2012
DOI: 10.1038/mp.2012.8
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Adenosine A2A receptor blockade reverts hippocampal stress-induced deficits and restores corticosterone circadian oscillation

Abstract: Maternal separation (MS) is an early life stress model that induces permanent changes in the central nervous system, impairing hippocampal long-term potentiation (LTP) and spatial working memory. There are compelling evidences for a role of hippocampal adenosine A(2A) receptors in stress-induced modifications related to cognition, thus opening a potential window for therapeutic intervention. Here, we submitted rats to MS and evaluated the long-lasting molecular, electrophysiological and behavioral impairments … Show more

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Cited by 123 publications
(127 citation statements)
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“…This A 2A R up-regulation is accompanied by an A 2A R gain of function (reviewed in ref. 33) that leads to synaptic dysfunction, as demonstrated by the ability of A 2A R antagonists to prevent synaptic plasticity dysfunction with aging (11) and maternal separation (12) and by the loss of synaptic markers in different noxious brain conditions (14,15,31), namely upon repeated restraint stress (32). How enhanced A 2A R function triggers synaptic dysfunction remains to be determined, given our current ignorance of the transducing systems operated by these pleiotropic A 2A R (34,35).…”
Section: Discussionmentioning
confidence: 99%
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“…This A 2A R up-regulation is accompanied by an A 2A R gain of function (reviewed in ref. 33) that leads to synaptic dysfunction, as demonstrated by the ability of A 2A R antagonists to prevent synaptic plasticity dysfunction with aging (11) and maternal separation (12) and by the loss of synaptic markers in different noxious brain conditions (14,15,31), namely upon repeated restraint stress (32). How enhanced A 2A R function triggers synaptic dysfunction remains to be determined, given our current ignorance of the transducing systems operated by these pleiotropic A 2A R (34,35).…”
Section: Discussionmentioning
confidence: 99%
“…The only molecular targets for caffeine at nontoxic doses are the main adenosine receptors in the brain, namely the inhibitory A 1 receptors (A 1 R) and the facilitatory A 2A receptors (A 2A R) (9). A 2A R blockade affords robust protection against noxious brain conditions (10), an effect that might result from the ability of neuronal A 2A R to control aberrant plasticity (11,12) and synaptotoxicity (13)(14)(15) or from A 2A R's impact on astrocytes (16) or microglia (17). The protection provided by A 2A R blockade prompts the hypothesis that A 2A R antagonism may underlie the beneficial effects of caffeine on chronic stress, in accordance with the role of synaptic (18,19) or glial dysfunction (20) in mood disorders.…”
mentioning
confidence: 99%
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“…The importance of this modulation system is best heralded by the observation that the overactivation of hippocampal A 2A Rs is necessary and sufficient to trigger spatial memory dysfunction (Li et al, 2015a;Pagnussat et al, 2015). Furthermore, conditions associated with memory deterioration trigger an upregulation of A 2A Rs in the hippocampus leading to abnormal synaptic plasticity (Costenla et al, 2011;Kaster et al, 2015), and A 2A R blockade prevent memory impairment in conditions such as stress, aging, or Alzheimer's disease (eg Batalha et al, 2013;Laurent et al, 2016;Oor et al, 2015;Prediger et al, 2005), an effect mimicked by caffeine (a nonselective adenosine receptor antagonist) both in animal models and in humans (reviewed in Cunha and Agostinho, 2010;Chen, 2014).…”
Section: Introductionmentioning
confidence: 99%
“…Chemoluminescence detection was performed with an ECL-PLUS Western blot detection reagent (GE Healthcare) using X-ray films (Fujifilm). The saturation binding experiments were adapted from a previous protocol (Batalha et al, 2013).…”
Section: Methodsmentioning
confidence: 99%