Felipe Siciliani Scalco
The Catholic University of America
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Featured researches published by Felipe Siciliani Scalco.
Neurobiology of Learning and Memory | 2011
Maria Noêmia Martins de Lima; Juliana Presti-Torres; Arethuza Dornelles; Felipe Siciliani Scalco; Rafael Roesler; Vanessa Athaíde Garcia; Nadja Schröder
The role of dopamine receptors in regulating the formation of recognition memory remains poorly understood. Here we show the effects of systemic administration of dopamine receptor agonists and antagonists on the formation of memory for novel object recognition in rats. In Experiment I, rats received an intraperitoneal (i.p.) injection of vehicle, the selective D1 receptor agonist SKF38393 (1.0 and 5.0mg/kg), or the D2 receptor agonist quinpirole (1.0 and 5.0mg/kg) immediately after training. In Experiment II, rats received an injection of vehicle, the dopamine receptor antagonist SCH23390 (0.1 and 0.05 mg/kg), or the D2 receptor antagonist raclopride (0.5 and 0.1mg/kg) before training, followed by an injection of vehicle or the nonselective dopamine receptor agonist apomorphine (0.05 mg/kg) immediately after training. SKF38393 at 5mg/kg produced an enhancement of novel object recognition memory measured at both 24 and 72 h after training, whereas the dose of 10mg/kg impaired 24-h retention. Posttraining administration of quinpirole did not affect 24-h retention. Apomorphine enhanced memory in rats given pretraining raclopride, suggesting that the effect was mediated by selective activation of D1 receptors. The results indicate that activation of D1 receptors can enhance recognition memory consolidation. Importantly, pharmacological activation of D1 receptors enhanced novel object recognition memory even under conditions in which control rats showed significant retention.
Neuropharmacology | 2008
M.N.M. de Lima; Juliana Presti-Torres; Vanessa Athaíde Garcia; Marcelo Reuwsaat Guimarães; Felipe Siciliani Scalco; Rafael Roesler; Nadja Schröder
Increasing evidence indicates that iron deposition in the brain might play a role in cognitive dysfunction associated with neurodegenerative disorders and aging. Previous studies have not examined whether iron-induced memory deficits can be attenuated by acute treatments with memory-enhancing agents. Phosphodiesterase type 4 (PDE4) inhibitors such as rolipram (ROL) ameliorate memory impairments in several rodent models of amnesia and have been proposed as candidate cognitive-enhancing drugs. Here we show that a single posttraining systemic injection of ROL dose-dependently attenuates the impairment of memory for novel object recognition (NOR) in rats given neonatal iron loading, a model of iron-induced cognitive impairment. Posttraining administration of ROL also recovered NOR deficits associated with aging in rats. These findings provide the first evidence that stimulation of an intracellular second messenger signaling pathway can attenuate iron-induced memory impairment, and support the view that PDE4 inhibitors might ameliorate cognitive dysfunction associated with aging and neurodegenerative disorders.
Neurobiology of Aging | 2008
Maria Noêmia Martins de Lima; Caroline Pietá Dias; Juliana Presti Torres; Arethuza Dornelles; Vanessa Athaíde Garcia; Felipe Siciliani Scalco; Marcelo R. Guimarães; Roberta Petry; Elke Bromberg; Larissa Constantino; Patrícia Budni; Felipe Dal-Pizzol; Nadja Schröder
It is now generally accepted that iron accumulates in the brain during the ageing process. Increasing evidence demonstrate that iron accumulation in selective regions of the brain may generate free radicals, thereby possessing implications for the etiology of neurodegenerative disorders. In a previous study we have reported that aged rats present recognition memory deficits. The aim of the present study was to evaluate the effect of desferoxamine (DFO), an iron chelator agent, on age-induced memory impairment. Aged Wistar rats received intraperitoneal injections of saline or DFO (300mg/kg) for 2 weeks. The animals were submitted to a novel object recognition task 24h after the last injection. DFO-treated rats showed normal recognition memory while the saline group showed long-term recognition memory deficits. The results show that DFO is able to reverse age-induced recognition memory deficits. We also demonstrated that DFO reduced the oxidative damage to proteins in cortex and hippocampus. Thus, the present findings provide the first evidence that iron chelators might prevent age-related memory dysfunction.
Neurobiology of Learning and Memory | 2007
Arethuza Dornelles; Maria Noêmia Martins de Lima; Manoela M. Grazziotin; Juliana Presti-Torres; Vanessa Athaíde Garcia; Felipe Siciliani Scalco; Rafael Roesler; Nadja Schröder
Extensive evidence indicates that epinephrine (EPI) modulates memory consolidation for emotionally arousing tasks in animals and human subjects. However, previous studies have not examined the effects of EPI on consolidation of recognition memory. Here we report that systemic administration of EPI enhances consolidation of memory for a novel object recognition (NOR) task under different training conditions. Control male rats given a systemic injection of saline (0.9% NaCl) immediately after NOR training showed significant memory retention when tested at 1.5 or 24, but not 96h after training. In contrast, rats given a post-training injection of EPI showed significant retention of NOR at all delays. In a second experiment using a different training condition, rats treated with EPI, but not SAL-treated animals, showed significant NOR retention at both 1.5 and 24-h delays. We next showed that the EPI-induced enhancement of retention tested at 96h after training was prevented by pretraining systemic administration of the beta-adrenoceptor antagonist propranolol. The findings suggest that, as previously observed in experiments using aversively motivated tasks, epinephrine modulates consolidation of recognition memory and that the effects require activation of beta-adrenoceptors.
Neuropharmacology | 2007
Juliana Presti-Torres; M.N.M. de Lima; Felipe Siciliani Scalco; Fábio Caldana; Vanessa Athaíde Garcia; Marcelo Reuwsaat Guimarães; Gilberto Schwartsmann; Rafael Roesler; Nadja Schröder
The gastrin-releasing peptide receptor (GRPR) has been implicated in central nervous system (CNS) diseases, including neurodevelopmental disorders associated with autism. In the present study we examined the effects of GRPR blockade during the neonatal period on behavioral measures relevant to animal models of neurodevelopmental disorders. Male Wistar rats were given an intraperitoneal (i.p.) injection of either saline (SAL) or the GRPR antagonist [D-Tpi(6), Leu(13) psi(CH(2)NH)-Leu(14)] bombesin (6-14) (RC-3095; 1 or 10mg/kg) twice daily for 10days from postnatal days (PN) 1 to 10. Animals treated with RC-3095 showed pronounced deficits in social interaction when tested at PN 30-35 and impaired 24-h retention of memory for both novel object recognition (NOR) and inhibitory avoidance (IA) tasks tested at PN 60-71. Neither short-term memory tested 1.5h posttraining nor open field behavior were affected by neonatal GRPR blockade. The implications of the findings for animal models of neurodevelopmental disorders are discussed.
European Journal of Pharmacology | 2007
Maria Noêmia Martins de Lima; Juliana Presti-Torres; Fábio Caldana; Manoela M. Grazziotin; Felipe Siciliani Scalco; Marcelo R. Guimarães; Elke Bromberg; Silvia Isabel Rech Franke; João Antonio Pêgas Henriques; Nadja Schröder
Neurotoxicity Research | 2011
Clívia Miwa; Maria Noêmia Martins de Lima; Felipe Siciliani Scalco; Gustavo Vedana; Raquel Mattos; Liana Lisboa Fernandez; Arlete Hilbig; Nadja Schröder; Mônica R. M. Vianna
Neurotoxicity Research | 2011
Liana Lisboa Fernandez; Maria Noêmia Martins de Lima; Felipe Siciliani Scalco; Gustavo Vedana; Clívia Miwa; Arlete Hilbig; Mônica R. M. Vianna; Nadja Schröder
Archive | 2007
Marcelo Reuwsaat Guimarães; Maria Noêmia Martins de Lima; Juliana Presti Torres; Vanessa Athaíde Garcia; Felipe Siciliani Scalco; Rafael Roesler
Archive | 2007
Felipe Siciliani Scalco; Maria Noêmia Martins de Lima; Juliana Presti Torres; Vanessa Athaíde Garcia; Marcelo Reuwsaat Guimarães