects, Body Temperature drug effects, Gastrointestinal Motility drug effects, Hyperalgesia drug therapy, Hyperalgesia physiopathology, Male, Neurotensin pharmacology, Pain physiopathology, Rats, Sprague-Dawley, Receptors, Neurotensin physiology, Analgesics therapeutic use, Neurotensin analogs & derivatives, Neurotensin therapeutic use, Pain drug therapy, Receptors, Neurotensin agonists

Abstract

Neurotensin (NT) exerts naloxone-insensitive antinociceptive action through its binding to both NTS 1 and NTS 2 receptors and NT analogs provide stronger pain relief than morphine on a molecular basis. Here, we examined the analgesic/adverse effect profile of a new NT(8-13) derivative denoted JMV2009, in which the Pro 10 residue was substituted by a silicon-containing unnatural amino acid silaproline. We first report the synthesis and in vitro characterization (receptor-binding affinity, functional activity and stability) of JMV2009. We next examined its analgesic activity in a battery of acute, tonic and chronic pain models. We finally evaluated its ability to induce adverse effects associated with chronic opioid use, such as constipation and analgesic tolerance or related to NTS 1 activation, like hypothermia. In in vitro assays, JMV2009 exhibited high binding affinity for both NTS 1 and NTS 2 , improved proteolytic resistance as well as agonistic activities similar to NT, inducing sustained activation of p42/p44 MAPK and receptor internalization. Intrathecal injection of JMV2009 produced dose-dependent antinociceptive responses in the tail-flick test and almost completely abolished the nociceptive-related behaviors induced by chemical somatic and visceral noxious stimuli. Likewise, increasing doses of JMV2009 significantly reduced tactile allodynia and weight bearing deficits in nerve-injured rats. Importantly, repeated agonist treatment did not result in the development of analgesic tolerance. Furthermore, JMV2009 did not cause constipation and was ineffective in inducing hypothermia. These findings suggest that NT drugs can act as an effective opioid-free medication for the management of pain or can serve as adjuvant analgesics to reduce the opioid adverse effects., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2020

17. Adenosine A 1 receptor agonist induces visceral antinociception via 5-HT 1A , 5-HT 2A , dopamine D 1 or cannabinoid CB 1 receptors, and the opioid system in the central nervous system.

Author

Okumura T, Nozu T, Ishioh M, Igarashi S, Kumei S, and Ohhira M

Subjects

Analgesics, Animals, Central Nervous System, Dopamine, Rats, Rats, Sprague-Dawley, Receptor, Cannabinoid, CB1, Receptor, Cannabinoid, CB2, Receptor, Serotonin, 5-HT1A, Receptor, Serotonin, 5-HT2A, Receptors, Dopamine D1, Serotonin, Adenosine A1 Receptor Agonists pharmacology, Analgesics, Opioid, Cannabinoids

Abstract

We have recently demonstrated that N(6)-cyclopentyladenosine (CPA), an adenosine A1 receptor agonist, acts centrally to induce a visceral antinociception. Since serotonin (5-HT), cannabinoid (CB), dopamine or opioid signaling in the central nervous system is involved in the regulation of visceral sensation, we made a hypothesis that the signaling may play a role in the CPA-induced visceral antinociception. Visceral sensation was evaluated by colonic distension-induced abdominal withdrawal reflex (AWR) in conscious rats. Subcutaneously administered CPA significantly increased the threshold of colonic distension-induced AWR. Intracisternal injection of either 5-HT 1A or 5-HT 2A receptor antagonist blocked the CPA-induced visceral antinociception while 5-HT 1B antagonist did not block the CPA-induced visceral antinociception. Subcutaneous injection of dopamine D 1 receptor antagonist, CB 1 receptor antagonist or naloxone significantly blocked the CPA-induced visceral antinociception while neither subcutaneous injection of dopamine D 2 receptor antagonist nor CB 2 receptor antagonist blocked the CPA-induced anti-pain action. These results suggest that 5-HT 1A , 5-HT 2A , dopamine D 1 , CB 1 receptors and the opioid system in the CNS may specifically mediate the CPA-induced visceral antinociception. These findings may help in understanding the physiological relevance of central adenosine with special reference to the pathophysiology of altered visceral sensation especially in irritable bowel syndrome., (Copyright © 2020 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2020

18. Dual dose-related effects evoked by CCL4 on thermal nociception after gene delivery or exogenous administration in mice.

Author

Aguirre A, González-Rodríguez S, García-Domínguez M, Lastra A, Gutiérrez-Fernández A, Hidalgo A, Menéndez L, and Baamonde A

Subjects

Animals, Chemokine CCL4 genetics, Dose-Response Relationship, Drug, Hyperalgesia genetics, Male, Mice, Nociception drug effects, Chemokine CCL4 administration & dosage, Gene Transfer Techniques, Hot Temperature adverse effects, Hyperalgesia drug therapy, Nociception physiology

Abstract

As recently described, the administration of extremely low doses (pg/kg) of CCL4 (Macrophage inflammatory protein 1β, MIP-1β) can induce antinociceptive effects in mice (García-Domínguez et al., 2019b). We describe here that hydrodynamic delivery of a plasmid containing CCL4 cDNA provokes a biphasic response consisting in an initial thermal hyperalgesic reaction for 8 days followed by analgesia at days 10-12, being both responses blocked after the administration of the CCR5 antagonist DAPTA. Both the luminiscence evoked in liver after the administration of a plasmid containing CCL4 and luciferase cDNAs and the hepatic concentration of CCL4 measured by ELISA were maximal 4 days after plasmid administration and markedly diminished at day 10. A dose-effect curve including a wide dose range of exogenous CCL4 revealed thermal analgesia after the administration of 10-100 pg/kg whereas 1000 times higher doses (30-100 ng/kg) induced, instead, thermal hyperalgesia inhibited by DAPTA. This hyperalgesia was absent in mice with reduced white blood cells after cyclophosphamide treatment, thus supporting the involvement of circulating leukocytes. A multiarray bioluminescent assay revealed increased plasma levels of IL-1α, CCL2, CXCL1, CXCL13, IL-16 and TIMP-1 in mice treated with 100 ng/kg of CCL4. The hyperalgesic response evoked by CCL4 was prevented by IL-1R, CXCR2 or CCR2 antagonists or by the neutralization of CXCL13 or IL-16, but not TIMP-1, with selective antibodies. The administration of the anti-IL-16 antibody was the unique treatment able to convert hyperalgesia evoked by 100 ng/kg of CCL4 in an analgesic effect. The ability of IL-16 to evoke hypernociception was confirmed by studying the response to its exogenous administration (10-30 ng/kg). In summary, the present results demonstrate that CCL4 induces a dual modulation of nociception and describe some mechanisms involved in the hyperalgesic response evoked by this chemokine., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2020 Elsevier Inc. All rights reserved.)

Published

2020

19. Intracerebroventricular administration of CYX-6, a potent μ-opioid receptor agonist, a δ- and κ-opioid receptor antagonist and a biased ligand at μ, δ & κ-opioid receptors, evokes antinociception with minimal constipation and respiratory depression in rats in contrast to morphine.

Author

Imam MZ, Kuo A, Ghassabian S, Cai Y, Qin Y, Li T, and Smith MT

Subjects

Analgesics, Opioid administration & dosage, Analgesics, Opioid adverse effects, Analgesics, Opioid metabolism, Animals, Infusions, Intraventricular, Ligands, Male, Morphine adverse effects, Opioid Peptides drug effects, Rats, Rats, Sprague-Dawley, Receptors, Opioid, delta metabolism, Receptors, Opioid, kappa metabolism, Receptors, Opioid, mu metabolism, Nociceptin, Analgesics, Opioid pharmacology, Constipation chemically induced, Morphine pharmacology, Receptors, Opioid, delta antagonists & inhibitors, Receptors, Opioid, kappa antagonists & inhibitors, Receptors, Opioid, mu agonists, Respiratory Insufficiency chemically induced

Abstract

Mu opioid receptor (MOPr) agonists are thought to produce analgesia via modulation of G-protein-coupled intracellular signalling pathways whereas the β-arrestin2 pathway is proposed to mediate opioid-related adverse effects. Here, we report the antinociception, constipation and respiratory depressant profile of CYX-6, a potent MOPr agonist that is also a delta and a kappa opioid receptor (DOPr/KOPr) antagonist and that lacks β-arrestin2 recruitment at each of the MOPr, DOPr and the KOPr. In anaesthetised male Sprague Dawley rats, an intracerebroventricular (i.c.v.) guide cannula was stereotaxically implanted. After 5-7 days post-surgical recovery, rats received a single i.c.v. bolus dose of CYX-6 (3-30 nmol), morphine (100 nmol) or vehicle. Antinociception was assessed using the warm water tail flick test (52.5 ± 0.5 °C). Constipation was assessed using the charcoal meal gut motility test and the castor oil-induced diarrhoea test. Respiratory depression was measured by whole-body plethysmography in awake, freely moving animals, upon exposure to a hypercapnic gas mixture (8% CO 2 , 21% O 2 and 71% N 2 ). The intrinsic pharmacology of CYX-6 given by the i.c.v. route in rats showed that it produced dose-dependent antinociception. It also produced respiratory stimulation rather than depression and it had a minimal effect on intestinal motility in contrast to the positive control, morphine. CYX-6 is an endomorphin-2 analogue that dissociates antinociception from constipation and respiratory depression in rats. Our findings provide useful insight to inform the discovery and development of novel opioid analgesics with a superior tolerability profile compared with morphine., Competing Interests: Declaration of competing interest None., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2020

20. The intraperitoneal administration of MOTS-c produces antinociceptive and anti-inflammatory effects through the activation of AMPK pathway in the mouse formalin test.

Author

Yin X, Jing Y, Chen Q, Abbas AB, Hu J, and Xu H

Subjects

Animals, Cytokines metabolism, Enzyme Activation drug effects, Extracellular Signal-Regulated MAP Kinases metabolism, Formaldehyde metabolism, Gene Expression Regulation, Enzymologic, Humans, Injections, Intraperitoneal, JNK Mitogen-Activated Protein Kinases metabolism, MAP Kinase Signaling System, Male, Mice, Mice, Inbred ICR, Nociception drug effects, Pain Measurement, Phosphorylation, Proto-Oncogene Proteins c-fos metabolism, Spinal Cord drug effects, p38 Mitogen-Activated Protein Kinases metabolism, AMP-Activated Protein Kinases metabolism, Analgesics administration & dosage, Anti-Inflammatory Agents administration & dosage, Mitochondrial Proteins administration & dosage, Neuralgia metabolism

Abstract

The activation of the AMP activated protein kinase (AMPK) exerts antinociceptive effects in acute and neuropathic pain models. Mitochondrial open-reading-frame of the twelve S rRNA-c (MOTS-c), a mitochondrial-derived peptide, regulates many biological activities via activating AMPK. However, the role of MOTS-c in the formalin-induced inflammatory nociception remains unclear. In this study, we investigated the role of MOTS-c in the formalin-induced inflammatory nociception. The antinociceptive effect of MOTS-c was assessed by recording the time spent licking paw. The anti-inflammatory effect of MOTS-c was evaluated by detecting the inflammatory cytokine level changes in the mouse serum. Western blot was used to detect the changes of protein phosphorylation levels in the mouse spinal cord. Changes of c-fos expression in the spinal cord were assessed by immunohistochemistry. Our results showed that the intraperitoneal administration of MOTS-c reduced the time spent on licking in phase 2 in a dose-dependent manner in the formalin test. The antinociceptive effects of MOTS-c (50 mg/kg, i.p.) were attenuated by the AMPK antagonist compound C (10 mg/kg, i.p.). MOTS-c (50 mg/kg, i.p.) significantly reduced pro-inflammatory cytokine levels and elevated the level of anti-inflammatory cytokine in mouse serum. In addition, MOTS-c treatment significantly increased AMPKα phosphorylation level and suppressed formalin-induced extracellular signal-regulated kinase (ERK), c-Jun amino-terminal kinases (JNK), and P38 activation and c-fos expression in the mouse spinal cord. These results suggest that systemic administration of MOTS-c exerts antinociceptive and anti-inflammatory effects, at least partially, through activating AMPK pathway and inhibiting MAP kinases-c-fos signaling pathway in the mouse formalin test., Competing Interests: Declaration of competing interest The authors declare that they have no conflict of interest., (Copyright © 2020 Elsevier B.V. All rights reserved.)

Published

2020

21. Design and synthesis of cyanamides as potent and selective N-acylethanolamine acid amidase inhibitors.

Author

Malamas MS, Farah SI, Lamani M, Pelekoudas DN, Perry NT, Rajarshi G, Miyabe CY, Chandrashekhar H, West J, Pavlopoulos S, and Makriyannis A

Subjects

Amidohydrolases metabolism, Animals, Cyanamide chemical synthesis, Cyanamide chemistry, Dose-Response Relationship, Drug, Enzyme Inhibitors chemical synthesis, Enzyme Inhibitors chemistry, Mice, Models, Molecular, Molecular Structure, Rats, Structure-Activity Relationship, Amidohydrolases antagonists & inhibitors, Cyanamide pharmacology, Drug Design, Enzyme Inhibitors pharmacology

Abstract

N-acylethanolamine acid amidase (NAAA) inhibition represents an exciting novel approach to treat inflammation and pain. NAAA is a cysteine amidase which preferentially hydrolyzes the endogenous biolipids palmitoylethanolamide (PEA) and oleoylethanolamide (OEA). PEA is an endogenous agonist of the nuclear peroxisome proliferator-activated receptor-α (PPAR-α), which is a key regulator of inflammation and pain. Thus, blocking the degradation of PEA with NAAA inhibitors results in augmentation of the PEA/PPAR-α signaling pathway and regulation of inflammatory and pain processes. We have prepared a new series of NAAA inhibitors exploring the azetidine-nitrile (cyanamide) pharmacophore that led to the discovery of highly potent and selective compounds. Key analogs demonstrated single-digit nanomolar potency for hNAAA and showed >100-fold selectivity against serine hydrolases FAAH, MGL and ABHD6, and cysteine protease cathepsin K. Additionally, we have identified potent and selective dual NAAA-FAAH inhibitors to investigate a potential synergism between two distinct anti-inflammatory molecular pathways, the PEA/PPAR-α anti-inflammatory signaling pathway, 1-4 and the cannabinoid receptors CB1 and CB2 pathways which are known for their antiinflammatory and antinociceptive properties. 5-8 Our ligand design strategy followed a traditional structure-activity relationship (SAR) approach and was supported by molecular modeling studies of reported X-ray structures of hNAAA. Several inhibitors were evaluated in stability assays and demonstrated very good plasma stability (t 1/2  > 2 h; human and rodents). The disclosed cyanamides represent promising new pharmacological tools to investigate the potential role of NAAA inhibitors and dual NAAA-FAAH inhibitors as therapeutic agents for the treatment of inflammation and pain., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2020

22. Involvement of Spinal Cannabinoid CB 2 Receptors in Exercise-Induced Antinociception.

Author

Dos Santos RS, Sorgi CA, Peti APF, Veras FP, Faccioli LH, and Galdino G

Subjects

Animals, Female, Hyperalgesia metabolism, Indoles pharmacology, Mice, Inbred C57BL, Pain chemically induced, Pain Management, Pain Measurement drug effects, Piperidines pharmacology, Receptor, Cannabinoid, CB1, Arachidonic Acids pharmacology, Endocannabinoids pharmacology, Pain physiopathology, Physical Conditioning, Animal methods, Polyunsaturated Alkamides pharmacology, Receptor, Cannabinoid, CB2 drug effects

Abstract

Muscle pain affects approximately 11-24% of the global population. Several studies have shown that exercise is a non-pharmacological therapy to pain control. It has been suggested that the endocannabinoid system is involved in this antinociceptive effect. However, the participation of this pathway is unclear. The present study aimed to investigate whether spinal cannabinoid CB 2 receptors participate in the exercise-induced antinociception. The inflammatory muscle pain model was induced by the intramuscular injection of carrageenan. Tactile allodynia and thermal hyperalgesia were determined with the von Frey filaments and hot-plate tests. C57BL/6J female mice underwent a swimming training protocol that lasted 3 weeks. This protocol of exercise reduced carrageenan-induced tactile allodynia and thermal hyperalgesia and this effect was prevented by the cannabinoid CB 2 receptors inverse agonist AM630 and potentiated by MAFP (inhibitor of the enzyme that metabolizes endocannabinoids) and minocycline (microglia inhibitor). In addition, exercise increased the endocannabinoid anandamide levels and cannabinoid CB 2 receptors expression whereas it reduced Iba1 (microglial marker) protein expression as well as pro-inflammatory cytokines (TNF-α and IL-1β) in the spinal cord of mice with inflammatory muscle pain. Swimming training also reduced muscle temperature of carrageen-treated animals. The present study suggests that activation of spinal cannabinoid CB 2 receptors and reduction of activated microglia are involved in exercise-induced antinociception., (Copyright © 2019 IBRO. Published by Elsevier Ltd. All rights reserved.)

Published

2019

23. Cellular Mechanism for Specific Mechanical Antinociception by D2-like Receptor at the Spinal Cord Level.

Author

Almanza A, Segura-Chama P, León-Olea M, Luis E, Garduño-Gutiérrez R, Mercado-Reyes J, Simón-Arceo K, Coffeen U, Hernández-Cruz A, Pellicer F, and Mercado F

Subjects

2,3,4,5-Tetrahydro-7,8-dihydroxy-1-phenyl-1H-3-benzazepine pharmacology, Animals, Calcium metabolism, Calcium physiology, Dopamine Agonists pharmacology, Ganglia, Spinal drug effects, Ganglia, Spinal metabolism, Ganglia, Spinal physiology, Male, Nociceptors drug effects, Nociceptors metabolism, Nociceptors physiology, Pramipexole pharmacology, Quinpirole pharmacology, Rats, Rats, Wistar, Spinal Cord metabolism, Nociception drug effects, Nociception physiology, Receptors, Dopamine D2 metabolism, Spinal Cord drug effects, Spinal Cord physiology

Abstract

Intrathecal (i.t.) administration of quinpirole, a dopamine (DA) D2-like receptor agonist, produces antinociception to mechanonociceptive stimuli but not to thermonociceptive stimuli. To determine a cellular mechanism for the specific antinociceptive effect of D2-like receptor activation on mechanonociception, we evaluated the effect of quinpirole on voltage-gated Ca 2+ influx in cultured dorsal root ganglion (DRG) neurons and the D2 DA receptor distribution in subpopulations of rat nociceptive DRG neurons. Small-diameter DRG neurons were classified into IB 4 + (nonpeptidergic) and IB 4 - (peptidergic). Intracellular [Ca 2+ ] microfluorometry and voltage-clamp experiments showed that quinpirole reduced Ca 2+ influx and inhibited the high voltage-activated Ca 2+ current (HVA-I Ca ) in half of IB 4 + neurons, leaving Ca 2+ entry and HVA-I Ca in IB 4 - neurons nearly unaffected. Pretreatment with ω-conotoxin MVIIA prevented the effect of quinpirole on HVA-I Ca from IB 4 + neurons, indicating that quinpirole mainly inhibits Ca V 2.2 channels. Immunofluorescence experiments showed that D2 DA receptor was present mainly in IB 4 + small DRG neurons. Finally, in behavioral experiments in rats, the clinically approved D2-like receptor agonist pramipexole produced spinal antinociception in a similar fashion to quinpirole, with a significant effect only in the mechanonociceptive test. Our results explain, at least in part, why D2-like receptor agonists produce antinociception on mechanonociceptors., (Copyright © 2019 IBRO. Published by Elsevier Ltd. All rights reserved.)

Published

2019

24. Natural chromones as potential anti-inflammatory agents: Pharmacological properties and related mechanisms.

Author

Opretzka LCF, Espírito-Santo RFD, Nascimento OA, Abreu LS, Alves IM, Döring E, Soares MBP, Velozo EDS, Laufer SA, and Villarreal CF

Subjects

Animals, Apoptosis drug effects, Cell Line, Cytokines immunology, Edema immunology, Humans, Liver metabolism, Macrophages drug effects, Macrophages metabolism, Male, Mice, Microsomes, Liver enzymology, NF-kappa B metabolism, Nitric Oxide biosynthesis, Plant Roots, Anti-Inflammatory Agents pharmacology, Anti-Inflammatory Agents therapeutic use, Chromones pharmacology, Chromones therapeutic use, Edema drug therapy, Rutaceae

Abstract

Chromones are a group of natural substances with a diversity of biological activities. Herein we assessed the pharmacological potential of three chromones (1, 2 and 3) isolated from Dictyoloma vandellianum as anti-inflammatory agents using in vitro and in vivo approaches. During in vitro screening, the production of NO and cytokines by macrophages stimulated with LPS and IFN-γ was inhibited by all chromones at concentrations (5-20 μM) that did not induce cytotoxicity. Analysis of pharmacokinetic parameters (in vitro half-life and intrinsic clearance) using human liver microsomes revealed that 3 has a superior pharmacokinetic profile, compared to 1 and 2. Treatment with 3 (100 mg/kg, ip) did not affect the mice motor performance, while 1 and 2 induced motor deficit. Taking into account the pharmacokinetic profile and absence of motor impairment, 3 was selected for further pharmacological characterization. Corroborating the data from in vitro screening, treatment of cell cultures with 3 (5-20 μM) reduced TNF-α, IL-6 and IL-1β production by stimulated macrophages. In the complete Freund's adjuvant-induced paw inflammation model in mice, 3 (25 and 50 mg/kg, ip) inhibited mechanical hyperalgesia, edema and cytokine production/release (IL-1β, IL-6 and TNF-α). 3 (5-20 μM) also reduced the transcriptional activity of NF-κB in stimulated macrophages. Furthermore, treatment with RU486, a glucocorticoid receptor (GR) antagonist, partially prevented the inhibitory effect of 3 on macrophages, indicating that this chromone exerts its anti-inflammatory effects in part through the activation of GR. The results presented herein demonstrate the pharmacological potential of natural chromones, highlighting 3 as a possible candidate for the drug discovery process targeting new anti-inflammatory drugs., (Copyright © 2019 Elsevier B.V. All rights reserved.)

Published

2019

25. The antinociceptive effects and molecular mechanisms of ghrelin(1-7)-NH 2 at the supraspinal level in acute pain in mice.

Author

Wu B, Liu Y, Liu F, Deng Q, Wang J, Han R, Zhang D, Chen J, and Wei J

Subjects

Analgesics administration & dosage, Analgesics, Opioid pharmacology, Animals, Injections, Intraventricular, Male, Mice, Morphine, Narcotic Antagonists administration & dosage, Oligopeptides administration & dosage, Peptide Fragments administration & dosage, Receptors, Ghrelin agonists, Receptors, Ghrelin metabolism, Receptors, Opioid drug effects, Ghrelin administration & dosage, Pain drug therapy

Abstract

Ghrelin(1-7)-NH 2 is the active N-terminal hepta-peptide of ghrelin as an agonist at the ghrelin receptor GHS-R1α. The biological functions of ghrelin(1-7)-NH 2 have not been well investigated. Therefore in this study, we were interested in exploring the effects and molecular mechanisms of ghrelin(1-7)-NH 2 in pain modulation at the supraspinal level using the tail withdrawal test in mice. Intracerebroventricular (i.c.v.) injection of ghrelin(1-7)-NH 2 (0.002, 0.02, 0.2 and 2 nmol/kg) induced a dose- and time-related antinociceptive effect. This antinociceptive effect was fully antagonized by co-injection with the GHS-R1α antagonist [D-Lys 3 ]-GHRP-6, indicating that this effect induced by ghrelin(1-7)-NH 2 was mediated through the activation of GHS-R1α. Interestingly, naloxone, β-funaltrexamine, naloxonazine, and naltrindole, but not nor-binaltorphimine, could also antagonize the antinociceptive effect markedly, suggesting that OPRM (primary μ 1 subtype) and OPRD were involved in the antinociceptive response induced by ghrelin(1-7)-NH 2 . Furthermore, the qRT-PCR and Western blot results indicated that both mRNA and protein levels of PENK and OPRD were up-regulated significantly. Using the fluorescence labeling method, our results showed that ghrelin(1-7)-NH 2 (i.c.v.) was mainly distributed at the dorsal 3rd ventricle and hippocampus where there are regions with high expressions of ghrelin, GHS-R1α and ORs. All these results indicated that ghrelin(1-7)-NH 2 initially activated the GHS-R1α, then activated the OPRM, as well as increased the release of endogenous PENK to activate of OPRD to produce antinociception. These results contributed to understanding the mechanisms of antinociception induced by ghrelin(1-7)-NH 2 . Furthermore, ghrelin(1-7)-NH 2 as the active fragment of ghrelin may be a promising peptide for developing new analgesic drugs., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2019

26. Discovery of two novel branched peptidomimetics containing endomorphin-2 and RF9 pharmacophores: Synthesis and neuropharmacological evaluation.

Author

Zhang T, Han Z, Shi X, Zhao W, Wang Z, Zhang R, Xu B, Zhang M, Zhang Q, Xiao J, Zhu H, Zheng T, and Fang Q

Subjects

Analgesics, Opioid chemical synthesis, Analgesics, Opioid therapeutic use, Animals, Cell Line, Tumor, Drug Partial Agonism, Gastrointestinal Transit drug effects, HEK293 Cells, Humans, Hyperalgesia drug therapy, Male, Mice, Morphine pharmacology, Naloxone pharmacology, Naltrexone analogs & derivatives, Naltrexone pharmacology, Neuronal Outgrowth drug effects, Peptidomimetics chemical synthesis, Peptidomimetics therapeutic use, Receptors, Neuropeptide agonists, Receptors, Neuropeptide antagonists & inhibitors, Receptors, Opioid, delta metabolism, Receptors, Opioid, mu metabolism, Analgesics, Opioid pharmacology, Drug Discovery, Peptidomimetics pharmacology

Abstract

It is well known that opioid analgesics produce side effects including tolerance and constipation. Since neuropeptide FF (NPFF) receptor antagonists reversed opioid-induced hyperalgesia and analgesic tolerance, the present work was performed to synthetize two branched peptidomimetics, EKR and RKE, containing the opioid peptide endomorphin-2 (EM-2) and the NPFF receptor antagonist RF9. Our data obtained from the in vitro cyclic adenosine monophosphate experiment demonstrated that EKR functioned as a mixed mu-, delta-opioid receptors agonist and NPFF 1 receptor antagonist/NPFF 2 receptor partial agonist, whereas RKE acted as a multi-functional peptidomimetic with the mu-opioid agonism and the NPFF 1 antagonism/NPFF 2 partial agonism. Furthermore, EKR and RKE completely blocked the NPFF 2 receptor-mediated neurite outgrowth of Neuro 2A cells. In vivo antinociception studies found that supraspinal administration of EKR and RKE dose-dependently produced potent antinociception via the mu-opioid receptor in the tail-flick test. In carrageenan inflammatory pain model, spinal administration of EKR and RKE induced dose-related analgesia, which was significantly reduced by the opioid antagonist naloxone and the NPFF antagonist RF9. Notably, compared with morphine, intracerebroventricular repeated administration of EKR and RKE maintained prolonged antinociceptive effectiveness. In addition, at the antinociceptive doses, these two branched peptidomimetics did not significantly inhibit gastrointestinal transit. Taken together, the present work suggest that EKR and RKE behave as multi-functional ligands with the opioid agonism and the NPFF 1 antagonism/NPFF 2 partial agonism, and produce prolonged antinociception with limited side effects. Moreover, our results imply that EKR and RKE might be interesting pharmacological tools for further investigating the biological function of the NPFF and opioid systems., (Copyright © 2019 Elsevier Ltd. All rights reserved.)

Published

2019

27. Role of mu-opioid agonist efficacy on antinociceptive interactions between mu agonists and the nociceptin opioid peptide agonist Ro 64-6198 in rhesus monkeys.

Author

Cornelissen JC, Steele FF, Tenney RD, Obeng S, Rice KC, Zhang Y, and Banks ML

Subjects

Animals, Macaca mulatta, Male, Analgesics, Opioid therapeutic use, Imidazoles therapeutic use, Opioid Peptides therapeutic use, Pain drug therapy, Receptors, Opioid agonists, Spiro Compounds therapeutic use

Abstract

Mu-opioid receptor agonists are clinically effective analgesics, but also produce undesirable effects that limit their clinical utility. The nociceptin opioid peptide (NOP) receptor system also modulates nociception, and NOP agonists might be useful adjuncts to enhance the analgesic effects or attenuate the undesirable effects of mu-opioid agonists. The present study determined behavioral interactions between the NOP agonist (-)-Ro 64-6198 and mu-opioid ligands that vary in mu-opioid receptor efficacy (17-cyclopropylmethyl-3,14β-dihyroxy-4,5α-epoxy-6α-[(3 ́-isoquinolyl)acetamindo]morphinan (NAQ) < buprenorphine < nalbuphine < morphine = oxycodone < methadone) in male rhesus monkeys. For comparison, Ro 64-6198 interactions were also examined with the kappa-opioid receptor agonist nalfurafine. Each opioid ligand was examined alone and following fixed-dose Ro 64-6198 pretreatments in assays of thermal nociception (n = 3-4) and schedule-controlled responding (n = 3). Ro 64-6198 alone failed to produce significant antinociception up to doses (0.32 mg/kg, IM) that significantly decreased rates of responding. All opioid ligands, except NAQ and nalfurafine, produced dose- and thermal intensity-dependent antinociception. Ro 64-6198 enhanced the antinociceptive potency of buprenorphine, nalbuphine, methadone, and nalfurafine. Ro 64-6198 enhancement of nalbuphine antinociception was NOP antagonist SB-612111 reversible and occurred under a narrow range of dose and time conditions. All opioid ligands, except NAQ and buprenorphine, produced dose-dependent decreases in rates of responding. Ro 64-6198 did not significantly alter mu-opioid ligand rate-decreasing effects. Although these results suggest that NOP agonists may selectively enhance the antinociceptive vs. rate-suppressant effects of some mu-opioid agonists, this small enhancement occurred under a narrow range of conditions dampening enthusiasm for NOP agonists as candidate "opioid-sparing" adjuncts., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2019

28. Antinociception by fluoro-loxoprofen, a novel non-steroidal anti-inflammatory drug with less ulcerogenic effects, in rat models of inflammatory pain.

Author

Asano T, Hattori T, Tanaka KI, Yamakawa N, Suemasu S, Aida S, Kataoka M, Mizushima T, and Takenaga M

Subjects

Acute Pain metabolism, Animals, Chronic Pain metabolism, Dinoprostone metabolism, Female, Foot, Male, Rats, Inbred Lew, Rats, Wistar, Acute Pain drug therapy, Analgesics therapeutic use, Anti-Inflammatory Agents, Non-Steroidal therapeutic use, Chronic Pain drug therapy, Phenylpropionates therapeutic use

Abstract

The use of non-steroidal anti-inflammatory drugs (NSAIDs) for the treatment of inflammatory pain is limited by gastrointestinal complications. The rapid action of NSAIDs is associated with better pain relief. Previously, we demonstrated that fluoro-loxoprofen, a novel NSAID, has less ulcerogenic potential than other NSAIDs, attributable to its gastroprotective properties. The aim of this study was to investigate and compare the effects of fluoro-loxoprofen on inflammatory pain in rats with those of other NSAIDs. Oral administration of fluoro-loxoprofen, loxoprofen, and celecoxib resulted in equivalent analgesic action against yeast-induced inflammatory pain. The antinociceptive effect of fluoro-loxoprofen was maximized within 1 h after administration, which is less time than that observed for loxoprofen (2 h) and celecoxib (3 h). We confirmed that both fluoro-loxoprofen and loxoprofen suppressed the increases in prostaglandin E 2 in inflamed paws. In addition to yeast-induced pain, fluoro-loxoprofen produced a similar effect against adjuvant-induced inflammatory pain, with faster peak analgesic effects than those observed for loxoprofen and celecoxib. Taken together, these results suggest that the analgesic effect of fluoro-loxoprofen is equivalent to that of loxoprofen and celecoxib. Moreover, the analgesic effect of fluoro-loxoprofen against inflammatory pain was more rapid than that of other NSAIDs, and this may be associated with its rapid absorption property., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2019

29. Systemic administration of the bifunctional opioid/neuropeptide FF receptors agonist BN-9 produced peripheral antinociception in preclinical mouse models of pain.

Author

Li N, Han ZL, Xu B, Zhang MN, Zhang T, Shi XR, Zhao WD, Guo YY, Zhang QQ, and Fang Q

Subjects

Animals, Disease Models, Animal, Dose-Response Relationship, Drug, Drug Stability, Drug Tolerance, Gastrointestinal Transit drug effects, Male, Mice, Oligopeptides chemistry, Oligopeptides pharmacology, Analgesics therapeutic use, Oligopeptides therapeutic use, Pain drug therapy, Receptors, Neuropeptide agonists

Abstract

We recently characterized a novel bifunctional agonist for opioid and neuropeptide FF receptors, named BN-9, which exhibited potent analgesia in the mouse tail-flick test when given centrally. To further evaluate its potential therapeutic efficacy for translational-medical development, the current work was performed to explore the antinociceptive activities of intraperitoneal (i.p.) administration of BN-9 in mouse models of tail-flick assay, formalin pain, visceral pain and post-operative pain. In the tail-flick test, BN-9 induced a dose-related antinociceptive effect, which was fully blocked by systemic pretreatment with the peripheral acting opioid receptor antagonist naloxone methiodide, but not supraspinal naloxone methiodide, implying the involvement of the peripheral opioid receptors. In addition, the systemic antinociception of BN-9 was antagonized by the selective antagonists of the μ- and κ-opioid receptors, independently of the δ-opioid and neuropeptide FF receptors. Similarly, dose-dependent analgesia was also produced by systemic BN-9 in different pain models via the peripheral opioid receptors, independently of the neuropeptide FF receptors. Furthermore, the side-effects of systemic BN-9 on motor performance, tolerance development and gastrointestinal transit inhibition were also evaluated. Repeated systemic injection of BN-9 produced non-tolerance analgesia over 8 days. Compared with morphine, intraperitoneal administration of BN-9 exerted less inhibition of gastrointestinal transit. These data show that BN-9 induced systemic analgesia with reduced side-effects on tolerance and constipation. This article suggests that systemic injection of BN-9 causes effective antinociception in different preclinical pain models via the peripheral opioid receptors, providing an attractive approach to develop peripherally acting opioid analgesics with multiple targeting properties., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

30. Sumatriptan effects on morphine-induced antinociceptive tolerance and physical dependence: The role of nitric oxide.

Author

Hassanipour M, Rajai N, Rahimi N, Fatemi I, Jalali M, Akbarian R, Shahabaddini A, Nazari A, Amini-Khoei H, and Dehpour AR

Subjects

Animals, Male, Mice, Naloxone pharmacology, Nitric Oxide Synthase antagonists & inhibitors, Nitric Oxide Synthase metabolism, Nitrites metabolism, Sumatriptan therapeutic use, Analgesics pharmacology, Drug Tolerance, Morphine pharmacology, Morphine Dependence drug therapy, Morphine Dependence metabolism, Nitric Oxide metabolism, Sumatriptan pharmacology

Abstract

Sumatriptan, a 5HT (5-hydroxytryptamine) 1B/1D receptor agonist, showed neuroprotection in different studies. The aim of the present study was to investigate the effect of sumatriptan on morphine-induced antinociceptive tolerance and physical dependence. We also investigated the possible role of nitric oxide (NO) on sumatriptan effects. Tolerance was induced by morphine injection (50, 50, 75 mg/kg) three times daily for five days. Antinociceptive latency after acute and chronic treatment with sumatriptan (0.001, 0.01, 0.1 and 1 mg/kg) was measured by hot plate test in morphine-dependent animals. To investigate the possible involvement of NO, different isoforms of nitric oxide synthase (NOS) inhibitors including L-NAME, aminoguanidine and 7-nitroindazole were co-administered with sumatriptan. Nitrite level in mice hippocampus was quantified by Griess method. To examine the role of sumatriptan on physical dependence, three parameters of withdrawal signs were recorded after injection of naloxone (4 mg/kg). Acute treatment with sumatriptan (0.01, 0.1 and 1 mg/kg) attenuated the antinociceptive tolerance (P < 0.001). Chronic injection of sumatriptan (0.001, 0.01 and 0.1 mg/kg), as well, decreased the antinociceptive tolerance (P < 0.001). Moreover, co-administration of NOS inhibitors prevented the effects of sumatriptan. Sumatriptan significantly increased the level of nitrite only after chronic administration. Sumatriptan administration showed no alteration in naloxone-precipitated withdrawal signs. Acute and chronic administration of sumatriptan attenuated morphine antinociceptive tolerance; at least in chronic phase via nitrergic pathway. Our data did not support beneficial effects of sumatriptan on morphine-induced physical dependence in mice., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

31. Phytohormone abscisic acid elicits antinociceptive effects in rats through the activation of opioid and peroxisome proliferator-activated receptors β/δ.

Author

Mollashahi M, Abbasnejad M, and Esmaeili-Mahani S

Subjects

Analgesics, Opioid pharmacology, Animals, Behavior, Animal drug effects, Dose-Response Relationship, Drug, Male, PPAR delta antagonists & inhibitors, PPAR-beta antagonists & inhibitors, Rats, Rats, Wistar, Signal Transduction drug effects, Abscisic Acid pharmacology, Analgesics pharmacology, PPAR delta metabolism, PPAR-beta metabolism, Plant Growth Regulators pharmacology, Receptors, Opioid metabolism

Abstract

The phytohormone abscisic acid exists in animal tissues particularly in the brain. However, its neurophysiological effects have not yet been fully clarified. This study was designed to evaluate the possible antinociceptive effects of abscisic acid on animal models of pain and determine its possible signaling mechanism. Tail-flick, hot-plate and formalin tests were used to assess the nociceptive threshold. All experiments were carried out on male Wistar rats. To determine the role of Peroxisome proliferator-activated receptor β/δ (PPARβ/δ) and opioid receptors on the induction of abscisic acid antinociception, specific antagonists were injected 15 min before abscisic acid. The data showed that abscisic acid (5, 10 and 15 µg/rat, i.c.v.) significantly decreased pain responses in formalin test. In addition, it could also produce dose-dependent antinociceptive effect in tail-flick and hot-plate tests. Administration of PPARβ/δ antagonist (GSK0660, 80 nM, i.c.v.) significantly attenuated the antinociceptive effect of abscisic acid in all tests. The antinociceptive effects of abscisic acid were completely inhibited by naloxone (6 µg, i.c.v.) during the time course of tail-flick and hot-plate tests. The results indicated that the central injection of abscisic acid has potent pain-relieving property which is mediated partly via the PPAR β/δ and opioid signaling., (Copyright © 2018 Elsevier B.V. All rights reserved.)

Published

2018

32. Antinociceptive effects of the endogenous cannabinoid peptide agonist VD-hemopressin(β) in mice.

Author

Wang P, Zheng T, Zhang M, Xu B, Zhang R, Zhang T, Zhao W, Shi X, Zhang Q, and Fang Q

Subjects

Acetic Acid toxicity, Animals, Area Under Curve, Disease Models, Animal, Dose-Response Relationship, Drug, Drug Administration Routes, Indoles administration & dosage, Male, Mice, Mice, Inbred Strains, Pain chemically induced, Pain Measurement, Piperidines administration & dosage, Pyrazoles administration & dosage, Rotarod Performance Test, Spinal Cord drug effects, Spinal Cord physiology, Analgesics therapeutic use, Oligopeptides therapeutic use, Pain drug therapy

Abstract

Cannabinoids (CBs) play important roles in pain modulation. Recently, VD-hemopressin(β) [VD-Hpβ], a 12-residue β-hemoglobin-derived peptide, was reported to activate both CB 1 and CB 2 receptors in vitro. To further characterize in vivo actions of VD-Hpβ, its antinociceptive activity and site(s) were evaluated in the mouse tail-flick test, and supraspinal antinociception of VD-Hpβ was further assessed in the writhing test. Our results demonstrated that supraspinal, intrathecal, subcutaneous and intraperitoneal administrations of VD-Hpβ produced analgesia in the tail-flick test. When given at the same levels, the CB 1 antagonist AM251, rather than the CB 2 antagonist AM630 diminished VD-Hpβ-induced antinociception. Furthermore, our results indicated that supraspinal, intrathecal or subcutaneous pretreatment with AM251 significantly inhibited VD-Hpβ-induced systemic antinociception. In the writhing test, supraspinal VD-Hpβ inhibited pain-related behaviors, which was partially prevented by AM251. Notably, supraspinal administration of VD-Hpβ failed to affect motor function at the antinociceptive doses. These findings suggest that VD-Hpβ induces CB 1 receptor-mediated antinociception in tail-flick test in various routes of administration, and its systemic antinociception is mediated by both central and peripheral CB 1 receptor. In addition, VD-Hpβ produces analgesic activity in the writhing test, which is at least partially mediated by CB 1 receptor. Therefore, our present animal models show a CB 1 agonistic character of VD-Hpβ, an endogenous cannabinoid peptide., (Copyright © 2018 Elsevier Inc. All rights reserved.)

Published

2018

33. Alterations in nociception and morphine antinociception in mice fed a high-fat diet.

Author

Nealon CM, Patel C, Worley BL, Henderson-Redmond AN, Morgan DJ, and Czyzyk TA

Subjects

Animals, Body Weight drug effects, Dose-Response Relationship, Drug, Female, Hyperalgesia drug therapy, Magnetic Resonance Spectroscopy, Male, Mice, Mice, Inbred C57BL, Pain drug therapy, Pain etiology, Pain Measurement drug effects, Sex Characteristics, Body Composition drug effects, Diet, High-Fat, Morphine pharmacology, Narcotics pharmacology, Nociception drug effects

Abstract

Currently, more than 78.6 million adults in the United States are obese. A majority of the patient population receiving treatment for pain symptoms is derived from this subpopulation. Environmental factors, including the increased availability of food high in fat and sugar, contribute to the continued rise in the rates of obesity. The focus of this study was to investigate whether long-term exposure to a high-fat, energy-dense diet enhances baseline thermal and inflammatory nociception while reducing sensitivity to morphine-induced antinociception. Antinociceptive and hypothermic responses to morphine were determined in male and female C57BL/6N mice fed either a "western-style" diet high in fat and sucrose (HED) or a standard low-fat chow diet for 15 weeks. Antinociception was assessed using both the hot plate and tail flick tests of acute thermal pain and the formalin test of inflammatory pain. Acute administration of morphine dose-dependently increased antinociception in the hot plate and tail flick assays for mice of both sexes fed chow and HED. However, female mice displayed lower antinociceptive response to morphine compared to males in the tail-flick test. Hypothermic responses to acute morphine were also assessed in mice fed chow or HED. Male and female mice fed chow, and female mice fed HED displayed similar hypothermic responses to morphine. However, males fed HED did not exhibit morphine-induced hypothermia. Tolerance to the antinociceptive and hypothermic effects of morphine was assessed after ten days of repeated daily administration (10mg/kg morphine). Male mice fed chow or HED developed tolerance to morphine in the hot plate test. However, females fed HED did not. In the tail flick assay, only mice fed HED developed tolerance to morphine. All groups showed tolerance to morphine-induced hypothermia. In the formalin test, we found that both male and female mice fed HED had reduced sensitivity to the antinociceptive effects of morphine (6mg/kg). Collectively, these data suggest that sensitivity and tolerance to the antinociceptive effects of morphine may be dependent on diet and sex in the hot plate and tail flick thermal pain models, and that the acute antinociceptive effects of morphine in the formalin inflammatory pain model may also be dependent on these two factors. In addition, diet and sex can influence morphine-induced hypothermia. Exposure to an HED may lead to changes in neuronal signaling pathways that alter nociceptive responses to noxious stimuli in a sex-specific manner. Thus, dietary modifications might be a useful way to impact pain therapy., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2018

34. Antinociceptive effects of mixtures of mu opioid receptor agonists and cannabinoid receptor agonists in rats: Impact of drug and fixed-dose ratio.

Author

Maguire DR and France CP

Subjects

Animals, Cyclohexanols pharmacology, Dose-Response Relationship, Drug, Dronabinol pharmacology, Drug Interactions, Male, Rats, Rats, Sprague-Dawley, Analgesics pharmacology, Cannabinoid Receptor Agonists pharmacology, Receptors, Opioid, mu metabolism

Abstract

Pain is a significant clinical problem, and there is a need for effective pharmacotherapies with fewer adverse effects than currently available drugs (e.g., mu opioid receptor agonists). Cannabinoid receptor agonists enhance the antinociceptive effects of mu opioid receptor agonists, but it remains unclear which drugs and in what proportion will yield the most effective and safest treatments. The antinociceptive effects of the mu opioid receptor agonists etorphine and morphine alone and in combination with the cannabinoid receptor agonists Δ 9 -THC and CP55940 were studied in male Sprague-Dawley rats (n = 16) using a warm water tail withdrawal procedure. The ratio of opioid to cannabinoid (3:1, 1:1, and 1:3) varied for each mixture. Drugs administered alone or as pairwise mixtures of an opioid and a cannabinoid dose-dependently increased tail withdrawal latency. Mixtures with morphine produced supra-additive (CP55940) and additive (Δ 9 -THC) effects, whereas mixtures with etorphine and either cannabinoid were sub-additive. The interactions were not different among ratios for a particular mixture. The nature of the interaction between opioids and cannabinoids with regard to antinociceptive effects varies with the particular drugs in the mixture, which can have implications for designing combination therapies for pain., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2018

35. Compound action potential inhibition produced by various antidepressants in the frog sciatic nerve.

Author

Hirao R, Fujita T, Sakai A, and Kumamoto E

Subjects

Animals, Dose-Response Relationship, Drug, Action Potentials drug effects, Antidepressive Agents pharmacology, Anura, Sciatic Nerve drug effects, Sciatic Nerve physiology

Abstract

Although an inhibition of action potential conduction in nerve fibers possibly contributes to at least a part of antinociception produced by analgesics and the adjuvants, it has not been fully examined yet how the conduction inhibition differs in extent among their drugs. We investigated the effects of various antidepressants used as analgesic adjuvants on compound action potentials (CAPs) recorded from the frog sciatic nerve by using the air-gap method. The results were compared with those of the other adjuvants that were reported previously. Antidepressants, duloxetine (serotonin and noradrenaline reuptake inhibitor, SNRI), fluoxetine (selective serotonin reuptake inhibitor, SSRI), amitriptyline (tricyclic tertiary amine), desipramine (tricyclic secondary amine) and maprotiline (tetracyclic secondary amine), reduced the peak amplitude of the CAP with half-maximal inhibitory concentration (IC 50 ) values of 0.23, 1.5, 0.26, 1.6 and 0.95mM, respectively. Trazodone (non-SNRI, -SSRI, -tricyclic and -tetracyclic antidepressant) at 1.0mM reduced CAP amplitude by about 50%. The duloxetine and amitriptyline values were comparable to those of lamotrigine and carbamazepine (antiepileptics), dexmedetomidine (α 2 -adrenoceptor agonist) and ropivacaine, levobupivacaine and pramoxine (local anesthetics). The fluoxetine, desipramine, maprotiline and trazodone values were similar to those of oxymetazoline (α 2 -adrenoceptor agonist) and lidocaine, cocaine, procaine and prilocaine (local anesthetics). The antidepressants' IC 50 values were much larger than that of tetracaine (local anesthetic). In conclusion, the six antidepressants inhibited CAPs with efficacies comparable to some antiepileptics, α 2 -adrenoceptor agonists and local anesthetics. It was suggested that antidepressants inhibit nerve conduction with efficacies comparable to those of the other adjuvants., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2018

36. Anti-migraine effect of ∆ 9 -tetrahydrocannabinol in the female rat.

Author

Kandasamy R, Dawson CT, Craft RM, and Morgan MM

Subjects

Animals, Dronabinol therapeutic use, Female, Migraine Disorders metabolism, Rats, Rats, Sprague-Dawley, Receptor, Cannabinoid, CB1 metabolism, Time Factors, Dronabinol pharmacology, Migraine Disorders drug therapy

Abstract

Current anti-migraine treatments have limited efficacy and many side effects. Although anecdotal evidence suggests that marijuana is useful for migraine, this hypothesis has not been tested in a controlled experiment. Thus, the present study tested whether administration of ∆ 9 -tetrahydrocannabinol (THC) produces anti-migraine effects in the female rat. Microinjection of the TRPA1 agonist allyl isothiocyanate (AITC) onto the dura mater produced migraine-like pain for 3h as measured by depression of home cage wheel running. Concurrent systemic administration of 0.32 but not 0.1mg/kg of THC prevented AITC-induced depression of wheel running. However, 0.32mg/kg was ineffective when administered 90min after AITC. Administration of a higher dose of THC (1.0mg/kg) depressed wheel running whether rats were injected with AITC or not. Administration of a CB 1 , but not a CB 2 , receptor antagonist attenuated the anti-migraine effect of THC. These data suggest that: 1) THC reduces migraine-like pain when administered at the right dose (0.32mg/kg) and time (immediately after AITC); 2) THC's anti-migraine effect is mediated by CB 1 receptors; and 3) Wheel running is an effective method to assess migraine treatments because only treatments producing antinociception without disruptive side effects will restore normal activity. These findings support anecdotal evidence for the use of cannabinoids as a treatment for migraine in humans and implicate the CB 1 receptor as a therapeutic target for migraine., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2018

37. 14-O-Methylmorphine: A Novel Selective Mu-Opioid Receptor Agonist with High Efficacy and Affinity.

Author

Zádor F, Balogh M, Váradi A, Zádori ZS, Király K, Szűcs E, Varga B, Lázár B, Hosztafi S, Riba P, Benyhe S, Fürst S, and Al-Khrasani M

Subjects

Animals, Binding, Competitive, Gastrointestinal Transit drug effects, Inhibitory Concentration 50, Male, Mice, Rats, Substrate Specificity, Vas Deferens drug effects, Vas Deferens metabolism, Analgesics metabolism, Analgesics pharmacology, Codeine metabolism, Codeine pharmacology, Receptors, Opioid, mu agonists, Receptors, Opioid, mu metabolism

Abstract

14-O-methyl (14-O-Me) group in morphine-6-O-sulfate (M6SU) or oxymorphone has been reported to be essential for enhanced affinity, potency and antinociceptive effect of these opioids. Herein we report on the pharmacological properties (potency, affinity and efficacy) of the new compound, 14-O-methylmorphine (14-O-MeM) in in vitro. Additionally, we also investigated the antinociceptive effect of the novel compound, as well as its inhibitory action on gastrointestinal transit in in vivo. The potency and efficacy of test compound were measured by [ 35 S]GTPγS binding, isolated mouse vas deferens (MVD) and rat vas deferens (RVD) assays. The affinity of 14-O-MeM for opioid receptors was assessed by radioligand binding and MVD assays. The antinociceptive and gastrointestinal effects of the novel compound were evaluated in the rat tail-flick test and charcoal meal test, respectively. Morphine, DAMGO, Ile 5,6 deltorphin II, deltorphin II and U-69593 were used as reference compounds. 14-O-MeM showed higher efficacy (E max ) and potency (EC 50 ) than morphine in MVD, RVD or [ 35 S]GTPγS binding. In addition, 14-O-MeM compared to morphine showed higher affinity for μ-opioid receptor (MOR). In vivo, in rat tail-flick test 14-O-MeM proved to be stronger antinociceptive agent than morphine after peripheral or central administration. Additionally, both compounds inhibited the gastrointestinal peristalsis. However, when the antinociceptive and antitransit doses for each test compound are compared, 14-O-MeM proved to have slightly more favorable pharmacological profile. Our results affirm that 14-O-MeM, an opioid of high efficacy and affinity for MOR can be considered as a novel analgesic agent of potential clinical value., (Copyright © 2017 Elsevier B.V. All rights reserved.)

Published

2017

38. Role of prefrontal cortical calcium-independent phospholipase A 2 in antinociceptive effect of the norepinephrine reuptake inhibitor antidepresssant maprotiline.

Author

Chew WS, Shalini SM, Torta F, Wenk MR, Stohler C, Yeo JF, Herr DR, and Ong WY

Subjects

Adrenergic Uptake Inhibitors pharmacology, Animals, Antidepressive Agents, Second-Generation pharmacology, Carrageenan, Disease Models, Animal, Docosahexaenoic Acids metabolism, Eicosapentaenoic Acid metabolism, Facial Pain immunology, Group VI Phospholipases A2 antagonists & inhibitors, Group VI Phospholipases A2 genetics, Male, Mice, Inbred C57BL, Pain Threshold drug effects, Pain Threshold physiology, Prefrontal Cortex immunology, RNA, Messenger metabolism, Somatosensory Cortex drug effects, Somatosensory Cortex metabolism, Analgesics pharmacology, Facial Pain drug therapy, Group VI Phospholipases A2 metabolism, Maprotiline pharmacology, Prefrontal Cortex drug effects

Abstract

The prefrontal cortex is essential for executive functions such as decision-making and planning. There is also accumulating evidence that it is important for the modulation of pain. In this study, we investigated a possible role of prefrontal cortical calcium-independent phospholipase A 2 (iPLA 2 ) in antinociception induced by the norepinephrine reuptake inhibitor (NRI) and tetracyclic (tricyclic) antidepressant, maprotiline. Intraperitoneal injections of maprotiline increased iPLA 2 mRNA and protein expression in the prefrontal cortex. This treatment also reduced grooming responses to von-Frey hair stimulation of the face after facial carrageenan injection, indicating decreased sensitivity to pain. The antinociceptive effect of maprotiline was abrogated by iPLA 2 antisense oligonucleotide injection to the prefrontal cortex, indicating a role of this enzyme in antinociception. In contrast, injection of iPLA 2 antisense oligonucleotide to the somatosensory cortex did not reduce the antinociceptive effect of maprotiline. Lipidomic analysis of the prefrontal cortex showed decrease in phosphatidylcholine species, but increase in lysophosphatidylcholine species, indicating increased PLA2 activity, and release of docosahexaenoic acid (DHA) and eicosapentaenoic acid (EPA) after maprotiline treatment. Differences in sphingomyelin/ceramide were also detected. These changes were not observed in maprotiline-treated mice that received iPLA 2 antisense oligonucleotide to the prefrontal cortex. Metabolites of DHA and EPA may help to strengthen a known supraspinal antinociceptive pathway from the prefrontal cortex to the periaqueductal gray. Together, results indicate a role of prefrontal cortical iPLA 2 and its enzymatic products in the antinociceptive effect of maprotiline., (Copyright © 2016 IBRO. Published by Elsevier Ltd. All rights reserved.)

Published

2017

39. Histone deacetylase inhibitor-induced emergence of synaptic δ-opioid receptors and behavioral antinociception in persistent neuropathic pain.

Author

Tao W, Zhou W, Wang Y, Sun T, Wang H, Zhang Z, and Jin Y

Subjects

Animals, Cell Membrane drug effects, Cell Membrane metabolism, Chronic Pain metabolism, Disease Models, Animal, Epigenesis, Genetic, Histones metabolism, Hydroxamic Acids metabolism, Male, Neuralgia metabolism, Nucleus Raphe Magnus drug effects, Nucleus Raphe Magnus metabolism, Rats, Wistar, Receptors, Opioid, delta agonists, Sciatic Nerve physiopathology, Synapses drug effects, Time Factors, Tissue Culture Techniques, Analgesics pharmacology, Chronic Pain drug therapy, Histone Deacetylase Inhibitors pharmacology, Neuralgia drug therapy, Receptors, Opioid, delta metabolism, Synapses metabolism

Abstract

The efficacy of opioids in patients with chronic neuropathic pain remains controversial. Although activation of δ-opioid receptors (DORs) in the brainstem reduces inflammation-induced persistent hyperalgesia, it is not effective under persistent neuropathic pain conditions and these clinical problems remain largely unknown. In this study, by using a chronic constriction injury (CCI) of the sciatic nerve in rats, we found that in the brainstem nucleus raphe magnus (NRM), DORs emerged on the surface membrane of central synaptic terminals on day 3 after CCI surgery and disappeared on day 14. Histone deacetylase (HDAC) inhibitors microinjected into the NRM in vivo increased the level of synaptosomal DOR protein and NRM infusion of DOR agonists producing an antinociceptive effect in a nerve growth factor (NGF) signaling-dependent manner. In vitro, in CCI rat slices incubated with HDAC inhibitors, DOR agonists significantly inhibited EPSCs. This effect was blocked by tyrosine receptor kinase A antagonists. Chromatin immunoprecipitation analysis revealed that NRM infusion of HDAC inhibitors in CCI rats increased the level of histone H4 acetylation at Ngf gene promoter regions. NGF was infused into the NRM or incubated CCI rat slices drove DORs to the surface membrane of synaptic terminals. Taken together, epigenetic upregulation of NGF activity by HDAC inhibitors in the NRM promotes the trafficking of DORs to pain-modulating neuronal synapses under neuropathic pain conditions, leading to δ-opioid analgesia. These findings indicate that therapeutic use of DOR agonists combined with HDAC inhibitors might be effective in chronic neuropathic pain managements., (Copyright © 2016 IBRO. Published by Elsevier Ltd. All rights reserved.)

Published

2016

40. Adenosine receptor targets for pain.

Author

Sawynok J

Subjects

Animals, Humans, Analgesics, Non-Narcotic pharmacology, Analgesics, Non-Narcotic therapeutic use, Pain drug therapy, Pain metabolism, Receptors, Purinergic P1 metabolism

Abstract

The main focus for the development of adenosine targets as analgesics to date has been A 1 Rs due to its antinociceptive profile in various preclinical pain models. The usefulness of systemic A 1 R agonists may be limited by other effects (cardiovascular, motor), but enhanced selectivity for pain might occur with partial agonists, potent and highly selective agonists, or allosteric modulators. A 2A R agonists exhibit some peripheral pronociceptive effects, but also act on immune cells to suppress inflammation and on spinal glia to suppress pain signaling and may be useful for inflammatory and neuropathic pain. A 2B R agonists exhibit peripheral proinflammatory effects on immune cells, but also spinal antinociceptive effects similar to A 2A R agonists. A 3 Rs are now demonstrated to produce antinociception in several preclinical neuropathic pain models, with mechanistic actions on glial cells, and may be useful for neuropathic pain. Endogenous adenosine levels can be augmented by inhibition of metabolism (via adenosine kinase) or increased generation (via nucleotidases), and these approaches have implications for pain. Endogenous adenosine contributes to antinociception by several pharmacological agents, herbal remedies, acupuncture, transcutaneous electrical nerve stimulation, exercise, joint mobilization, and water immersion via spinal and/or peripheral effects, such that this system appears to constitute a major pain regulatory system. Finally, caffeine inhibits A 1 -, A 2A - and A 3 Rs with similar potency, and dietary caffeine intake will need attention in trials of: (a) agonists and/or modulators acting at these receptors, (b) some pharmacological and herbal analgesics, and (c) manipulations that enhance endogenous adenosine levels, all of which are inhibited by caffeine and/or A 1 R antagonists in preclinical studies. All adenosine receptors have effects on spinal glial cells in regulating nociception, and gender differences in the involvement of such cells in chronic neuropathic pain indicate gender may also need attention in preclinical and human trials evaluating the efficacy of adenosine-based analgesics., (Copyright © 2015 IBRO. Published by Elsevier Ltd. All rights reserved.)

Published

2016

41. Analysis of morphine-induced changes in the activity of periaqueductal gray neurons in the intact rat.

Author

Tryon VL, Mizumori SJ, and Morgan MM

Subjects

Animals, Drug Tolerance physiology, Male, Medulla Oblongata drug effects, Microinjections methods, Pain drug therapy, Pain Measurement drug effects, Periaqueductal Gray physiopathology, Rats, Sprague-Dawley, Analgesics, Opioid pharmacology, Morphine pharmacology, Neurons drug effects, Periaqueductal Gray drug effects

Abstract

Microinjection of morphine into the periaqueductal gray (PAG) produces antinociception. In vitro slice recordings indicate that all PAG neurons are sensitive to morphine either by direct inhibition or indirect disinhibition. We tested the hypothesis that all PAG neurons respond to opioids in vivo by examining the extracellular activity of PAG neurons recorded in lightly anesthetized and awake rats. Spontaneous activity was less than 1Hz in most neurons. Noxious stimuli (heat, pinch) caused an increase in activity in 57% and 75% of the neurons recorded in anesthetized and awake rats, respectively. The same noxious stimuli caused a decrease in activity in only 17% and 6% of neurons recorded in anesthetized and awake rats. Systemic administration of morphine caused approximately equal numbers of neurons to increase, decrease, or show no change in activity in lightly anesthetized rats. In contrast, administration of morphine caused an increase in the activity of 22 of the 27 neurons recorded in awake rats. No change in activity was evident in the remaining five neurons. Changes in activity caused by morphine were surprisingly modest (a median increase from 0.7 to 1.3Hz). The small inconsistent effects of morphine are in stark contrast to the large changes produced by morphine on the activity of rostral ventromedial medulla (RVM) neurons or the widespread inhibition and excitation of PAG neurons treated with opioids in in vitro slice experiments. The relatively modest effects of morphine in the present study suggest that morphine produces antinociception by causing small changes in the activity of many PAG neurons., (Copyright © 2016 IBRO. Published by Elsevier Ltd. All rights reserved.)

Published

2016

42. Prohormone convertase 2 (PC2) null mice have increased mu opioid receptor levels accompanied by altered morphine-induced antinociception, tolerance and dependence.

Author

Lutfy K, Parikh D, Lee DL, Liu Y, Ferrini MG, Hamid A, and Friedman TC

Subjects

Animals, Brain drug effects, Brain metabolism, Brain pathology, Dose-Response Relationship, Drug, Drug Tolerance physiology, Male, Mice, 129 Strain, Mice, Inbred C57BL, Mice, Knockout, Morphine Dependence pathology, Naloxone pharmacology, Narcotic Antagonists pharmacology, Nociceptive Pain metabolism, Proprotein Convertase 2 genetics, Substance Withdrawal Syndrome metabolism, Substance Withdrawal Syndrome pathology, Analgesics, Opioid pharmacology, Morphine pharmacology, Morphine Dependence metabolism, Nociceptive Pain drug therapy, Proprotein Convertase 2 deficiency, Receptors, Opioid, mu metabolism

Abstract

Chronic morphine treatment increases the levels of prohormone convertase 2 (PC2) in brain regions involved in nociception, tolerance and dependence. Thus, we tested if PC2 null mice exhibit altered morphine-induced antinociception, tolerance and dependence. PC2 null mice and their wild-type controls were tested for baseline hot plate latency, injected with morphine (1.25-10mg/kg) and tested for antinociception 30min later. For tolerance studies, mice were tested in the hot plate test before and 30min following morphine (5mg/kg) on day 1. Mice then received an additional dose so that the final dose of morphine was 10mg/kg on this day. On days 2-4, mice received additional doses of morphine (20, 40 and 80mg/kg on days 1, 2, 3, and 4, respectively). On day 5, mice were tested in the hot plate test before and 30min following morphine (5mg/kg). For withdrawal studies, mice were treated with the escalating doses of morphine (10, 20, 40 and 80mg/kg) for 4days, implanted with a morphine pellet on day 5 and 3 days later injected with naloxone (1mg/kg) and signs of withdrawal were recorded. Morphine dose-dependently induced antinociception and the magnitude of this response was greater in PC2 null mice. Tolerance to morphine was observed in wild-type mice and this phenomenon was blunted in PC2 null mice. Withdrawal signs were also reduced in PC2 null mice. Immunohistochemical studies showed up-regulation of the mu opioid receptor (MOP) protein expression in the periaqueductal gray area, ventral tegmental area, lateral hypothalamus, medial hypothalamus, nucleus accumbens, and somatosensory cortex in PC2 null mice. Likewise, naloxone specific binding was increased in the brains of these mice compared to their wild-type controls. The results suggest that the PC2-derived peptides may play a functional role in morphine-induced antinociception, tolerance and dependence. Alternatively, lack of opioid peptides led to up-regulation of the MOP and altered morphine-induced antinociception, tolerance and dependence., (Copyright © 2016 IBRO. Published by Elsevier Ltd. All rights reserved.)

Published

2016

43. Increasing the availability of l-arginine and nitric oxide increases sensitivity of nitrous oxide (N2O)-insensitive inbred mice to N2O-induced antinociception.

Author

Chung E, Ohgami Y, and Quock RM

Subjects

Abdominal Pain complications, Analysis of Variance, Animals, Disease Models, Animal, Dose-Response Relationship, Drug, Drug Synergism, Male, Mice, Mice, Inbred C57BL, Mice, Inbred DBA, Molsidomine analogs & derivatives, Molsidomine pharmacology, Nitric Oxide Donors pharmacology, Species Specificity, Abdominal Pain drug therapy, Analgesics therapeutic use, Arginine therapeutic use, Nitric Oxide therapeutic use, Nitrous Oxide therapeutic use, Pain Threshold drug effects

Abstract

Nitrous oxide (N2O)-induced antinociception in mice is dependent on the neuromodulator nitric oxide (NO). In contrast to C57BL/6J (B6) mice, DBA/2J (D2) mice fail to respond to N2O with a robust antinociceptive response or with an increase in brain nitric oxide synthase (NOS) enzyme activity, suggesting that failure of D2 mice to respond to N2O might result from a deficit of NO function. Therefore, it was of interest to determine whether increasing the availability of NO might increase sensitivity of D2 mice to N2O. Male D2 mice were pretreated with sub-antinociceptive intracerebroventricular doses of the NO donor 3-morpholinosydnoimine or the NO precursor l-arginine then assessed for responsiveness to N2O-induced antinociception using the acetic acid abdominal constriction test. Both pretreatments increased the antinociceptive responsiveness of D2 mice to N2O. These results indicate that the NOS enzyme in D2 mice is functional and that the deficit in NO function that obstructs sensitivity to N2O-induced antinociception may lie in availability or utilization of l-arginine., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

44. Atorvastatin attenuates the antinociceptive tolerance of morphine via nitric oxide dependent pathway in male mice.

Author

Hassanipour M, Amini-Khoei H, Shafaroodi H, Shirzadian A, Rahimi N, Imran-Khan M, Rezayat SM, and Dehpour A

Subjects

Animals, Arginine pharmacology, Disease Models, Animal, Dose-Response Relationship, Drug, Drug Tolerance, Enzyme Inhibitors pharmacology, Hydroxymethylglutaryl-CoA Reductase Inhibitors pharmacology, Hydroxymethylglutaryl-CoA Reductase Inhibitors therapeutic use, Male, Mice, NG-Nitroarginine Methyl Ester pharmacology, Narcotics adverse effects, Pain Measurement, Atorvastatin pharmacology, Atorvastatin therapeutic use, Morphine adverse effects, Nitric Oxide metabolism, Opioid-Related Disorders drug therapy, Pain Threshold drug effects, Signal Transduction drug effects

Abstract

The development of morphine-induced antinociceptive tolerance limits its therapeutic efficacy in pain management. Atorvastatin, or competitive inhibitor of 3-hydroxy-methyl-glutaryl coenzyme A (HMG-CoA) reductase, is mainstay agent in hypercholesterolemia treatment. Beyond the cholesterol-lowering activity, exploration of neuroprotective properties of this statin indicates its potential benefit in central nervous disorders. The aim of the present study was to assess the effects of atorvastatin in development and expression of morphine-induced analgesic tolerance in male mice and probable involvement of nitric oxide. Chronic and acute treatment with atorvastatin 10 and 20mg/kg, respectively, could alleviate morphine tolerance in development and expression phases. Chronic co-administration of nitric oxide synthase (NOS) inhibitors including L-NAME (non selective NOS inhibitor; 2mg/kg), aminoguanidine (selective inducible NOS inhibitor; 50mg/kg) and 7-NI (selective neuronal NOS inhibitor; 15mg/kg) with atorvastatin blocked the protective effect of atorvastatin in tolerance reversal. Moreover, reversing the atorvastatin effect was also observed in acute simultaneous treatment of L-NAME (5mg/kg) and aminoguanidine (100mg/kg) with atorvastatin. Co-treatment of guanylyl cyclase inhibitor, ODQ (chronic dose: 10mg/kg and acute dose: 20mg/kg) was associated with prevention of atorvastatin anti-tolerance properties. Our results revealed that the atorvastatin modulating role in morphine antinociceptive tolerance is mediated at least in part via nitric oxide in animal pain models of hot plate and tail flick., (Copyright © 2016 Elsevier Inc. All rights reserved.)

Published

2016

45. Sex differences in hypothalamic-mediated tonic norepinephrine release for thermal hyperalgesia in rats.

Author

Wagner M, Banerjee T, Jeong Y, and Holden JE

Subjects

Adrenergic alpha-Antagonists pharmacology, Animals, Cobalt pharmacology, Constriction, Pathologic, Dioxanes pharmacology, Disease Models, Animal, Female, Hot Temperature, Hyperalgesia drug therapy, Hypothalamus drug effects, Male, Random Allocation, Rats, Sprague-Dawley, Receptors, Adrenergic, alpha-1 metabolism, Receptors, Adrenergic, alpha-2 metabolism, Sciatic Nerve injuries, Yohimbine pharmacology, Hyperalgesia physiopathology, Hypothalamus physiopathology, Neuralgia physiopathology, Nociceptive Pain physiopathology, Norepinephrine metabolism, Sex Characteristics

Abstract

Neuropathic pain is treated using serotonin norepinephrine reuptake inhibitors with mixed results. Pain facilitation mediated by α1-adrenoceptors may be involved, but whether norepinephrine (NE) is tonically released is unclear. The aim of this study was to determine whether NE is tonically released from A7 cells following chronic constriction injury (CCI), and if the lateral hypothalamus (LH) plays a role in this release in male and female rats with nociceptive and neuropathic pain types. Neuropathic groups received left CCI while nociceptive groups remained naïve to injury. Fourteen days later, rats were given intrathecal infusion of either the α1-adrenoceptor antagonist WB4101, the α2-adrenoceptor antagonist yohimbine (74 μg), or normal saline for control. Paw withdrawal latency (PWL) from a thermal stimulus was measured. The generalized estimated equation method was used for statistical analysis. Nociceptive rats given WB4101 had a PWL significantly longer than saline control (7.89 ± 0.63 vs. 5.87 ± 0.52 s), while the PWL of neuropathic rats given WB4101 was 13.20 ± 0.52 s compared to 6.78 ± 0.52 s for the saline control rats. Yohimbine had no significant effect. Microinjection of cobalt chloride (CoCl) in the A7 catecholamine cell group to prevent synaptic transmission blocked the effect of WB4101 in all groups, supporting the notion that spinally descending A7 cells tonically release NE that contributes to α1-mediated nociceptive facilitation. Microinjection of CoCl into the left LH blocked the effect of WB4101 in nociceptive and neuropathic male rats, but had no effect in female rats of either pain type, suggesting differential innervation. These findings indicate that tonic release of NE acts at pronociceptive α1-adrenoceptors, that this effect is greater in rats with nerve damage, and that, while NE comes primarily from the A7 cell group, LH innervation of the A7 cell group is different between the sexes., (Copyright © 2016 IBRO. Published by Elsevier Ltd. All rights reserved.)

Published

2016

46. Involvement of opioid receptors in the systemic and peripheral antinociceptive actions of montelukast in the animal models of pain.

Author

Ghorbanzadeh B, Mansouri MT, Sahraei H, and Alboghobeish S

Subjects

Acetates therapeutic use, Acetic Acid adverse effects, Analgesics therapeutic use, Animals, Behavior, Animal drug effects, Cyclopropanes, Disease Models, Animal, Drug Synergism, Formaldehyde adverse effects, Male, Mice, Naloxone pharmacology, Pain chemically induced, Quinolines therapeutic use, Rats, Sulfides, Visceral Pain drug therapy, Acetates administration & dosage, Acetates pharmacology, Analgesics pharmacology, Pain drug therapy, Pain metabolism, Quinolines administration & dosage, Quinolines pharmacology, Receptors, Opioid metabolism

Abstract

This study aimed to investigate the involvement of opioid receptors in the systemic and peripheral antinociceptive activities of montelukast in different animal models of pain. Rats and mice were injected with montelukast to produce analgesia. The formalin and acetic acid-induced writhing tests were used to assess the nociceptive activity. The results showed that i.p. administration of montelukast (0.3-10mg/kg) dose-dependently reduced flinching behavior in both the first and second phases of formalin test with mean ED50 of 0.55 and 5.31mg/kg, respectively. Also, intraplantar administration of montelukast (3-30μg/paw) produced antinociception against the two phases of formalin assay in a dose-dependent way with mean ED30 of 2.92 and 8.11μg/paw, respectively. Furthermore, pre-treatment with naloxone (a non-selective opioid receptor antagonist) significantly inhibited both the systemic and also peripheral antinociceptive actions of montelukast in formalin test. In writhing test, the results showed that intraperitoneal administration of montelukast (3-10mg/kg) significantly reduced the writhe number induced by acetic acid in mice. Moreover, co-administration of non-effective doses of montelukast (0.3 and 1mg/kg; i.p.) and morphine (0.25mg/kg; i.p.) significantly decreased the writhes number induced by acetic acid. Also, this effect was naloxone-reversible. These findings suggest that the systemic and peripheral antinociception produced by montelukast were mediated through the opioid receptors in central and peripheral nervous systems. Moreover, combination of montelukast and morphine could be noted as a new strategy for pain relief., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

47. Morphine-induced antinociception and reward in "humanized" mice expressing the mu opioid receptor A118G polymorphism.

Author

Henderson-Redmond AN, Yuill MB, Lowe TE, Kline AM, Zee ML, Guindon J, and Morgan DJ

Subjects

Alleles, Analgesics metabolism, Analgesics pharmacology, Analgesics, Opioid pharmacology, Animals, Drug Tolerance genetics, Female, Male, Mice, Mice, Transgenic, Morphine pharmacology, Pain drug therapy, Pain Measurement drug effects, Polymorphism, Single Nucleotide genetics, Pain genetics, Receptors, Opioid, mu genetics, Receptors, Opioid, mu metabolism

Abstract

The rewarding and antinociceptive effects of opioids are mediated through the mu-opioid receptor. The A118G single nucleotide polymorphism in this receptor has been implicated in drug addiction and differences in pain response. Clinical and preclinical studies have found that the G allele is associated with increased heroin reward and self-administration, elevated post-operative pain, and reduced analgesic responsiveness to opioids. Male and female mice homozygous for the "humanized" 118AA or 118GG alleles were evaluated to test the hypothesis that 118GG mice are less sensitive to the rewarding and antinociceptive effects of morphine. We found that 118AA and 118GG mice of both genders developed conditioned place preference for morphine. All mice developed tolerance to the antinociceptive and hypothermic effects of morphine. However, morphine tolerance was not different between AA and GG mice. We also examined sensitivity to the antinociceptive and hypothermic effects of cumulative morphine doses. We found that 118GG mice show reduced hypothermic and antinociceptive responses on the hotplate for 10mg/kg morphine. Finally, we examined basal pain response and morphine-induced antinociception in the formalin test for inflammatory pain. We found no gender or genotype differences in either basal pain response or morphine-induced antinociception in the formalin test. Our data suggests that homozygous expression of the GG allele in mice blunts morphine-induced hypothermia and hotplate antinociception but does not alter morphine CPP, morphine tolerance, or basal inflammatory pain response., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2016

48. Distinguishing subgroups among μ-opioid receptor agonists using Na(+),K(+)-ATPase as an effector mechanism.

Author

Masocha W, González LG, and Agil A

Subjects

Animals, Female, Mice, Neurons cytology, Ouabain pharmacology, Sodium-Potassium-Exchanging ATPase antagonists & inhibitors, Synaptosomes drug effects, Synaptosomes enzymology, Analgesics pharmacology, Receptors, Opioid, mu agonists, Sodium-Potassium-Exchanging ATPase metabolism

Abstract

We evaluated the effects of intracerebroventricular administration of ouabain on the antinociception induced by five μ-opioid receptor agonists in a tail flick test on female CD-1 mice and the effects of these μ-opioid receptor agonists on mice forebrain synaptosomal ouabain-sensitive Na(+),K(+)-ATPase activity. The subcutaneous administration of the μ-opioid receptor agonists tested produced a dose-dependent antinociceptive effect. The antinociception induced by morphine (1-32 mg/kg), levorphanol (0.4-6.4 mg/kg), and buprenorphine (0.02-0.64 mg/kg) was antagonised in a dose-dependent manner by ouabain (0.001-10 ng, i.c.v.), whilst the antinociception produced by fentanyl (0.02-0.16 mg/kg) and methadone (2-10 mg/kg) was not influenced significantly by ouabain (1-100 ng, i.c.v.). Incubation in vitro of forebrain synaptosomes with morphine (10(-9)-10(-4) M), levorphanol (10(-10)-10(-4) M), buprenorphine (10(-10)-10(-5) M), or fentanyl (10(-10)-10(-5) M) stimulated significantly ouabain-sensitive Na(+),K(+)-ATPase activity in a concentration-dependent way. The order of efficacy (using the Emax as a measure of intrinsic efficacy) was: morphine (29.83±0.56%)>levorphanol (18.61±1.26%)>buprenorphine (14.91±0.74%)>fentanyl (10.10±1.73%). On the other hand, methadone (10(-10)-10(-5) M) did not significantly modify the ouabain-sensitive Na(+),K(+)-ATPase activity (Emax=5.11±0.92%). These results suggest that Na(+),K(+)-ATPase activity is involved in the antinociceptive effects of morphine, levorphanol and buprenorphine, but not in that produced by fentanyl and methadone. Thus, we can conclude that at least two subgroups can be distinguished among the μ-opioid receptor agonists taking into consideration the role of Na(+),K(+)-ATPase in their antinociceptive effects., (Copyright © 2016 Elsevier B.V. All rights reserved.)

Published

2016

49. Antinociception of spirocyclopiperazinium salt compound LXM-10-M targeting α7 nicotinic receptor and M4 muscarinic receptor and inhibiting CaMKIIα/CREB/CGRP signaling pathway in mice.

Author

Wan D, Wang D, Sun Q, Song Y, Jiang Y, Li R, and Ye J

Subjects

Analgesics chemistry, Analgesics pharmacology, Analgesics toxicity, Animals, Calcitonin Gene-Related Peptide metabolism, Calcium-Calmodulin-Dependent Protein Kinase Type 2 metabolism, Cyclic AMP Response Element-Binding Protein metabolism, Female, Gene Expression Regulation drug effects, Male, Mice, Piperazines toxicity, Spinal Cord drug effects, Spinal Cord metabolism, Spiro Compounds pharmacology, Spiro Compounds toxicity, Piperazines chemistry, Piperazines pharmacology, Receptor, Muscarinic M4 metabolism, Salts chemistry, Signal Transduction drug effects, Spiro Compounds chemistry, alpha7 Nicotinic Acetylcholine Receptor metabolism

Abstract

The present study was designed to investigate the antinociception of spirocyclopiperazinium salt compound LXM-10-M (2,4-dimethyl-9-β-m-hydroxyphenylethyl-3-oxo-6, 9-diazaspiro [5.5] undecane chloride) in thermal and chemical pain models, and further to explore the molecular target and potential signal pathway. We assessed the antinociception of LXM-10-M in hot-plate test, formalin test and acetic acid writhing test in mice. The possible changes of calcium/calmodulin-dependent protein kinase IIα (CaMKIIα)/cAMP response element-binding protein (CREB)/calcitonin gene related peptide (CGRP) signaling pathway were detected by Western Blot in mice. Administration of LXM-10-M produced significant antinociception in hot-plate test, formalin test and acetic acid writhing test in mice, with no obvious toxicity. The antinociceptive effects were blocked by pretreatment with methyllycaconitine citrate (MLA, α7 nicotinic receptor antagonist) or tropicamide (TRO, M4 muscarinic receptor antagonist). Western blot analysis showed that the upregulations of p-CaMKIIα, p-CREB and CGRP in the spinal cord were reduced by LXM-10-M in chemical pain model in mice, and the effects were blocked by MLA or TRO pretreatment. This is the first paper to report that LXM-10-M exerted significant antinociception, which may be attributed to the activation of α7 nicotinic receptor and M4 muscarinic receptor and thereby triggering the inhibition of CaMKIIα/CREB/CGRP signaling pathway in mice., (Copyright © 2015 Elsevier B.V. All rights reserved.)

Published

2016

50. Differential effects of lacosamide, phenytoin and topiramate on peripheral nerve excitability: An ex vivo electrophysiological study.

Author

Zafeiridou G, Spilioti M, Kagiava A, Krikonis K, Kosmidis EK, Karlovasitou A, and Kimiskidis VK

Subjects

Animals, Dose-Response Relationship, Drug, Electric Stimulation, Female, Fructose adverse effects, In Vitro Techniques, Lacosamide, Male, Rats, Sciatic Nerve physiology, Topiramate, Acetamides adverse effects, Action Potentials drug effects, Fructose analogs & derivatives, Phenytoin adverse effects, Sciatic Nerve drug effects

Abstract

Background: Antiepileptic drugs (AEDs) are mainly used to control cortical hyperexcitability. Some of them (e.g. phenytoin (PHT) and topiramate (TPM)) have also effects on the peripheral nervous system (PNS). Lacosamide (LCM) is a novel AED that stabilizes hyperexcitable neuronal membranes by selectively enhancing the slow inactivation of voltage-gated sodium channels (VGSCs). Although the mechanism of action of LCM is fairly well understood, there are no in vitro data available regarding any possible PNS effects of LCM., Objective: To investigate, in vitro, the effects of LCM on peripheral nerve excitability in comparison with PHT and TPM, two AEDs that act, in part, by stabilizing the fast inactivation state of VGSCs., Methods: Experiments were conducted on the isolated sciatic nerve of the adult rat using standard electrophysiological methods. The effects of LCM on the amplitude and latency of the evoked compound action potential (CAP) during a 48h period of drug exposure were recorded and compared with the effects of PHT and TPM., Results: LCM produced inhibitory effects on CAP at concentrations significantly higher than the therapeutic levels (>25μg/ml). At these concentrations (62.57-125.15μg/ml), an acute and immediate increment of the latency and decrement of the amplitude of the CAP were observed. In contrast to LCM, PHT caused an acute decrement in the amplitude as well as an increment in the latency of the CAP even at subtherapeutic levels (5μg/ml). With regard to TPM, the amplitude of the CAP was not affected at the supratherapeutic concentrations but at the therapeutic concentration of 33.94μg/ml a reduced decrement of the CAP amplitude compared to the controls was observed., Conclusions: LCM, PHT and TPM exert differential effects on peripheral nerve excitability. PHT inhibited the sciatic nerve CAP even at subtherapeutic levels whereas LCM was safe within the therapeutic concentration range. TPM did not affect the CAP amplitude even at high supratherapeutic concentrations whereas in the therapeutic range a neuroprotective effect was observed. Possible underlying mechanisms and the clinical implications of these findings are discussed., (Copyright © 2015 Elsevier Inc. All rights reserved.)

Published

2016