7 results on '"Merlo-Pich E"'
Search Results
2. Involvement of α6 nicotinic receptor subunit in nicotine-elicited locomotion, demonstrated by in vivo antisense oligonucleotide infusion
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Merlo-Pich E, Jean-Pierre Changeux, le Novère N, Clément Léna, Marina R. Picciotto, Michele Zoli, and Rosaria Ferrari
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Male ,medicine.medical_specialty ,Nicotine ,Protein subunit ,Molecular Sequence Data ,Pharmacology ,Biology ,Receptors, Nicotinic ,Rats, Sprague-Dawley ,chemistry.chemical_compound ,In vivo ,Mesencephalon ,Internal medicine ,medicine ,acetylcholine ,cholinergic behavior ,dopaminergic system ,Animals ,Amino Acid Sequence ,Neurotransmitter ,Cells, Cultured ,Acetylcholine receptor ,Neurons ,General Neuroscience ,Dopaminergic ,Infusion Pumps, Implantable ,Oligonucleotides, Antisense ,Peptide Fragments ,Rats ,Endocrinology ,Nicotinic agonist ,chemistry ,Acetylcholine ,Locomotion ,medicine.drug - Abstract
Enhanced locomotion in a habituated environment is a well documented effect of nicotine mediated by the mesotelencephalic dopaminergic system. The nicotinic receptor subunit alpha6 is, among other subunits, strongly expressed in the dopaminergic neurons of the mesencephalon. To examine the functional role of this subunit, we inhibited its expression in vivo using antisense oligonucleotides. In vitro treatments of embryonic mesencephalic neuron cultures demonstrated that the alpha6 antisense oligonucleotides caused a marked decrease in the level of alpha6 subunit protein. In vivo, 1 week infusion of alpha6 antisense oligonucleotides by osmotic mini-pump reduced the effect of nicotine on locomotor activity in habituated environment by 70%. These data support the notion that the effects of nicotine on the dopaminergic system involve alpha6 subunit containing nAChRs.
3. Social dysfunction in mood disorders and schizophrenia
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Dan Rujescu, Daniel Souery, Brenda W.J.H. Penninx, Emilio Merlo Pich, Alessandro Serretti, Julien Mendlewicz, Siegfried Kasper, Stuart Montgomery, Joseph Zohar, Stefano Porcelli, Stephane Pollentier, Panagiotis Ferentinos, Porcelli S., Kasper S., Zohar J., Souery D., Montgomery S., Ferentinos P., Rujescu D., Mendlewicz J., Merlo Pich E., Pollentier S., Penninx B.W.J.H., Serretti A., Psychiatry, APH - Mental Health, Amsterdam Neuroscience - Mood, Anxiety, Psychosis, Stress & Sleep, and APH - Digital Health
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Adult ,Male ,Social adjustment ,Younger age ,Bipolar Disorder ,Mood disorder ,Pharmacologie ,Lifestyle factors ,03 medical and health sciences ,Young Adult ,0302 clinical medicine ,Physiopsychologie et psychologie biologique [psychiatrie] ,Independent samples ,Medicine ,Humans ,Social Behavior ,Biological Psychiatry ,Pharmacology ,Depressive Disorder, Major ,business.industry ,Mood Disorders ,Lifestyle factor ,medicine.disease ,Socio-demographic factors ,030227 psychiatry ,Cross-Sectional Studies ,Mood disorders ,Schizophrenia ,Marital status ,Social dysfunction ,Female ,Schizophrenic Psychology ,business ,Psychopathology ,Clinical psychology - Abstract
Introduction: Social dysfunction is a common symptom of several neuropsychiatric disorders. However, only in the last few years research began to systematically investigate clinical aspects of this relevant outcome. Interestingly, its distribution and link with other clinical variables is still unclear. This study investigated social dysfunction in 4 different cohorts of patients affected by mood disorders and schizophrenia to evaluate 1) the degree of social dysfunction in these populations; 2) the associations among social dysfunction and socio-demographic and psychopathological features. Methods: Data from 4 independent studies (CATIE, GSRD ES1, ES2 and ES3, STAR*D, STEP-BD) were investigated. Behavioural and affective indicators of social dysfunction were derived and operationalized from scales or questionnaire items related to the interaction with relatives, friends and significant people in patients affected by schizophrenia (N = 765) and mood disorders (N = 2278 + 1954 + 1829). In particular the social dysfunction indicator was derived from Sheehan Disability Scale (SDS) for GSRD sample, from the Work and Social Adjustment Scale (WSAS) for STAR*D sample, from the Life-Range of Impaired Functioning Tool (LRIFT) for STEP-BD sample, and from the Quality of Life Scale (QOLS) for CATIE sample. The distribution of social dysfunction was described and association with socio-demographic and psychopathological characteristics were analysed. Results: Social dysfunction indicators showed a broad distribution in all samples investigated. Consistently across studies, social dysfunction was associated with higher psychopathological severity (all samples except CATIE) and suicide risk (GSRD ES1 and ES2, STAR*D, and STEP-BD) that explain up to 47% of the variance, but also to lower education level (GSRD ES2, STAR*D, CATIE, and STEP-BD), poorer professional/work status (GSRD ES2 and ES3, STAR*D, CATIE, and STEP-BD), marital status (STAR*D and CATIE), age (younger age in GSRD ES1 and STAR*D, older age in CATIE), higher BMI (GSRD ES2 and ES3, and STEP-BD), and smoking (GSRD ES2 and ES3). Conclusion: Our results demonstrated that a significant percentage of patients affected by both mood disorders and schizophrenia shows relevant social dysfunction. Social dysfunction is related, but not completely explained by psychopathological severity. In several patients, it tends to persist also during remission state. Socio-demographic and lifestyle factors were also found to play a role and should therefore be taken into consideration in further studies investigating social dysfunction., SCOPUS: ar.j, info:eu-repo/semantics/published
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- 2020
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4. Negative Symptoms of Schizophrenia and Dopaminergic Transmission: Translational Models and Perspectives Opened by iPSC Techniques
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Ginetta Collo, Armida Mucci, Giulia M. Giordano, Emilio Merlo Pich, Silvana Galderisi, Collo, G., Mucci, A., Giordano, G. M., Merlo Pich, E., and Galderisi, S.
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Review ,Biology ,lcsh:RC321-571 ,Dopamine receptor D1 ,Dopamine receptor D3 ,Dopamine ,medicine ,negative symptom ,Induced pluripotent stem cell ,Prefrontal cortex ,Receptor ,lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry ,negative symptoms ,iPSC ,General Neuroscience ,animal model ,Dopaminergic ,Correction ,medicine.disease ,animal models ,schizophrenia ,Schizophrenia ,dopamine ,Neuroscience ,medicine.drug - Abstract
Negative symptoms (NS) represent a heterogeneous dimension of schizophrenia (SCZ), associated with a poor functional outcome. A dysregulated dopamine (DA) system, including a reduced D1 receptor activation in the prefrontal cortex, DA hypoactivity in the caudate and alterations in D3 receptor activity, seems to contribute to the pathogenesis of NS. However, failure to take into account the NS heterogeneity has slowed down progress in research on their neurobiological correlates and discoveries of new effective treatments. A better neurobiological characterization of NS is needed, and this requires objective quantification of their features that can be applied in translational models, such as animal models and human inducible pluripotent stem cells (iPSC). In this review we summarize the evidence for dopaminergic alterations relevant to NS in translational animal models focusing on dysfunctional motivation, a core aspect of NS. Among others, experiments on mutant rodents with an overexpression of DA D2 or D3 receptors and the dopamine deficient mice are discussed. In the second part we summarize the findings from recent studies using iPSC to model the pathogenesis of SCZ. By retaining the genetic background of risk genetic variants, iPSC offer the possibility to study the effect of de novo mutations or inherited polymorphisms from subgroups of patients and their response to drugs, adding an important tool for personalized psychiatry. Given the key role of DA in NS, we focus on findings of iPSC-derived DA neurons. Since implementation of iPSC-derived neurons to study the neurobiology of SCZ is a relatively recent acquisition, the available data are limited. We highlight some methodological aspects of relevance in the interpretation of in vitro testing results, including limitations and strengths, offering a critical viewpoint for the implementation of future pharmacological studies aimed to the discovery and characterization of novel treatments for NS.
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- 2020
5. Relating constructs of attention and working memory to social withdrawal in Alzheimer's disease and schizophrenia: issues regarding paradigm selection
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Gerard R. Dawson, Stefano Porcelli, Valerie Bertaina-Anglade, Jeffrey C. Glennon, Estibaliz Arce, Emilio Merlo Pich, Hugh Marston, Rouba Kozak, Alessandro Serretti, Brian T. Harel, Juergen Dukart, Antonio Lobo, Darrel J. Pemberton, Raúl López-Antón, Gary Gilmour, Martha N. Havenith, Anja Hayen, Gilmour G., Porcelli S., Bertaina-Anglade V., Arce E., Dukart J., Hayen A., Lobo A., Lopez-Anton R., Merlo Pich E., Pemberton D.J., Havenith M.N., Glennon J.C., Harel B.T., Dawson G., Marston H., Kozak R., and Serretti A.
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Research design ,PRISM ,social withdrawal ,Interpersonal Relation ,translation ,Disease ,Neuropsychological Tests ,Alzheimer's Disease ,Spatial memory ,Behavioral Neuroscience ,0302 clinical medicine ,IMI ,Attention ,Social isolation ,Brain Mapping ,05 social sciences ,Neuropsychology ,Brain ,Electroencephalography ,Magnetic Resonance Imaging ,Memory, Short-Term ,Neuropsychology and Physiological Psychology ,Social Isolation ,Research Design ,Neuropsychological Test ,Schizophrenic Psychology ,Alzheimer's disease ,medicine.symptom ,Psychology ,Human ,Cognitive psychology ,Neuroinformatics ,Cognitive Neuroscience ,working memory ,03 medical and health sciences ,Interpersonal relationship ,All institutes and research themes of the Radboud University Medical Center ,Alzheimer Disease ,medicine ,Animals ,Humans ,Interpersonal Relations ,0501 psychology and cognitive sciences ,050102 behavioral science & comparative psychology ,Neurodevelopmental disorders Donders Center for Medical Neuroscience [Radboudumc 7] ,Animal ,Working memory ,medicine.disease ,schizophrenia ,Disease Models, Animal ,030217 neurology & neurosurgery - Abstract
Central nervous system diseases are not currently diagnosed based on knowledge of biological mechanisms underlying their symptoms. Greater understanding may be offered through an agnostic approach to traditional disease categories, where learning more about shared biological mechanisms across conditions could potentially reclassify sub-groups of patients to allow realisation of more effective treatments. This review represents the output of the collaborative group “PRISM”, tasked with considering assay choices for assessment of attention and working memory in a transdiagnostic cohort of Alzheimer''s disease and schizophrenia patients exhibiting symptomatic spectra of social withdrawal. A multidimensional analysis of this nature has not been previously attempted. Nominated assays (continuous performance test III, attention network test, digit symbol substitution, N-back, complex span, spatial navigation in a virtual environment) reflected a necessary compromise between the need for broad assessment of the neuropsychological constructs in question with several pragmatic criteria: patient burden, compatibility with neurophysiologic measures and availability of preclinical homologues.
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- 2019
6. Pressor responses to hyperventilation in elderly subjects differentiate essential from secondary hypertension
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Pasquale Bernardi, Carmine Pizzi, Fiorella Fontana, Emilio Merlo Pich, Fontana F, Bernardi P, Pizzi C, and Merlo Pich E.
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education.field_of_study ,Ambulatory blood pressure ,HYPERVENTILATION ,HYPERTENSION ,business.industry ,Population ,Secondary hypertension ,White coat hypertension ,General Medicine ,medicine.disease ,Essential hypertension ,Blood pressure ,ELDERLY SUBJECTS ,Anesthesia ,Respiratory alkalosis ,Hyperventilation ,Medicine ,medicine.symptom ,business ,education - Abstract
We evaluated pressor responses to the hyperventilation test in elderly normotensive (n=43, mean age 82 ± 5 years) and elderly hypertensive subjects (n=45 with essential hypertension, mean age 82 ± 2 years, and n=49 with secondary hypertension, mean age 82 ± 3 years). Hyperventilation did not change blood pressure (BP) in normotensive and secondary hypertensive subjects, whereas it decreased BP in essential hypertensives. Hierarchical cluster analysis based on BP responses to hyperventilation disclosed three groups of subjects in each population: group 1 exhibited a reduction in BP (essential hypertensives: 76%), group 2 no change (normotensives: 70%, secondary hypertensives: 76%), and group 3 an increase (normotensives: 19%, essential hypertensives: 13%, secondary hypertensives: 14%). Ambulatory BP monitoring found significant differences in pressor daytime profiles of hypertensive patients according to pressor responses to hyperventilation showing wide fluctuations in group 1 and 3 patients. Interestingly, the peak ambulatory SBP values correlated to the pre-hyperventilation SBP values in group 1, and to the hyperventilation peak SBP values in group 3. In conclusion: 1) Aging decreases reactivity to respiratory alkalosis in elderly normotensives; 2) hyperventilation induces significant pressor changes frequently in essential hypertension, but rarely in secondary hypertension; 3) the significant pressor responses to hyperventilation reflect the daytime pressor profiles predicting the highest daily fluctuations of BP values.
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- 2009
7. Plasma nociceptin/orphanin FQ levels rise after spontaneous episodes of angina, but not during induced myocardial ischemia
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Pasquale Bernardi, Santi Mario Spampinato, Fiorella Fontana, Andrea Bedini, Emilio Merlo Pich, Carmine Pizzi, FONTANA F, BERNARDI P, PIZZI C, SPAMPINATO S, BEDINI A, and MERLO PICH E.
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Male ,Adenosine ,Physiology ,Hemodynamics ,Blood Pressure ,Chest pain ,Biochemistry ,Coronary artery disease ,Angina ,Cellular and Molecular Neuroscience ,Myocardial perfusion imaging ,Endocrinology ,Heart Rate ,Heart rate ,medicine ,Humans ,Angina, Unstable ,cardiovascular diseases ,MYOCARDIAL ISCHEMIA ,Aged ,Tomography, Emission-Computed, Single-Photon ,medicine.diagnostic_test ,business.industry ,Unstable angina ,PLASMA NOCICEPTIN/ORPHANIN FQ ,Myocardial Perfusion Imaging ,Middle Aged ,medicine.disease ,Blood pressure ,Opioid Peptides ,Anesthesia ,Female ,medicine.symptom ,business - Abstract
The aim of our study was to evaluate the effects of repeated episodes of angina and induced myocardial ischemia on plasma nociceptin/orphanin FQ (N/OFQ) levels. Patients with unstable angina (23 with new onset severe angina or accelerated angina and 18 with subacute angina at rest) who had had repeated spontaneous episodes of chest pain in the last week before the study underwent myocardial perfusion single-photon emission computed tomography using adenosine infusion. Twenty subjects without clinical symptoms of angina matched for age, sex and cardiac risk factors served as a control group. N/OFQ levels were significantly (P
- Published
- 2009
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