2012
DOI: 10.1016/j.neuropharm.2012.03.008
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Orally administered oleoylethanolamide protects mice from focal cerebral ischemic injury by activating peroxisome proliferator-activated receptor α

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Cited by 67 publications
(82 citation statements)
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“…Human and animal in vivo data have shown increases in neurological and circulating plasma levels of AEA, 2-AG, OEA and PEA after stroke (Schabitz et al 2002;Hillard 2008;Naccarato et al 2010). As in other cardiovascular disorders, the hypothesis is that upregulation of the endocannabinoid system is protective in stroke, and this is supported by numerous studies showing that 2-AG (Wang et al 2009), AEA (Wang et al 2009) as well as the endocannabinoid-like compounds, OEA (Sun et al 2007;Zhou et al 2012) and PEA (Schomacher et al 2008;Garg et al 2010;Ahmad et al 2012b), offer protection against ischaemic/reperfusion injury. N-acylethanolamine compounds such as lauroylethanolamide and linoleoylethanolamide have also been shown to be protective against stroke (Garg et al 2011).…”
Section: Endocannabinoids and Cerebral Ischaemia/strokementioning
confidence: 93%
“…Human and animal in vivo data have shown increases in neurological and circulating plasma levels of AEA, 2-AG, OEA and PEA after stroke (Schabitz et al 2002;Hillard 2008;Naccarato et al 2010). As in other cardiovascular disorders, the hypothesis is that upregulation of the endocannabinoid system is protective in stroke, and this is supported by numerous studies showing that 2-AG (Wang et al 2009), AEA (Wang et al 2009) as well as the endocannabinoid-like compounds, OEA (Sun et al 2007;Zhou et al 2012) and PEA (Schomacher et al 2008;Garg et al 2010;Ahmad et al 2012b), offer protection against ischaemic/reperfusion injury. N-acylethanolamine compounds such as lauroylethanolamide and linoleoylethanolamide have also been shown to be protective against stroke (Garg et al 2011).…”
Section: Endocannabinoids and Cerebral Ischaemia/strokementioning
confidence: 93%
“…1) is an endocannabinoid analogy that belongs to a family of endogenous acylethanolamides [2]. Increasing evidence suggests that OEA may act as an endogenous neuroprotective factor and participate in the control of reward-related behaviors [1,8]. Systemic administration of OEA to rats results in elevated OEA plasma levels, as has also been reported in patients with post-traumatic stress disorder [9].…”
Section: Introductionmentioning
confidence: 90%
“…Thus, the effects observed here upon um-PEA administration can be due to PEA activating its molecular targets, and also to PEA favoring the actions of other NAEs (e.g., AEA and OEA). Indeed, anti-inflammatory, neuroprotective, and analgesic effects have been reported for AEA and OEA in several preclinical models [69][70][71][72][73].…”
Section: Discussionmentioning
confidence: 99%