11 results on '"Melloni, Elisa Maria Teresa"'
Search Results
2. Machine learning approaches for prediction of bipolar disorder based on biological, clinical and neuropsychological markers: A systematic review and meta-analysis
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Colombo, Federica, Calesella, Federico, Mazza, Mario Gennaro, Melloni, Elisa Maria Teresa, Morelli, Marco J., Scotti, Giulia Maria, Benedetti, Francesco, Bollettini, Irene, and Vai, Benedetta
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- 2022
- Full Text
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3. One-year mental health outcomes in a cohort of COVID-19 survivors
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Vai, Benedetta, Bollettini, Irene, Melloni, Elisa Maria Teresa, Mazza, Elena Beatrice, Aggio, Veronica, Calesella, Federico, Paolini, Marco, Caselani, Elisa, Colombo, Federica, D’orsi, Greta, Di Pasquasio, Camilla, Fiore, Paola, Calvisi, Stefania, Canti, Valentina, Castellani, Jacopo, Cilla, Marta, Cinel, Elena, Damanti, Sarah, Ferrante, Marica, Martinenghi, Sabina, Santini, Chiara, Vitali, Giordano, Mazza, Mario Gennaro, Palladini, Mariagrazia, De Lorenzo, Rebecca, Bravi, Beatrice, Poletti, Sara, Furlan, Roberto, Ciceri, Fabio, Rovere-Querini, Patrizia, and Benedetti, Francesco
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- 2022
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4. Anxiety and depression in COVID-19 survivors: Role of inflammatory and clinical predictors
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Mazza, Mario Gennaro, De Lorenzo, Rebecca, Conte, Caterina, Poletti, Sara, Vai, Benedetta, Bollettini, Irene, Melloni, Elisa Maria Teresa, Furlan, Roberto, Ciceri, Fabio, Rovere-Querini, Patrizia, and Benedetti, Francesco
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- 2020
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5. The parental psychological distress caused by separation from their critically ill child during the COVID-19 pandemic: A tale of two cities
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Camporesi, Anna, Abecasis, Francisco, Torres, Erica M., Zoia, Elena, Izzo, Francesca, Ferrario, Stefania, and Melloni, Elisa Maria Teresa
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Pediatrics, Perinatology and Child Health - Abstract
IntroductionA child’s critical illness is a stressful event for the entire family, causing significant emotional distress among parents and changes to family functioning. The Severe Acute Respiratory Syndrome-Related Coronavirus 2 (SARS-CoV-2) pandemic has abruptly caused modifications in visitation policies of Pediatric Intensive Care Units (PICUs) in many countries. We hypothesized that caregivers with no or severely restricted access to PICUs would demonstrate increased psychological distress as compared to those who had limitless access (LA) to PICUs.MethodsSociodemographic variables, levels of psychological distress, ratings of family functioning, and ability to cope with stressful events were collected with an online survey in a group of caregivers after their child’s hospitalization. Ratings of psychological distress were compared between caregivers with no/severely restricted (NA) and with LA to PICUs.ResultsMeasures of depression, anxiety, and global severity index (GSI) of psychological distress were significantly higher in NA caregivers as compared to LA. Among demographic characteristics of the sample, only gender influenced the severity of psychological symptoms: women showed an increased score on levels of somatization, depression, anxiety, and GSI. Avoidant coping style positively correlated with measures of depression. Univariate General Linear Model (GLM) analyses of the effects of sex, age, visitation policies of PICUs, and score of avoidant coping strategies on measures of psychological distress confirmed a significant univariate effect of no access to PICUs on parents’ psychopathological scores.ConclusionRestrictions imposed on visitation policies in PICU during the pandemic negatively impacted families’ psychological wellbeing. A balance between the safety of patients, families, and health care professionals and meeting the needs of families is of utmost importance.
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- 2022
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6. One-year mental health outcomes in a cohort of COVID-19 survivors
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Mazza, Mario Gennaro, primary, Palladini, Mariagrazia, additional, De Lorenzo, Rebecca, additional, Bravi, Beatrice, additional, Poletti, Sara, additional, Furlan, Roberto, additional, Ciceri, Fabio, additional, Rovere-Querini, Patrizia, additional, Benedetti, Francesco, additional, Vai, Benedetta, additional, Bollettini, Irene, additional, Melloni, Elisa Maria Teresa, additional, Mazza, Elena Beatrice, additional, Aggio, Veronica, additional, Calesella, Federico, additional, Paolini, Marco, additional, Caselani, Elisa, additional, Colombo, Federica, additional, D’orsi, Greta, additional, Di Pasquasio, Camilla, additional, Fiore, Paola, additional, Calvisi, Stefania, additional, Canti, Valentina, additional, Castellani, Jacopo, additional, Cilla, Marta, additional, Cinel, Elena, additional, Damanti, Sarah, additional, Ferrante, Marica, additional, Martinenghi, Sabina, additional, Santini, Chiara, additional, and Vitali, Giordano, additional
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- 2022
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7. Effective Antidepressant Chronotherapeutics (Sleep Deprivation and Light Therapy) Normalize the IL-1β:IL-1ra Ratio in Bipolar Depression
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Benedetti, Francesco, primary, Dallaspezia, Sara, additional, Melloni, Elisa Maria Teresa, additional, Lorenzi, Cristina, additional, Zanardi, Raffaella, additional, Barbini, Barbara, additional, and Colombo, Cristina, additional
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- 2021
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8. Clock genes associate with white matter integrity in depressed bipolar patients
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Bollettini, Irene, primary, Melloni, Elisa Maria Teresa, additional, Aggio, Veronica, additional, Poletti, Sara, additional, Lorenzi, Cristina, additional, Pirovano, Adele, additional, Vai, Benedetta, additional, Dallaspezia, Sara, additional, Colombo, Cristina, additional, and Benedetti, Francesco, additional
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- 2016
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9. Clock genes associate with white matter integrity in depressed bipolar patients.
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Bollettini, Irene, Melloni, Elisa Maria Teresa, Aggio, Veronica, Poletti, Sara, Lorenzi, Cristina, Pirovano, Adele, Vai, Benedetta, Dallaspezia, Sara, Colombo, Cristina, and Benedetti, Francesco
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GENETICS of bipolar disorder , *MENTAL depression genetics , *CLOCK genes , *WHITE matter (Nerve tissue) , *HUMAN genetics , *CIRCADIAN rhythms - Abstract
Human genetic studies have implicated specific genes that constitute the molecular clock in the manifestation of bipolar disorder (BD). Among the clock genes involved in the control system of circadian rhythms, CLOCK 3111 T/C and Period3 (PER3) influence core psychopathological features of mood disorders, such as patterns of sleep, rest, and activity, diurnal preference, cognitive performances after sleep loss, age at the onset of the illness, and response to antidepressant treatment. Furthermore, several studies pointed out that bipolar symptomatology is associated with dysfunctions in white matter (WM) integrity, suggesting these structural alterations as a possible biomarker of the disorder. We hypothesise that CLOCK and PER3 polymorphisms could be potential factors affecting WM microstructure integrity in bipolar patients. The relationship between these clock genes and DTI measures of WM integrity in a sample of 140 (53 M; 87 F) patients affected by BD type I was studied. Tract-based spatial statistics analyses on DTI measures of WM integrity were performed for each clock gene polymorphism, between the genetic groups. We accounted for the effect of nuisance covariates known to influence WM microstructure: age, sex, lithium treatment, age at the onset of the illness, and the number of illness episodes. We found that compared to T homozygotes, CLOCK C carriers showed a widespread increase of the mean diffusivity in several WM tracts. Compared with PER35/5homozygotes, PER34/4homozygotes showed significantly increased radial diffusivity and reduced fractional anisotropy in several brain WM tracts. No significant difference was observed between heterozygotes and the other subgroups. Altogether, this pattern of results suggests WM disruption in CLOCK C carrier and in PER34homozygotes. Sleep promotes myelination and oligodendrocyte precursor cell proliferation and associates with higher expression of genes coding for phospholipid synthesis and myelination in oligodendrocytes. These clock genes play a pivotal role in maintaining circadian rhythms and the sleep-wake cycle. Thus, it may be suggested that CLOCK rs1801260*C and PER34/4influence myelination processes by regulating sleep quality and quantity. [ABSTRACT FROM PUBLISHER]
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- 2017
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10. Abnormal choroid plexus, hippocampus, and lateral ventricles volumes as markers of treatment‐resistant major depressive disorder.
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Bravi, Beatrice, Paolini, Marco, Maccario, Melania, Milano, Chiara, Raffaelli, Laura, Melloni, Elisa Maria Teresa, Zanardi, Raffaella, Colombo, Cristina, and Benedetti, Francesco
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CHOROID plexus , *MENTAL depression , *MEDICAL care costs , *BIOMARKERS , *NEUROINFLAMMATION - Abstract
Aim Methods Results Conclusions One‐third of patients with major depressive disorder (MDD) do not achieve full remission and have high relapse rates even after treatment, leading to increased medical costs and reduced quality of life and health status. The possible specificity of treatment‐resistant depression (TRD) neurobiology is still under investigation, with risk factors such as higher inflammatory markers being identified. Given recent findings on the role of choroid plexus (ChP) in neuroinflammation and hippocampus in treatment response, the aim of the present study was to evaluate inflammatory‐ and trophic‐related differences in these regions along with ventricular volumes among patients with treatment‐sensitive depression (TSD), TRD, and healthy controls (HCs).ChP, hippocampal, and ventricular volumes were assessed in 197 patients with MDD and 58 age‐ and sex‐matched HCs. Volumes were estimated using FreeSurfer 7.2. Treatment resistance status was defined as failure to respond to at least two separate antidepressant treatments. Region of interest volumes were then compared among groups.We found higher ChP volumes in patients with TRD compared with patients with TSD and HCs. Our results also showed lower hippocampal volumes and higher lateral ventricular volumes in TRD compared with both patients without TRD and HCs.These findings corroborate the link between TRD and neuroinflammation, as ChP volume could be considered a putative marker of central immune activity. The lack of significant differences in all of the region of interest volumes between patients with TSD and HCs may highlight the specificity of these features to TRD, possibly providing new insights into the specific neurobiological underpinnings of this condition. [ABSTRACT FROM AUTHOR]
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- 2024
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11. Clock genes associate with white matter integrity in depressed bipolar patients
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Sara Dallaspezia, Cristina Colombo, Benedetta Vai, Irene Bollettini, Adele Pirovano, Elisa Melloni, Veronica Aggio, Sara Poletti, Cristina Lorenzi, Francesco Benedetti, Bollettini, Irene, Melloni, Elisa Maria Teresa, Aggio, Veronica, Poletti, Sara, Lorenzi, Cristina, Pirovano, Adele, Vai, Benedetta, Dallaspezia, Sara, Colombo, CRISTINA ANNA, and Benedetti, Francesco
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circadian rhythm ,Adult ,Male ,Sleep Wake Disorders ,medicine.medical_specialty ,Heterozygote ,Bipolar Disorder ,Genotype ,Physiology ,Bipolar depression ,clock gene ,CLOCK Proteins ,White matter ,03 medical and health sciences ,0302 clinical medicine ,Physiology (medical) ,Internal medicine ,Fractional anisotropy ,medicine ,Image Processing, Computer-Assisted ,Humans ,Bipolar disorder ,Circadian rhythm ,Molecular clock ,Myelin Sheath ,Cell Proliferation ,Brain Mapping ,Depression ,Homozygote ,Period Circadian Proteins ,Middle Aged ,diffusion tensor imaging ,medicine.disease ,White Matter ,Antidepressive Agents ,030227 psychiatry ,Circadian Rhythm ,CLOCK ,PER3 ,medicine.anatomical_structure ,Endocrinology ,Mood disorders ,Anisotropy ,Female ,myelin alteration ,Psychology ,Sleep ,Neuroscience ,030217 neurology & neurosurgery - Abstract
Human genetic studies have implicated specific genes that constitute the molecular clock in the manifestation of bipolar disorder (BD). Among the clock genes involved in the control system of circadian rhythms, CLOCK 3111 T/C and Period3 (PER3) influence core psychopathological features of mood disorders, such as patterns of sleep, rest, and activity, diurnal preference, cognitive performances after sleep loss, age at the onset of the illness, and response to antidepressant treatment. Furthermore, several studies pointed out that bipolar symptomatology is associated with dysfunctions in white matter (WM) integrity, suggesting these structural alterations as a possible biomarker of the disorder. We hypothesise that CLOCK and PER3 polymorphisms could be potential factors affecting WM microstructure integrity in bipolar patients. The relationship between these clock genes and DTI measures of WM integrity in a sample of 140 (53 M; 87 F) patients affected by BD type I was studied. Tract-based spatial statistics analyses on DTI measures of WM integrity were performed for each clock gene polymorphism, between the genetic groups. We accounted for the effect of nuisance covariates known to influence WM microstructure: age, sex, lithium treatment, age at the onset of the illness, and the number of illness episodes. We found that compared to T homozygotes, CLOCK C carriers showed a widespread increase of the mean diffusivity in several WM tracts. Compared with PER35/5 homozygotes, PER34/4 homozygotes showed significantly increased radial diffusivity and reduced fractional anisotropy in several brain WM tracts. No significant difference was observed between heterozygotes and the other subgroups. Altogether, this pattern of results suggests WM disruption in CLOCK C carrier and in PER34 homozygotes. Sleep promotes myelination and oligodendrocyte precursor cell proliferation and associates with higher expression of genes coding for phospholipid synthesis and myelination in oligodendrocytes. These clock genes play a pivotal role in maintaining circadian rhythms and the sleep-wake cycle. Thus, it may be suggested that CLOCK rs1801260*C and PER34/4 influence myelination processes by regulating sleep quality and quantity.
- Published
- 2016
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