2013
DOI: 10.1016/j.bbr.2012.09.030
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D1 receptor agonists reverse the subchronic phencyclidine (PCP)-induced novel object recognition (NOR) deficit in female rats

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Cited by 38 publications
(30 citation statements)
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“…Indeed, some treatments for some domains of cognition may impair other domains, e.g. over stimulation of dopamine (DA) D 1 receptors (Horiguchi et al, 2011a).…”
Section: Introductionmentioning
confidence: 99%
“…Indeed, some treatments for some domains of cognition may impair other domains, e.g. over stimulation of dopamine (DA) D 1 receptors (Horiguchi et al, 2011a).…”
Section: Introductionmentioning
confidence: 99%
“…88,[93][94][95] In addition, several studies analyzing the effects of pharmacological or nonpharmacological treatments on cognitive function and memory revealed a stimulation with increasing doses up to a maximum, following an inhibition at higher doses. 90,91,96,97 In another example related to vaccine development, the authors observed a similar immune suppression effect at above threshold doses. 98 In the present study, we have shown that Lymphomyosot improves wound repair, modulates macrophage activity, and reduces acute lymphedema.…”
mentioning
confidence: 52%
“…The release of cortical and hippocampal DA and ACh, two neurotransmitters, in cortex and hippocampus, has been shown by microdialysis in freely moving rodents to be selectively enhanced by AAPDs, but not typical APDs [44]. It has been suggested that this produces cognitive enhancement, in part, through stimulation of D 1 , D 4 , nicotinic and muscarinic receptors [37,[44][45][46][47]. DA and ACh efflux may also overcome possible adverse effects of APD-induced D 2 or muscarinic receptor blockade, or both [12,44].…”
Section: The Neuropharmacologic Basis For Efficacy Of Aapds To Treat Cismentioning
confidence: 97%
“…Unfortunately, like most CIS, studies, they did not report the percentages of patients who experience improvement that would be expected to be clinically significant, and beyond practice levels, 0.5 or 1.0 SD, respectively [36]. Similarly, the majority of CIS studies are 4-8 weeks in duration, which may be an insufficient length of time for significant benefit (see Ref [24 ]) because of the time needed for some of the emergent adaptive changes in synaptic function produced by AAPDs [37]. A test of the concepts advocated here to better evaluate the efficacy of AAPDs, as well as adjunctive treatments for AAPDs, would include as many of the following features as possible: random assignment of drug-free patients or patients taking typical APDs, to monotherapy with an AAPD which the patient had not recently received, a control group treated with typical APDs, treatment duration at least six months, no concomitant psychotropic medications, inclusion of only non-treatment resistant schizophrenia patients, and primary endpoints of proportions of subjects showing improvement 0.5 SD in each of the key domains of cognition.…”
Section: Introductionmentioning
confidence: 95%
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