2003
DOI: 10.1016/s0091-3057(03)00151-5
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Anxiety does not affect the antinociceptive effect of Δ9-THC in mice: participation of cannabinoid and opioid receptors

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Cited by 4 publications
(7 citation statements)
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“…Further, the use of a CB1 receptor antagonist has been found to fully reverse the effects of THC [41]. However, other non-CB1 receptors are also believed to be involved including serotonin 5-HT1A receptors [42] and the opioid system [20,43,44]. There has also been research in recent years to determine the neural site at which these interactions take place.…”
mentioning
confidence: 99%
“…Further, the use of a CB1 receptor antagonist has been found to fully reverse the effects of THC [41]. However, other non-CB1 receptors are also believed to be involved including serotonin 5-HT1A receptors [42] and the opioid system [20,43,44]. There has also been research in recent years to determine the neural site at which these interactions take place.…”
mentioning
confidence: 99%
“…THC has shown to exert an antinociceptive effect in a wide range of preclinical acute nociception tests as the acetic acid model (Booker et al, 2009), tail flick test (Mason et al, 1999) or paw pressure test (Smith et al, 1998;Tseng and Craft, 2001), and also in chronic pain assays as inflammatory pain (Moss and Johnson, 1980;Takahashi et al, 2003), arthritic pain (Cox et al, 2007) or neuropathic pain (De Vry et al, 2004). Now, we show the effect of THC in two models of muscle pain and to our knowledge the results from this study are the first to demonstrate the efficacy of THC in animal models of acute muscle pain.…”
Section: Discussionmentioning
confidence: 99%
“…Despite the hypothesis that the degree of anxiety may contribute to the perception of and response to the noxious stimulus, both anxious and nonanxious animals displayed comparable formalin-evoked biphasic nociceptive profiles. Systemic pretreatment with Δ 9 -THC elicited an analgesic effect in both groups of animals, an effect blocked by systemic pretreatment with a CB 1 receptor antagonist, rimonabant ( Takahashi et al, 2003 ). These data suggested that the endocannabinoid system (and in particular the CB 1 receptor) may represent a potential treatment strategy for inflammatory pain in the presence and/or absence of anxiety and possibly other neuropsychiatric disorders.…”
Section: The Role Of the Endocannabinoid System In Depression-pain Inmentioning
confidence: 99%
“…Despite numerous reports of altered endocannabinoid signaling in various animal models of pain ( Lim et al, 2003 ; Zhang et al, 2003 ; Walczak et al, 2005 ; Mitrirattanakul et al, 2006 ) and mood-related behavior ( Vinod et al, 2012 ; Marco et al, 2014 ; Navarria et al, 2014 ), there is limited direct evidence available identifying alterations in endocannabinoid function in animal models of coexistent depressive and pain behavior ( Tables 2 and 3 ). One of the first studies examining the role of the endocannabinoid system in the interaction between affect and pain was conducted by Takahashi and colleagues (2003) . In this study, outbred Swiss-albino mice were stratified into groups of anxious and nonanxious animals as determined by behavioral responses in the elevated plus maze, before subsequent exposure to intraplantar formalin administration ( Takahashi et al, 2003 ).…”
Section: The Role Of the Endocannabinoid System In Depression-pain Inmentioning
confidence: 99%
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