Your search keyword '"Tomasetti, Carmine"' showing total 25 results

1. The Homer1 family of proteins at the crossroad of dopamine-glutamate signaling: An emerging molecular "Lego" in the pathophysiology of psychiatric disorders. A systematic review and translational insight.

Author

de Bartolomeis A, Barone A, Buonaguro EF, Tomasetti C, Vellucci L, and Iasevoli F

Subjects

Carrier Proteins metabolism, Glutamates therapeutic use, Homer Scaffolding Proteins metabolism, Humans, Signal Transduction, Dopamine metabolism, Mental Disorders metabolism

Abstract

Once considered only scaffolding proteins at glutamatergic postsynaptic density (PSD), Homer1 proteins are increasingly emerging as multimodal adaptors that integrate different signal transduction pathways within PSD, involved in motor and cognitive functions, with putative implications in psychiatric disorders. Regulation of type I metabotropic glutamate receptor trafficking, modulation of calcium signaling, tuning of long-term potentiation, organization of dendritic spines' growth, as well as meta- and homeostatic plasticity control are only a few of the multiple endocellular and synaptic functions that have been linked to Homer1. Findings from preclinical studies, as well as genetic studies conducted in humans, suggest that both constitutive (Homer1b/c) and inducible (Homer1a) isoforms of Homer1 play a role in the neurobiology of several psychiatric disorders, including psychosis, mood disorders, neurodevelopmental disorders, and addiction. On this background, Homer1 has been proposed as a putative novel target in psychopharmacological treatments. The aim of this review is to summarize and systematize the growing body of evidence on Homer proteins, highlighting the role of Homer1 in the pathophysiology and therapy of mental diseases., (Copyright © 2022 Elsevier Ltd. All rights reserved.)

Published

2022

2. Treating the Synapse in Major Psychiatric Disorders: The Role of Postsynaptic Density Network in Dopamine-Glutamate Interplay and Psychopharmacologic Drugs Molecular Actions.

Author

Tomasetti C, Iasevoli F, Buonaguro EF, De Berardis D, Fornaro M, Fiengo AL, Martinotti G, Orsolini L, Valchera A, Di Giannantonio M, and de Bartolomeis A

Subjects

Animals, Humans, Intracellular Signaling Peptides and Proteins metabolism, Models, Biological, Psychotic Disorders metabolism, Antipsychotic Agents therapeutic use, Dopamine metabolism, Glutamic Acid metabolism, Post-Synaptic Density metabolism, Psychotic Disorders drug therapy, Signal Transduction drug effects

Abstract

Dopamine-glutamate interplay dysfunctions have been suggested as pathophysiological key determinants of major psychotic disorders, above all schizophrenia and mood disorders. For the most part, synaptic interactions between dopamine and glutamate signaling pathways take part in the postsynaptic density, a specialized ultrastructure localized under the membrane of glutamatergic excitatory synapses. Multiple proteins, with the role of adaptors, regulators, effectors, and scaffolds compose the postsynaptic density network. They form structural and functional crossroads where multiple signals, starting at membrane receptors, are received, elaborated, integrated, and routed to appropriate nuclear targets. Moreover, transductional pathways belonging to different receptors may be functionally interconnected through postsynaptic density molecules. Several studies have demonstrated that psychopharmacologic drugs may differentially affect the expression and function of postsynaptic genes and proteins, depending upon the peculiar receptor profile of each compound. Thus, through postsynaptic network modulation, these drugs may induce dopamine-glutamate synaptic remodeling, which is at the basis of their long-term physiologic effects. In this review, we will discuss the role of postsynaptic proteins in dopamine-glutamate signals integration, as well as the peculiar impact of different psychotropic drugs used in clinical practice on postsynaptic remodeling, thereby trying to point out the possible future molecular targets of "synapse-based" psychiatric therapeutic strategies., Competing Interests: The authors declare no conflict of interest.

Published

2017

3. MicroRNAs in Schizophrenia: Implications for Synaptic Plasticity and Dopamine-Glutamate Interaction at the Postsynaptic Density. New Avenues for Antipsychotic Treatment Under a Theranostic Perspective.

Author

de Bartolomeis A, Iasevoli F, Tomasetti C, and Buonaguro EF

Subjects

Animals, Humans, Schizophrenia metabolism, Antipsychotic Agents therapeutic use, Dopamine metabolism, Glutamic Acid metabolism, MicroRNAs metabolism, Neuronal Plasticity drug effects, Schizophrenia drug therapy

Abstract

Despite dopamine-glutamate aberrant interaction that has long been considered a relevant landmark of psychosis pathophysiology, several aspects of these two neurotransmitters reciprocal interaction remain to be defined. The emerging role of postsynaptic density (PSD) proteins at glutamate synapse as a molecular "lego" making a functional hub where different signals converge may add a new piece of information to understand how dopamine-glutamate interaction may work with regard to schizophrenia pathophysiology and treatment. More recently, compelling evidence suggests a relevant role for microRNA (miRNA) as a new class of dopamine and glutamate modulators with regulatory functions in the reciprocal interaction of these two neurotransmitters. Here, we aimed at addressing the following issues: (i) Do miRNAs have a role in schizophrenia pathophysiology in the context of dopamine-glutamate aberrant interaction? (ii) If miRNAs are relevant for dopamine-glutamate interaction, at what level this modulation takes place? (iii) Finally, will this knowledge open the door to innovative diagnostic and therapeutic tools? The biogenesis of miRNAs and their role in synaptic plasticity with relevance to schizophrenia will be considered in the context of dopamine-glutamate interaction, with special focus on miRNA interaction with PSD elements. From this framework, implications both for biomarkers identification and potential innovative interventions will be considered.

Published

2015

4. Regulation of postsynaptic plasticity genes' expression and topography by sustained dopamine perturbation and modulation by acute memantine: relevance to schizophrenia.

Author

Iasevoli F, Buonaguro EF, Sarappa C, Marmo F, Latte G, Rossi R, Eramo A, Tomasetti C, and de Bartolomeis A

Subjects

Animals, Benzazepines pharmacology, Brain drug effects, Brain metabolism, Disks Large Homolog 4 Protein, Dopamine Antagonists pharmacology, Dopamine Uptake Inhibitors pharmacology, Gene Expression drug effects, Haloperidol pharmacology, Homer Scaffolding Proteins, Male, Piperazines pharmacology, RNA, Messenger metabolism, Random Allocation, Rats, Sprague-Dawley, Schizophrenia drug therapy, Schizophrenia physiopathology, Carrier Proteins metabolism, Dopamine metabolism, Dopamine Agents pharmacology, Intracellular Signaling Peptides and Proteins metabolism, Memantine pharmacology, Membrane Proteins metabolism

Abstract

A relevant role for dopamine-glutamate interaction has been reported in the pathophysiology and treatment of psychoses. Dopamine and glutamate may interact at multiple levels, including the glutamatergic postsynaptic density (PSD), an electron-dense thickening that has gained recent attention as a switchboard of dopamine-glutamate interactions and for its role in synaptic plasticity. Recently, glutamate-based strategies, such as memantine add-on to antipsychotics, have been proposed for refractory symptoms of schizophrenia, e.g. cognitive impairment. Both antipsychotics and memantine regulate PSD transcripts but sparse information is available on memantine's effects under dopamine perturbation. We tested gene expression changes of the Homer1 and PSD-95 PSD proteins in models of sustained dopamine perturbation, i.e. subchronic treatment by: a) GBR-12909, a dopamine receptor indirect agonist; b) haloperidol, a D2R antagonist; c) SCH-23390, a dopamine D1 receptor (D1R) antagonist; and d) SCH-23390+haloperidol. On the last day of treatment, rats were acutely treated with vehicle or memantine. The Homer1a immediate-early gene was significantly induced by haloperidol and by haloperidol+SCH-23390. The gene was not induced by SCH-23390 per se or by GBR-12909. Expression of the constitutive genes Homer1b/c and PSD-95 was less affected by these dopaminergic paradigms. Acute memantine administration significantly increased Homer1a expression by the dopaminergic compounds used herein. Both haloperidol and haloperidol+SCH-23390 shifted Homer1a/Homer1b/c ratio of expression toward Homer1a. This pattern was sharpened by acute memantine. Dopaminergic compounds and acute memantine also differentially affected topographic distribution of gene expression and coordinated expression of Homer1a among cortical-subcortical regions. These results indicate that dopaminergic perturbations may affect glutamatergic signaling in different directions. Memantine may help partially revert dopamine-mediated glutamatergic dysfunctions., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014

5. The emerging role of dopamine-glutamate interaction and of the postsynaptic density in bipolar disorder pathophysiology: Implications for treatment.

Author

de Bartolomeis A, Buonaguro EF, Iasevoli F, and Tomasetti C

Subjects

Antipsychotic Agents therapeutic use, Bipolar Disorder drug therapy, Bipolar Disorder physiopathology, Bipolar Disorder psychology, Brain drug effects, Brain physiopathology, Dopaminergic Neurons drug effects, Humans, Neuronal Plasticity, Post-Synaptic Density drug effects, Synaptic Transmission, Affect drug effects, Bipolar Disorder metabolism, Brain metabolism, Dopamine metabolism, Dopaminergic Neurons metabolism, Glutamic Acid metabolism, Post-Synaptic Density metabolism

Abstract

Aberrant synaptic plasticity, originating from abnormalities in dopamine and/or glutamate transduction pathways, may contribute to the complex clinical manifestations of bipolar disorder (BD). Dopamine and glutamate systems cross-talk at multiple levels, such as at the postsynaptic density (PSD). The PSD is a structural and functional protein mesh implicated in dopamine and glutamate-mediated synaptic plasticity. Proteins at PSD have been demonstrated to be involved in mood disorders pathophysiology and to be modulated by antipsychotics and mood stabilizers. On the other side, post-receptor effectors such as protein kinase B (Akt), glycogen synthase kinase-3 (GSK-3) and the extracellular signal-regulated kinase (Erk), which are implicated in both molecular abnormalities and treatment of BD, may interact with PSD proteins, and participate in the interplay of the dopamine-glutamate signalling pathway. In this review, we describe emerging evidence on the molecular cross-talk between dopamine and glutamate signalling in BD pathophysiology and pharmacological treatment, mainly focusing on dysfunctions in PSD molecules. We also aim to discuss future therapeutic strategies that could selectively target the PSD-mediated signalling cascade at the crossroads of dopamine-glutamate neurotransmission., (© The Author(s) 2014.)

Published

2014

6. Calcium-dependent networks in dopamine-glutamate interaction: the role of postsynaptic scaffolding proteins.

Author

de Bartolomeis A and Tomasetti C

Subjects

Animals, Antipsychotic Agents pharmacology, Humans, Nerve Net drug effects, Calcium metabolism, Dopamine metabolism, Glutamic Acid metabolism, Nerve Net metabolism, Nerve Tissue Proteins metabolism

Abstract

Dopamine and glutamate systems are both involved in cognitive, behavioral, and motor processes. Dysfunction of dopamine-glutamate interplay has been suggested in several psychotic diseases, above all in schizophrenia, for which there exists a need for novel medications. Intracellular calcium-dependent transduction pathways are key determinants of dopamine-glutamate interactions, which take place mainly, albeit not exclusively, in the postsynaptic density (PSD), a highly specialized postsynaptic ultrastructure. Stimulation of dopamine and glutamate receptors modulates the gene expression and the function of specific PSD proteins, the "scaffolding" proteins (Homer, Shank, and PSD95), belonging to a complex Ca(2+)-regulated network that integrates and converges dopamine and glutamate signaling to appropriate nuclear targets. Dysfunction of scaffolding proteins leads to severe impairment of Ca(2+)-dependent signaling, which may underlie the dopamine-glutamate aberrations putatively implicated in the pathogenesis of psychotic disorders. Antipsychotic therapy has been demonstrated to directly and indirectly affect the neuronal Ca(2+)-dependent pathways through the modulation of PSD scaffolding proteins, such as Homer, therefore influencing both dopaminergic and glutamatergic functions and enforcing Ca(2+)-mediated long-term synaptic changes. In this review, we will discuss the role of PSD scaffolding proteins in routing Ca(2+)-dependent signals to the nucleus. In particular, we will address the implication of PSD scaffolding proteins in the intracellular connections between dopamine and glutamate pathways, which involve both Ca(2+)-dependent and Ca(2+)-independent mechanisms. Finally, we will discuss how new strategies for the treatment of psychosis aim at developing antipsychotics that may impact both glutamate and dopamine signaling, and what should be the possible role of PSD scaffolding proteins.

Published

2012

7. Otx genes in neurogenesis of mesencephalic dopaminergic neurons.

Author

Simeone A, Puelles E, Omodei D, Acampora D, Di Giovannantonio LG, Di Salvio M, Mancuso P, and Tomasetti C

Subjects

Humans, Mesencephalon metabolism, Otx Transcription Factors metabolism, Dopamine metabolism, Mesencephalon growth & development, Neurogenesis physiology, Neurons metabolism, Otx Transcription Factors genetics

Abstract

Mesencephalic-diencephalic dopaminergic (mdDA) neurons play a relevant role in the control of movement, behavior, and cognition. Indeed loss and/or abnormal functioning of mdDA neurons are responsible for Parkinson's disease as well as for addictive and psychiatric disorders. In the last years a wealth of information has been provided on gene functions controlling identity, fate, and proliferation of mdDA progenitors. This review will focus on the role exerted by Otx genes in early decisions regulating sequential steps required for the neurogenesis of mesencephalic dopaminergic (mesDA) neurons. In this context, the regulatory network involving Otx functional interactions with signaling molecules and transcription factors required to promote or prevent the development of mesDA neurons will be analyzed in detail., (Copyright © 2011 Wiley Periodicals, Inc.)

Published

2011

8. The role of otx2 in adult mesencephalic-diencephalic dopaminergic neurons.

Author

Simeone A, Di Salvio M, Di Giovannantonio LG, Acampora D, Omodei D, and Tomasetti C

Subjects

Animals, Diencephalon metabolism, Aging metabolism, Dopamine metabolism, Mesencephalon metabolism, Neurons metabolism, Otx Transcription Factors metabolism

Abstract

Mesencephalic and diencephalic dopaminergic (mdDA) progenitors generate two major groups of neurons corresponding to the A9 neurons of the substantia nigra pars compacta (SNpc) and the A10 neurons of the ventral tegmental area (VTA). MdDA neurons control motor, sensorimotor and motivated behaviour and their degeneration or abnormal functioning is associated to Parkinson's disease and psychiatric disorders. Although relevant advances have been made, the molecular basis controlling identity, survival and vulnerability to neurodegeneration of SNpc and VTA neurons remains poorly understood. Here, we will review recent findings on the role exerted by the transcription factor Otx2 in adult mdDA neurons. Otx2 expression is restricted to a relevant fraction of VTA neurons and absent in the SNpc. In particular, Otx2 is prevalently excluded from neurons of the dorsal-lateral VTA, which expressed Girk2 and high level of the dopamine transporter (Dat). Loss and gain of function mouse models revealed that Otx2 controls neuron subtype identity by antagonizing molecular and functional features of the dorsal-lateral VTA such as Girk2 and Dat expression as well as vulnerability to the parkinsonian MPTP toxin. Furthermore, when ectopically expressed in the SNpc, Otx2 suppresses Dat expression and confers efficient neuroprotection to MPTP toxicity by suppressing efficient DA uptake.

Published

2011

9. Differential expression of Homer 1 gene by acute and chronic administration of antipsychotics and dopamine transporter inhibitors in the rat forebrain.

Author

Ambesi-Impiombato A, Panariello F, Dell'aversano C, Tomasetti C, Muscettola G, and de Bartolomeis A

Subjects

Animals, Basal Ganglia drug effects, Basal Ganglia metabolism, Biomarkers metabolism, Dibenzothiazepines pharmacology, Dopamine Plasma Membrane Transport Proteins metabolism, Dopamine Uptake Inhibitors pharmacology, Drug Administration Schedule, Gene Expression physiology, Haloperidol pharmacology, Homer Scaffolding Proteins, Male, Parietal Lobe drug effects, Parietal Lobe metabolism, Piperazines pharmacology, Prosencephalon drug effects, Quetiapine Fumarate, Rats, Rats, Sprague-Dawley, Receptors, Dopamine D2 drug effects, Receptors, Dopamine D2 metabolism, Antipsychotic Agents pharmacology, Carrier Proteins genetics, Dopamine metabolism, Dopamine Plasma Membrane Transport Proteins antagonists & inhibitors, Gene Expression drug effects, Prosencephalon metabolism

Abstract

Neuronal expression of immediate-early genes in response to a drug is a powerful screening tool for dissecting anatomical and functional brain circuitry affected by psychoactive compounds. We examined the effect of dopaminergic perturbation on two Homer 1 gene splice variants, Homer 1a and ania-3, in rat forebrain. Rats were treated with the "typical" antipsychotic haloperidol, the "atypical" quetiapine, or the selective dopamine transporter (DAT) inhibitor GBR 12909 in acute and chronic paradigms. Our results show that the high affinity dopamine D(2) receptor antagonist haloperidol strongly induces Homer 1 gene expression in the caudate-putamen, whereas quetiapine, a fast D2R dissociating antagonist, does not. This confirms that Homer 1 may be considered a predictor of "atypicality" of antipsychotic compounds in acute and also chronic regimens. Chronic treatment with GBR 12909 showed a strong induction in the parietal cortex, resembling the activation of "sensitization" circuitry by stimulants. Finally, we describe a differential spatial induction pattern of Homer 1 gene within the caudate-putamen by typical antipsychotics and DAT blockers, and propose a novel method to quantitate it.

Published

2007

10. Divergent acute and chronic modulation of glutamatergic postsynaptic density genes expression by the antipsychotics haloperidol and sertindole

Author

Iasevoli, Felice, Tomasetti, Carmine, Marmo, Federica, Bravi, Daniele, Arnt, Jørn, and de Bartolomeis, Andrea

Published

2010

11. Agomelatine beyond Borders: Current Evidences of Its Efficacy in Disorders Other than Major Depression.

Author

De Berardis, Domenico, Fornaro, Michele, Serroni, Nicola, Campanella, Daniela, Rapini, Gabriella, Olivieri, Luigi, Srinivasan, Venkataramanujam, Iasevoli, Felice, Tomasetti, Carmine, De Bartolomeis, Andrea, Valchera, Alessandro, Perna, Giampaolo, Mazza, Monica, Di Nicola, Marco, Martinotti, Giovanni, and Di Giannantonio, Massimo

Subjects

THERAPEUTICS, MENTAL depression, PHYSIOLOGICAL effects of antidepressants, DRUG efficacy, SEASONAL affective disorder, MENTAL illness treatment, PATHOLOGICAL psychology, CIRCADIAN rhythms

Abstract

Agomelatine, a melatonergic antidepressant with a rapid onset of action, is one of the most recent drugs in the antidepressant category. Agomelatine's antidepressant actions are attributed to its sleep-promoting and chronobiotic actions mediated by MT1 and MT2 receptors present in the suprachiasmatic nucleus, as well as to its effects on the blockade of 5-HT2c receptors. Blockade of 5-HT2c receptors causes release of both noradrenaline and dopamine at the fronto-cortical dopaminergic and noradrenergic pathways. The combined actions of agomelatine on MT1/MT2 and 5-HT2c receptors facilitate the resynchronization of altered circadian rhythms and abnormal sleep patterns. Agomelatine appeared to be effective in treating major depression. Moreover, evidence exists that points out a possible efficacy of such drug in the treatment of bipolar depression, anxiety disorders, alcohol dependence, migraines etc. Thus, the aim of this narrative review was to elucidate current evidences on the role of agomelatine in disorders other than major depression. [ABSTRACT FROM AUTHOR]

Published

2015

12. The Melatonergic System in Mood and Anxiety Disorders and the Role of Agomelatine: Implications for Clinical Practice.

Author

De Berardis, Domenico, Marini, Stefano, Fornaro, Michele, Srinivasan, Venkataramanujam, Iasevoli, Felice, Tomasetti, Carmine, Valchera, Alessandro, Perna, Giampaolo, Quera-Salva, Maria-Antonia, Martinotti, Giovanni, and Giannantonio, Massimo di

Subjects

MELATONIN, G protein coupled receptors, AFFECTIVE disorders, ANXIETY disorders, MENTAL depression, DEPRESSED persons, BIOMARKERS, CHRONOBIOLOGY disorders

Abstract

Melatonin exerts its actions through membrane MT1/MT2 melatonin receptors, which belong to the super family of G-protein-coupled receptors consisting of the typical seven transmembrane domains. MT1 and MT2 receptors are expressed in various tissues of the body either as single ones or together. A growing literature suggests that the melatonergic system may be involved in the pathophysiology of mood and anxiety disorders. In fact, some core symptoms of depression show disturbance of the circadian rhythm in their clinical expression, such as diurnal mood and other symptomatic variation, or are closely linked to circadian system functioning, such as sleep-wake cycle alterations. In addition, alterations have been described in the circadian rhythms of several biological markers in depressed patients. Therefore, there is interest in developing antidepressants that have a chronobiotic effect (i.e., treatment of circadian rhythm disorders). As melatonin produces chronobiotic effects, efforts have been aimed at developing agomelatine, an antidepressant with melatonin agonist activity. The present paper reviews the role of the melatonergic system in the pathophysiology of mood and anxiety disorders and the clinical characteristics of agomelatine. Implications of agomelatine in "real world" clinical practice will be also discussed. [ABSTRACT FROM AUTHOR]

Published

2013

13. The acute and chronic effects of combined antipsychotic–mood stabilizing treatment on the expression of cortical and striatal postsynaptic density genes

Author

Tomasetti, Carmine, Dell'Aversano, Carmela, Iasevoli, Felice, Marmo, Federica, and de Bartolomeis, Andrea

Subjects

*MOOD stabilizers, *ANTIPSYCHOTIC agents, *BIPOLAR disorder, *ANTIDEPRESSANTS, *ANALYSIS of variance, *DOPAMINE, *GENE expression, *VALPROIC acid, *EXTRACELLULAR enzymes

Abstract

Abstract: The detection of changes in postsynaptic gene expression after the administration of mood stabilizers, alone or in combination with antipsychotics, and antidepressants in animal models of drug treatment, may represent a valuable strategy to explore the molecular targets of the mainstay treatments for bipolar disorder. In this study we investigated, in both acute and chronic paradigms, the expression of specific postsynaptic density genes (Homer1a, Homer1b/c, and PSD95) and genes putatively implicated in mood stabilizers mechanism of action (GSK3b, ERK) after administration of first (haloperidol) or second generation antipsychotics (quetiapine 30mg/kg), alone or in combination with valproate. Moreover, we compared the effects of an antidepressant agent widely used in bipolar depression (citalopram) with a low dose of quetiapine (15mg/kg), which has been demonstrated to display antidepressant action in bipolar depression. In striatal regions, Homer1a expression was strongly induced by haloperidol compared to all the other treatments. Haloperidol plus valproate also markedly induced Homer1a, but to a significant lesser extent than haloperidol alone. Also in the chronic paradigm haloperidol, but not haloperidol plus valproate, induced Homer1a expression in all the subregions of the caudate-putamen and in the nucleus accumbens core. The high dose of quetiapine significantly induced Homer1a in anterior cingulated, premotor and motor subregions of the cortex, and the extent of induction was significantly higher as compared to the lower dose. Oppositely, Homer1a expression was decreased in the cortex by citalopram acute administration. ERK gene was upregulated in cortex and striatum by the acute treatment with valproate and with the combination of haloperidol or quetiapine plus valproate, whereas no significant differences were noticed in GSK3b expression among treatments. PSD95 showed a significant upregulation by acute citalopram and by haloperidol plus valproate in both cortical and subcortical regions. Haloperidol and quetiapine 30mg/kg, oppositely, significantly reduced the expression of the gene in the cortex. In conclusion, these results suggest that the combined treatment with a typical or an atypical antipsychotic plus valproate may induce differential modulation of postsynaptic genes expression when compared to the effects of these drugs individually administered. [Copyright &y& Elsevier]

Published

2011

14. Antipsychotic and antidepressant co-treatment: Effects on transcripts of inducible postsynaptic density genes possibly implicated in behavioural disorders

Author

Dell’Aversano, Carmela, Tomasetti, Carmine, Iasevoli, Felice, and de Bartolomeis, Andrea

Subjects

*COMBINATION drug therapy, *SEROTONIN uptake inhibitors, *DRUG efficacy, *SCHIZOPHRENIA treatment, *GENETIC transcription, *ANTIPSYCHOTIC agents, *ANTIDEPRESSANTS, *ANALYSIS of variance

Abstract

Abstract: Selective serotonin reuptake inhibitors (SSRIs) and antipsychotics co-administration is a widely used strategy to treat both psychotic depression and depressive symptoms in schizophrenia. Nonetheless, the molecular mechanisms involved in the therapeutic benefits of antidepressant–antipsychotic combination are still elusive. It has been suggested that co-administration of SSRIs and antipsychotics may result in molecular changes different from their individual effects. In the present study, we evaluated the acute effects of two SSRIs, citalopram and escitalopram, alone or in combination with haloperidol, on the expression of Homer1a together with its splice variant ania-3, and p11, two genes linked respectively to dopaminergic and serotonergic neurotransmission and involved in synaptic plasticity. Homer1a and ania-3 were induced in the striatum by haloperidol, alone and in combination with SSRIs, but not by SSRIs only. Haloperidol+citalopram co-administration induced a stronger Homer1a expression than haloperidol alone in the ventrolateral caudate-putamen. No signal was detected for p11 in striatum, while there were no significant differences among treatments in cortical subregions. Homer1a was significantly down-regulated in the parietal cortex by all treatments. These results demonstrated that haloperidol+citalopram combination exerts synergistic effects on Homer expression, suggesting that citalopram may influence the impact by haloperidol on the dopaminergic neurotransmission. Moreover, present findings confirm that Homer1a and ania-3 are strongly induced in striatum by haloperidol, while they are not influenced by citalopram or escitalopram in this region. Oppositely, in the cortex the two transcripts are modulated by both haloperidol and SSRIs, suggesting a possible role of both dopamine and serotonin in their cortical regulation. [Copyright &y& Elsevier]

Published

2009

15. Eradicating Suicide at Its Roots: Preclinical Bases and Clinical Evidence of the Efficacy of Ketamine in the Treatment of Suicidal Behaviors.

Author

De Berardis, Domenico, Fornaro, Michele, Valchera, Alessandro, Cavuto, Marilde, Perna, Giampaolo, Di Nicola, Marco, Serafini, Gianluca, Carano, Alessandro, Pompili, Maurizio, Vellante, Federica, Orsolini, Laura, Fiengo, Annastasia, Ventriglio, Antonio, Yong-Ku, Kim, Martinotti, Giovanni, Di Giannantonio, Massimo, and Tomasetti, Carmine

Subjects

SUICIDAL behavior treatment, KETAMINE, DRUG efficacy, NEUROBIOLOGY, BIOLOGICAL tags

Abstract

Despite the continuous advancement in neurosciences as well as in the knowledge of human behaviors pathophysiology, currently suicide represents a puzzling challenge. The World Health Organization (WHO) has established that one million people die by suicide every year, with the impressive daily rate of a suicide every 40 s. The weightiest concern about suicidal behavior is how difficult it is for healthcare professionals to predict. However, recent evidence in genomic studies has pointed out the essential role that genetics could play in influencing person's suicide risk. Combining genomic and clinical risk assessment approaches, some studies have identified a number of biomarkers for suicidal ideation, which are involved in neural connectivity, neural activity, mood, as well as in immune and inflammatory response, such as the mammalian target of rapamycin (mTOR) signaling. This interesting discovery provides the neurobiological bases for the use of drugs that impact these specific signaling pathways in the treatment of suicidality, such as ketamine. Ketamine, an N-methyl-d-aspartate glutamate (NMDA) antagonist agent, has recently hit the headlines because of its rapid antidepressant and concurrent anti-suicidal action. Here we review the preclinical and clinical evidence that lay the foundations of the efficacy of ketamine in the treatment of suicidal ideation in mood disorders, thereby also approaching the essential question of the understanding of neurobiological processes of suicide and the potential therapeutics. [ABSTRACT FROM AUTHOR]

Published

2018

16. Imaging brain gene expression profiles by antipsychotics: Region-specific action of amisulpride on postsynaptic density transcripts compared to haloperidol.

Author

de Bartolomeis, Andrea, Marmo, Federica, Buonaguro, Elisabetta Filomena, Rossi, Rodolfo, Tomasetti, Carmine, and Iasevoli, Felice

Subjects

*BRAIN imaging, *GENE expression, *ANTIPSYCHOTIC agents, *AMISULPRIDE, *HALOPERIDOL, *MOVEMENT disorders

Abstract

Abstract: Induction of motor disorders is considered the clinical landmark differentiating typical from atypical antipsychotics, and has been mainly correlated to dopamine D2 receptors blockade in striatum. This view is challenged by benzamides, such as amisulpride, which display low liability for motor side effects despite being D2/D3 receptors high-affinity blocking agents. These effects have been explained with the prominent presynaptic action of amisulpride or with the fast dissociation at D2 receptors, but there is scarce information on the effects of amisulpride on postsynaptic signaling. We carried out a molecular imaging study of gene expression after acute administration of haloperidol (0.8mg/kg), amisulpride (10 or 35mg/kg), or vehicle, focusing on postsynaptic genes that are key regulators of synaptic plasticity, such as Arc, c-fos, Zif-268, Norbin, Homer. The last one has been associated to schizophrenia both in clinical and preclinical studies, and is differentially induced by antipsychotics with different D2 receptors affinity. Topography of gene expression revealed that amisulpride, unlike haloperidol, triggers transcripts expression peak in medial striatal regions. Correlation analysis of gene expression revealed a prevalent correlated gene induction within motor corticostriatal regions by haloperidol and a more balanced gene induction within limbic and motor corticostriatal regions by amisulpride. Despite the selective dopaminergic profile of both compounds, our results demonstrated a differential modulation of postsynaptic molecules by amisulpride and haloperidol, the former impacting preferentially medial regions of striatum whereas the latter inducing strong gene expression in lateral regions. Thus, we provided a possible molecular profile of amisulpride, putatively explaining its “atypical atypicality”. [Copyright &y& Elsevier]

Published

2013

17. Different effects of the NMDA receptor antagonists ketamine, MK-801, and memantine on postsynaptic density transcripts and their topography: Role of Homer signaling, and implications for novel antipsychotic and pro-cognitive targets in psychosis.

Author

de Bartolomeis, Andrea, Sarappa, Chiara, Buonaguro, Elisabetta F., Marmo, Federica, Eramo, Anna, Tomasetti, Carmine, and Iasevoli, Felice

Subjects

*METHYL aspartate receptors, *KETAMINE, *MEMANTINE, *POSTSYNAPTIC density protein, *BRAIN mapping, *SCAFFOLD proteins, *ANTIPSYCHOTIC agents, *COGNITION

Abstract

Abstract: Administration of NMDA receptor antagonists, such as ketamine and MK-801, may induce psychotic-like behaviors in preclinical models of schizophrenia. Ketamine has also been observed to exacerbate psychotic symptoms in schizophrenia patients. However, memantine, a non-competitive NMDA receptor antagonist approved for Alzheimer's disease and proposed for antipsychotic augmentation, may challenge this view. To date, the molecular mechanisms by which these NMDA receptor antagonists cause different neurochemical, behavioral, and clinical effects are still a matter of debate. Here, we investigated by molecular imaging whether these agents could differently modulate gene expression and topographical distribution of glutamatergic postsynaptic density (PSD) proteins. We focused on Homer1a/Homer1b/PSD-95 signaling network, which may be implicated in glutamate-dependent synaptic plasticity, as well as in psychosis pathophysiology and treatment. Ketamine (25 and 50mg/kg) and MK-801 (0.8mg/kg) significantly induced the transcripts of immediate-early genes (Arc, c-fos, and Homer1a) in cortical regions compared to vehicle, whereas they reduced Homer1b and PSD-95 expression in cortical and striatal regions. Differently, memantine (5mg/kg) did not increase Homer1a signal compared to vehicle, whereas it induced c-fos in the somatosensory and in the medial agranular cortices. Moreover, memantine did not affect Homer1b and PSD-95 expression. When compared to ketamine and MK-801, memantine significantly increased the expression of c-fos, Homer1b and PSD-95. Overall, ketamine and MK-801 prominently increased Homer1a/Homer1b expression ratio, whereas memantine elicited the opposite effect. These data may support the view that ketamine, MK-801 and memantine exert divergent effects on PSD transcripts, which may contribute to their partially different behavioral and clinical effects. [Copyright &y& Elsevier]

Published

2013

18. Nicotine and caffeine modulate haloperidol-induced changes in postsynaptic density transcripts expression: Translational insights in psychosis therapy and treatment resistance

Author

Gianmarco Latte, Carmine Tomasetti, Federica Marmo, Andrea de Bartolomeis, Livia Avvisati, Felice Iasevoli, Elisabetta F. Buonaguro, de Bartolomeis, Andrea, Iasevoli, Felice, Marmo, Federica, Buonaguro, Elisabetta Filomena, Avvisati, Livia, Latte, Gianmarco, and Tomasetti, Carmine

Subjects

Male, medicine.medical_treatment, Drug Resistance, Pharmacology, Nicotine, Rats, Sprague-Dawley, chemistry.chemical_compound, Random Allocation, 0302 clinical medicine, Homer Scaffolding Proteins, Haloperidol, Medicine, Drug Interactions, Pharmacology (medical), Arc (protein), Brain, Arc, Neurology, Psychiatry and Mental Health, Caffeine, medicine.drug, Psychosis, Homer1, HOMER1, Nerve Tissue Proteins, Motor Activity, behavioral disciplines and activities, 03 medical and health sciences, Dopamine, Animals, RNA, Messenger, Antipsychotic, Biological Psychiatry, business.industry, Post-Synaptic Density, medicine.disease, 030227 psychiatry, Cytoskeletal Proteins, chemistry, Psychotic Disorders, Schizophrenia, Gene expression, Neurology (clinical), business, 030217 neurology & neurosurgery, PSD protein, Central Nervous System Agents

Abstract

Caffeine and nicotine are widely used by schizophrenia patients and may worsen psychosis and affect antipsychotic therapies. However, they have also been accounted as augmentation strategies in treatment-resistant schizophrenia. Despite both substances are known to modulate dopamine and glutamate transmission, little is known about the molecular changes induced by these compounds in association to antipsychotics, mostly at the level of the postsynaptic density (PSD), a site of dopamine-glutamate interplay. Here we investigated whether caffeine and nicotine, alone or combined with haloperidol, elicited significant changes in the levels of both transcripts and proteins of the PSD members Homer1 and Arc, which have been implicated in synaptic plasticity, schizophrenia pathophysiology, and antipsychotics molecular action. Homer1a mRNA expression was significantly reduced by caffeine and nicotine, alone or combined with haloperidol, compared to haloperidol. Haloperidol induced significantly higher Arc mRNA levels than both caffeine and caffeine plus haloperidol in the striatum. Arc mRNA expression was significantly higher by nicotine plus haloperidol vs. haloperidol in the cortex, while in striatum gene expression by nicotine was significantly lower than that by both haloperidol and nicotine plus haloperidol. Both Homer1a and Arc protein levels were significantly increased by caffeine, nicotine, and nicotine plus haloperidol. Homer1b mRNA expression was significantly increased by nicotine and nicotine plus haloperidol, while protein levels were unaffected. Locomotor activity was not significantly affected by caffeine, while it was reduced by nicotine. These data indicate that both caffeine and nicotine trigger relevant molecular changes in PSD sites when given in association with haloperidol.

Published

2018

19. Treating the Synapse in Major Psychiatric Disorders: The Role of Postsynaptic Density Network in Dopamine-Glutamate Interplay and Psychopharmacologic Drugs Molecular Actions

Author

Michele Fornaro, Felice Iasevoli, Andrea de Bartolomeis, Giovanni Martinotti, Carmine Tomasetti, Massimo Di Giannantonio, Elisabetta F. Buonaguro, Domenico De Berardis, Laura Orsolini, Annastasia L.C. Fiengo, Alessandro Valchera, Tomasetti, Carmine, Iasevoli, Felice, Buonaguro, ELISABETTA FILOMENA, De Berardis, Domenico, Fornaro, Michele, Fiengo, ANNASTASIA LUCIA CARMELA, Martinotti, Giovanni, Orsolini, Laura, Valchera, Alessandro, Di Giannantonio, Massimo, and DE BARTOLOMEIS, Andrea

Subjects

0301 basic medicine, medicine.medical_specialty, Dopamine, Glutamic Acid, Review, Neurotransmission, Biology, Models, Biological, Catalysis, transductional pathways, Inorganic Chemistry, Synapse, lcsh:Chemistry, 03 medical and health sciences, Glutamatergic, 0302 clinical medicine, Postsynaptic potential, medicine, Animals, Humans, Physical and Theoretical Chemistry, Psychiatry, Molecular Biology, lcsh:QH301-705.5, Spectroscopy, postsynaptic density (PSD), bipolar disorder, Organic Chemistry, Glutamate receptor, Intracellular Signaling Peptides and Proteins, Post-Synaptic Density, General Medicine, Computer Science Applications, schizophrenia, 030104 developmental biology, Homer, Psychotic Disorders, lcsh:Biology (General), lcsh:QD1-999, Excitatory postsynaptic potential, gene expression, Postsynaptic density, 030217 neurology & neurosurgery, medicine.drug, Antipsychotic Agents, Signal Transduction

Abstract

Dopamine-glutamate interplay dysfunctions have been suggested as pathophysiological key determinants of major psychotic disorders, above all schizophrenia and mood disorders. For the most part, synaptic interactions between dopamine and glutamate signaling pathways take part in the postsynaptic density, a specialized ultrastructure localized under the membrane of glutamatergic excitatory synapses. Multiple proteins, with the role of adaptors, regulators, effectors, and scaffolds compose the postsynaptic density network. They form structural and functional crossroads where multiple signals, starting at membrane receptors, are received, elaborated, integrated, and routed to appropriate nuclear targets. Moreover, transductional pathways belonging to different receptors may be functionally interconnected through postsynaptic density molecules. Several studies have demonstrated that psychopharmacologic drugs may differentially affect the expression and function of postsynaptic genes and proteins, depending upon the peculiar receptor profile of each compound. Thus, through postsynaptic network modulation, these drugs may induce dopamine-glutamate synaptic remodeling, which is at the basis of their long-term physiologic effects. In this review, we will discuss the role of postsynaptic proteins in dopamine-glutamate signals integration, as well as the peculiar impact of different psychotropic drugs used in clinical practice on postsynaptic remodeling, thereby trying to point out the possible future molecular targets of "synapse-based" psychiatric therapeutic strategies.

Published

2017

20. Differential Adaptive Changes in Dopaminergic System by Acute vs. Subchronic Ketamine: Relevance for Psychosis Pathophysiology and Treatment

Author

Carmine Tomasetti, Andrea de Bartolomeis, Gianmarco Latte, Felice Iasevoli, Livia Avvisati, Luigi Aloj, Elisabetta F. Buonaguro, Iasevoli, Felice, Avvisati, Livia, Latte, Gianmarco, Buonaguro, ELISABETTA FILOMENA, Tomasetti, Carmine, Aloj, Luigi, and DE BARTOLOMEIS, Andrea

Subjects

Psychosis, business.industry, Dopaminergic, Glutamate receptor, medicine.disease, Bioinformatics, Pathophysiology, Endocrinology, Schizophrenia, Dopamine, Anesthesia, Dopamine receptor D2, Medicine, Pharmacology (medical), Ketamine, business, medicine.drug

Published

2013

21. The acute and chronic effects of combined antipsychotic–mood stabilizing treatment on the expression of cortical and striatal postsynaptic density genes

Author

Carmine Tomasetti, Andrea de Bartolomeis, Felice Iasevoli, Federica Marmo, Carmela Dell'Aversano, Tomasetti, Carmine, Dell'Aversano, Carmela, Iasevoli, Felice, Marmo, Federica, and DE BARTOLOMEIS, Andrea

Subjects

Male, medicine.medical_specialty, Time Factors, Bipolar disorder, medicine.drug_class, Dopamine, medicine.medical_treatment, Atypical antipsychotic, Nerve Tissue Proteins, Citalopram, behavioral disciplines and activities, Rats, Sprague-Dawley, Glycogen Synthase Kinase 3, Homer Scaffolding Proteins, Antimanic Agents, Internal medicine, Homer1a, medicine, Haloperidol, Animals, RNA, Messenger, Extracellular Signal-Regulated MAP Kinases, Antipsychotic, Biological Psychiatry, Cerebral Cortex, Pharmacology, Valproate, Analysis of Variance, Glycogen Synthase Kinase 3 beta, Quetiapine, Intracellular Signaling Peptides and Proteins, Membrane Proteins, Mood stabilizer, Corpus Striatum, Rats, Drug Combinations, Endocrinology, Anticonvulsant, Gene Expression Regulation, Autoradiography, Antidepressant, Carrier Proteins, Psychology, Disks Large Homolog 4 Protein, Antipsychotic Agents, medicine.drug

Abstract

The detection of changes in postsynaptic gene expression after the administration of mood stabilizers, alone or in combination with antipsychotics, and antidepressants in animal models of drug treatment, may represent a valuable strategy to explore the molecular targets of the mainstay treatments for bipolar disorder. In this study we investigated, in both acute and chronic paradigms, the expression of specific postsynaptic density genes ( Homer1a, Homer1b/c , and PSD95) and genes putatively implicated in mood stabilizers mechanism of action ( GSK3b, ERK ) after administration of first (haloperidol) or second generation antipsychotics (quetiapine 30 mg/kg), alone or in combination with valproate. Moreover, we compared the effects of an antidepressant agent widely used in bipolar depression (citalopram) with a low dose of quetiapine (15 mg/kg), which has been demonstrated to display antidepressant action in bipolar depression. In striatal regions, Homer1a expression was strongly induced by haloperidol compared to all the other treatments. Haloperidol plus valproate also markedly induced Homer1a , but to a significant lesser extent than haloperidol alone. Also in the chronic paradigm haloperidol, but not haloperidol plus valproate, induced Homer1a expression in all the subregions of the caudate-putamen and in the nucleus accumbens core. The high dose of quetiapine significantly induced Homer1a in anterior cingulated, premotor and motor subregions of the cortex, and the extent of induction was significantly higher as compared to the lower dose. Oppositely, Homer1a expression was decreased in the cortex by citalopram acute administration. ERK gene was upregulated in cortex and striatum by the acute treatment with valproate and with the combination of haloperidol or quetiapine plus valproate, whereas no significant differences were noticed in GSK3b expression among treatments. PSD95 showed a significant upregulation by acute citalopram and by haloperidol plus valproate in both cortical and subcortical regions. Haloperidol and quetiapine 30 mg/kg, oppositely, significantly reduced the expression of the gene in the cortex. In conclusion, these results suggest that the combined treatment with a typical or an atypical antipsychotic plus valproate may induce differential modulation of postsynaptic genes expression when compared to the effects of these drugs individually administered.

Published

2011

22. Agomelatine beyond borders: current evidences of its efficacy in disorders other than major depression

Author

Nicola Serroni, Andrea de Bartolomeis, Massimo Di Giannantonio, Luigi Olivieri, Monica Mazza, Domenico De Berardis, Giampaolo Perna, Alessandro Valchera, Daniela Campanella, Michele Fornaro, Carmine Tomasetti, Gabriella Rapini, Giovanni Martinotti, Marco Di Nicola, Felice Iasevoli, Venkataramanujam Srinivasan, Psychiatrie & Neuropsychologie, RS: MHeNs - R2 - Mental Health, De Berardis, Domenico, Fornaro, Michele, Serroni, Nicola, Campanella, Daniela, Rapini, Gabriella, Olivieri, Luigi, Srinivasan, Venkataramanujam, Iasevoli, Felice, Tomasetti, Carmine, DE BARTOLOMEIS, Andrea, Valchera, Alessandro, Perna, Giampaolo, Mazza, Monica, Di Nicola, Marco, Martinotti, Giovanni, and Di Giannantonio, Massimo

Subjects

migraines, Bipolar Disorder, Chronobiotic, alcohol dependence, melatonin, Review, lcsh:Chemistry, melatonergic receptors, Migraine Disorder, Acetamides, Receptor, Serotonin, 5-HT2C, lcsh:QH301-705.5, Spectroscopy, bipolar depression, Dopaminergic, General Medicine, anxiety, Antidepressive Agents, Computer Science Applications, serotonin, psychiatric disorders, Schizophrenia, Antidepressant, Antidepressive Agent, fibromyalgia, dopamine, agomelatine, medicine.drug, Human, Sleep Wake Disorders, medicine.medical_specialty, Migraine Disorders, Catalysis, Inorganic Chemistry, Dopamine, seasonal affective disorder, Internal medicine, medicine, Agomelatine, Humans, Bipolar disorder, Physical and Theoretical Chemistry, Molecular Biology, Depressive Disorder, business.industry, Receptor, Melatonin, MT2, Receptor, Melatonin, MT1, Organic Chemistry, medicine.disease, schizophrenia, Endocrinology, lcsh:Biology (General), lcsh:QD1-999, noradrenaline, Serotonin, business, Neuroscience, Acetamide

Abstract

Agomelatine, a melatonergic antidepressant with a rapid onset of action, is one of the most recent drugs in the antidepressant category. Agomelatine's antidepressant actions are attributed to its sleep-promoting and chronobiotic actions mediated by MT1 and MT2 receptors present in the suprachiasmatic nucleus, as well as to its effects on the blockade of 5-HT2c receptors. Blockade of 5-HT2c receptors causes release of both noradrenaline and dopamine at the fronto-cortical dopaminergic and noradrenergic pathways. The combined actions of agomelatine on MT1/MT2 and 5-HT2c receptors facilitate the resynchronization of altered circadian rhythms and abnormal sleep patterns. Agomelatine appeared to be effective in treating major depression. Moreover, evidence exists that points out a possible efficacy of such drug in the treatment of bipolar depression, anxiety disorders, alcohol dependence, migraines etc. Thus, the aim of this narrative review was to elucidate current evidences on the role of agomelatine in disorders other than major depression.

Published

2015

23. MicroRNAs in Schizophrenia: Implications for Synaptic Plasticity and Dopamine-Glutamate Interaction at the Postsynaptic Density. New Avenues for Antipsychotic Treatment Under a Theranostic Perspective

Author

Andrea de Bartolomeis, Carmine Tomasetti, Elisabetta F. Buonaguro, Felice Iasevoli, DE BARTOLOMEIS, Andrea, Iasevoli, Felice, Tomasetti, Carmine, and Buonaguro, ELISABETTA FILOMENA

Subjects

Psychosis, Dopamine, Negative symptom, Neuroscience (miscellaneous), Glutamic Acid, Psychosi, Context (language use), Antipsychotic, Synapse, Cellular and Molecular Neuroscience, medicine, Animals, Humans, PSD-95, Neuronal Plasticity, Glutamate receptor, Mood stabilizer, medicine.disease, MicroRNAs, Homer, Neurology, Schizophrenia, Synaptic plasticity, Psychology, Postsynaptic density, Neuroscience, medicine.drug, Antipsychotic Agents

Abstract

Despite dopamine-glutamate aberrant interaction that has long been considered a relevant landmark of psychosis pathophysiology, several aspects of these two neurotransmitters reciprocal interaction remain to be defined. The emerging role of postsynaptic density (PSD) proteins at glutamate synapse as a molecular "lego" making a functional hub where different signals converge may add a new piece of information to understand how dopamine-glutamate interaction may work with regard to schizophrenia pathophysiology and treatment. More recently, compelling evidence suggests a relevant role for microRNA (miRNA) as a new class of dopamine and glutamate modulators with regulatory functions in the reciprocal interaction of these two neurotransmitters. Here, we aimed at addressing the following issues: (i) Do miRNAs have a role in schizophrenia pathophysiology in the context of dopamine-glutamate aberrant interaction? (ii) If miRNAs are relevant for dopamine-glutamate interaction, at what level this modulation takes place? (iii) Finally, will this knowledge open the door to innovative diagnostic and therapeutic tools? The biogenesis of miRNAs and their role in synaptic plasticity with relevance to schizophrenia will be considered in the context of dopamine-glutamate interaction, with special focus on miRNA interaction with PSD elements. From this framework, implications both for biomarkers identification and potential innovative interventions will be considered.

Published

2014

24. The Glucocorticoid Analog Dexamethasone Alters the Expression and the Distribution of Dopamine Receptors and Enkephalin within Cortico-subcortical Regions

Author

Federica Marmo, Luigi Aloj, Carmine Tomasetti, Annamaria Colao, Rosario Pivonello, Gianmarco Latte, Chiara Simeoli, Felice Iasevoli, Livia Avvisati, Andrea de Bartolomeis, Elisabetta F. Buonaguro, Iasevoli, Felice, Aloj, L, Latte, Gianmarco, Avvisati, Livia, Marmo, Federica, Tomasetti, Carmine, Buonaguro, ELISABETTA FILOMENA, Simeoli, Chiara, Pivonello, Rosario, Colao, Annamaria, and DE BARTOLOMEIS, Andrea

Subjects

Male, medicine.medical_specialty, Enkephalin, Dexamethasone, Rats, Sprague-Dawley, Cerebellar Cortex, Dopamine receptor D1, Glucocorticoid receptor, Dopamine, Mesencephalon, Internal medicine, Dopamine receptor D2, medicine, dopamine receptor, Animals, RNA, Messenger, glucocorticoids, Chemistry, Receptors, Dopamine D2, Receptors, Dopamine D1, Dopaminergic, General Medicine, Enkephalins, Corpus Striatum, Rats, Endocrinology, nervous system, Gene Expression Regulation, Dopamine receptor, Glucocorticoid, medicine.drug

Abstract

In humans, glucocorticoid excess may cause neuropsychiatric symptoms, including psychosis and cognitive impairment, and glucocorticoid signaling hyperactivation may sensitize to substance of abuse. The aim of this work was to evaluate whether exposure to glucocorticoid excess triggers molecular changes in dopaminergic and opioidergic systems within relevant forebrain areas. Methods: We acutely exposed Sprague-Dawley rats to dexamethasone, a glucocorticoid analogue, or vehicle and evaluated the mRNA expression of dopamine D1 and D2 receptors and enkephalin within the cortex, the striatum, and the midbrain. Results: Dexamethasone reduced mRNA expression of D1 receptor and enkephalin in the cortex. In the striatum, dexamethasone reduced the expression of D1 receptor mRNA, but not that of D2 receptor and enkephalin. No significant changes in D2 receptor mRNA expression were observed in the midbrain. Basal distribution of D1 and D2 receptor mRNA showed a clear-cut striatal/cortical gradient, while this distribution was less obvious for enkephalin mRNA. Dexamethasone increased the cortico-striatal separation in terms of D1 and D2 receptor mRNA expression. Discussion: These molecular changes may represent adaptive mechanisms to dexamethasone-induced potentiation of dopaminergic and opioidergic transmission, mostly in cortical areas.

Published

2013

25. Calcium-dependent networks in dopamine-glutamate interaction: the role of postsynaptic scaffolding proteins

Author

Carmine Tomasetti, Andrea de Bartolomeis, DE BARTOLOMEIS, Andrea, and Tomasetti, Carmine

Subjects

Scaffold protein, Psychosis, Dopamine, Neuroscience (miscellaneous), Glutamic Acid, Psychosi, Nerve Tissue Proteins, Shank, Cellular and Molecular Neuroscience, Glutamatergic, Postsynaptic potential, medicine, Antipsychotics, Animals, Humans, Dopaminergic, Glutamate receptor, Postsynaptic density, PSD95, medicine.disease, Homer, Neurology, Calcium, Nerve Net, Psychology, Neuroscience, medicine.drug, Antipsychotic Agents

Abstract

Dopamine and glutamate systems are both involved in cognitive, behavioral, and motor processes. Dysfunction of dopamine-glutamate interplay has been suggested in several psychotic diseases, above all in schizophrenia, for which there exists a need for novel medications. Intracellular calcium-dependent transduction pathways are key determinants of dopamine-glutamate interactions, which take place mainly, albeit not exclusively, in the postsynaptic density (PSD), a highly specialized postsynaptic ultrastructure. Stimulation of dopamine and glutamate receptors modulates the gene expression and the function of specific PSD proteins, the "scaffolding" proteins (Homer, Shank, and PSD95), belonging to a complex Ca(2+)-regulated network that integrates and converges dopamine and glutamate signaling to appropriate nuclear targets. Dysfunction of scaffolding proteins leads to severe impairment of Ca(2+)-dependent signaling, which may underlie the dopamine-glutamate aberrations putatively implicated in the pathogenesis of psychotic disorders. Antipsychotic therapy has been demonstrated to directly and indirectly affect the neuronal Ca(2+)-dependent pathways through the modulation of PSD scaffolding proteins, such as Homer, therefore influencing both dopaminergic and glutamatergic functions and enforcing Ca(2+)-mediated long-term synaptic changes. In this review, we will discuss the role of PSD scaffolding proteins in routing Ca(2+)-dependent signals to the nucleus. In particular, we will address the implication of PSD scaffolding proteins in the intracellular connections between dopamine and glutamate pathways, which involve both Ca(2+)-dependent and Ca(2+)-independent mechanisms. Finally, we will discuss how new strategies for the treatment of psychosis aim at developing antipsychotics that may impact both glutamate and dopamine signaling, and what should be the possible role of PSD scaffolding proteins.

Published

2012