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2. COVID-19 pandemic stressors are associated with reported increases in frequency of drunkenness among individuals with a history of alcohol use disorder

Author

Meyers, Jacquelyn L, McCutcheon, Vivia V, Horne-Osipenko, Kristina A, Waters, Lawrence R, Barr, Peter, Chan, Grace, Chorlian, David B, Johnson, Emma C, Kuo, Sally I-Chun, Kramer, John R, Dick, Danielle M, Kuperman, Samuel, Kamarajan, Chella, Pandey, Gayathri, Singman, Dzov, de Viteri, Stacey Subbie-Saenz, Salvatore, Jessica E, Bierut, Laura J, Foroud, Tatiana, Goate, Alison, Hesselbrock, Victor, Nurnberger, John, Plaweck, Martin H, Schuckit, Marc A, Agrawal, Arpana, Edenberg, Howard J, Bucholz, Kathleen K, and Porjesz, Bernice

Subjects
Biological Psychology, Biomedical and Clinical Sciences, Psychology, Alcoholism, Alcohol Use and Health, Mental Health, Substance Misuse, Pediatric, Behavioral and Social Science, Clinical Research, Brain Disorders, Prevention, Aetiology, 2.3 Psychological, social and economic factors, Mental health, Good Health and Well Being, Clinical Sciences, Public Health and Health Services, Clinical sciences, Neurosciences, Biological psychology
Abstract

Some sources report increases in alcohol use have been observed since the start of the COVID-19 pandemic, particularly among women. Cross-sectional studies suggest that specific COVID-19-related stressful experiences (e.g., social disconnection) may be driving such increases in the general population. Few studies have explored these topics among individuals with a history of Alcohol Use Disorders (AUD), an especially vulnerable population. Drawing on recent data collected by the Collaborative Study on the Genetics of Alcoholism (COGA; COVID-19 study N = 1651, 62% women, age range: 30-91) in conjunction with AUD history data collected on the sample since 1990, we investigated associations of COVID-19 related stressors and coping activities with changes in drunkenness frequency since the start of the pandemic. Analyses were conducted for those without a history of AUD (N: 645) and three groups of participants with a history of AUD prior to the start of the pandemic: (1) those experiencing AUD symptoms (N: 606), (2) those in remission who were drinking (N: 231), and (3) those in remission who were abstinent (had not consumed alcohol for 5+ years; N: 169). Gender-stratified models were also examined. Exploratory analyses examined the moderating effects of 'problematic alcohol use' polygenic risk scores (PRS) and neural connectivity (i.e., posterior interhemispheric alpha EEG coherence) on associations between COVID-19 stressors and coping activities with changes in the frequency of drunkenness. Increases in drunkenness frequency since the start of the pandemic were higher among those with a lifetime AUD diagnosis experiencing symptoms prior to the start of the pandemic (14% reported increased drunkenness) when compared to those without a history of AUD (5% reported increased drunkenness). Among individuals in remission from AUD prior to the start of the pandemic, rates of increased drunkenness were 10% for those who were drinking pre-pandemic and 4% for those who had previously been abstinent. Across all groups, women reported nominally greater increases in drunkenness frequency when compared with men, although only women experiencing pre-pandemic AUD symptoms reported significantly greater rates of increased drunkenness since the start of the pandemic compared to men in this group (17% of women vs. 5% of men). Among those without a prior history of AUD, associations between COVID-19 risk and protective factors with increases in drunkenness frequency were not observed. Among all groups with a history of AUD (including those with AUD symptoms and those remitted from AUD), perceived stress was associated with increases in drunkenness. Among the remitted-abstinent group, essential worker status was associated with increases in drunkenness. Gender differences in these associations were observed: among women in the remitted-abstinent group, essential worker status, perceived stress, media consumption, and decreased social interactions were associated with increases in drunkenness. Among men in the remitted-drinking group, perceived stress was associated with increases in drunkenness, and increased relationship quality was associated with decreases in drunkenness. Exploratory analyses indicated that associations between family illness or death with increases in drunkenness and increased relationship quality with decreases in drunkenness were more pronounced among the remitted-drinking participants with higher PRS. Associations between family illness or death, media consumption, and economic hardships with increases in drunkenness and healthy coping with decreases in drunkenness were more pronounced among the remitted-abstinent group with lower interhemispheric alpha EEG connectivity. Our results demonstrated that only individuals with pre-pandemic AUD symptoms reported greater increases in drunkenness frequency since the start of the COVID-19 pandemic compared to those without a lifetime history of AUD. This increase was more pronounced among women than men in this group. However, COVID-19-related stressors and coping activities were associated with changes in the frequency of drunkenness among all groups of participants with a prior history of AUD, including those experiencing AUD symptoms, as well as abstinent and non-abstinent participants in remission. Perceived stress, essential worker status, media consumption, social connections (especially for women), and relationship quality (especially for men) are specific areas of focus for designing intervention and prevention strategies aimed at reducing pandemic-related alcohol misuse among this particularly vulnerable group. Interestingly, these associations were not observed for individuals without a prior history of AUD, supporting prior literature that demonstrates that widespread stressors (e.g., pandemics, terrorist attacks) disproportionately impact the mental health and alcohol use of those with a prior history of problems.

Published
2023

3. Parsing genetically influenced risk pathways: genetic loci impact problematic alcohol use via externalizing and specific risk

Author

Barr, Peter B, Mallard, Travis T, Sanchez-Roige, Sandra, Poore, Holly E, Linnér, Richard Karlsson, Waldman, Irwin D, Palmer, Abraham A, Harden, K Paige, and Dick, Danielle M

Subjects
Biological Psychology, Biomedical and Clinical Sciences, Psychology, Human Genome, Genetics, Underage Drinking, Prevention, Substance Misuse, Brain Disorders, Alcoholism, Alcohol Use and Health, Mental Health, Pediatric, 2.1 Biological and endogenous factors, Aetiology, Mental health, Cardiovascular, Oral and gastrointestinal, Good Health and Well Being, Alcohol Drinking, Genetic Loci, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Multifactorial Inheritance, Substance-Related Disorders, COGA Collaborators, Clinical Sciences, Public Health and Health Services, Clinical sciences, Neurosciences, Biological psychology
Abstract

Genome-wide association studies (GWAS) identify genetic variants associated with a trait, regardless of how those variants are associated with the outcome. Characterizing whether variants for psychiatric outcomes operate via specific versus general pathways provides more informative measures of genetic risk. In the current analysis, we used multivariate GWAS to tease apart variants associated with problematic alcohol use (ALCP-total) through either a shared risk for externalizing (EXT) or a problematic alcohol use-specific risk (ALCP-specific). SNPs associated with ALCP-specific were primarily related to alcohol metabolism. Genetic correlations showed ALCP-specific was predominantly associated with alcohol use and other forms of psychopathology, but not other forms of substance use. Polygenic scores for ALCP-total were associated with multiple forms of substance use, but polygenic scores for ALCP-specific were only associated with alcohol phenotypes. Polygenic scores for both ALCP-specific and EXT show different patterns of associations with alcohol misuse across development. Our results demonstrate that focusing on both shared and specific risk can better characterize pathways of risk for substance use disorders. Parsing risk pathways will become increasingly relevant as genetic information is incorporated into clinical practice.

Published
2022

4. Predicting alcohol use disorder remission: a longitudinal multimodal multi-featured machine learning approach.

Author

Kinreich, Sivan, McCutcheon, Vivia V, Aliev, Fazil, Meyers, Jacquelyn L, Kamarajan, Chella, Pandey, Ashwini K, Chorlian, David B, Zhang, Jian, Kuang, Weipeng, Pandey, Gayathri, Viteri, Stacey Subbie-Saenz de, Francis, Meredith W, Chan, Grace, Bourdon, Jessica L, Dick, Danielle M, Anokhin, Andrey P, Bauer, Lance, Hesselbrock, Victor, Schuckit, Marc A, Nurnberger, John I, Foroud, Tatiana M, Salvatore, Jessica E, Bucholz, Kathleen K, and Porjesz, Bernice

Subjects
Clinical Sciences, Public Health and Health Services, Psychology
Abstract

Predictive models for recovering from alcohol use disorder (AUD) and identifying related predisposition biomarkers can have a tremendous impact on addiction treatment outcomes and cost reduction. Our sample (N = 1376) included individuals of European (EA) and African (AA) ancestry from the Collaborative Study on the Genetics of Alcoholism (COGA) who were initially assessed as having AUD (DSM-5) and reassessed years later as either having AUD or in remission. To predict this difference in AUD recovery status, we analyzed the initial data using multimodal, multi-features machine learning applications including EEG source-level functional brain connectivity, Polygenic Risk Scores (PRS), medications, and demographic information. Sex and ancestry age-matched stratified analyses were performed with supervised linear Support Vector Machine application and were calculated twice, once when the ancestry was defined by self-report and once defined by genetic data. Multifeatured prediction models achieved higher accuracy scores than models based on a single domain and higher scores in male models when the ancestry was based on genetic data. The AA male group model with PRS, EEG functional connectivity, marital and employment status features achieved the highest accuracy of 86.04%. Several discriminative features were identified, including collections of PRS related to neuroticism, depression, aggression, years of education, and alcohol consumption phenotypes. Other discriminated features included being married, employed, medication, lower default mode network and fusiform connectivity, and higher insula connectivity. Results highlight the importance of increasing genetic homogeneity of analyzed groups, identifying sex, and ancestry-specific features to increase prediction scores revealing biomarkers related to AUD remission.

Published
2021

5. Cortical and subcortical brain structure in generalized anxiety disorder: findings from 28 research sites in the ENIGMA-Anxiety Working Group

Author

Harrewijn, Anita, Cardinale, Elise M, Groenewold, Nynke A, Bas-Hoogendam, Janna Marie, Aghajani, Moji, Hilbert, Kevin, Cardoner, Narcis, Porta-Casteràs, Daniel, Gosnell, Savannah, Salas, Ramiro, Jackowski, Andrea P, Pan, Pedro M, Salum, Giovanni A, Blair, Karina S, Blair, James R, Hammoud, Mira Z, Milad, Mohammed R, Burkhouse, Katie L, Phan, K Luan, Schroeder, Heidi K, Strawn, Jeffrey R, Beesdo-Baum, Katja, Jahanshad, Neda, Thomopoulos, Sophia I, Buckner, Randy, Nielsen, Jared A, Smoller, Jordan W, Soares, Jair C, Mwangi, Benson, Wu, Mon-Ju, Zunta-Soares, Giovana B, Assaf, Michal, Diefenbach, Gretchen J, Brambilla, Paolo, Maggioni, Eleonora, Hofmann, David, Straube, Thomas, Andreescu, Carmen, Berta, Rachel, Tamburo, Erica, Price, Rebecca B, Manfro, Gisele G, Agosta, Federica, Canu, Elisa, Cividini, Camilla, Filippi, Massimo, Kostić, Milutin, Munjiza Jovanovic, Ana, Alberton, Bianca AV, Benson, Brenda, Freitag, Gabrielle F, Filippi, Courtney A, Gold, Andrea L, Leibenluft, Ellen, Ringlein, Grace V, Werwath, Kathryn E, Zwiebel, Hannah, Zugman, André, Grabe, Hans J, Van der Auwera, Sandra, Wittfeld, Katharina, Völzke, Henry, Bülow, Robin, Balderston, Nicholas L, Ernst, Monique, Grillon, Christian, Mujica-Parodi, Lilianne R, van Nieuwenhuizen, Helena, Critchley, Hugo D, Makovac, Elena, Mancini, Matteo, Meeten, Frances, Ottaviani, Cristina, Ball, Tali M, Fonzo, Gregory A, Paulus, Martin P, Stein, Murray B, Gur, Raquel E, Gur, Ruben C, Kaczkurkin, Antonia N, Larsen, Bart, Satterthwaite, Theodore D, Harper, Jennifer, Myers, Michael, Perino, Michael T, Sylvester, Chad M, Yu, Qiongru, Lueken, Ulrike, Veltman, Dick J, Thompson, Paul M, Stein, Dan J, Van der Wee, Nic JA, Winkler, Anderson M, and Pine, Daniel S

Subjects
Biological Psychology, Biomedical and Clinical Sciences, Clinical Sciences, Psychology, Neurosciences, Women's Health, Brain Disorders, Behavioral and Social Science, Biomedical Imaging, 4.2 Evaluation of markers and technologies, Mental health, Adult, Anxiety, Anxiety Disorders, Brain, Child, Female, Humans, Magnetic Resonance Imaging, Male, Public Health and Health Services, Clinical sciences, Biological psychology
Abstract

The goal of this study was to compare brain structure between individuals with generalized anxiety disorder (GAD) and healthy controls. Previous studies have generated inconsistent findings, possibly due to small sample sizes, or clinical/analytic heterogeneity. To address these concerns, we combined data from 28 research sites worldwide through the ENIGMA-Anxiety Working Group, using a single, pre-registered mega-analysis. Structural magnetic resonance imaging data from children and adults (5-90 years) were processed using FreeSurfer. The main analysis included the regional and vertex-wise cortical thickness, cortical surface area, and subcortical volume as dependent variables, and GAD, age, age-squared, sex, and their interactions as independent variables. Nuisance variables included IQ, years of education, medication use, comorbidities, and global brain measures. The main analysis (1020 individuals with GAD and 2999 healthy controls) included random slopes per site and random intercepts per scanner. A secondary analysis (1112 individuals with GAD and 3282 healthy controls) included fixed slopes and random intercepts per scanner with the same variables. The main analysis showed no effect of GAD on brain structure, nor interactions involving GAD, age, or sex. The secondary analysis showed increased volume in the right ventral diencephalon in male individuals with GAD compared to male healthy controls, whereas female individuals with GAD did not differ from female healthy controls. This mega-analysis combining worldwide data showed that differences in brain structure related to GAD are small, possibly reflecting heterogeneity or those structural alterations are not a major component of its pathophysiology.

Published
2021

6. Using polygenic scores for identifying individuals at increased risk of substance use disorders in clinical and population samples.

Author

Barr, Peter B, Ksinan, Albert, Su, Jinni, Johnson, Emma C, Meyers, Jacquelyn L, Wetherill, Leah, Latvala, Antti, Aliev, Fazil, Chan, Grace, Kuperman, Samuel, Nurnberger, John, Kamarajan, Chella, Anokhin, Andrey, Agrawal, Arpana, Rose, Richard J, Edenberg, Howard J, Schuckit, Marc, Kaprio, Jaakko, and Dick, Danielle M

Subjects
Clinical Sciences, Public Health and Health Services, Psychology
Abstract

Genome-wide, polygenic risk scores (PRS) have emerged as a useful way to characterize genetic liability. There is growing evidence that PRS may prove useful for early identification of those at increased risk for certain diseases. The current potential of PRS for alcohol use disorders (AUD) remains an open question. Using data from both a population-based sample [the FinnTwin12 (FT12) study] and a high-risk sample [the Collaborative Study on the Genetics of Alcoholism (COGA)], we examined the association between PRSs derived from genome-wide association studies (GWASs) of (1) alcohol dependence/alcohol problems, (2) alcohol consumption, and (3) risky behaviors with AUD and other substance use disorder (SUD) criteria. These PRSs explain ~2.5-3.5% of the variance in AUD (across FT12 and COGA) when all PRSs are included in the same model. Calculations of area under the curve (AUC) show PRS provide only a slight improvement over a model with age, sex, and ancestral principal components as covariates. While individuals in the top 20, 10, and 5% of the PRS distribution had greater odds of having an AUD compared to the lower end of the continuum in both COGA and FT12, the point estimates at each threshold were statistically indistinguishable. Those in the top 5% reported greater levels of licit (alcohol and nicotine) and illicit (cannabis and opioid) SUD criteria. PRSs are associated with risk for SUD in independent samples. However, usefulness for identifying those at increased risk in their current form is modest, at best. Improvement in predictive ability will likely be dependent on increasing the size of well-phenotyped discovery samples.

Published
2020

8. Genome-wide association data suggest ABCB1 and immune-related gene sets may be involved in adult antisocial behavior.

Author

Salvatore, JE, Edwards, AC, McClintick, JN, Bigdeli, TB, Adkins, A, Aliev, F, Edenberg, HJ, Foroud, T, Hesselbrock, V, Kramer, J, Nurnberger, JI, Schuckit, M, Tischfield, JA, Xuei, X, and Dick, DM

Subjects
Brain, Humans, Alcoholism, Cocaine-Related Disorders, Genetic Predisposition to Disease, P-Glycoproteins, Interferon Type I, Case-Control Studies, Antisocial Personality Disorder, Polymorphism, Single Nucleotide, Adult, Female, Male, Genome-Wide Association Study, ATP Binding Cassette Transporter, Subfamily B, Human Genome, Substance Abuse, Brain Disorders, Mental Health, Genetics, Violence Research, Polymorphism, Single Nucleotide, ATP Binding Cassette Transporter, Subfamily B, Psychology, Clinical Sciences, Public Health and Health Services
Abstract

Adult antisocial behavior (AAB) is moderately heritable, relatively common and has adverse consequences for individuals and society. We examined the molecular genetic basis of AAB in 1379 participants from a case-control study in which the cases met criteria for alcohol dependence. We also examined whether genes of interest were expressed in human brain. AAB was measured using a count of the number of Antisocial Personality Disorder criteria endorsed under criterion A from the Diagnostic and Statistical Manual of Mental Disorders, 4th Edition (DSM-IV). Participants were genotyped on the Illumina Human 1M BeadChip. In total, all single-nucleotide polymorphisms (SNPs) accounted for 25% of the variance in AAB, although this estimate was not significant (P=0.09). Enrichment tests indicated that more significantly associated genes were over-represented in seven gene sets, and most were immune related. Our most highly associated SNP (rs4728702, P=5.77 × 10(-7)) was located in the protein-coding adenosine triphosphate-binding cassette, sub-family B (MDR/TAP), member 1 (ABCB1). In a gene-based test, ABCB1 was genome-wide significant (q=0.03). Expression analyses indicated that ABCB1 was robustly expressed in the brain. ABCB1 has been implicated in substance use, and in post hoc tests we found that variation in ABCB1 was associated with DSM-IV alcohol and cocaine dependence criterion counts. These results suggest that ABCB1 may confer risk across externalizing behaviors, and are consistent with previous suggestions that immune pathways are associated with externalizing behaviors. The results should be tempered by the fact that we did not replicate the associations for ABCB1 or the gene sets in a less-affected independent sample.

Published
2015

10. Genetic association study of childhood aggression across raters, instruments, and age

Author

Ip, Hill F., van der Laan, Camiel M., Krapohl, Eva M. L., Brikell, Isabell, Sánchez-Mora, Cristina, Nolte, Ilja M., St Pourcain, Beate, Bolhuis, Koen, Palviainen, Teemu, Zafarmand, Hadi, Colodro-Conde, Lucía, Gordon, Scott, Zayats, Tetyana, Aliev, Fazil, Jiang, Chang, Wang, Carol A., Saunders, Gretchen, Karhunen, Ville, Hammerschlag, Anke R., Adkins, Daniel E., Border, Richard, Peterson, Roseann E., Prinz, Joseph A., Thiering, Elisabeth, Seppälä, Ilkka, Vilor-Tejedor, Natàlia, Ahluwalia, Tarunveer S., Day, Felix R., Hottenga, Jouke-Jan, Allegrini, Andrea G., Rimfeld, Kaili, Chen, Qi, Lu, Yi, Martin, Joanna, Soler Artigas, María, Rovira, Paula, Bosch, Rosa, Español, Gemma, Ramos Quiroga, Josep Antoni, Neumann, Alexander, Ensink, Judith, Grasby, Katrina, Morosoli, José J., Tong, Xiaoran, Marrington, Shelby, Middeldorp, Christel, Scott, James G., Vinkhuyzen, Anna, Shabalin, Andrey A., Corley, Robin, Evans, Luke M., Sugden, Karen, Alemany, Silvia, Sass, Lærke, Vinding, Rebecca, Ruth, Kate, Tyrrell, Jess, Davies, Gareth E., Ehli, Erik A., Hagenbeek, Fiona A., De Zeeuw, Eveline, Van Beijsterveldt, Toos C.E.M., Larsson, Henrik, Snieder, Harold, Verhulst, Frank C., Amin, Najaf, Whipp, Alyce M., Korhonen, Tellervo, Vuoksimaa, Eero, Rose, Richard J., Uitterlinden, André G., Heath, Andrew C., Madden, Pamela, Haavik, Jan, Harris, Jennifer R., Helgeland, Øyvind, Johansson, Stefan, Knudsen, Gun Peggy S., Njolstad, Pal Rasmus, Lu, Qing, Rodriguez, Alina, Henders, Anjali K., Mamun, Abdullah, Najman, Jackob M., Brown, Sandy, Hopfer, Christian, Krauter, Kenneth, Reynolds, Chandra, Smolen, Andrew, Stallings, Michael, Wadsworth, Sally, Wall, Tamara L., Silberg, Judy L., Miller, Allison, Keltikangas-Järvinen, Liisa, Hakulinen, Christian, Pulkki-Råback, Laura, Havdahl, Alexandra, Magnus, Per, Raitakari, Olli T., Perry, John R. B., Llop, Sabrina, Lopez-Espinosa, Maria-Jose, Bønnelykke, Klaus, Bisgaard, Hans, Sunyer, Jordi, Lehtimäki, Terho, Arseneault, Louise, Standl, Marie, Heinrich, Joachim, Boden, Joseph, Pearson, John, Horwood, L. John, Kennedy, Martin, Poulton, Richie, Eaves, Lindon J., Maes, Hermine H., Hewitt, John, Copeland, William E., Costello, Elizabeth J., Williams, Gail M., Wray, Naomi, Järvelin, Marjo-Riitta, McGue, Matt, Iacono, William, Caspi, Avshalom, Moffitt, Terrie E., Whitehouse, Andrew, Pennell, Craig E., Klump, Kelly L., Burt, S. Alexandra, Dick, Danielle M., Reichborn-Kjennerud, Ted, Martin, Nicholas G., Medland, Sarah E., Vrijkotte, Tanja, Kaprio, Jaakko, Tiemeier, Henning, Davey Smith, George, Hartman, Catharina A., Oldehinkel, Albertine J., Casas, Miquel, Ribasés, Marta, Lichtenstein, Paul, Lundström, Sebastian, Plomin, Robert, Bartels, Meike, Nivard, Michel G., and Boomsma, Dorret I.

Published
2021
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12. Psycho-social factors associated with mental resilience in the Corona lockdown

Author

Veer, Ilya M., Riepenhausen, Antje, Zerban, Matthias, Wackerhagen, Carolin, Puhlmann, Lara M. C., Engen, Haakon, Köber, Göran, Bögemann, Sophie A., Weermeijer, Jeroen, Uściłko, Aleksandra, Mor, Netali, Marciniak, Marta A., Askelund, Adrian Dahl, Al-Kamel, Abbas, Ayash, Sarah, Barsuola, Giulia, Bartkute-Norkuniene, Vaida, Battaglia, Simone, Bobko, Yaryna, Bölte, Sven, Cardone, Paolo, Chvojková, Edita, Damnjanović, Kaja, De Calheiros Velozo, Joana, de Thurah, Lena, Deza-Araujo, Yacila I., Dimitrov, Annika, Farkas, Kinga, Feller, Clémence, Gazea, Mary, Gilan, Donya, Gnjidić, Vedrana, Hajduk, Michal, Hiekkaranta, Anu P., Hofgaard, Live S., Ilen, Laura, Kasanova, Zuzana, Khanpour, Mohsen, Lau, Bobo Hi Po, Lenferink, Dionne B., Lindhardt, Thomas B., Magas, Dávid Á., Mituniewicz, Julian, Moreno-López, Laura, Muzychka, Sofiia, Ntafouli, Maria, O’Leary, Aet, Paparella, Ilenia, Põldver, Nele, Rintala, Aki, Robak, Natalia, Rosická, Anna M., Røysamb, Espen, Sadeghi, Siavash, Schneider, Maude, Siugzdaite, Roma, Stantić, Mirta, Teixeira, Ana, Todorovic, Ana, Wan, Wendy W. N., van Dick, Rolf, Lieb, Klaus, Kleim, Birgit, Hermans, Erno J., Kobylińska, Dorota, Hendler, Talma, Binder, Harald, Myin-Germeys, Inez, van Leeuwen, Judith M. C., Tüscher, Oliver, Yuen, Kenneth S. L., Walter, Henrik, and Kalisch, Raffael

Published
2021
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13. Sex differences in the neuroanatomy of alcohol dependence: hippocampus and amygdala subregions in a sample of 966 people from the ENIGMA Addiction Working Group

Author

Grace, Sally, Rossetti, Maria Gloria, Allen, Nicholas, Batalla, Albert, Bellani, Marcella, Brambilla, Paolo, Chye, Yann, Cousijn, Janna, Goudriaan, Anna E, Hester, Robert, Hutchison, Kent, Labuschagne, Izelle, Momenan, Reza, Martin-Santos, Rocio, Rendell, Peter, Solowij, Nadia, Sinha, Rajita, Li, Chiang-shan Ray, Schmaal, Lianne, Sjoerds, Zsuzsika, Suo, Chao, Terrett, Gill, van Holst, Ruth J., Veltman, Dick J., Yücel, Murat, Thompson, Paul, Conrod, Patricia, Mackey, Scott, Garavan, Hugh, and Lorenzetti, Valentina

Published
2021
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14. ENIGMA MDD: seven years of global neuroimaging studies of major depression through worldwide data sharing

Author

Schmaal, Lianne, Pozzi, Elena, C. Ho, Tiffany, van Velzen, Laura S., Veer, Ilya M., Opel, Nils, Van Someren, Eus J. W., Han, Laura K. M., Aftanas, Lybomir, Aleman, André, Baune, Bernhard T., Berger, Klaus, Blanken, Tessa F., Capitão, Liliana, Couvy-Duchesne, Baptiste, R. Cullen, Kathryn, Dannlowski, Udo, Davey, Christopher, Erwin-Grabner, Tracy, Evans, Jennifer, Frodl, Thomas, Fu, Cynthia H. Y., Godlewska, Beata, Gotlib, Ian H., Goya-Maldonado, Roberto, Grabe, Hans J., Groenewold, Nynke A., Grotegerd, Dominik, Gruber, Oliver, Gutman, Boris A., Hall, Geoffrey B., Harrison, Ben J., Hatton, Sean N., Hermesdorf, Marco, Hickie, Ian B., Hilland, Eva, Irungu, Benson, Jonassen, Rune, Kelly, Sinead, Kircher, Tilo, Klimes-Dougan, Bonnie, Krug, Axel, Landrø, Nils Inge, Lagopoulos, Jim, Leerssen, Jeanne, Li, Meng, Linden, David E. J., MacMaster, Frank P., M. McIntosh, Andrew, Mehler, David M. A., Nenadić, Igor, Penninx, Brenda W. J. H., Portella, Maria J., Reneman, Liesbeth, Rentería, Miguel E., Sacchet, Matthew D., G. Sämann, Philipp, Schrantee, Anouk, Sim, Kang, Soares, Jair C., Stein, Dan J., Tozzi, Leonardo, van Der Wee, Nic J. A., van Tol, Marie-José, Vermeiren, Robert, Vives-Gilabert, Yolanda, Walter, Henrik, Walter, Martin, Whalley, Heather C., Wittfeld, Katharina, Whittle, Sarah, Wright, Margaret J., Yang, Tony T., Zarate, Jr, Carlos, Thomopoulos, Sophia I., Jahanshad, Neda, Thompson, Paul M., and Veltman, Dick J.

Published
2020
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15. Brain structural correlates of insomnia severity in 1053 individuals with major depressive disorder: results from the ENIGMA MDD Working Group

Author

Leerssen, Jeanne, Blanken, Tessa F., Pozzi, Elena, Jahanshad, Neda, Aftanas, Lyubomir, Andreassen, Ole A., Baune, Bernhard T., Brack, Ivan, Carballedo, Angela, Ching, Christopher R. K., Dannlowski, Udo, Dohm, Katharina, Enneking, Verena, Filimonova, Elena, Fingas, Stella M., Frodl, Thomas, Godlewska, Beata R., Goltermann, Janik, Gotlib, Ian H., Grotegerd, Dominik, Gruber, Oliver, Harris, Mathew A., Hatton, Sean N., Hawkins, Emma, Hickie, Ian B., Jaworska, Natalia, Kircher, Tilo, Krug, Axel, Lagopoulos, Jim, Lemke, Hannah, Li, Meng, MacMaster, Frank P., McIntosh, Andrew M., McLellan, Quinn, Meinert, Susanne, Mwangi, Benson, Nenadić, Igor, Osipov, Evgeny, Portella, Maria J., Redlich, Ronny, Repple, Jonathan, Sacchet, Matthew D., Sämann, Philipp G., Simulionyte, Egle, Soares, Jair C., Walter, Martin, Watanabe, Norio, Whalley, Heather C., Yüksel, Dilara, Veltman, Dick J., Thompson, Paul M., Schmaal, Lianne, and Van Someren, Eus J. W.

Published
2020
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17. Psychosocial moderation of polygenic risk for cannabis involvement: the role of trauma exposure and frequency of religious service attendance

Author

Meyers, Jacquelyn L., Salvatore, Jessica E., Aliev, Fazil, Johnson, Emma C., McCutcheon, Vivia V., Su, Jinni, Kuo, Sally I-Chun, Lai, Dongbing, Wetherill, Leah, Wang, Jen C., Chan, Grace, Hesselbrock, Victor, Foroud, Tatiana, Bucholz, Kathleen K., Edenberg, Howard J., Dick, Danielle M., Porjesz, Bernice, and Agrawal, Arpana

Published
2019
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