Your search keyword '"Magno, Marta"' showing total 4 results

1. Medical comorbidities in bipolar disorder (BIPCOM): clinical validation of risk factors and biomarkers to improve prevention and treatment. Study protocol

Author

de Girolamo, Giovanni, Andreassen, Ole A., Bauer, Michael, Brambilla, Paolo, Calza, Stefano, Citerà, Nicholas, Corcoy, Rosa, Fagiolini, Andrea, Garcia-Argibay, Miguel, Godin, Ophélia, Klingler, Florian, Kobayashi, Nene F., Larsson, Henrik, Leboyer, Marion, Matura, Silke, Martinelli, Alessandra, De la Peña-Arteaga, Víctor, Poli, Roberto, Reif, Andreas, Ritter, Philipp, Rødevand, Linn N., Magno, Marta, and Caselani, Elisa

Published

2024

2. Age of onset and cumulative risk of mental disorders: a cross-national analysis of population surveys from 29 countries

Author

Aguilar-Gaxiola, Sergio, Al-Hamzawi, Ali, Alonso, Jordi, Altwaijri, Yasmin A., Andrade, Laura Helena, Atwoli, Lukoye, Benjet, Corina, Bromet, Evelyn J., Bruffaerts, Ronny, Bunting, Brendan, Caldas-de-Almeida, José Miguel, Cardoso, Graça, Chardoul, Stephanie, Cía, Alfredo H., Degenhardt, Louisa, De Girolamo, Giovanni, Gureje, Oye, Haro, Josep Maria, Harris, Meredith G., Hinkov, Hristo, Hu, Chi-yi, De Jonge, Peter, Karam, Aimee N., Karam, Elie G., Karam, Georges, Kazdin, Alan E., Kawakami, Norito, Kessler, Ronald C., Kiejna, Andrzej, Kovess-Masfety, Viviane, McGrath, John J., Medina-Mora, Maria Elena, Moskalewicz, Jacek, Navarro-Mateu, Fernando, Nishi, Daisuke, Piazza, Marina, Posada-Villa, José, Scott, Kate M., Stagnaro, Juan Carlos, Stein, Dan J., Ten Have, Margreet, Torres, Yolanda, Viana, Maria Carmen, Vigo, Daniel V., Vladescu, Cristian, Williams, David R., Woodruff, Peter, Wojtyniak, Bogdan, Xavier, Miguel, Zaslavsky, Alan M., McGrath, John J, Altwaijri, Yasmin, Andrade, Laura H, Bromet, Evelyn J, de Almeida, José Miguel Caldas, Chiu, Wai Tat, Demler, Olga V, Ferry, Finola, Karam, Elie G, Khaled, Salma M, Magno, Marta, Plana-Ripoll, Oleguer, Rapsey, Charlene, Sampson, Nancy A, Stein, Dan J, ten Have, Margreet, Woodruff, Peter W, Zarkov, Zahari, and Kessler, Ronald C

Published

2023

3. Metabolic Syndrome in people treated with Antipsychotics (RISKMet): A multimethod study protocol investigating genetic, behavioural, and environmental risk factors.

Author

de Girolamo, Giovanni, La Cascia, Caterina, Macchia, Paolo Emidio, Nobile, Maria, Calza, Stefano, Camillo, Laura, Mauri, Maddalena, Pozzi, Marco, Tripoli, Giada, Vetrani, Claudia, Caselani, Elisa, and Magno, Marta

Subjects

METABOLIC syndrome, CHILD patients, DIETARY patterns, FOOD habits, RESEARCH protocols, ORAL habits, ARIPIPRAZOLE, AMISULPRIDE

Abstract

Introduction: The RISKMet project aims to: (1) identify risk factors for metabolic syndrome (MetS) by comparing patients with and without MetS; (2) characterise patients treated with second-generation antipsychotics (SGAs) about MetS diagnosis; (3) study behavioural patterns, including physical activity (PA) and dietary habits, in patients and healthy individuals using a prospective cohort design. Method: The RISKMet project investigates MetS in individuals treated with SGAs, focusing on both adult and paediatric populations. The study utilizes a case-control design to examine potential risk factors for MetS, categorizing participants as MetS+ considered as "Cases" and MetS- considered as "Controls" matched by sex and age. The evaluation of factors such as MetS, lifestyle habits, and environmental influences is conducted at two time points, T0 and T3, after 3 months. Subsequently, the project aims to assess body parameters, including physical examinations, and blood, and stool sample collection, to evaluate metabolic markers and the impact of SGAs. The analysis includes pharmacological treatment data and genetic variability. Behavioural markers related to lifestyle, eating behaviour, PA, and mood are assessed at both T0 and T3 using interviews, accelerometers, and a mobile app. The study aims to improve mental and physical well-being in SGA-treated individuals, establish a biobank for MetS research, build an evidence base for physical health programs, and develop preventive strategies for SGA-related comorbidities. Conclusions: This project innovates MetS monitoring in psychiatry by using intensive digital phenotyping, identifying biochemical markers, assessing familial risks, and including genetically similar healthy controls. Study registration number: ISRCTN18419418 at www.isrctn.com. [ABSTRACT FROM AUTHOR]

Published

2024

4. Age of onset and cumulative risk of mental disorders: a cross-national analysis of population surveys from 29 countries.

Author

McGrath JJ, Al-Hamzawi A, Alonso J, Altwaijri Y, Andrade LH, Bromet EJ, Bruffaerts R, de Almeida JMC, Chardoul S, Chiu WT, Degenhardt L, Demler OV, Ferry F, Gureje O, Haro JM, Karam EG, Karam G, Khaled SM, Kovess-Masfety V, Magno M, Medina-Mora ME, Moskalewicz J, Navarro-Mateu F, Nishi D, Plana-Ripoll O, Posada-Villa J, Rapsey C, Sampson NA, Stagnaro JC, Stein DJ, Ten Have M, Torres Y, Vladescu C, Woodruff PW, Zarkov Z, and Kessler RC

Subjects

Adolescent, Humans, Male, Female, Young Adult, Adult, Age of Onset, Cross-Sectional Studies, Health Surveys, Surveys and Questionnaires, Prevalence, Diagnostic and Statistical Manual of Mental Disorders, Comorbidity, Depressive Disorder, Major epidemiology, Mental Disorders epidemiology, Phobic Disorders epidemiology

Abstract

Background: Information on the frequency and timing of mental disorder onsets across the lifespan is of fundamental importance for public health planning. Broad, cross-national estimates of this information from coordinated general population surveys were last updated in 2007. We aimed to provide updated and improved estimates of age-of-onset distributions, lifetime prevalence, and morbid risk., Methods: In this cross-national analysis, we analysed data from respondents aged 18 years or older to the World Mental Health surveys, a coordinated series of cross-sectional, face-to-face community epidemiological surveys administered between 2001 and 2022. In the surveys, the WHO Composite International Diagnostic Interview, a fully structured psychiatric diagnostic interview, was used to assess age of onset, lifetime prevalence, and morbid risk of 13 DSM-IV mental disorders until age 75 years across surveys by sex. We did not assess ethnicity. The surveys were geographically clustered and weighted to adjust for selection probability, and standard errors of incidence rates and cumulative incidence curves were calculated using the jackknife repeated replications simulation method, taking weighting and geographical clustering of data into account., Findings: We included 156 331 respondents from 32 surveys in 29 countries, including 12 low-income and middle-income countries and 17 high-income countries, and including 85 308 (54·5%) female respondents and 71 023 (45·4%) male respondents. The lifetime prevalence of any mental disorder was 28·6% (95% CI 27·9-29·2) for male respondents and 29·8% (29·2-30·3) for female respondents. Morbid risk of any mental disorder by age 75 years was 46·4% (44·9-47·8) for male respondents and 53·1% (51·9-54·3) for female respondents. Conditional probabilities of first onset peaked at approximately age 15 years, with a median age of onset of 19 years (IQR 14-32) for male respondents and 20 years (12-36) for female respondents. The two most prevalent disorders were alcohol use disorder and major depressive disorder for male respondents and major depressive disorder and specific phobia for female respondents., Interpretation: By age 75 years, approximately half the population can expect to develop one or more of the 13 mental disorders considered in this Article. These disorders typically first emerge in childhood, adolescence, or young adulthood. Services should have the capacity to detect and treat common mental disorders promptly and to optimise care that suits people at these crucial parts of the life course., Funding: None., Competing Interests: Declaration of interests LD receives educational grants from Indivior and Seqirus. OVD receives funding from Kowa Research Institute and has been an advisor in the PROMINENT trial. SMK and PWW receive grant funding from Hamad Medical Corporation through the Cambridgeshire and Peterborough National Health Service Foundation trust and from Qatar University. PWW has received financial support from the Qatar National Research Fund and an honorarium from Gresham College. RCK has been a consultant for Cambridge Health Alliance, Canandaigua Veterans Affairs Medical Center, Holmusk, Partners Healthcare, RallyPoint Networks, and Sage Therapeutics. He holds stock options in Cerebral, Mirah, Prepare Your Mind, Roga Sciences, and Verisense Health. DN receives honoraria from AIG General Insurance and Takeda Pharmaceutical and financial support from Startia, En-power, and MD.net. DJS receives royalties from American Psychiatric Press, Cambridge University Press, and Elsevier–Academic Press. He has received honoraria from Discovery Vitality, Johnson & Johnson, Kanna, L'Oreal, Lundbeck, Orion, Sanofi, Servier, Takeda, and Vistagen. He was the president of the African College of Neuropsychopharmacology and is financially supported by the Medical Research Council of South Africa. All other authors declare no competing interests., (Copyright © 2023 Elsevier Ltd. All rights reserved.)

Published

2023