Synergistic antinociceptive effects of anandamide, an endocannabinoid, and nonsteroidal anti-inflammatory drugs in peripheral tissue: A role for endogenous fatty-acid ethanolamides?

Guindon, Josée; LoVerme, Jesse; Léan, André De; Piomelli, Daniele; Beaulieu, Pierre

doi:10.1016/j.ejphar.2006.08.045

Cited by 51 publications

(43 citation statements)

References 51 publications

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“…The PPAR-α receptor agonist GW7647 and anandamide were found to produce synergistic antinociception in this same study. In addition combination of anandamide and the COX-2 inhibitor, rofecoxib, synergistically decrease pain in the formalin model and to increase levels of AEA, OEA, and PEA in the formalin treated paw (Guindon et al, 2006). These findings suggest that the antiedema effects of FAAH inhibition may be mediated by multiple mechanisms and that the results from these combination studies should be extended to investigate their effects on inflammation.…”

Section: Discussionmentioning

confidence: 89%

Evaluation of fatty acid amides in the carrageenan-induced paw edema model

et al. 2008

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While it has long been recognized that Δ 9 -tetrahydrocannabinol (THC), the primary psychoactive constituent of cannabis, and other cannabinoid receptor agonists possess anti-inflammatory properties, their well known CNS effects have dampened enthusiasm for therapeutic development. On the other hand, genetic deletion of fatty acid amide hydrolase (FAAH), the enzyme responsible for degradation of fatty acid amides, including endogenous cannabinoid N-arachidonoyl ethanolamine (anandamide; AEA), N-palmitoyl ethanolamine (PEA), N-oleoyl ethanolamine (OEA), and oleamide, also elicits anti-edema, but does not produce any apparent cannabinoid effects. The purpose of the present study was to investigate whether exogenous administration of FAAs would augment the anti-inflammatory phenotype of FAAH (-/-) mice in the carrageenan model. Thus, we evaluated the effects of the FAAs AEA, PEA, OEA, and oleamide in wild-type and FAAH (-/-) mice. For comparison, we evaluated the anti-edema effects of THC, dexamethasone (DEX), a synthetic glucocorticoid, diclofenac (DIC), a nonselective cyclooxygenase (COX) inhibitor, in both genotypes. A final study determined if tolerance to the anti-edema effects of PEA occurs after repeated dosing. PEA, THC, DEX, DIC elicited significant decreases in carrageenan-induced paw edema in wild type mice. In contrast OEA produced a less reliable anti-edema effect than these other drugs, and AEA and oleamide failed to produce any significant decreases in paw edema. Moreover, none of the agents evaluated augmented the anti-edema phenotype of FAAH (-/-) mice, suggesting that maximal antiedema effects had already been established. PEA was the most effective FAA in preventing paw edema and its effects did not undergo tolerance. While the present findings do not support a role for AEA in preventing carrageenan-induced edema, PEA administration and FAAH blockade elicited anti-edema effects of an equivalent magnitude as produced by THC, DEX, and DIC in this assay.

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Section: Discussionmentioning

confidence: 89%

Evaluation of fatty acid amides in the carrageenan-induced paw edema model

et al. 2008

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“…Allosteric modulators of CB 1 receptors may therefore be a useful strategy for amplifying effects of ECs only at sites where they are produced and released on demand (Laprairie et al, 2017). Nonetheless, multifunctional compounds targeting the ECS allied to inhibition of COX2 (Grim et al, 2014), antagonism of TRPV1 (Maione et al, 2006; or in combination with opioids (Wilson-Poe et al, 2013) or non-steroidal anti-inflammatory drugs (Guindon et al, 2006) have great potential to produce a superior therapeutic profile with minimized unwanted cannabimimetic side effects. A novel therapeutic approach in many pathological states can be the possible modulation of EC activity through the regulation of their synthesis or degradation.…”

Section: Figure 10mentioning

confidence: 99%

Effects of centrally administered endocannabinoids and opioids on orofacial pain perception in rats

Zubrzycki

Janecka

Liebold

et al. 2017

British J Pharmacology

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BACKGROUND AND PURPOSEEndocannabinoids and opioids play a vital role in mediating pain-induced analgesia. The specific effects of these compounds within the orofacial region are largely unknown. In this study, we tried to determine whether an increase in cannabinoid and opioid concentration in the CSF affects impulse transmission between the motor centres localized in the vicinity of the third and fourth cerebral ventricles. EXPERIMENTAL APPROACHThe study objectives were realized on rats using a method that allows the recording of the amplitude of evoked tongue jerks (ETJ) in response to noxious tooth pulp stimulation. The amplitude of ETJ was a measure of the effect of neurotransmitters on neural structures. KEY RESULTSPerfusion of cerebral ventricles with anandamide (AEA), endomorphin-2 (EM-2), URB597, an inhibitor of fatty acid amide hydrolase (FAAH) and JZL195, a dual inhibitor of FAAH and monoacylglycerol lipase (MAGL) reduced the ETJ amplitude. The antinociceptive effect of AEA, EM-2, URB597 and JZL195 was blocked by CB 1 receptor antagonist, AM251 and by μ receptorantagonist, β-funaltrexamine. In contrast to AEA, 2-arachidonoylglycerol alone did not decrease ETJ amplitude. CONCLUSIONS AND IMPLICATIONSWe demonstrated that in the orofacial area, analgesic activity is modulated by AEA and that EM-2-induced antinociception was mediated by μ and CB 1 receptors. The action of AEA and EM-2 is tightly regulated by FAAH and FAAH/MAGL, by preventing the breakdown of endogenous cannabinoids in regions where they are produced on demand. Therefore, the current findings support the therapeutic potential of FAAH and FAAH/MAGL inhibitors as novel pharmacotherapeutic agents for orofacial pain. IntroductionOrofacial pain disorders are frequent in the general population; up to 26% adults suffer from such problems at some point of their life. Pharmacological treatment of orofacial pain is difficult and controversial (Tzabazis et al., 2014;Weiss et al., 2017). It has been demonstrated that the endogenous opioid system could be involved in cannabinoid antinociception, and recent data have also provided evidence for a role of the endogenous cannabinoid system in opioid antinociception (Cichewicz, 2004;Bushlin et al., 2010;Wilson-Poe et al., 2013).The opioid receptor system includes three subtypes of receptors, μ, δ and κ, and the endogenous opioid peptides, β-endorphin, enkephalins, dynorphins and endomorphins, that can activate these receptors (Kieffer, 1995). The cannabinoid system comprises the two major cannabinoid receptors, CB 1 and CB 2 receptors, their endogenous ligands, anandamide (AEA) and 2-arachidonoylglycerol (2-AG) and enzymes, fatty acid amide hydrolase (FAAH) and monoacylglycerol lipase (MAGL), which regulate their biosynthesis and degradation (Di Marzo et al., 2004). Simultaneous activation of opioid and cannabinoid receptors can produce synergistic analgesic effects (Smith et al., 1998;Seely et al., 2012). Opioids and cannabinoids produce antinociception through separate (although possibly interrelated) mech...

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“…These drugs produce, however, a variety of psychotropic side effects that severely limit their therapeutic utility (Piomelli, 2005). Alternative cannabinoid-based therapeutic strategies are being explored, therefore, which include activating peripheral cannabinoid receptors with brain impermeant receptor agonists, prolonging the half-life time of endocannabinoids by inhibiting their degradation (Bari et al, 2006;Piomelli et al, 2006) or using low-dose combinations of cannabinoid receptor agonists in conjunction with other analgesic agents to produce synergistic reductions in pain (Calignano et al, 2001;Cichewicz, 2004;Guindon et al, 2006). An example of the combination approach is when anandamide is administered together with the naturally occurring analgesic and antiinflammatory factor palmitoylethanolamide (PEA) (Calignano et al, 1998;Jaggar et al, 1998;Mazzari et al, 1996) -the two agents exert a synergistic antinociceptive effect in mice without eliciting overt psychotropic responses (Calignano et al, 2001).…”

Section: Introductionmentioning

confidence: 99%

Synergistic antinociception by the cannabinoid receptor agonist anandamide and the PPAR-α receptor agonist GW7647

Russo

LoVerme

Rana

et al. 2007

European Journal of Pharmacology

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The analgesic properties of cannabinoid receptor agonists are well characterized. However, numerous side effects limit the therapeutic potential of these agents. Here we report a synergistic antinociceptive interaction between the endogenous cannabinoid receptor agonist anandamide and the synthetic peroxisome proliferator-activated receptor-α (PPAR-α) agonist 2-(4-(2-(1-Cyclohexanebutyl)-3-cyclohexylureido)ethyl)phenylthio)-2-methylpropionic acid (GW7647) in a model of acute chemical-induced pain. Moreover, we show that anandamide synergistically interacts with the largeconductance potassium channel (K Ca 1.1, BK) activator isopimaric acid. These findings reveal a synergistic interaction between the endocannabinoid and PPAR-α systems that might be exploited clinically and identify a new pharmacological effect of the BK channel activator isopimaric acid.

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Synergistic antinociceptive effects of anandamide, an endocannabinoid, and nonsteroidal anti-inflammatory drugs in peripheral tissue: A role for endogenous fatty-acid ethanolamides?

Cited by 51 publications

References 51 publications

Evaluation of fatty acid amides in the carrageenan-induced paw edema model

Evaluation of fatty acid amides in the carrageenan-induced paw edema model

Effects of centrally administered endocannabinoids and opioids on orofacial pain perception in rats

Synergistic antinociception by the cannabinoid receptor agonist anandamide and the PPAR-α receptor agonist GW7647

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