Your search keyword '"Maihofer, Adam"' showing total 668 results

1. Effects of genetically predicted posttraumatic stress disorder on autoimmune phenotypes.

Author

Maihofer, Adam, Ratanatharathorn, Andrew, Hemmings, Sian, Costenbader, Karen, Michopoulos, Vasiliki, Polimanti, Renato, Rothbaum, Alex, Seedat, Soraya, Mikita, Elizabeth, Smith, Alicia, Salem, Rany, Shaffer, Richard, Wu, Tianying, Sebat, Jonathan, Ressler, Kerry, Stein, Murray, Koenen, Karestan, Wolf, Erika, Sumner, Jennifer, and Nievergelt, Caroline

Subjects

Humans, Stress Disorders, Post-Traumatic, Phenotype, C-Reactive Protein, Autoimmune Diseases, Hashimoto Disease, Biomarkers, Genome-Wide Association Study

Abstract

Observational studies suggest that posttraumatic stress disorder (PTSD) increases risk for various autoimmune diseases. Insights into shared biology and causal relationships between these diseases may inform intervention approaches to PTSD and co-morbid autoimmune conditions. We investigated the shared genetic contributions and causal relationships between PTSD, 18 autoimmune diseases, and 3 immune/inflammatory biomarkers. Univariate MiXeR was used to contrast the genetic architectures of phenotypes. Genetic correlations were estimated using linkage disequilibrium score regression. Bi-directional, two-sample Mendelian randomization (MR) was performed using independent, genome-wide significant single nucleotide polymorphisms; inverse variance weighted and weighted median MR estimates were evaluated. Sensitivity analyses for uncorrelated (MR PRESSO) and correlated horizontal pleiotropy (CAUSE) were also performed. PTSD was considerably more polygenic (10,863 influential variants) than autoimmune diseases (median 255 influential variants). However, PTSD evidenced significant genetic correlation with nine autoimmune diseases and three inflammatory biomarkers. PTSD had putative causal effects on autoimmune thyroid disease (p = 0.00009) and C-reactive protein (CRP) (p = 4.3 × 10-7). Inferences were not substantially altered by sensitivity analyses. Additionally, the PTSD-autoimmune thyroid disease association remained significant in multivariable MR analysis adjusted for genetically predicted inflammatory biomarkers as potential mechanistic pathway variables. No autoimmune disease had a significant causal effect on PTSD (all p values > 0.05). Although causal effect models were supported for associations of PTSD with CRP, shared pleiotropy was adequate to explain a putative causal effect of CRP on PTSD (p = 0.18). In summary, our results suggest a significant genetic overlap between PTSD, autoimmune diseases, and biomarkers of inflammation. PTSD has a putative causal effect on autoimmune thyroid disease, consistent with existing epidemiologic evidence. A previously reported causal effect of CRP on PTSD is potentially confounded by shared genetics. Together, results highlight the nuanced links between PTSD, autoimmune disorders, and associated inflammatory signatures, and suggest the importance of targeting related pathways to protect against disease and disability.

Published

2024

2. Genetic architecture distinguishes tinnitus from hearing loss

Author

Clifford, Royce E, Maihofer, Adam X, Chatzinakos, Chris, Coleman, Jonathan RI, Daskalakis, Nikolaos P, Gasperi, Marianna, Hogan, Kelleigh, Mikita, Elizabeth A, Stein, Murray B, Tcheandjieu, Catherine, Telese, Francesca, Zuo, Yanning, Ryan, Allen F, and Nievergelt, Caroline M

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Allied Health and Rehabilitation Science, Health Sciences, Clinical Sciences, Brain Disorders, Neurosciences, Human Genome, Aetiology, 2.1 Biological and endogenous factors, Mental health, Ear, Cochlea, Humans, Deafness, Hearing Loss, Noise-Induced, Tinnitus

Abstract

Tinnitus is a heritable, highly prevalent auditory disorder treated by multiple medical specialties. Previous GWAS indicated high genetic correlations between tinnitus and hearing loss, with little indication of differentiating signals. We present a GWAS meta-analysis, triple previous sample sizes, and expand to non-European ancestries. GWAS in 596,905 Million Veteran Program subjects identified 39 tinnitus loci, and identified genes related to neuronal synapses and cochlear structural support. Applying state-of-the-art analytic tools, we confirm a large number of shared variants, but also a distinct genetic architecture of tinnitus, with higher polygenicity and large proportion of variants not shared with hearing difficulty. Tissue-expression analysis for tinnitus infers broad enrichment across most brain tissues, in contrast to hearing difficulty. Finally, tinnitus is not only correlated with hearing loss, but also with a spectrum of psychiatric disorders, providing potential new avenues for treatment. This study establishes tinnitus as a distinct disorder separate from hearing difficulties.

Published

2024

3. Focal adhesion is associated with lithium response in bipolar disorder: evidence from a network-based multi-omics analysis

Author

Niemsiri, Vipavee, Rosenthal, Sara Brin, Nievergelt, Caroline M, Maihofer, Adam X, Marchetto, Maria C, Santos, Renata, Shekhtman, Tatyana, Alliey-Rodriguez, Ney, Anand, Amit, Balaraman, Yokesh, Berrettini, Wade H, Bertram, Holli, Burdick, Katherine E, Calabrese, Joseph R, Calkin, Cynthia V, Conroy, Carla, Coryell, William H, DeModena, Anna, Eyler, Lisa T, Feeder, Scott, Fisher, Carrie, Frazier, Nicole, Frye, Mark A, Gao, Keming, Garnham, Julie, Gershon, Elliot S, Goes, Fernando S, Goto, Toyomi, Harrington, Gloria J, Jakobsen, Petter, Kamali, Masoud, Kelly, Marisa, Leckband, Susan G, Lohoff, Falk W, McCarthy, Michael J, McInnis, Melvin G, Craig, David, Millett, Caitlin E, Mondimore, Francis, Morken, Gunnar, Nurnberger, John I, Donovan, Claire O’, Øedegaard, Ketil J, Ryan, Kelly, Schinagle, Martha, Shilling, Paul D, Slaney, Claire, Stapp, Emma K, Stautland, Andrea, Tarwater, Bruce, Zandi, Peter P, Alda, Martin, Fisch, Kathleen M, Gage, Fred H, and Kelsoe, John R

Subjects

Biomedical and Clinical Sciences, Biological Psychology, Clinical and Health Psychology, Clinical Sciences, Psychology, Serious Mental Illness, Genetics, Mental Health, Brain Disorders, Human Genome, Mental health, Bipolar Disorder, Humans, Lithium, Gene Regulatory Networks, Focal Adhesions, Transcriptome, Genome-Wide Association Study, Neurons, Induced Pluripotent Stem Cells, Pharmacogenetics, Antimanic Agents, Male, Female, Lithium Compounds, Gene Expression Profiling, Genomics, Multiomics, Biological Sciences, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry, Clinical sciences, Biological psychology, Clinical and health psychology

Abstract

Lithium (Li) is one of the most effective drugs for treating bipolar disorder (BD), however, there is presently no way to predict response to guide treatment. The aim of this study is to identify functional genes and pathways that distinguish BD Li responders (LR) from BD Li non-responders (NR). An initial Pharmacogenomics of Bipolar Disorder study (PGBD) GWAS of lithium response did not provide any significant results. As a result, we then employed network-based integrative analysis of transcriptomic and genomic data. In transcriptomic study of iPSC-derived neurons, 41 significantly differentially expressed (DE) genes were identified in LR vs NR regardless of lithium exposure. In the PGBD, post-GWAS gene prioritization using the GWA-boosting (GWAB) approach identified 1119 candidate genes. Following DE-derived network propagation, there was a highly significant overlap of genes between the top 500- and top 2000-proximal gene networks and the GWAB gene list (Phypergeometric = 1.28E-09 and 4.10E-18, respectively). Functional enrichment analyses of the top 500 proximal network genes identified focal adhesion and the extracellular matrix (ECM) as the most significant functions. Our findings suggest that the difference between LR and NR was a much greater effect than that of lithium. The direct impact of dysregulation of focal adhesion on axon guidance and neuronal circuits could underpin mechanisms of response to lithium, as well as underlying BD. It also highlights the power of integrative multi-omics analysis of transcriptomic and genomic profiling to gain molecular insights into lithium response in BD.

Published

2024

4. Genomic structural equation modeling reveals latent phenotypes in the human cortex with distinct genetic architecture

Author

Morey, Rajendra A., Zheng, Yuanchao, Bayly, Henry, Sun, Delin, Garrett, Melanie E., Gasperi, Marianna, Maihofer, Adam X., Baird, C. Lexi, Grasby, Katrina L., Huggins, Ashley A., Haswell, Courtney C., Thompson, Paul M., Medland, Sarah, Gustavson, Daniel E., Panizzon, Matthew S., Kremen, William S., Nievergelt, Caroline M., Ashley-Koch, Allison E., and Logue, Mark W.

Published

2024

5. Blood-based DNA methylation and exposure risk scores predict PTSD with high accuracy in military and civilian cohorts

Author

Wani, Agaz H., Katrinli, Seyma, Zhao, Xiang, Daskalakis, Nikolaos P., Zannas, Anthony S., Aiello, Allison E., Baker, Dewleen G., Boks, Marco P., Brick, Leslie A., Chen, Chia-Yen, Dalvie, Shareefa, Fortier, Catherine, Geuze, Elbert, Hayes, Jasmeet P., Kessler, Ronald C., King, Anthony P., Koen, Nastassja, Liberzon, Israel, Lori, Adriana, Luykx, Jurjen J., Maihofer, Adam X., Milberg, William, Miller, Mark W., Mufford, Mary S., Nugent, Nicole R., Rauch, Sheila, Ressler, Kerry J., Risbrough, Victoria B., Rutten, Bart P. F., Stein, Dan J., Stein, Murray B., Ursano, Robert J., Verfaellie, Mieke H., Vermetten, Eric, Vinkers, Christiaan H., Ware, Erin B., Wildman, Derek E., Wolf, Erika J., Nievergelt, Caroline M., Logue, Mark W., Smith, Alicia K., and Uddin, Monica

Published

2024

6. Genome-wide association analyses identify 95 risk loci and provide insights into the neurobiology of post-traumatic stress disorder

Author

Nievergelt, Caroline M., Maihofer, Adam X., Atkinson, Elizabeth G., Chen, Chia-Yen, Choi, Karmel W., Coleman, Jonathan R. I., Daskalakis, Nikolaos P., Duncan, Laramie E., Polimanti, Renato, Aaronson, Cindy, Amstadter, Ananda B., Andersen, Soren B., Andreassen, Ole A., Arbisi, Paul A., Ashley-Koch, Allison E., Austin, S. Bryn, Avdibegoviç, Esmina, Babić, Dragan, Bacanu, Silviu-Alin, Baker, Dewleen G., Batzler, Anthony, Beckham, Jean C., Belangero, Sintia, Benjet, Corina, Bergner, Carisa, Bierer, Linda M., Biernacka, Joanna M., Bierut, Laura J., Bisson, Jonathan I., Boks, Marco P., Bolger, Elizabeth A., Brandolino, Amber, Breen, Gerome, Bressan, Rodrigo Affonseca, Bryant, Richard A., Bustamante, Angela C., Bybjerg-Grauholm, Jonas, Bækvad-Hansen, Marie, Børglum, Anders D., Børte, Sigrid, Cahn, Leah, Calabrese, Joseph R., Caldas-de-Almeida, Jose Miguel, Chatzinakos, Chris, Cheema, Sheraz, Clouston, Sean A. P., Colodro-Conde, Lucía, Coombes, Brandon J., Cruz-Fuentes, Carlos S., Dale, Anders M., Dalvie, Shareefa, Davis, Lea K., Deckert, Jürgen, Delahanty, Douglas L., Dennis, Michelle F., Desarnaud, Frank, DiPietro, Christopher P., Disner, Seth G., Docherty, Anna R., Domschke, Katharina, Dyb, Grete, Kulenović, Alma Džubur, Edenberg, Howard J., Evans, Alexandra, Fabbri, Chiara, Fani, Negar, Farrer, Lindsay A., Feder, Adriana, Feeny, Norah C., Flory, Janine D., Forbes, David, Franz, Carol E., Galea, Sandro, Garrett, Melanie E., Gelaye, Bizu, Gelernter, Joel, Geuze, Elbert, Gillespie, Charles F., Goleva, Slavina B., Gordon, Scott D., Goçi, Aferdita, Grasser, Lana Ruvolo, Guindalini, Camila, Haas, Magali, Hagenaars, Saskia, Hauser, Michael A., Heath, Andrew C., Hemmings, Sian M. J., Hesselbrock, Victor, Hickie, Ian B., Hogan, Kelleigh, Hougaard, David Michael, Huang, Hailiang, Huckins, Laura M., Hveem, Kristian, Jakovljević, Miro, Javanbakht, Arash, Jenkins, Gregory D., Johnson, Jessica, Jones, Ian, Jovanovic, Tanja, Karstoft, Karen-Inge, Kaufman, Milissa L., Kennedy, James L., Kessler, Ronald C., Khan, Alaptagin, Kimbrel, Nathan A., King, Anthony P., Koen, Nastassja, Kotov, Roman, Kranzler, Henry R., Krebs, Kristi, Kremen, William S., Kuan, Pei-Fen, Lawford, Bruce R., Lebois, Lauren A. M., Lehto, Kelli, Levey, Daniel F., Lewis, Catrin, Liberzon, Israel, Linnstaedt, Sarah D., Logue, Mark W., Lori, Adriana, Lu, Yi, Luft, Benjamin J., Lupton, Michelle K., Luykx, Jurjen J., Makotkine, Iouri, Maples-Keller, Jessica L., Marchese, Shelby, Marmar, Charles, Martin, Nicholas G., Martínez-Levy, Gabriela A., McAloney, Kerrie, McFarlane, Alexander, McLaughlin, Katie A., McLean, Samuel A., Medland, Sarah E., Mehta, Divya, Meyers, Jacquelyn, Michopoulos, Vasiliki, Mikita, Elizabeth A., Milani, Lili, Milberg, William, Miller, Mark W., Morey, Rajendra A., Morris, Charles Phillip, Mors, Ole, Mortensen, Preben Bo, Mufford, Mary S., Nelson, Elliot C., Nordentoft, Merete, Norman, Sonya B., Nugent, Nicole R., O’Donnell, Meaghan, Orcutt, Holly K., Pan, Pedro M., Panizzon, Matthew S., Pathak, Gita A., Peters, Edward S., Peterson, Alan L., Peverill, Matthew, Pietrzak, Robert H., Polusny, Melissa A., Porjesz, Bernice, Powers, Abigail, Qin, Xue-Jun, Ratanatharathorn, Andrew, Risbrough, Victoria B., Roberts, Andrea L., Rothbaum, Alex O., Rothbaum, Barbara O., Roy-Byrne, Peter, Ruggiero, Kenneth J., Rung, Ariane, Runz, Heiko, Rutten, Bart P. F., de Viteri, Stacey Saenz, Salum, Giovanni Abrahão, Sampson, Laura, Sanchez, Sixto E., Santoro, Marcos, Seah, Carina, Seedat, Soraya, Seng, Julia S., Shabalin, Andrey, Sheerin, Christina M., Silove, Derrick, Smith, Alicia K., Smoller, Jordan W., Sponheim, Scott R., Stein, Dan J., Stensland, Synne, Stevens, Jennifer S., Sumner, Jennifer A., Teicher, Martin H., Thompson, Wesley K., Tiwari, Arun K., Trapido, Edward, Uddin, Monica, Ursano, Robert J., Valdimarsdóttir, Unnur, Van Hooff, Miranda, Vermetten, Eric, Vinkers, Christiaan H., Voisey, Joanne, Wang, Yunpeng, Wang, Zhewu, Waszczuk, Monika, Weber, Heike, Wendt, Frank R., Werge, Thomas, Williams, Michelle A., Williamson, Douglas E., Winsvold, Bendik S., Winternitz, Sherry, Wolf, Christiane, Wolf, Erika J., Xia, Yan, Xiong, Ying, Yehuda, Rachel, Young, Keith A., Young, Ross McD, Zai, Clement C., Zai, Gwyneth C., Zervas, Mark, Zhao, Hongyu, Zoellner, Lori A., Zwart, John-Anker, deRoon-Cassini, Terri, van Rooij, Sanne J. H., van den Heuvel, Leigh L., Stein, Murray B., Ressler, Kerry J., and Koenen, Karestan C.

Published

2024

7. Genome-wide association study of traumatic brain injury in U.S. military veterans enrolled in the VA million veteran program

Author

Merritt, Victoria C., Maihofer, Adam X., Gasperi, Marianna, Chanfreau-Coffinier, Catherine, Stein, Murray B., Panizzon, Matthew S., Hauger, Richard L., Logue, Mark W., Delano-Wood, Lisa, and Nievergelt, Caroline M.

Published

2024

8. Sex differences in the polygenic architecture of hearing problems in adults

Author

De Angelis, Flavio, Zeleznik, Oana A, Wendt, Frank R, Pathak, Gita A, Tylee, Daniel S, De Lillo, Antonella, Koller, Dora, Cabrera-Mendoza, Brenda, Clifford, Royce E, Maihofer, Adam X, Nievergelt, Caroline M, Curhan, Gary C, Curhan, Sharon G, and Polimanti, Renato

Subjects

Biological Sciences, Genetics, Aging, Brain Disorders, Human Genome, Prevention, Aetiology, 2.1 Biological and endogenous factors, Good Health and Well Being, Humans, Adult, Male, Female, Follow-Up Studies, Sex Characteristics, Genetic Predisposition to Disease, Multifactorial Inheritance, Hearing, Genome-Wide Association Study, Hearing problems, Genome-wide association study, Ancestry, Polygenic risk scores, Transcriptomic regulation, Sex differences, Pleiotropy, Causal inference, Genome-wide gene-by-environment interaction, Ancestry, Polygenic risk scores, Clinical Sciences

Abstract

BackgroundHearing problems (HP) in adults are common and are associated with several comorbid conditions. Its prevalence increases with age, reflecting the cumulative effect of environmental factors and genetic predisposition. Although several risk loci have been already identified, HP biology and epidemiology are still insufficiently investigated by large-scale genetic studies.MethodsLeveraging the UK Biobank, the Nurses' Health Studies (I and II), the Health Professionals Follow-up Study, and the Million Veteran Program, we conducted a comprehensive genome-wide investigation of HP in 748,668 adult participants (discovery N = 501,825; replication N = 226,043; cross-ancestry replication N = 20,800). We leveraged the GWAS findings to characterize HP polygenic architecture, exploring sex differences, polygenic risk across ancestries, tissue-specific transcriptomic regulation, cause-effect relationships with genetically correlated traits, and gene interactions with HP environmental risk factors.ResultsWe identified 54 risk loci and demonstrated that HP polygenic risk is shared across ancestry groups. Our transcriptomic regulation analysis highlighted the potential role of the central nervous system in HP pathogenesis. The sex-stratified analyses showed several additional associations related to peripheral hormonally regulated tissues reflecting a potential role of estrogen in hearing function. This evidence was supported by the multivariate interaction analysis that showed how genes involved in brain development interact with sex, noise pollution, and tobacco smoking in relation to their HP associations. Additionally, the genetically informed causal inference analysis showed that HP is linked to many physical and mental health outcomes.ConclusionsThe results provide many novel insights into the biology and epidemiology of HP in adults. Our sex-specific analyses and transcriptomic associations highlighted molecular pathways that may be targeted for drug development or repurposing. Additionally, the potential causal relationships identified may support novel preventive screening programs to identify individuals at risk.

Published

2023

9. Polygenic risk for mental disorders as predictors of posttraumatic stress disorder after mild traumatic brain injury.

Author

Stein, Murray B, Jain, Sonia, Parodi, Livia, Choi, Karmel W, Maihofer, Adam X, Nelson, Lindsay D, Mukherjee, Pratik, Sun, Xiaoying, He, Feng, Okonkwo, David O, Giacino, Joseph T, Korley, Frederick K, Vassar, Mary J, Robertson, Claudia S, McCrea, Michael A, Temkin, Nancy, Markowitz, Amy J, Diaz-Arrastia, Ramon, Rosand, Jonathan, Manley, Geoffrey T, and TRACK-TBI Investigators

Subjects

TRACK-TBI Investigators, Humans, Brain Concussion, Longitudinal Studies, Prospective Studies, Stress Disorders, Post-Traumatic, Depressive Disorder, Major, Traumatic Head and Spine Injury, Mental Health, Post-Traumatic Stress Disorder (PTSD), Neurosciences, Brain Disorders, Physical Injury - Accidents and Adverse Effects, Anxiety Disorders, Clinical Research, Traumatic Brain Injury (TBI), Serious Mental Illness, Mental health, Good Health and Well Being, Clinical Sciences, Public Health and Health Services, Psychology

Abstract

Many patients with mild traumatic brain injury (mTBI) are at risk for mental health problems such as posttraumatic stress disorder (PTSD). The objective of this study was to determine whether the polygenic risk for PTSD (or for related mental health disorders or traits including major depressive disorder [MDD] and neuroticism [NEU]) was associated with an increased likelihood of PTSD in the aftermath of mTBI. We used data from individuals of European ancestry with mTBI enrolled in TRACK-TBI (n = 714), a prospective longitudinal study of level 1 trauma center patients. One hundred and sixteen mTBI patients (16.3%) had probable PTSD (PCL-5 score ≥33) at 6 months post-injury. We used summary statistics from recent GWAS studies of PTSD, MDD, and NEU to generate polygenic risk scores (PRS) for individuals in our sample. A multivariable model that included age, sex, pre-injury history of mental disorder, and cause of injury explained 7% of the variance in the PTSD outcome; the addition of the PTSD-PRS (and five ancestral principal components) significantly increased the variance explained to 11%. The adjusted odds of PTSD in the uppermost PTSD-PRS quintile was nearly four times higher (aOR = 3.71, 95% CI 1.80-7.65) than in the lowest PTSD-PRS quintile. There was no evidence of a statistically significant interaction between PTSD-PRS and prior history of mental disorder, indicating that PTSD-PRS had similar predictive utility among those with and without pre-injury psychiatric illness. When added to the model, neither MDD-PRS nor NEU-PRS were significantly associated with the PTSD outcome. These findings show that the risk for PTSD in the context of mTBI is, in part, genetically influenced. They also raise the possibility that an individual's PRS could be clinically actionable if used-possibly with other non-genetic predictors-to signal the need for enhanced follow-up and early intervention; this precision medicine approach needs to be prospectively studied.

Published

2023

10. Deriving psychiatric symptom-based biomarkers from multivariate relationships between psychophysiological and biochemical measures

Author

Stout, Daniel M, Simmons, Alan N, Nievergelt, Caroline M, Minassian, Arpi, Biswas, Nilima, Maihofer, Adam X, Risbrough, Victoria B, and Baker, Dewleen G

Subjects

Clinical and Health Psychology, Psychology, Brain Disorders, Neurosciences, Anxiety Disorders, Mind and Body, Mental Illness, Behavioral and Social Science, Depression, Basic Behavioral and Social Science, Clinical Research, Mental Health, 2.1 Biological and endogenous factors, Mental health, Humans, Anhedonia, Stress Disorders, Post-Traumatic, Anxiety, Biomarkers, Fatigue, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry, Biological psychology

Abstract

Identification of biomarkers for psychiatric disorders remains very challenging due to substantial symptom heterogeneity and diagnostic comorbidity, limiting the ability to map symptoms to underlying neurobiology. Dimensional symptom clusters, such as anhedonia, hyperarousal, etc., are complex and arise due to interactions of a multitude of complex biological relationships. The primary aim of the current investigation was to use multi-set canonical correlation analysis (mCCA) to derive biomarkers (biochemical, physiological) linked to dimensional symptoms across the anxiety and depressive spectrum. Active-duty service members (N = 2,592) completed standardized depression, anxiety and posttraumatic stress questionnaires and several psychophysiological and biochemical assays. Using this approach, we identified two phenotype associations between distinct physiological and biological phenotypes. One was characterized by symptoms of dysphoric arousal (anhedonia, anxiety, hypervigilance) which was associated with low blood pressure and startle reactivity. This finding is in line with previous studies suggesting blunted physiological reactivity is associated with subpopulations endorsing anxiety with comorbid depressive features. A second phenotype of anxious fatigue (high anxiety and reexperiencing/avoidance symptoms coupled with fatigue) was associated with elevated blood levels of norepinephrine and the inflammatory marker C-reactive protein in conjunction with high blood pressure. This second phenotype may describe populations in which inflammation and high sympathetic outflow might contribute to anxious fatigue. Overall, these findings support the growing consensus that distinct neuropsychiatric symptom patterns are associated with differential physiological and blood-based biological profiles and highlight the potential of mCCA to reveal important psychiatric symptom biomarkers from several psychophysiological and biochemical measures.

Published

2022

11. Rare copy number variation in posttraumatic stress disorder

Author

Maihofer, Adam X, Engchuan, Worrawat, Huguet, Guillaume, Klein, Marieke, MacDonald, Jeffrey R, Shanta, Omar, Thiruvahindrapuram, Bhooma, Jean-louis, Martineau, Saci, Zohra, Jacquemont, Sebastien, Scherer, Stephen W, Ketema, Elizabeth, Aiello, Allison E, Amstadter, Ananda B, Avdibegović, Esmina, Babic, Dragan, Baker, Dewleen G, Bisson, Jonathan I, Boks, Marco P, Bolger, Elizabeth A, Bryant, Richard A, Bustamante, Angela C, Caldas-de-Almeida, Jose Miguel, Cardoso, Graça, Deckert, Jurgen, Delahanty, Douglas L, Domschke, Katharina, Dunlop, Boadie W, Dzubur-Kulenovic, Alma, Evans, Alexandra, Feeny, Norah C, Franz, Carol E, Gautam, Aarti, Geuze, Elbert, Goci, Aferdita, Hammamieh, Rasha, Jakovljevic, Miro, Jett, Marti, Jones, Ian, Kaufman, Milissa L, Kessler, Ronald C, King, Anthony P, Kremen, William S, Lawford, Bruce R, Lebois, Lauren AM, Lewis, Catrin, Liberzon, Israel, Linnstaedt, Sarah D, Lugonja, Bozo, Luykx, Jurjen J, Lyons, Michael J, Mavissakalian, Matig R, McLaughlin, Katie A, McLean, Samuel A, Mehta, Divya, Mellor, Rebecca, Morris, Charles Phillip, Muhie, Seid, Orcutt, Holly K, Peverill, Matthew, Ratanatharathorn, Andrew, Risbrough, Victoria B, Rizzo, Albert, Roberts, Andrea L, Rothbaum, Alex O, Rothbaum, Barbara O, Roy-Byrne, Peter, Ruggiero, Kenneth J, Rutten, Bart PF, Schijven, Dick, Seng, Julia S, Sheerin, Christina M, Sorenson, Michael A, Teicher, Martin H, Uddin, Monica, Ursano, Robert J, Vinkers, Christiaan H, Voisey, Joanne, Weber, Heike, Winternitz, Sherry, Xavier, Miguel, Yang, Ruoting, McD Young, Ross, Zoellner, Lori A, Salem, Rany M, Shaffer, Richard A, Wu, Tianying, Ressler, Kerry J, Stein, Murray B, Koenen, Karestan C, Sebat, Jonathan, and Nievergelt, Caroline M

Subjects

Post-Traumatic Stress Disorder (PTSD), Mental Health, Human Genome, Genetics, Neurosciences, Brain Disorders, Mental health, Humans, DNA Copy Number Variations, Stress Disorders, Post-Traumatic, Genome, Brain, Genome-Wide Association Study, Polymorphism, Single Nucleotide, Genetic Predisposition to Disease, Psychiatric Genomics Consortium PTSD Working Group, Psychiatric Genomics Consortium CNV Working Group, Biological Sciences, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

Posttraumatic stress disorder (PTSD) is a heritable (h2 = 24-71%) psychiatric illness. Copy number variation (CNV) is a form of rare genetic variation that has been implicated in the etiology of psychiatric disorders, but no large-scale investigation of CNV in PTSD has been performed. We present an association study of CNV burden and PTSD symptoms in a sample of 114,383 participants (13,036 cases and 101,347 controls) of European ancestry. CNVs were called using two calling algorithms and intersected to a consensus set. Quality control was performed to remove strong outlier samples. CNVs were examined for association with PTSD within each cohort using linear or logistic regression analysis adjusted for population structure and CNV quality metrics, then inverse variance weighted meta-analyzed across cohorts. We examined the genome-wide total span of CNVs, enrichment of CNVs within specified gene-sets, and CNVs overlapping individual genes and implicated neurodevelopmental regions. The total distance covered by deletions crossing over known neurodevelopmental CNV regions was significant (beta = 0.029, SE = 0.005, P = 6.3 × 10-8). The genome-wide neurodevelopmental CNV burden identified explains 0.034% of the variation in PTSD symptoms. The 15q11.2 BP1-BP2 microdeletion region was significantly associated with PTSD (beta = 0.0206, SE = 0.0056, P = 0.0002). No individual significant genes interrupted by CNV were identified. 22 gene pathways related to the function of the nervous system and brain were significant in pathway analysis (FDR q

Published

2022

12. Psychological trauma and the genetic overlap between posttraumatic stress disorder and major depressive disorder

Author

Mundy, Jessica, Hübel, Christopher, Gelernter, Joel, Levey, Daniel, Murray, Robin M, Skelton, Megan, Stein, Murray B, Maihofer, Adam X, Nievergelt, Caroline M, Baker, Dewlen G, Risborough, Victoria B, Calabrese, Joseph R, Galea, Sandro, Stein, Dan J, Koen, Nastassja, Dalvie, Shareefa, Aiello, Allison E, Roberts, Andrea L, Koenen, KC, Solovieff, Nadia, Kranzler, Henry R, Zhao, Hongyu, Farrer, Lindsay A, Johnson, Eric Otto, Rice, John P, Bierut, Laura J, Saccone, Nancy L, McFarlane, Alexander, Forbes, David, Silove, Derrick, O'Donnell, Meaghan, Bryant, Richard A, van Hooff, Miranda, Sponheim, Scott R, Disner, Seth G, Pietrzak, Robert H, Chen, Chia-Yen, Smoller, Jordan W, Ursano, Robert J, Kessler, Ronald C, Junglen, Angela G, Delahanty, Douglas L, Amstadter, Ananda B, Sheerin, Christina M, Ruggiero, Ken, McLaughlin, Katie A, Peverill, Matthew, Caldas-de-Almeida, JM, Austin, S Bryn, Gelaye, Bizu, Williams, Michelle A, Sanchez, Sixto E, Franz, Carol E, Panizzon, Matthew S, Lyons, Michael J, Kremen, William S, Andreassen, Ole A, Dale, Anders M, Rutten, Bart PF, Vinkers, Christiaan, Schijven, Dick, Geuze, Elbert, Vermetten, Eric, Luykx, Jurjen J, Boks, Marco P, Ashley-Koch, Allison E, Beckham, Jean C, Garrett, Melanie E, Hauser, Michael A, Dennis, Michelle F, Kimbrel, Nathan A, Qin, Xue-Jun, Karstoft, Karen-Inge, Andersen, Soren B, Borglum, Anders D, Hougaard, David Michael, Bybjerg-Grauholm, Jonas, Duncan, Laramie E, Bµkvad-Hansen, Marie, Nordentoft, Merete, Mors, Ole, Mortensen, PB, Werge, Thomas, Thompson, Wesley K, Wang, Yunpeng, Heath, Andrew C, Nelson, Elliot C, Martin, Nicholas G, Gordon, Scott D, Wolf, Erika J, Logue, Mark W, Miller, Mark W, McGlinchey, Regina E, Milberg, William, Erbes, Christopher R, Polusny, Melissa A, Arbisi, Paul A, and Peterson, Alan L

Subjects

Prevention, Clinical Research, Genetics, Serious Mental Illness, Depression, Post-Traumatic Stress Disorder (PTSD), Mental Health, Brain Disorders, Anxiety Disorders, Major Depressive Disorder, Human Genome, 2.3 Psychological, social and economic factors, Aetiology, Mental health, Good Health and Well Being, Posttraumatic stress disorder, major depressive disorder, psychological trauma, genetics, genetic correlations, polygenic risk scores, Million Veteran Program, Post Traumatic Stress Disorder Working Group of the Psychiatric Genomics Consortium, Neurosciences, Public Health and Health Services, Psychology, Psychiatry

Abstract

BackgroundPosttraumatic stress disorder (PTSD) and major depressive disorder (MDD) are commonly reported co-occurring mental health consequences of psychological trauma exposure. The disorders have high genetic overlap. Trauma is a complex phenotype but research suggests that trauma sensitivity has a heritable basis. We investigated whether sensitivity to trauma in those with MDD reflects a similar genetic component in those with PTSD.MethodsGenetic correlations between PTSD and MDD in individuals reporting trauma and MDD in individuals not reporting trauma were estimated, as well as with recurrent MDD and single-episode MDD, using genome-wide association study (GWAS) summary statistics. Genetic correlations were replicated using PTSD data from the Psychiatric Genomics Consortium and the Million Veteran Program. Polygenic risk scores were generated in UK Biobank participants who met the criteria for lifetime MDD (N = 29 471). We investigated whether genetic loading for PTSD was associated with reporting trauma in these individuals.ResultsGenetic loading for PTSD was significantly associated with reporting trauma in individuals with MDD [OR 1.04 (95% CI 1.01-1.07), Empirical-p = 0.02]. PTSD was significantly more genetically correlated with recurrent MDD than with MDD in individuals not reporting trauma (rg differences = ~0.2, p < 0.008). Participants who had experienced recurrent MDD reported significantly higher rates of trauma than participants who had experienced single-episode MDD (χ2 > 166, p < 0.001).ConclusionsOur findings point towards the existence of genetic variants associated with trauma sensitivity that might be shared between PTSD and MDD, although replication with better powered GWAS is needed. Our findings corroborate previous research highlighting trauma exposure as a key risk factor for recurrent MDD.

Published

2022

13. A phenotypic spectrum of autism is attributable to the combined effects of rare variants, polygenic risk and sex

Author

Antaki, Danny, Guevara, James, Maihofer, Adam X, Klein, Marieke, Gujral, Madhusudan, Grove, Jakob, Carey, Caitlin E, Hong, Oanh, Arranz, Maria J, Hervas, Amaia, Corsello, Christina, Vaux, Keith K, Muotri, Alysson R, Iakoucheva, Lilia M, Courchesne, Eric, Pierce, Karen, Gleeson, Joseph G, Robinson, Elise B, Nievergelt, Caroline M, and Sebat, Jonathan

Subjects

Genetic Testing, Prevention, Intellectual and Developmental Disabilities (IDD), Brain Disorders, Mental Health, Genetics, Autism, Neurosciences, Pediatric, 2.1 Biological and endogenous factors, Aetiology, Autism Spectrum Disorder, Autistic Disorder, Child, Family, Female, Genetic Predisposition to Disease, Humans, Male, Multifactorial Inheritance, Biological Sciences, Medical and Health Sciences, Developmental Biology

Abstract

The genetic etiology of autism spectrum disorder (ASD) is multifactorial, but how combinations of genetic factors determine risk is unclear. In a large family sample, we show that genetic loads of rare and polygenic risk are inversely correlated in cases and greater in females than in males, consistent with a liability threshold that differs by sex. De novo mutations (DNMs), rare inherited variants and polygenic scores were associated with various dimensions of symptom severity in children and parents. Parental age effects on risk for ASD in offspring were attributable to a combination of genetic mechanisms, including DNMs that accumulate in the paternal germline and inherited risk that influences behavior in parents. Genes implicated by rare variants were enriched in excitatory and inhibitory neurons compared with genes implicated by common variants. Our results suggest that a phenotypic spectrum of ASD is attributable to a spectrum of genetic factors that impact different neurodevelopmental processes.

Published

2022

14. Enhancing Discovery of Genetic Variants for Posttraumatic Stress Disorder Through Integration of Quantitative Phenotypes and Trauma Exposure Information

Author

Maihofer, Adam X, Choi, Karmel W, Coleman, Jonathan RI, Daskalakis, Nikolaos P, Denckla, Christy A, Ketema, Elizabeth, Morey, Rajendra A, Polimanti, Renato, Ratanatharathorn, Andrew, Torres, Katy, Wingo, Aliza P, Zai, Clement C, Aiello, Allison E, Almli, Lynn M, Amstadter, Ananda B, Andersen, Soren B, Andreassen, Ole A, Arbisi, Paul A, Ashley-Koch, Allison E, Austin, S Bryn, Avdibegović, Esmina, Borglum, Anders D, Babić, Dragan, Bækvad-Hansen, Marie, Baker, Dewleen G, Beckham, Jean C, Bierut, Laura J, Bisson, Jonathan I, Boks, Marco P, Bolger, Elizabeth A, Bradley, Bekh, Brashear, Meghan, Breen, Gerome, Bryant, Richard A, Bustamante, Angela C, Bybjerg-Grauholm, Jonas, Calabrese, Joseph R, Caldas-de-Almeida, José M, Chen, Chia-Yen, Dale, Anders M, Dalvie, Shareefa, Deckert, Jürgen, Delahanty, Douglas L, Dennis, Michelle F, Disner, Seth G, Domschke, Katharina, Duncan, Laramie E, Džubur Kulenović, Alma, Erbes, Christopher R, Evans, Alexandra, Farrer, Lindsay A, Feeny, Norah C, Flory, Janine D, Forbes, David, Franz, Carol E, Galea, Sandro, Garrett, Melanie E, Gautam, Aarti, Gelaye, Bizu, Gelernter, Joel, Geuze, Elbert, Gillespie, Charles F, Goçi, Aferdita, Gordon, Scott D, Guffanti, Guia, Hammamieh, Rasha, Hauser, Michael A, Heath, Andrew C, Hemmings, Sian MJ, Hougaard, David Michael, Jakovljević, Miro, Jett, Marti, Johnson, Eric Otto, Jones, Ian, Jovanovic, Tanja, Qin, Xue-Jun, Karstoft, Karen-Inge, Kaufman, Milissa L, Kessler, Ronald C, Khan, Alaptagin, Kimbrel, Nathan A, King, Anthony P, Koen, Nastassja, Kranzler, Henry R, Kremen, William S, Lawford, Bruce R, Lebois, Lauren AM, Lewis, Catrin, Liberzon, Israel, Linnstaedt, Sarah D, Logue, Mark W, Lori, Adriana, Lugonja, Božo, Luykx, Jurjen J, Lyons, Michael J, Maples-Keller, Jessica L, Marmar, Charles, Martin, Nicholas G, Maurer, Douglas, and Mavissakalian, Matig R

Subjects

Biological Sciences, Genetics, Anxiety Disorders, Mental Health, Brain Disorders, Post-Traumatic Stress Disorder (PTSD), Prevention, Human Genome, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Phenotype, Polymorphism, Single Nucleotide, Stress Disorders, Post-Traumatic, GWAS, Heritability, PTSD, PheWAS, Trauma, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry, Biological sciences, Biomedical and clinical sciences, Psychology

Abstract

BackgroundPosttraumatic stress disorder (PTSD) is heritable and a potential consequence of exposure to traumatic stress. Evidence suggests that a quantitative approach to PTSD phenotype measurement and incorporation of lifetime trauma exposure (LTE) information could enhance the discovery power of PTSD genome-wide association studies (GWASs).MethodsA GWAS on PTSD symptoms was performed in 51 cohorts followed by a fixed-effects meta-analysis (N = 182,199 European ancestry participants). A GWAS of LTE burden was performed in the UK Biobank cohort (N = 132,988). Genetic correlations were evaluated with linkage disequilibrium score regression. Multivariate analysis was performed using Multi-Trait Analysis of GWAS. Functional mapping and annotation of leading loci was performed with FUMA. Replication was evaluated using the Million Veteran Program GWAS of PTSD total symptoms.ResultsGWASs of PTSD symptoms and LTE burden identified 5 and 6 independent genome-wide significant loci, respectively. There was a 72% genetic correlation between PTSD and LTE. PTSD and LTE showed largely similar patterns of genetic correlation with other traits, albeit with some distinctions. Adjusting PTSD for LTE reduced PTSD heritability by 31%. Multivariate analysis of PTSD and LTE increased the effective sample size of the PTSD GWAS by 20% and identified 4 additional loci. Four of these 9 PTSD loci were independently replicated in the Million Veteran Program.ConclusionsThrough using a quantitative trait measure of PTSD, we identified novel risk loci not previously identified using prior case-control analyses. PTSD and LTE have a high genetic overlap that can be leveraged to increase discovery power through multivariate methods.

Published

2022

15. Epigenome-wide meta-analysis of PTSD symptom severity in three military cohorts implicates DNA methylation changes in genes involved in immune system and oxidative stress

Author

Katrinli, Seyma, Maihofer, Adam X, Wani, Agaz H, Pfeiffer, John R, Ketema, Elizabeth, Ratanatharathorn, Andrew, Baker, Dewleen G, Boks, Marco P, Geuze, Elbert, Kessler, Ronald C, Risbrough, Victoria B, Rutten, Bart PF, Stein, Murray B, Ursano, Robert J, Vermetten, Eric, Logue, Mark W, Nievergelt, Caroline M, Smith, Alicia K, and Uddin, Monica

Subjects

Human Genome, Mental Health, Post-Traumatic Stress Disorder (PTSD), Genetics, 2.1 Biological and endogenous factors, Aetiology, Good Health and Well Being, Adaptor Proteins, Signal Transducing, DNA Methylation, Epigenesis, Genetic, Epigenome, Humans, Immune System, Male, Military Personnel, Oxidative Stress, Stress Disorders, Post-Traumatic, Biological Sciences, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

Epigenetic factors modify the effects of environmental factors on biological outcomes. Identification of epigenetic changes that associate with PTSD is therefore a crucial step in deciphering mechanisms of risk and resilience. In this study, our goal is to identify epigenetic signatures associated with PTSD symptom severity (PTSS) and changes in PTSS over time, using whole blood DNA methylation (DNAm) data (MethylationEPIC BeadChip) of military personnel prior to and following combat deployment. A total of 429 subjects (858 samples across 2 time points) from three male military cohorts were included in the analyses. We conducted two different meta-analyses to answer two different scientific questions: one to identify a DNAm profile of PTSS using a random effects model including both time points for each subject, and the other to identify a DNAm profile of change in PTSS conditioned on pre-deployment DNAm. Four CpGs near four genes (F2R, CNPY2, BAIAP2L1, and TBXAS1) and 88 differentially methylated regions (DMRs) were associated with PTSS. Change in PTSS after deployment was associated with 15 DMRs, of those 2 DMRs near OTUD5 and ELF4 were also associated with PTSS. Notably, three PTSS-associated CpGs near F2R, BAIAP2L1 and TBXAS1 also showed nominal evidence of association with change in PTSS. This study, which identifies PTSD-associated changes in genes involved in oxidative stress and immune system, provides novel evidence that epigenetic differences are associated with PTSS.

Published

2022

16. Testing the causal relationships of physical activity and sedentary behaviour with mental health and substance use disorders: a Mendelian randomisation study

Author

Iob, Eleonora, Pingault, Jean-Baptiste, Munafò, Marcus R., Stubbs, Brendon, Gilthorpe, Mark S., Maihofer, Adam X., and Danese, Andrea

Published

2023

17. Dissecting the genetic association of C-reactive protein with PTSD, traumatic events, and social support

Author

Muniz Carvalho, Carolina, Wendt, Frank R, Maihofer, Adam X, Stein, Dan J, Stein, Murray B, Sumner, Jennifer A, Hemmings, Sian MJ, Nievergelt, Caroline M, Koenen, Karestan C, Gelernter, Joel, Belangero, Sintia I, and Polimanti, Renato

Subjects

Biological Psychology, Biomedical and Clinical Sciences, Neurosciences, Psychology, Post-Traumatic Stress Disorder (PTSD), Mental Health, Brain Disorders, Anxiety Disorders, Behavioral and Social Science, Genetics, 2.3 Psychological, social and economic factors, Aetiology, 2.1 Biological and endogenous factors, C-Reactive Protein, Child, Genome-Wide Association Study, Humans, Polymorphism, Single Nucleotide, Social Support, Stress Disorders, Post-Traumatic, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry, Biological psychology

Abstract

Inflammatory markers like C-reactive protein (CRP) have been associated with post-traumatic stress disorder (PTSD) and traumatic experiences, but the underlying mechanisms are unclear. We investigated the relationship among serum CRP, PTSD, and traits related to traumatic events and social support using genetic association data from the Psychiatric Genomics Consortium (23,185 PTSD cases and 151,309 controls), the UK Biobank (UKB; up to 117,900 individuals), and the CHARGE study (Cohorts for Heart and Aging Research in Genomic Epidemiology, 148,164 individual). Linkage disequilibrium score regression, polygenic risk scoring, and two-sample Mendelian randomization (MR) analyses were used to investigate genetic overlap and causal relationships. Genetic correlations of CRP were observed with PTSD (rg = 0.16, p = 0.026) and traits related to traumatic events, and the presence of social support (-0.28

Published

2021

18. Contributions of circadian clock genes to cell survival in fibroblast models of lithium-responsive bipolar disorder

Author

Mishra, Himanshu K., Wei, Heather, Rohr, Kayla E., Ko, Insu, Nievergelt, Caroline M., Maihofer, Adam X., Shilling, Paul D., Alda, Martin, Berrettini, Wade H., Brennand, Kristen J., Calabrese, Joseph R., Coryell, William H., Frye, Mark, Gage, Fred, Gershon, Elliot, McInnis, Melvin G., Nurnberger, John, Oedegaard, Ketil J., Zandi, Peter P., Kelsoe, John R., and McCarthy, Michael J.

Published

2023

19. Trauma and posttraumatic stress disorder modulate polygenic predictors of hippocampal and amygdala volume

Author

Zheng, Yuanchao, Garrett, Melanie E, Sun, Delin, Clarke-Rubright, Emily K, Haswell, Courtney C, Maihofer, Adam X, Elman, Jeremy A, Franz, Carol E, Lyons, Michael J, Kremen, William S, Peverill, Matthew, Sambrook, Kelly, McLaughlin, Katie A, Davenport, Nicholas D, Disner, Seth, Sponheim, Scott R, Andrew, Elpiniki, Korgaonkar, Mayuresh, Bryant, Richard, Varkevisser, Tim, Geuze, Elbert, Coleman, Jonathan, Beckham, Jean C, Kimbrel, Nathan A, Sullivan, Danielle, Miller, Mark, Hayes, Jasmeet, Verfaellie, Mieke, Wolf, Erika, Salat, David, Spielberg, Jeffrey M, Milberg, William, McGlinchey, Regina, Dennis, Emily L, Thompson, Paul M, Medland, Sarah, Jahanshad, Neda, Nievergelt, Caroline M, Ashley-Koch, Allison E, Logue, Mark W, and Morey, Rajendra A

Subjects

Biological Psychology, Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Psychology, Neurosciences, Mental Health, Behavioral and Social Science, Brain Disorders, Post-Traumatic Stress Disorder (PTSD), Genetics, Anxiety Disorders, Aetiology, 2.1 Biological and endogenous factors, Good Health and Well Being, Amygdala, Brain, Hippocampus, Humans, Magnetic Resonance Imaging, Stress Disorders, Post-Traumatic, Clinical Sciences, Public Health and Health Services, Clinical sciences, Biological psychology

Abstract

The volume of subcortical structures represents a reliable, quantitative, and objective phenotype that captures genetic effects, environmental effects such as trauma, and disease effects such as posttraumatic stress disorder (PTSD). Trauma and PTSD represent potent exposures that may interact with genetic markers to influence brain structure and function. Genetic variants, associated with subcortical volumes in two large normative discovery samples, were used to compute polygenic scores (PGS) for the volume of seven subcortical structures. These were applied to a target sample enriched for childhood trauma and PTSD. Subcortical volume PGS from the discovery sample were strongly associated in our trauma/PTSD enriched sample (n = 7580) with respective subcortical volumes of the hippocampus (p = 1.10 × 10-20), thalamus (p = 7.46 × 10-10), caudate (p = 1.97 × 10-18), putamen (p = 1.7 × 10-12), and nucleus accumbens (p = 1.99 × 10-7). We found a significant association between the hippocampal volume PGS and hippocampal volume in control subjects from our sample, but was absent in individuals with PTSD (GxE; (beta = -0.10, p = 0.027)). This significant GxE (PGS × PTSD) relationship persisted (p

Published

2021

20. Examining Individual and Synergistic Contributions of PTSD and Genetics to Blood Pressure: A Trans-Ethnic Meta-Analysis

Author

Sumner, Jennifer A, Maihofer, Adam X, Michopoulos, Vasiliki, Rothbaum, Alex O, Almli, Lynn M, Andreassen, Ole A, Ashley-Koch, Allison E, Baker, Dewleen G, Beckham, Jean C, Bradley, Bekh, Breen, Gerome, Coleman, Jonathan RI, Dale, Anders M, Dennis, Michelle F, Feeny, Norah C, Franz, Carol E, Garrett, Melanie E, Gillespie, Charles F, Guffanti, Guia, Hauser, Michael A, Hemmings, Sian MJ, Jovanovic, Tanja, Kimbrel, Nathan A, Kremen, William S, Lawford, Bruce R, Logue, Mark W, Lori, Adriana, Lyons, Michael J, Maples-Keller, Jessica, Mavissakalian, Matig R, McGlinchey, Regina E, Mehta, Divya, Mellor, Rebecca, Milberg, William, Miller, Mark W, Morris, Charles Phillip, Panizzon, Matthew S, Ressler, Kerry J, Risbrough, Victoria B, Rothbaum, Barbara O, Roy-Byrne, Peter, Seedat, Soraya, Smith, Alicia K, Stevens, Jennifer S, van den Heuvel, Leigh Luella, Voisey, Joanne, Young, Ross McD, Zoellner, Lori A, Nievergelt, Caroline M, and Wolf, Erika J

Subjects

Biological Psychology, Biomedical and Clinical Sciences, Neurosciences, Psychology, Hypertension, Mental Health, Post-Traumatic Stress Disorder (PTSD), Anxiety Disorders, Cardiovascular, Mental Illness, Brain Disorders, Prevention, Good Health and Well Being, posttraumatic stress disorder, genetics, blood pressure, trans-ethnic, meta-analysis, Cognitive Sciences, Biological psychology

Abstract

Growing research suggests that posttraumatic stress disorder (PTSD) may be a risk factor for poor cardiovascular health, and yet our understanding of who might be at greatest risk of adverse cardiovascular outcomes after trauma is limited. In this study, we conducted the first examination of the individual and synergistic contributions of PTSD symptoms and blood pressure genetics to continuous blood pressure levels. We harnessed the power of the Psychiatric Genomics Consortium-PTSD Physical Health Working Group and investigated these associations across 11 studies of 72,224 trauma-exposed individuals of European (n = 70,870) and African (n = 1,354) ancestry. Genetic contributions to blood pressure were modeled via polygenic scores (PGS) for systolic blood pressure (SBP) and diastolic blood pressure (DBP) that were derived from a prior trans-ethnic blood pressure genome-wide association study (GWAS). Results of trans-ethnic meta-analyses revealed significant main effects of the PGS on blood pressure levels [SBP: β = 2.83, standard error (SE) = 0.06, p < 1E-20; DBP: β = 1.32, SE = 0.04, p < 1E-20]. Significant main effects of PTSD symptoms were also detected for SBP and DBP in trans-ethnic meta-analyses, though there was significant heterogeneity in these results. When including data from the largest contributing study - United Kingdom Biobank - PTSD symptoms were negatively associated with SBP levels (β = -1.46, SE = 0.44, p = 9.8E-4) and positively associated with DBP levels (β = 0.70, SE = 0.26, p = 8.1E-3). However, when excluding the United Kingdom Biobank cohort in trans-ethnic meta-analyses, there was a nominally significant positive association between PTSD symptoms and SBP levels (β = 2.81, SE = 1.13, p = 0.01); no significant association was observed for DBP (β = 0.43, SE = 0.78, p = 0.58). Blood pressure PGS did not significantly moderate the associations between PTSD symptoms and blood pressure levels in meta-analyses. Additional research is needed to better understand the extent to which PTSD is associated with high blood pressure and how genetic as well as contextual factors may play a role in influencing cardiovascular risk.

Published

2021

21. Longitudinal epigenome-wide association studies of three male military cohorts reveal multiple CpG sites associated with post-traumatic stress disorder

Author

Snijders, Clara, Maihofer, Adam X, Ratanatharathorn, Andrew, Baker, Dewleen G, Boks, Marco P, Geuze, Elbert, Jain, Sonia, Kessler, Ronald C, Pishva, Ehsan, Risbrough, Victoria B, Stein, Murray B, Ursano, Robert J, Vermetten, Eric, Vinkers, Christiaan H, Smith, Alicia K, Uddin, Monica, Rutten, Bart PF, and Nievergelt, Caroline M

Subjects

Mental Health, Post-Traumatic Stress Disorder (PTSD), Anxiety Disorders, Human Genome, Genetics, 2.1 Biological and endogenous factors, Aetiology, Adult, Case-Control Studies, Cell Cycle Proteins, Cohort Studies, CpG Islands, DNA Methylation, Epigenesis, Genetic, Epigenome, Genomics, Humans, Longitudinal Studies, Male, Military Personnel, Polymorphism, Single Nucleotide, Stress Disorders, Post-Traumatic, EWAS, Longitudinal, DNA methylation, Meta-analysis, Trauma, PTSD, Epigenetics, PGC PTSD EWAS Consortium, Clinical Sciences, Paediatrics and Reproductive Medicine

Abstract

BackgroundEpigenetic mechanisms have been suggested to play a role in the development of post-traumatic stress disorder (PTSD). Here, blood-derived DNA methylation data (HumanMethylation450 BeadChip) collected prior to and following combat exposure in three cohorts of male military members were analyzed to assess whether DNA methylation profiles are associated with the development of PTSD. A total of 123 PTSD cases and 143 trauma-exposed controls were included in the analyses. The Psychiatric Genomics Consortium (PGC) PTSD EWAS QC pipeline was used on all cohorts, and results were combined using a sample size weighted meta-analysis in a two-stage design. In stage one, we jointly analyzed data of two new cohorts (N = 126 and 78) for gene discovery, and sought to replicate significant findings in a third, previously published cohort (N = 62) to assess the robustness of our results. In stage 2, we aimed at maximizing power for gene discovery by combining all three cohorts in a meta-analysis.ResultsStage 1 analyses identified four CpG sites in which, conditional on pre-deployment DNA methylation, post-deployment DNA methylation was significantly associated with PTSD status after epigenome-wide adjustment for multiple comparisons. The most significant (intergenic) CpG cg05656210 (p = 1.0 × 10-08) was located on 5q31 and significantly replicated in the third cohort. In addition, 19 differentially methylated regions (DMRs) were identified, but failed replication. Stage 2 analyses identified three epigenome-wide significant CpGs, the intergenic CpG cg05656210 and two additional CpGs located in MAD1L1 (cg12169700) and HEXDC (cg20756026). Interestingly, cg12169700 had an underlying single nucleotide polymorphism (SNP) which was located within the same LD block as a recently identified PTSD-associated SNP in MAD1L1. Stage 2 analyses further identified 12 significant differential methylated regions (DMRs), 1 of which was located in MAD1L1 and 4 were situated in the human leukocyte antigen (HLA) region.ConclusionsThis study suggests that the development of combat-related PTSD is associated with distinct methylation patterns in several genomic positions and regions. Our most prominent findings suggest the involvement of the immune system through the HLA region and HEXDC, and MAD1L1 which was previously associated with PTSD.

Published

2020

22. Epigenome-wide meta-analysis of PTSD across 10 military and civilian cohorts identifies methylation changes in AHRR.

Author

Smith, Alicia K, Ratanatharathorn, Andrew, Maihofer, Adam X, Naviaux, Robert K, Aiello, Allison E, Amstadter, Ananda B, Ashley-Koch, Allison E, Baker, Dewleen G, Beckham, Jean C, Boks, Marco P, Bromet, Evelyn, Dennis, Michelle, Galea, Sandro, Garrett, Melanie E, Geuze, Elbert, Guffanti, Guia, Hauser, Michael A, Katrinli, Seyma, Kilaru, Varun, Kessler, Ronald C, Kimbrel, Nathan A, Koenen, Karestan C, Kuan, Pei-Fen, Li, Kefeng, Logue, Mark W, Lori, Adriana, Luft, Benjamin J, Miller, Mark W, Naviaux, Jane C, Nugent, Nicole R, Qin, Xuejun, Ressler, Kerry J, Risbrough, Victoria B, Rutten, Bart PF, Stein, Murray B, Ursano, Robert J, Vermetten, Eric, Vinkers, Christiaan H, Wang, Lin, Youssef, Nagy A, INTRuST Clinical Consortium, VA Mid-Atlantic MIRECC Workgroup, PGC PTSD Epigenetics Workgroup, Uddin, Monica, and Nievergelt, Caroline M

Subjects

INTRuST Clinical Consortium, VA Mid-Atlantic MIRECC Workgroup, PGC PTSD Epigenetics Workgroup, Humans, Wounds and Injuries, Kynurenine, Repressor Proteins, Case-Control Studies, Cohort Studies, Stress Disorders, Post-Traumatic, DNA Methylation, Epigenesis, Genetic, Military Personnel, Female, Male, Basic Helix-Loop-Helix Transcription Factors, Epigenome, Stress Disorders, Post-Traumatic, Epigenesis, Genetic

Abstract

Epigenetic differences may help to distinguish between PTSD cases and trauma-exposed controls. Here, we describe the results of the largest DNA methylation meta-analysis of PTSD to date. Ten cohorts, military and civilian, contribute blood-derived DNA methylation data from 1,896 PTSD cases and trauma-exposed controls. Four CpG sites within the aryl-hydrocarbon receptor repressor (AHRR) associate with PTSD after adjustment for multiple comparisons, with lower DNA methylation in PTSD cases relative to controls. Although AHRR methylation is known to associate with smoking, the AHRR association with PTSD is most pronounced in non-smokers, suggesting the result was independent of smoking status. Evaluation of metabolomics data reveals that AHRR methylation associated with kynurenine levels, which are lower among subjects with PTSD. This study supports epigenetic differences in those with PTSD and suggests a role for decreased kynurenine as a contributor to immune dysregulation in PTSD.

Published

2020

23. The association between lithium use and neurocognitive performance in patients with bipolar disorder

Author

Burdick, Katherine E, Millett, Caitlin E, Russo, Manuela, Alda, Martin, Alliey-Rodriguez, Ney, Anand, Amit, Balaraman, Yokesh, Berrettini, Wade, Bertram, Holli, Calabrese, Joseph R, Calkin, Cynthia, Conroy, Carla, Coryell, William, DeModena, Anna, Feeder, Scott, Fisher, Carrie, Frazier, Nicole, Frye, Mark, Gao, Keming, Garnham, Julie, Gershon, Elliot S, Glazer, Kara, Goes, Fernando S, Goto, Toyomi, Harrington, Gloria J, Jakobsen, Petter, Kamali, Masoud, Kelly, Marisa, Leckband, Susan, Løberg, Else Marie, Lohoff, Falk W, Maihofer, Adam X, McCarthy, Michael J, McInnis, Melvin, Morken, Gunnar, Nievergelt, Caroline M, Nurnberger, John, Oedegaard, Ketil J, Ortiz, Abigail, Ritchey, Megan, Ryan, Kelly, Schinagle, Martha, Schwebel, Candice, Shaw, Martha, Shilling, Paul, Slaney, Claire, Stapp, Emma, Tarwater, Bruce, Zandi, Peter, and Kelsoe, John R

Subjects

Biological Psychology, Biomedical and Clinical Sciences, Psychology, Mental Health, Serious Mental Illness, Brain Disorders, Behavioral and Social Science, Clinical Research, Bipolar Disorder, Clinical Trials and Supportive Activities, Mental health, Cognition, Cross-Sectional Studies, Humans, Lithium, Neuropsychological Tests, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry, Neurosciences, Biological psychology

Abstract

Lithium remains the gold standard for the treatment of bipolar disorder (BD); however, its use has declined over the years mainly due to the side effects and the subjective experience of cognitive numbness reported by patients. In the present study, we aim to methodically test the effects of lithium on neurocognitive functioning in the largest single cohort (n = 262) of BD patients reported to date by harnessing the power of a multi-site, ongoing clinical trial of lithium monotherapy. At the cross-sectional level, multivariate analysis of covariance (MANCOVA) was conducted to examine potential group differences across neurocognitive tests [California Verbal Learning Test (CVLT trials 1-5,CVLT delayed recall), Wechsler Digit Symbol, Trail-making Test parts A and B (TMT-A; TMT-B), and a global cognition index]. At the longitudinal level, on a subset of patients (n = 88) who achieved mood stabilization with lithium monotherapy, we explored the effect of lithium treatment across time on neurocognitive functioning. There were no differences at baseline between BD patients that were taking lithium compared with those that were not. At follow-up a significant neurocognitive improvement in the global cognitive index score [F = 31.69; p

Published

2020

24. Analysis of Genetically Regulated Gene Expression Identifies a Prefrontal PTSD Gene, SNRNP35, Specific to Military Cohorts

Author

Huckins, Laura M, Chatzinakos, Chris, Breen, Michael S, Hartmann, Jakob, Klengel, Torsten, da Silva Almeida, Ana C, Dobbyn, Amanda, Girdhar, Kiran, Hoffman, Gabriel E, Klengel, Claudia, Logue, Mark W, Lori, Adriana, Maihofer, Adam X, Morrison, Filomene G, Nguyen, Hoang T, Park, Yongjin, Ruderfer, Douglas, Sloofman, Laura G, van Rooij, Sanne JH, Consortium, PTSD Working Group of Psychiatric Genomics, Baker, Dewleen G, Chen, Chia-Yen, Cox, Nancy, Duncan, Laramie E, Geyer, Mark A, Glatt, Stephen J, Im, Hae Kyung, Risbrough, Victoria B, Smoller, Jordan W, Stein, Dan J, Yehuda, Rachel, Liberzon, Israel, Koenen, Karestan C, Jovanovic, Tanja, Kellis, Manolis, Miller, Mark W, Bacanu, Silviu-Alin, Nievergelt, Caroline M, Buxbaum, Joseph D, Sklar, Pamela, Ressler, Kerry J, Stahl, Eli A, and Daskalakis, Nikolaos P

Subjects

Genetics, Brain Disorders, Post-Traumatic Stress Disorder (PTSD), Mental Health, Neurosciences, 1.1 Normal biological development and functioning, Underpinning research, Neurological, Animals, Case-Control Studies, Cohort Studies, Dexamethasone, Down-Regulation, Gene Expression Regulation, Gene Regulatory Networks, Genetic Predisposition to Disease, Humans, Leukocytes, Male, Mice, Mice, Inbred C57BL, Military Personnel, Prefrontal Cortex, RNA Interference, RNA, Small Interfering, Repressor Proteins, Ribonucleoproteins, Small Nuclear, Stress Disorders, Post-Traumatic, PTSD Working Group of Psychiatric Genomics Consortium, GWAS, PTSD, blood, civilian, glucocorticoid, military, prefrontal cortex, sex, splicing, transcriptomic imputation, genetics, Transcriptomic Imputation, trauma, Biochemistry and Cell Biology, Medical Physiology

Abstract

To reveal post-traumatic stress disorder (PTSD) genetic risk influences on tissue-specific gene expression, we use brain and non-brain transcriptomic imputation. We impute genetically regulated gene expression (GReX) in 29,539 PTSD cases and 166,145 controls from 70 ancestry-specific cohorts and identify 18 significant GReX-PTSD associations corresponding to specific tissue-gene pairs. The results suggest substantial genetic heterogeneity based on ancestry, cohort type (military versus civilian), and sex. Two study-wide significant PTSD associations are identified in European and military European cohorts; ZNF140 is predicted to be upregulated in whole blood, and SNRNP35 is predicted to be downregulated in dorsolateral prefrontal cortex, respectively. In peripheral leukocytes from 175 marines, the observed PTSD differential gene expression correlates with the predicted differences for these individuals, and deployment stress produces glucocorticoid-regulated expression changes that include downregulation of both ZNF140 and SNRNP35. SNRNP35 knockdown in cells validates its functional role in U12-intron splicing. Finally, exogenous glucocorticoids in mice downregulate prefrontal Snrnp35 expression.

Published

2020

25. Genomic influences on self-reported childhood maltreatment.

Author

Dalvie, Shareefa, Maihofer, Adam X, Coleman, Jonathan RI, Bradley, Bekh, Breen, Gerome, Brick, Leslie A, Chen, Chia-Yen, Choi, Karmel W, Duncan, Laramie E, Guffanti, Guia, Haas, Magali, Harnal, Supriya, Liberzon, Israel, Nugent, Nicole R, Provost, Allison C, Ressler, Kerry J, Torres, Katy, Amstadter, Ananda B, Bryn Austin, S, Baker, Dewleen G, Bolger, Elizabeth A, Bryant, Richard A, Calabrese, Joseph R, Delahanty, Douglas L, Farrer, Lindsay A, Feeny, Norah C, Flory, Janine D, Forbes, David, Galea, Sandro, Gautam, Aarti, Gelernter, Joel, Hammamieh, Rasha, Jett, Marti, Junglen, Angela G, Kaufman, Milissa L, Kessler, Ronald C, Khan, Alaptagin, Kranzler, Henry R, Lebois, Lauren AM, Marmar, Charles, Mavissakalian, Matig R, McFarlane, Alexander, Donnell, Meaghan O', Orcutt, Holly K, Pietrzak, Robert H, Risbrough, Victoria B, Roberts, Andrea L, Rothbaum, Alex O, Roy-Byrne, Peter, Ruggiero, Ken, Seligowski, Antonia V, Sheerin, Christina M, Silove, Derrick, Smoller, Jordan W, Stein, Murray B, Teicher, Martin H, Ursano, Robert J, Van Hooff, Miranda, Winternitz, Sherry, Wolff, Jonathan D, Yehuda, Rachel, Zhao, Hongyu, Zoellner, Lori A, Stein, Dan J, Koenen, Karestan C, and Nievergelt, Caroline M

Subjects

Clinical Sciences, Public Health and Health Services, Psychology

Abstract

Childhood maltreatment is highly prevalent and serves as a risk factor for mental and physical disorders. Self-reported childhood maltreatment appears heritable, but the specific genetic influences on this phenotype are largely unknown. The aims of this study were to (1) identify genetic variation associated with self-reported childhood maltreatment, (2) estimate SNP-based heritability (h2snp), (3) assess predictive value of polygenic risk scores (PRS) for childhood maltreatment, and (4) quantify genetic overlap of childhood maltreatment with mental and physical health-related phenotypes, and condition the top hits from our analyses when such overlap is present. Genome-wide association analysis for childhood maltreatment was undertaken, using a discovery sample from the UK Biobank (UKBB) (n = 124,000) and a replication sample from the Psychiatric Genomics Consortium-posttraumatic stress disorder group (PGC-PTSD) (n = 26,290). h2snp for childhood maltreatment and genetic correlations with mental/physical health traits were calculated using linkage disequilibrium score regression. PRS was calculated using PRSice and mtCOJO was used to perform conditional analysis. Two genome-wide significant loci associated with childhood maltreatment (rs142346759, p = 4.35 × 10-8, FOXP1; rs10262462, p = 3.24 × 10-8, FOXP2) were identified in the discovery dataset but were not replicated in PGC-PTSD. h2snp for childhood maltreatment was ~6% and the PRS derived from the UKBB was significantly predictive of childhood maltreatment in PGC-PTSD (r2 = 0.0025; p = 1.8 × 10-15). The most significant genetic correlation of childhood maltreatment was with depressive symptoms (rg = 0.70, p = 4.65 × 10-40), although we show evidence that our top hits may be specific to childhood maltreatment. This is the first large-scale genetic study to identify specific variants associated with self-reported childhood maltreatment. Speculatively, FOXP genes might influence externalizing traits and so be relevant to childhood maltreatment. Alternatively, these variants may be associated with a greater likelihood of reporting maltreatment. A clearer understanding of the genetic relationships of childhood maltreatment, including particular abuse subtypes, with a range of phenotypes, may ultimately be useful in in developing targeted treatment and prevention strategies.

Published

2020

26. Sleep disturbance at pre-deployment is a significant predictor of post-deployment re-experiencing symptoms

Author

Acheson, Dean T, Kwan, Brian, Maihofer, Adam X, Risbrough, Victoria B, Nievergelt, Caroline M, Clark, Jacob W, Tu, Xin M, Irwin, Michael R, and Baker, Dewleen G

Subjects

Clinical Research, Sleep Research, Post-Traumatic Stress Disorder (PTSD), Brain Disorders, Mental Health, Behavioral and Social Science, Mental health, Good Health and Well Being, Sleep, insomnia, PTSD, re-experiencing, longitudinal, Clinical Sciences, Psychology

Abstract

Background: Insomnia is common in service members and associated with many mental and physical health problems. Recently, longitudinal data have been used to assess the impact of disturbed sleep on mental health outcomes. These studies have consistently shown relationships between sleep disturbance and development of mental illness. Objective: The present study examined the longitudinal relationship between sleep disturbance and PTSD symptomatology in a cohort of Marines and Navy Corpsmen deployed to Iraq and Afghanistan (n = 2,404) assessed prior to deployment, as well as at -3 and 6 months post-deployment. Additionally, we aimed to investigate the extent to which these relationships are moderated by combat-stress severity, and to what extent these findings are replicated in a second, separate cohort of Marines and Navy corpsmen (n = 938) assessed with identical measures prior to deployment and within 3 months of return. Method: The present study employed latent variable path models to examine the relationships between pre-deployment sleep disturbance and post-deployment re-experiencing symptoms. Initial cross-lagged path models were conducted on discovery and replication samples to validate the hypothesized predictive relationships. Follow up moderation path models were then conducted to include the effect of combat-stress severity on these relationships. Results: Initial cross-lagged models supported a significant relationship between pre-deployment sleep disturbance and future re-experiencing PTSD symptoms at all time points. Initial moderation models showed a small moderator effect of combat-stress severity, though the main predictive relationship between pre-deployment sleep disturbance and PTSD symptoms remained significant. The moderator effect was not significant in the replication sample. Conclusions: The results of this study support pre-deployment sleep disturbance as a risk factor for development of post-deployment PTSD symptoms. Interventions aimed at normalizing sleep may be important in preventive measures for PTSD.

Published

2019

27. Genome-wide Association of Endophenotypes for Schizophrenia From the Consortium on the Genetics of Schizophrenia (COGS) Study

Author

Greenwood, Tiffany A, Lazzeroni, Laura C, Maihofer, Adam X, Swerdlow, Neal R, Calkins, Monica E, Freedman, Robert, Green, Michael F, Light, Gregory A, Nievergelt, Caroline M, Nuechterlein, Keith H, Radant, Allen D, Siever, Larry J, Silverman, Jeremy M, Stone, William S, Sugar, Catherine A, Tsuang, Debby W, Tsuang, Ming T, Turetsky, Bruce I, Gur, Ruben C, Gur, Raquel E, and Braff, David L

Subjects

Schizophrenia, Neurosciences, Human Genome, Genetics, Mental Health, Clinical Research, Brain Disorders, 2.1 Biological and endogenous factors, Aetiology, Mental health, Good Health and Well Being, Adult, Cognitive Dysfunction, Endophenotypes, Female, Genome-Wide Association Study, Humans, Hyperpolarization-Activated Cyclic Nucleotide-Gated Channels, Male, Middle Aged, Neuregulins, Potassium Channels, Other Medical and Health Sciences, Psychology, Cognitive Sciences

Abstract

ImportanceThe Consortium on the Genetics of Schizophrenia (COGS) uses quantitative neurophysiological and neurocognitive endophenotypes with demonstrated deficits in schizophrenia as a platform from which to explore the underlying neural circuitry and genetic architecture. Many of these endophenotypes are associated with poor functional outcome in schizophrenia. Some are also endorsed as potential treatment targets by the US Food and Drug Administration.ObjectiveTo build on prior assessments of heritability, association, and linkage in the COGS phase 1 (COGS-1) families by reporting a genome-wide association study (GWAS) of 11 schizophrenia-related endophenotypes in the independent phase 2 (COGS-2) cohort of patients with schizophrenia and healthy comparison participants (HCPs).Design, setting, and participantsA total of 1789 patients with schizophrenia and HCPs of self-reported European or Latino ancestry were recruited through a collaborative effort across the COGS sites and genotyped using the PsychChip. Standard quality control filters were applied, and more than 6.2 million variants with a genotyping call rate of greater than 0.99 were available after imputation. Association was performed for data sets stratified by diagnosis and ancestry using linear regression and adjusting for age, sex, and 5 principal components, with results combined through weighted meta-analysis. Data for COGS-1 were collected from January 6, 2003, to August 6, 2008; data for COGS-2, from June 30, 2010, to February 14, 2014. Data were analyzed from October 28, 2016, to May 4, 2018.Main outcomes and measuresA genome-wide association study was performed to evaluate association for 11 neurophysiological and neurocognitive endophenotypes targeting key domains of schizophrenia related to inhibition, attention, vigilance, learning, working memory, executive function, episodic memory, and social cognition.ResultsThe final sample of 1533 participants included 861 male participants (56.2%), and the mean (SD) age was 41.8 (13.6) years. In total, 7 genome-wide significant regions (P

Published

2019

28. Neural progenitor cells derived from lithium responsive and non-responsive bipolar disorder patients exhibit distinct sensitivity to cell death following methamphetamine

Author

Mishra, Himanshu K., Mandyam, Atulya D., Trenet, Wulfran, Wei, Heather, Nievergelt, Caroline M., Maihofer, Adam X., Shilling, Paul D., Alda, Martin, Gershon, Elliot, McInnis, Melvin G., Kelsoe, John R., and McCarthy, Michael J.

Published

2023

29. The Relationship of Attention-Deficit/Hyperactivity Disorder With Posttraumatic Stress Disorder: A Two-Sample Mendelian Randomization and Population-Based Sibling Comparison Study

Author

Maihofer, Adam X., Choi, Karmel W., Coleman, Jonathan R.I., Daskalakis, Nikolaos P., Denckla, Christy A., Ketema, Elizabeth, Morey, Rajendra A., Polimanti, Renato, Ratanatharathorn, Andrew, Torres, Katy, Wingo, Aliza P., Zai, Clement C., Aiello, Allison E., Almli, Lynn M., Amstadter, Ananda B., Andersen, Soren B., Andreassen, Ole A., Arbisi, Paul A., Ashley-Koch, Allison E., Austin, S. Bryn, Avdibegovic, Esmina, Borglum, Anders D., Babic, Dragan, Bækvad-Hansen, Marie, Baker, Dewleen G., Beckham, Jean C., Bierut, Laura J., Bisson, Jonathan I., Boks, Marco P., Bolger, Elizabeth A., Bradley, Bekh, Brashear, Meghan, Breen, Gerome, Bryant, Richard A., Bustamante, Angela C., Bybjerg-Grauholm, Jonas, Calabrese, Joseph R., Caldas-de-Almeida, Jose Miguel, Chen, Chia-Yen, Dale, Anders M., Dalvie, Shareefa, Deckert, Jürgen, Delahanty, Douglas L., Dennis, Michelle F., Disner, Seth G., Domschke, Katharina, Duncan, Laramie E., Kulenovic, Alma Dzubur, Erbes, Christopher R., Evans, Alexandra, Farrer, Lindsay A., Feeny, Norah C., Flory, Janine D., Forbes, David, Franz, Carol E., Galea, Sandro, Garrett, Melanie E., Gautam, Aarti, Gelaye, Bizu, Gelernter, Joel, Geuze, Elbert, Gillespie, Charles F., Uka, Aferdita Goci, Gordon, Scott D., Guffanti, Guia, Hammamieh, Rasha, Hauser, Michael A., Heath, Andrew C., Hemmings, Sian M.J., Hougaard, David Michael, Jakovljevic, Miro, Jett, Marti, Johnson, Eric Otto, Jones, Ian, Jovanovic, Tanja, Qin, Xue-Jun, Karstoft, Karen-Inge, Kaufman, Milissa L., Kessler, Ronald C., Khan, Alaptagin, Kimbrel, Nathan A., King, Anthony P., Koen, Nastassja, Kranzler, Henry R., Kremen, William S., Lawford, Bruce R., Lebois, Lauren A.M., Lewis, Catrin, Liberzon, Israel, Linnstaedt, Sarah D., Logue, Mark W., Lori, Adriana, Lugonja, Bozo, Luykx, Jurjen J., Lyons, Michael J., Maples-Keller, Jessica L., Marmar, Charles, Martin, Nicholas G., Maurer, Douglas, Mavissakalian, Matig R., McFarlane, Alexander, McGlinchey, Regina E., McLaughlin, Katie A., McLean, Samuel A., Mehta, Divya, Mellor, Rebecca, Michopoulos, Vasiliki, Milberg, William, Miller, Mark W., Morris, Charles Phillip, Mors, Ole, Mortensen, Preben Bo, Nelson, Elliot C., Nordentoft, Merete, Norman, Sonya B., O’Donnell, Meaghan, Orcutt, Holly K., Panizzon, Matthew S., Peters, Edward S., Peterson, Alan L., Peverill, Matthew, Pietrzak, Robert H., Polusny, Melissa A., Rice, John P., Risbrough, Victoria B., Roberts, Andrea L., Rothbaum, Alex O., Rothbaum, Barbara O., Roy-Byrne, Peter, Ruggiero, Kenneth J., Rung, Ariane, Rutten, Bart P.F., Saccone, Nancy L., Sanchez, Sixto E., Schijven, Dick, Seedat, Soraya, Seligowski, Antonia V., Seng, Julia S., Sheerin, Christina M., Silove, Derrick, Smith, Alicia K., Smoller, Jordan W., Sponheim, Scott R., Stein, Dan J., Stevens, Jennifer S., Teicher, Martin H., Thompson, Wesley K., Trapido, Edward, Uddin, Monica, Ursano, Robert J., Luella van den Heuvel, Leigh, Van Hooff, Miranda, Vermetten, Eric, Vinkers, Christiaan, Voisey, Joanne, Wang, Yunpeng, Wang, Zhewu, Werge, Thomas, Williams, Michelle A., Williamson, Douglas E., Winternitz, Sherry, Wolf, Christiane, Wolf, Erika J., Yehuda, Rachel, Young, Keith A., Young, Ross McD., Zhao, Hongyu, Zoellner, Lori A., Haas, Magali, Lasseter, Heather, Provost, Allison C., Salem, Rany M., Sebat, Jonathan, Shaffer, Richard, Wu, Tianying, Ripke, Stephan, Daly, Mark J., Ressler, Kerry J., Koenen, Karestan C., Stein, Murray B., Nievergelt, Caroline M., Wendt, Frank R., Garcia-Argibay, Miguel, Cabrera-Mendoza, Brenda, Valdimarsdóttir, Unnur A., Nivard, Michel G., Larsson, Henrik, Mattheisen, Manuel, and Meier, Sandra M.

Published

2023

30. Integrating human brain proteomes with genome-wide association data implicates novel proteins in post-traumatic stress disorder

Author

Wingo, Thomas S., Gerasimov, Ekaterina S., Liu, Yue, Duong, Duc M., Vattathil, Selina M., Lori, Adriana, Gockley, Jake, Breen, Michael S., Maihofer, Adam X., Nievergelt, Caroline M., Koenen, Karestan C., Levey, Daniel F., Gelernter, Joel, Stein, Murray B., Ressler, Kerry J., Bennett, David A., Levey, Allan I., Seyfried, Nicholas T., and Wingo, Aliza P.

Published

2022

31. Association of polygenic risk scores, traumatic life events and coping strategies with war-related PTSD diagnosis and symptom severity in the South Eastern Europe (SEE)-PTSD cohort

Author

Weber, Heike, Maihofer, Adam X., Jaksic, Nenad, Bojic, Elma Feric, Kucukalic, Sabina, Dzananovic, Emina Sabic, Uka, Aferdita Goci, Hoxha, Blerina, Haxhibeqiri, Valdete, Haxhibeqiri, Shpend, Kravic, Nermina, Umihanic, Mirnesa Muminovic, Franc, Ana Cima, Babic, Romana, Pavlovic, Marko, Mehmedbasic, Alma Bravo, Aukst-Margetic, Branka, Kucukalic, Abdulah, Marjanovic, Damir, Babic, Dragan, Bozina, Nada, Jakovljevic, Miro, Sinanovic, Osman, Avdibegović, Esmina, Agani, Ferid, Warrings, Bodo, Domschke, Katharina, Nievergelt, Caroline M., Deckert, Jürgen, Dzubur-Kulenovic, Alma, and Erhardt, Angelika

Published

2022

32. International meta-analysis of PTSD genome-wide association studies identifies sex- and ancestry-specific genetic risk loci.

Author

Nievergelt, Caroline M, Maihofer, Adam X, Klengel, Torsten, Atkinson, Elizabeth G, Chen, Chia-Yen, Choi, Karmel W, Coleman, Jonathan RI, Dalvie, Shareefa, Duncan, Laramie E, Gelernter, Joel, Levey, Daniel F, Logue, Mark W, Polimanti, Renato, Provost, Allison C, Ratanatharathorn, Andrew, Stein, Murray B, Torres, Katy, Aiello, Allison E, Almli, Lynn M, Amstadter, Ananda B, Andersen, Søren B, Andreassen, Ole A, Arbisi, Paul A, Ashley-Koch, Allison E, Austin, S Bryn, Avdibegovic, Esmina, Babić, Dragan, Bækvad-Hansen, Marie, Baker, Dewleen G, Beckham, Jean C, Bierut, Laura J, Bisson, Jonathan I, Boks, Marco P, Bolger, Elizabeth A, Børglum, Anders D, Bradley, Bekh, Brashear, Megan, Breen, Gerome, Bryant, Richard A, Bustamante, Angela C, Bybjerg-Grauholm, Jonas, Calabrese, Joseph R, Caldas-de-Almeida, José M, Dale, Anders M, Daly, Mark J, Daskalakis, Nikolaos P, Deckert, Jürgen, Delahanty, Douglas L, Dennis, Michelle F, Disner, Seth G, Domschke, Katharina, Dzubur-Kulenovic, Alma, Erbes, Christopher R, Evans, Alexandra, Farrer, Lindsay A, Feeny, Norah C, Flory, Janine D, Forbes, David, Franz, Carol E, Galea, Sandro, Garrett, Melanie E, Gelaye, Bizu, Geuze, Elbert, Gillespie, Charles, Uka, Aferdita Goci, Gordon, Scott D, Guffanti, Guia, Hammamieh, Rasha, Harnal, Supriya, Hauser, Michael A, Heath, Andrew C, Hemmings, Sian MJ, Hougaard, David Michael, Jakovljevic, Miro, Jett, Marti, Johnson, Eric Otto, Jones, Ian, Jovanovic, Tanja, Qin, Xue-Jun, Junglen, Angela G, Karstoft, Karen-Inge, Kaufman, Milissa L, Kessler, Ronald C, Khan, Alaptagin, Kimbrel, Nathan A, King, Anthony P, Koen, Nastassja, Kranzler, Henry R, Kremen, William S, Lawford, Bruce R, Lebois, Lauren AM, Lewis, Catrin E, Linnstaedt, Sarah D, Lori, Adriana, Lugonja, Bozo, Luykx, Jurjen J, Lyons, Michael J, Maples-Keller, Jessica, Marmar, Charles, and Martin, Alicia R

Subjects

Humans, Genetic Predisposition to Disease, Ubiquitin-Protein Ligases, Stress Disorders, Post-Traumatic, Sex Factors, African Continental Ancestry Group, European Continental Ancestry Group, Veterans, Female, Male, Genome-Wide Association Study, Genetic Loci, Datasets as Topic, Human Genome, Mental Health, Biotechnology, Clinical Research, Post-Traumatic Stress Disorder (PTSD), Anxiety Disorders, Prevention, Genetics

Abstract

The risk of posttraumatic stress disorder (PTSD) following trauma is heritable, but robust common variants have yet to be identified. In a multi-ethnic cohort including over 30,000 PTSD cases and 170,000 controls we conduct a genome-wide association study of PTSD. We demonstrate SNP-based heritability estimates of 5-20%, varying by sex. Three genome-wide significant loci are identified, 2 in European and 1 in African-ancestry analyses. Analyses stratified by sex implicate 3 additional loci in men. Along with other novel genes and non-coding RNAs, a Parkinson's disease gene involved in dopamine regulation, PARK2, is associated with PTSD. Finally, we demonstrate that polygenic risk for PTSD is significantly predictive of re-experiencing symptoms in the Million Veteran Program dataset, although specific loci did not replicate. These results demonstrate the role of genetic variation in the biology of risk for PTSD and highlight the necessity of conducting sex-stratified analyses and expanding GWAS beyond European ancestry populations.

Published

2019

33. Chronotype and cellular circadian rhythms predict the clinical response to lithium maintenance treatment in patients with bipolar disorder

Author

McCarthy, Michael J, Wei, Heather, Nievergelt, Caroline M, Stautland, Andrea, Maihofer, Adam X, Welsh, David K, Shilling, Paul, Alda, Martin, Alliey-Rodriguez, Ney, Anand, Amit, Andreasson, Ole A, Balaraman, Yokesh, Berrettini, Wade H, Bertram, Holli, Brennand, Kristen J, Calabrese, Joseph R, Calkin, Cynthia V, Claasen, Ana, Conroy, Clara, Coryell, William H, Craig, David W, D’Arcangelo, Nicole, Demodena, Anna, Djurovic, Srdjan, Feeder, Scott, Fisher, Carrie, Frazier, Nicole, Frye, Mark A, Gage, Fred H, Gao, Keming, Garnham, Julie, Gershon, Elliot S, Glazer, Kara, Goes, Fernando, Goto, Toyomi, Harrington, Gloria, Jakobsen, Petter, Kamali, Masoud, Karberg, Elizabeth, Kelly, Marisa, Leckband, Susan G, Lohoff, Falk, McInnis, Melvin G, Mondimore, Francis, Morken, Gunnar, Nurnberger, John I, Obral, Sarah, Oedegaard, Ketil J, Ortiz, Abigail, Ritchey, Megan, Ryan, Kelly, Schinagle, Martha, Schoeyen, Helle, Schwebel, Candice, Shaw, Martha, Shekhtman, Tatyana, Slaney, Claire, Stapp, Emma, Szelinger, Szabolcs, Tarwater, Bruce, Zandi, Peter P, and Kelsoe, John R

Subjects

Bipolar Disorder, Depression, Sleep Research, Serious Mental Illness, Brain Disorders, Clinical Research, Mental Health, Mental health, Adult, Animals, Antimanic Agents, Cells, Cultured, Circadian Rhythm, Fibroblasts, Genotyping Techniques, Humans, Inositol 1, 4, 5-Trisphosphate Receptors, Lithium Compounds, Luminescent Measurements, Mice, NIH 3T3 Cells, Period Circadian Proteins, Polymorphism, Single Nucleotide, Prospective Studies, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

Bipolar disorder (BD) is a serious mood disorder associated with circadian rhythm abnormalities. Risk for BD is genetically encoded and overlaps with systems that maintain circadian rhythms. Lithium is an effective mood stabilizer treatment for BD, but only a minority of patients fully respond to monotherapy. Presently, we hypothesized that lithium-responsive BD patients (Li-R) would show characteristic differences in chronotype and cellular circadian rhythms compared to lithium non-responders (Li-NR). Selecting patients from a prospective, multi-center, clinical trial of lithium monotherapy, we examined morning vs. evening preference (chronotype) as a dimension of circadian rhythm function in 193 Li-R and Li-NR BD patients. From a subset of 59 patient donors, we measured circadian rhythms in skin fibroblasts longitudinally over 5 days using a bioluminescent reporter (Per2-luc). We then estimated circadian rhythm parameters (amplitude, period, phase) and the pharmacological effects of lithium on rhythms in cells from Li-R and Li-NR donors. Compared to Li-NRs, Li-Rs showed a difference in chronotype, with higher levels of morningness. Evening chronotype was associated with increased mood symptoms at baseline, including depression, mania, and insomnia. Cells from Li-Rs were more likely to exhibit a short circadian period, a linear relationship between period and phase, and period shortening effects of lithium. Common genetic variation in the IP3 signaling pathway may account for some of the individual differences in the effects of lithium on cellular rhythms. We conclude that circadian rhythms may influence response to lithium in maintenance treatment of BD.

Published

2019

34. Entrainment of Circadian Rhythms to Temperature Reveals Amplitude Deficits in Fibroblasts from Patients with Bipolar Disorder and Possible Links to Calcium Channels

Author

Nudell, Victoria, Wei, Heather, Nievergelt, Caroline, Maihofer, Adam X, Shilling, Paul, Alda, Martin, Berrettini, Wade H, Brennand, Kristen J, Calabrese, Joseph R, Coryell, William H, Covault, Jonathan M, Frye, Mark A, Gage, Fred, Gershon, Elliot, McInnis, Melvin G, Nurnberger, John I, Oedegaard, Ketil J, Shekhtman, Tatyana, Zandi, Peter P, Kelsoe, John R, and McCarthy, Michael J

Subjects

Medical Physiology, Biomedical and Clinical Sciences, Bipolar Disorder, Sleep Research, Brain Disorders, Bipolar disorder, Calcium channel, Circadian rhythm, Gene expression

Abstract

Bipolar disorder (BD) is characterized by recurrent mood episodes, and circadian rhythm disturbances. Past studies have identified calcium channel genes as risk loci for BD. CACNA1C encodes an L-type calcium channel (LTCC) involved in the entrainment of circadian rhythms to light. Another calcium channel, i.e., the ryanodine receptor (RYR), is involved in -circadian phase delays. It is unknown whether variants in CACNA1C or other calcium channels contribute to the circadian phenotype in BD. We hypothesized that, by using temperature cycles, we could model circadian entrainment in fibroblasts from BD patients and controls to interrogate the circadian functions of LTCCs. Using Per2-luc, a bioluminescent reporter, we verified that cells entrain to temperature rhythms in vitro. Under constant temperature conditions, the LTCC antagonist verapamil shortened the circadian period, and the RYR antagonist dantrolene lengthened the period. However, neither drug affected temperature entrainment. Fibroblasts from BD patients and controls also entrained to temperature. In cells from BD patients, the rhythm amplitude was lower under entrained, but not constant, conditions. Temperature entrainment was otherwise similar between BD and control cells. However, the CACNA1C genotype among BD cells predicted the degree to which cells entrained. We conclude that assessment of rhythms under entrained conditions reveals additional rhythm abnormalities in BD that are not observable under constant temperature conditions.

Published

2019

35. Alcohol use and alcohol use disorder differ in their genetic relationships with PTSD: A genomic structural equation modelling approach

Author

Bountress, Kaitlin E., Brick, Leslie A., Sheerin, Christina, Grotzinger, Andrew, Bustamante, Daniel, Hawn, Sage E., Gillespie, Nathan, Kirkpatrick, Robert M., Kranzler, Henry, Morey, Rajendra, Edenberg, Howard J., Maihofer, Adam X., Disner, Seth, Ashley-Koch, Allison, Peterson, Roseann, Lori, Adriana, Stein, Dan J., Kimbrel, Nathan, Nievergelt, Caroline, Andreassen, Ole A., Luykx, Jurjen, Javanbakht, Arash, Youssef, Nagy A., and Amstadter, Ananda B.

Published

2022

36. Problematic alcohol use associates with sodium channel and clathrin linker 1 (SCLT1) in trauma‐exposed populations

Author

Almli, Lynn M, Lori, Adriana, Meyers, Jacquelyn L, Shin, Jaemin, Fani, Negar, Maihofer, Adam X, Nievergelt, Caroline M, Smith, Alicia K, Mercer, Kristina B, Kerley, Kimberly, Leveille, Jennifer M, Feng, Hao, Abu‐Amara, Duna, Flory, Janine D, Yehuda, Rachel, Marmar, Charles R, Baker, Dewleen G, Bradley, Bekh, Koenen, Karestan C, Conneely, Karen N, and Ressler, Kerry J

Subjects

Human Genome, Genetics, Substance Misuse, Alcoholism, Alcohol Use and Health, Prevention, Physical Injury - Accidents and Adverse Effects, Mental health, Cardiovascular, Good Health and Well Being, Adolescent, Adult, Black or African American, Aged, Alcoholism, Brain, Cohort Studies, Female, Genome-Wide Association Study, Georgia, Humans, Magnetic Resonance Imaging, Male, Middle Aged, Polymorphism, Single Nucleotide, Sodium Channels, Stress Disorders, Post-Traumatic, Young Adult, alcohol consumption, alcohol use disorder, AUDIT, expression QTL, fMRI, genome-wide association study, Medical and Health Sciences, Psychology and Cognitive Sciences, Substance Abuse

Abstract

Excessive alcohol use is extremely prevalent in the United States, particularly among trauma-exposed individuals. While several studies have examined genetic influences on alcohol use and related problems, this has not been studied in the context of trauma-exposed populations. We report results from a genome-wide association study of alcohol consumption and associated problems as measured by the alcohol use disorders identification test (AUDIT) in a trauma-exposed cohort. Results indicate a genome-wide significant association between total AUDIT score and rs1433375 [N = 1036, P = 2.61 × 10-8 (dominant model), P = 7.76 × 10-8 (additive model)], an intergenic single-nucleotide polymorphism located 323 kb upstream of the sodium channel and clathrin linker 1 (SCLT1) at 4q28. rs1433375 was also significant in a meta-analysis of two similar, but independent, cohorts (N = 1394, P = 0.0004), the Marine Resiliency Study and Systems Biology PTSD Biomarkers Consortium. Functional analysis indicated that rs1433375 was associated with SCLT1 gene expression and cortical-cerebellar functional connectivity measured via resting state functional magnetic resonance imaging. Together, findings suggest a role for sodium channel regulation and cerebellar functioning in alcohol use behavior. Identifying mechanisms underlying risk for problematic alcohol use in trauma-exposed populations is critical for future treatment and prevention efforts.

Published

2018

37. PTSD Blood Transcriptome Mega-Analysis: Shared Inflammatory Pathways across Biological Sex and Modes of Trauma

Author

Breen, Michael S, Tylee, Daniel S, Maihofer, Adam X, Neylan, Thomas C, Mehta, Divya, Binder, Elisabeth B, Chandler, Sharon D, Hess, Jonathan L, Kremen, William S, Risbrough, Victoria B, Woelk, Christopher H, Baker, Dewleen G, Nievergelt, Caroline M, Tsuang, Ming T, Buxbaum, Joseph D, and Glatt, Stephen J

Subjects

Biological Psychology, Biomedical and Clinical Sciences, Neurosciences, Psychology, Genetics, Anxiety Disorders, Mental Illness, Mental Health, Brain Disorders, Post-Traumatic Stress Disorder (PTSD), 2.1 Biological and endogenous factors, Inflammatory and immune system, Female, Humans, Male, Sex Characteristics, Stress Disorders, Post-Traumatic, Transcriptome, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry, Biological psychology

Abstract

Transcriptome-wide screens of peripheral blood during the onset and development of posttraumatic stress disorder (PTSD) indicate widespread immune dysregulation. However, little is known as to whether biological sex and the type of traumatic event influence shared or distinct biological pathways in PTSD. We performed a combined analysis of five independent PTSD blood transcriptome studies covering seven types of trauma in 229 PTSD and 311 comparison individuals to synthesize the extant data. Analyses by trauma type revealed a clear pattern of PTSD gene expression signatures distinguishing interpersonal (IP)-related traumas from combat-related traumas. Co-expression network analyses integrated all data and identified distinct gene expression perturbations across sex and modes of trauma in PTSD, including one wound-healing module downregulated in men exposed to combat traumas, one IL-12-mediated signaling module upregulated in men exposed to IP-related traumas, and two modules associated with lipid metabolism and mitogen-activated protein kinase activity upregulated in women exposed to IP-related traumas. Remarkably, a high degree of sharing of transcriptional dysregulation across sex and modes of trauma in PTSD was also observed converging on common signaling cascades, including cytokine, innate immune, and type I interferon pathways. Collectively, these findings provide a broad view of immune dysregulation in PTSD and demonstrate inflammatory pathways of molecular convergence and specificity, which may inform mechanisms and diagnostic biomarkers for the disorder.

Published

2018

38. COMT val158met polymorphism links to altered fear conditioning and extinction are modulated by PTSD and childhood trauma

Author

Deslauriers, Jessica, Acheson, Dean T, Maihofer, Adam X, Nievergelt, Caroline M, Baker, Dewleen G, Geyer, Mark A, Risbrough, Victoria B, and Team, Marine Resiliency Study

Subjects

Behavioral and Social Science, Clinical Research, Pediatric, Brain Disorders, Anxiety Disorders, Post-Traumatic Stress Disorder (PTSD), Genetics, Mental Health, Aetiology, 2.1 Biological and endogenous factors, Adult, Adult Survivors of Child Adverse Events, Catechol O-Methyltransferase, Conditioning, Psychological, Extinction, Psychological, Fear, Gene-Environment Interaction, Humans, Male, Military Personnel, Polymorphism, Genetic, Stress Disorders, Post-Traumatic, Young Adult, childhood trauma, COMT polymorphism, fear extinction, PTSD, Marines, trauma, Marine Resiliency Study Team, Clinical Sciences, Psychology, Psychiatry

Abstract

BackgroundRisk for posttraumatic stress disorder (PTSD) is thought to be mediated by gene × environment (G × E) interactions that affect core cognitive processes such as fear learning. The catechol-O-methyltransferase (COMT) val158met polymorphism has been associated with risk for PTSD and impaired fear inhibition. We used a large, relatively homogenous population to (1) replicate previous findings of poor fear inhibition in COMT Met/Met carriers with PTSD; (2) determine if COMT association with fear inhibition is moderated by childhood trauma (CT), an environmental risk factor for PTSD; and (3) determine if COMT is associated with altered fear processes after recent exposure to combat trauma.MethodsMale Marines and Navy Corpsmen of European-American ancestry were assessed prior to (n = 714) and 4-6 months after deployment to Afghanistan (n = 452). Acquisition and extinction of fear-potentiated startle, childhood and combat trauma history, and PTSD diagnosis were assessed at both time points.ResultsBefore deployment, Met/Met genotype was associated with fear inhibition deficits in participants with current PTSD; however, this association was dependent on CT exposure. After deployment, combat trauma was associated with a modest reduction in fear extinction in Met/Met compared with Val/Val carriers. There were no associations of COMT genotype with fear extinction within healthy and non-traumatized individuals.ConclusionsThese findings support the hypothesis that G × E interactions underlie associations of COMT val158met with fear inhibition deficits. These studies confirm that Met/Met carriers with PTSD have poor fear inhibition, and support further research in understanding how this polymorphism might impact response to extinction-based therapies.

Published

2018

39. Effects of military service and deployment on clinical symptomatology: The role of trauma exposure and social support

Author

Moore, Tyler M, Risbrough, Victoria B, Baker, Dewleen G, Larson, Gerald E, Glenn, Daniel E, Nievergelt, Caroline M, Maihofer, Adam, Port, Allison M, Jackson, Chad T, Ruparel, Kosha, and Gur, Ruben C

Subjects

Post-Traumatic Stress Disorder (PTSD), Anxiety Disorders, Mental Health, Good Health and Well Being, Adolescent, Adult, Afghan Campaign 2001-, Anxiety, Combat Disorders, Humans, Male, Military Personnel, Psychological Trauma, Sleep Initiation and Maintenance Disorders, Social Perception, Social Support, Stress Disorders, Post-Traumatic, United States, Young Adult, Marine resiliency study 2, Posttraumatic stress disorder, Computerized neurocognitive battery, Psychometrics, Social support, Medical and Health Sciences, Psychology and Cognitive Sciences, Psychiatry

Abstract

The Marine Resiliency Study-II examined changes in symptomatology across a deployment cycle to Afghanistan. U.S. Servicemembers (N = 1041) received clinical testing at two time points either bracketing a deployment (855) or not (186). Factor analyses were used to generate summary and change scores from Time 1 to Time 2. A between-subject design was used to examine changes across the deployment cycle with deployment (low-trauma, high-trauma, and non-deployed) and social support (low vs. high) as the grouping variables. Insomnia increased post-deployment regardless of deployment trauma (std. effect for high-trauma and low-trauma = 0.39 and 0.26, respectively). Only the high-trauma group showed increased PTSD symptoms and non-perspective-taking (std. effect = 0.40 and 0.30, respectively), while low-trauma showed decreased anxiety symptoms after deployment (std. effect = -0.17). These associations also depend on social support, with std. effects ranging from -0.22 to 0.51. When the groups were compared, the high-trauma deployed group showed significantly worse PTSD and non-perspective-taking than all other groups. Similar to studies in other military divisions, increased clinical symptoms were associated with high deployment stress in active duty Servicemembers, and social support shows promise as a moderator of said association.

Published

2017

40. A putative causal relationship between genetically determined female body shape and posttraumatic stress disorder

Author

Polimanti, Renato, Amstadter, Ananda B, Stein, Murray B, Almli, Lynn M, Baker, Dewleen G, Bierut, Laura J, Bradley, Bekh, Farrer, Lindsay A, Johnson, Eric O, King, Anthony, Kranzler, Henry R, Maihofer, Adam X, Rice, John P, Roberts, Andrea L, Saccone, Nancy L, Zhao, Hongyu, Liberzon, Israel, Ressler, Kerry J, Nievergelt, Caroline M, Koenen, Karestan C, Gelernter, Joel, and for The Psychiatric Genomics Consortium Posttraumatic Stress Disorder Workgroup

Subjects

Behavioral and Social Science, Post-Traumatic Stress Disorder (PTSD), Mental Health, Genetics, Anxiety Disorders, Prevention, Aetiology, 2.1 Biological and endogenous factors, Reproductive health and childbirth, Body Weights and Measures, Female, Genetic Predisposition to Disease, Humans, Male, Middle Aged, Polymorphism, Single Nucleotide, Reproduction, Risk, Sexual Behavior, Stress Disorders, Post-Traumatic, Trauma, Women, Anthropometric traits, Psychiatric Genomics Consortium Posttraumatic Stress Disorder Workgroup, Clinical Sciences

Abstract

BACKGROUND:The nature and underlying mechanisms of the observed increased vulnerability to posttraumatic stress disorder (PTSD) in women are unclear. METHODS:We investigated the genetic overlap of PTSD with anthropometric traits and reproductive behaviors and functions in women. The analysis was conducted using female-specific summary statistics from large genome-wide association studies (GWAS) and a cohort of 3577 European American women (966 PTSD cases and 2611 trauma-exposed controls). We applied a high-resolution polygenic score approach and Mendelian randomization analysis to investigate genetic correlations and causal relationships. RESULTS:We observed an inverse association of PTSD with genetically determined anthropometric traits related to body shape, independent of body mass index (BMI). The top association was related to BMI-adjusted waist circumference (WCadj; R = -0.079, P

Published

2017

41. Integrative Omic Approaches to Link PTSD Risk Variation to Function

Author

Maihofer, Adam, primary, Chen, Chia-Yen, additional, Coleman, Jonathan, additional, Daskalakis, Nikos, additional, Stein, Murray, additional, Ressler, Kerry, additional, Koenen, Karestan, additional, and Nievergelt, Caroline, additional

Published

2024

42. Epigenome-Wide Meta-Analysis of 11 Military and Civilian Cohorts Reveals Cell-Type Specific and Inflammatory DNA Methylation Patterns Associated With PTSD

Author

Katrinli, Seyma, primary, Wani, Agaz, additional, Zhao, Xiang, additional, Maihofer, Adam X., additional, Zhao, Ying, additional, Nunez, Diana, additional, Montalvo-Ortiz, Janitza, additional, Zannas, Anthony, additional, Logue, Mark W., additional, Nievergelt, Caroline M., additional, Uddin, Monica, additional, and Smith, Alicia, additional

Published

2024

43. Differential contributions of circadian clock genes to cell survival in bipolar disorder patient derived neuronal progenitor cells distinguishes lithium responders and non-responders

Author

Mishra, Himanshu K., primary, Wei, Heather, additional, LeRoux, Melissa, additional, Ko, Insu, additional, Rohr, Kayla E., additional, Nievergelt, Caroline M, additional, Maihofer, Adam X, additional, Shilling, Paul, additional, Alda, Martin, additional, Berrettini, Wade H, additional, Calabrese, Joseph R., additional, Coryell, William H., additional, Frye, Mark, additional, Gershon, Elliot, additional, McInnis, Melvin G., additional, Nurnberger, John, additional, Oedegaard, Ketil J., additional, Zandi, Peter P., additional, Kelsoe, John R., additional, and McCarthy, Michael J., additional

Published

2024

44. Exploring the Genetic Basis of Chronic Prostatitis/Chronic Pelvic Pain Syndrome: Insights from a Large-Scale Multi-Ancestry Study

Author

Rosenthal, Sara Brin, primary, Whisenant, Thomas, additional, Maihofer, Adam, additional, Afari, Niloofar, additional, Dochtermann, Daniel, additional, Pyarajan, Saiju, additional, Gerstenberger, Armand, additional, Nievergelt, Caroline, additional, and Program, Marianna Gasperi on behalf of the VA Million Veteran, additional

Published

2024

45. Epigenome‐wide association of PTSD from heterogeneous cohorts with a common multi‐site analysis pipeline

Author

Ratanatharathorn, Andrew, Boks, Marco P, Maihofer, Adam X, Aiello, Allison E, Amstadter, Ananda B, Ashley‐Koch, Allison E, Baker, Dewleen G, Beckham, Jean C, Bromet, Evelyn, Dennis, Michelle, Garrett, Melanie E, Geuze, Elbert, Guffanti, Guia, Hauser, Michael A, Kilaru, Varun, Kimbrel, Nathan A, Koenen, Karestan C, Kuan, Pei‐Fen, Logue, Mark W, Luft, Benjamin J, Miller, Mark W, Mitchell, Colter, Nugent, Nicole R, Ressler, Kerry J, Rutten, Bart PF, Stein, Murray B, Vermetten, Eric, Vinkers, Christiaan H, Youssef, Nagy A, Workgroup, VA Mid‐Atlantic MIRECC, Workgroup, PGC PTSD Epigenetics, Uddin, Monica, Nievergelt, Caroline M, and Smith, Alicia K

Subjects

Human Genome, Genetics, Post-Traumatic Stress Disorder (PTSD), Mental Health, Anxiety Disorders, Brain Disorders, 2.1 Biological and endogenous factors, Aetiology, Adult, Cohort Studies, DNA Methylation, Epigenomics, Female, Genetic Predisposition to Disease, Genome-Wide Association Study, Genomics, Humans, Male, Middle Aged, Phenotype, Stress Disorders, Post-Traumatic, EWAS, meta-analysis, stress, trauma, VA Mid-Atlantic MIRECC Workgroup, PGC PTSD Epigenetics Workgroup, Clinical Sciences, Neurosciences

Abstract

Compelling evidence suggests that epigenetic mechanisms such as DNA methylation play a role in stress regulation and in the etiologic basis of stress related disorders such as Post traumatic Stress Disorder (PTSD). Here we describe the purpose and methods of an international consortium that was developed to study the role of epigenetics in PTSD. Inspired by the approach used in the Psychiatric Genomics Consortium, we brought together investigators representing seven cohorts with a collective sample size of N = 1147 that included detailed information on trauma exposure, PTSD symptoms, and genome-wide DNA methylation data. The objective of this consortium is to increase the analytical sample size by pooling data and combining expertise so that DNA methylation patterns associated with PTSD can be identified. Several quality control and analytical pipelines were evaluated for their control of genomic inflation and technical artifacts with a joint analysis procedure established to derive comparable data over the cohorts for meta-analysis. We propose methods to deal with ancestry population stratification and type I error inflation and discuss the advantages and disadvantages of applying robust error estimates. To evaluate our pipeline, we report results from an epigenome-wide association study (EWAS) of age, which is a well-characterized phenotype with known epigenetic associations. Overall, while EWAS are highly complex and subject to similar challenges as genome-wide association studies (GWAS), we demonstrate that an epigenetic meta-analysis with a relatively modest sample size can be well-powered to identify epigenetic associations. Our pipeline can be used as a framework for consortium efforts for EWAS.

Published

2017

46. Erratum: Genetic loci associated with heart rate variability and their effects on cardiac disease risk.

Author

Nolte, Ilja, Munoz, M, Tragante, Vinicius, Amare, Azmeraw, Jansen, Rick, Vaez, Ahmad, von der Heyde, Benedikt, Avery, Christy, Bis, Joshua, Dierckx, Bram, van Dongen, Jenny, Gogarten, Stephanie, Goyette, Philippe, Hernesniemi, Jussi, Huikari, Ville, Hwang, Shih-Jen, Jaju, Deepali, Kerr, Kathleen, Kluttig, Alexander, Krijthe, Bouwe, Kumar, Jitender, van der Laan, Sander, Lyytikäinen, Leo-Pekka, Maihofer, Adam, Minassian, Arpi, van der Most, Peter, Müller-Nurasyid, Martina, Nivard, Michel, Salvi, Erika, Stewart, James, Thayer, Julian, Verweij, Niek, Wong, Andrew, Zabaneh, Delilah, Zafarmand, Mohammad, Abdellaoui, Abdel, Albarwani, Sulayma, Albert, Christine, Alonso, Alvaro, Ashar, Foram, Auvinen, Juha, Axelsson, Tomas, Baker, Dewleen, de Bakker, Paul, Barcella, Matteo, Bayoumi, Riad, Bieringa, Rob, Boomsma, Dorret, Boucher, Gabrielle, Britton, Annie, Christophersen, Ingrid, Dietrich, Andrea, Ehret, George, Ellinor, Patrick, Eskola, Markku, Felix, Janine, Floras, John, Franco, Oscar, Friberg, Peter, Gademan, Maaike, Geyer, Mark, Giedraitis, Vilmantas, Hartman, Catharina, Hemerich, Daiane, Hofman, Albert, Hottenga, Jouke-Jan, Huikuri, Heikki, Hutri-Kähönen, Nina, Jouven, Xavier, Junttila, Juhani, Juonala, Markus, Kiviniemi, Antti, Kors, Jan, Kumari, Meena, Kuznetsova, Tatiana, Laurie, Cathy, Lefrandt, Joop, Li, Yong, Li, Yun, Liao, Duanping, Limacher, Marian, Lin, Henry, Lindgren, Cecilia, Lubitz, Steven, Mahajan, Anubha, McKnight, Barbara, Zu Schwabedissen, Henriette, Milaneschi, Yuri, Mononen, Nina, Morris, Andrew, Nalls, Mike, Navis, Gerjan, Neijts, Melanie, Nikus, Kjell, North, Kari, OConnor, Daniel, Ormel, Johan, Perz, Siegfried, Peters, Annette, and Psaty, Bruce

Abstract

This corrects the article DOI: 10.1038/ncomms15805.

Published

2017

47. Genetic loci associated with heart rate variability and their effects on cardiac disease risk.

Author

Nolte, Ilja M, Munoz, M Loretto, Tragante, Vinicius, Amare, Azmeraw T, Jansen, Rick, Vaez, Ahmad, von der Heyde, Benedikt, Avery, Christy L, Bis, Joshua C, Dierckx, Bram, van Dongen, Jenny, Gogarten, Stephanie M, Goyette, Philippe, Hernesniemi, Jussi, Huikari, Ville, Hwang, Shih-Jen, Jaju, Deepali, Kerr, Kathleen F, Kluttig, Alexander, Krijthe, Bouwe P, Kumar, Jitender, van der Laan, Sander W, Lyytikäinen, Leo-Pekka, Maihofer, Adam X, Minassian, Arpi, van der Most, Peter J, Müller-Nurasyid, Martina, Nivard, Michel, Salvi, Erika, Stewart, James D, Thayer, Julian F, Verweij, Niek, Wong, Andrew, Zabaneh, Delilah, Zafarmand, Mohammad H, Abdellaoui, Abdel, Albarwani, Sulayma, Albert, Christine, Alonso, Alvaro, Ashar, Foram, Auvinen, Juha, Axelsson, Tomas, Baker, Dewleen G, de Bakker, Paul IW, Barcella, Matteo, Bayoumi, Riad, Bieringa, Rob J, Boomsma, Dorret, Boucher, Gabrielle, Britton, Annie R, Christophersen, Ingrid, Dietrich, Andrea, Ehret, George B, Ellinor, Patrick T, Eskola, Markku, Felix, Janine F, Floras, John S, Franco, Oscar H, Friberg, Peter, Gademan, Maaike GJ, Geyer, Mark A, Giedraitis, Vilmantas, Hartman, Catharina A, Hemerich, Daiane, Hofman, Albert, Hottenga, Jouke-Jan, Huikuri, Heikki, Hutri-Kähönen, Nina, Jouven, Xavier, Junttila, Juhani, Juonala, Markus, Kiviniemi, Antti M, Kors, Jan A, Kumari, Meena, Kuznetsova, Tatiana, Laurie, Cathy C, Lefrandt, Joop D, Li, Yong, Li, Yun, Liao, Duanping, Limacher, Marian C, Lin, Henry J, Lindgren, Cecilia M, Lubitz, Steven A, Mahajan, Anubha, McKnight, Barbara, Zu Schwabedissen, Henriette Meyer, Milaneschi, Yuri, Mononen, Nina, Morris, Andrew P, Nalls, Mike A, Navis, Gerjan, Neijts, Melanie, Nikus, Kjell, North, Kari E, O'Connor, Daniel T, Ormel, Johan, Perz, Siegfried, Peters, Annette, and Psaty, Bruce M

Subjects

Humans, Heart Diseases, Genetic Predisposition to Disease, RGS Proteins, Potassium Channels, Muscle Proteins, Risk Factors, Cohort Studies, Blood Pressure, Heart Rate, Polymorphism, Single Nucleotide, Quantitative Trait Loci, European Continental Ancestry Group, Genome-Wide Association Study, Hyperpolarization-Activated Cyclic Nucleotide-Gated Channels, Cardiovascular, Genetics, Heart Disease

Abstract

Reduced cardiac vagal control reflected in low heart rate variability (HRV) is associated with greater risks for cardiac morbidity and mortality. In two-stage meta-analyses of genome-wide association studies for three HRV traits in up to 53,174 individuals of European ancestry, we detect 17 genome-wide significant SNPs in eight loci. HRV SNPs tag non-synonymous SNPs (in NDUFA11 and KIAA1755), expression quantitative trait loci (eQTLs) (influencing GNG11, RGS6 and NEO1), or are located in genes preferentially expressed in the sinoatrial node (GNG11, RGS6 and HCN4). Genetic risk scores account for 0.9 to 2.6% of the HRV variance. Significant genetic correlation is found for HRV with heart rate (-0.74g

Published

2017

48. Identification of novel loci affecting circulating chromogranins and related peptides

Author

Benyamin, Beben, Maihofer, Adam X, Schork, Andrew J, Hamilton, Bruce A, Rao, Fangwen, Schmid-Schönbein, Geert W, Zhang, Kuixing, Mahata, Manjula, Stridsberg, Mats, Schork, Nicholas J, Biswas, Nilima, Hook, Vivian Y, Wei, Zhiyun, Montgomery, Grant W, Martin, Nicholas G, Nievergelt, Caroline M, Whitfield, John B, and O’Connor, Daniel T

Subjects

Adolescent, Adrenal Glands, Adult, Aged, Animals, Australia, Biomarkers, Catecholamines, Cells, Cultured, Chromaffin Cells, Chromogranin A, Factor XII, Female, Genetic Loci, Genome-Wide Association Study, Humans, Hypertension, Kallikreins, Male, Mice, Middle Aged, Peptide Fragments, Rats, United States, Young Adult, Biological Sciences, Medical and Health Sciences, Genetics & Heredity

Abstract

Chromogranins are pro-hormone secretory proteins released from neuroendocrine cells, with effects on control of blood pressure. We conducted a genome-wide association study for plasma catestatin, the catecholamine release inhibitory peptide derived from chromogranin A (CHGA), and other CHGA- or chromogranin B (CHGB)-related peptides, in 545 US and 1252 Australian subjects. This identified loci on chromosomes 4q35 and 5q34 affecting catestatin concentration (P = 3.40 × 10-30 for rs4253311 and 1.85 × 10-19 for rs2731672, respectively). Genes in these regions include the proteolytic enzymes kallikrein (KLKB1) and Factor XII (F12). In chromaffin cells, CHGA and KLKB1 proteins co-localized in catecholamine storage granules. In vitro, kallikrein cleaved recombinant human CHGA to catestatin, verified by mass spectrometry. The peptide identified from this digestion (CHGA360-373) selectively inhibited nicotinic cholinergic stimulated catecholamine release from chromaffin cells. A proteolytic cascade involving kallikrein and Factor XII cleaves chromogranins to active compounds both in vivo and in vitro.

Published

2017

49. Genome-wide association study of more than 40,000 bipolar disorder cases provides new insights into the underlying biology

Author

Mullins, Niamh, Forstner, Andreas J., O’Connell, Kevin S., Coombes, Brandon, Coleman, Jonathan R. I., Qiao, Zhen, Als, Thomas D., Bigdeli, Tim B., Børte, Sigrid, Bryois, Julien, Charney, Alexander W., Drange, Ole Kristian, Gandal, Michael J., Hagenaars, Saskia P., Ikeda, Masashi, Kamitaki, Nolan, Kim, Minsoo, Krebs, Kristi, Panagiotaropoulou, Georgia, Schilder, Brian M., Sloofman, Laura G., Steinberg, Stacy, Trubetskoy, Vassily, Winsvold, Bendik S., Won, Hong-Hee, Abramova, Liliya, Adorjan, Kristina, Agerbo, Esben, Al Eissa, Mariam, Albani, Diego, Alliey-Rodriguez, Ney, Anjorin, Adebayo, Antilla, Verneri, Antoniou, Anastasia, Awasthi, Swapnil, Baek, Ji Hyun, Bækvad-Hansen, Marie, Bass, Nicholas, Bauer, Michael, Beins, Eva C., Bergen, Sarah E., Birner, Armin, Bøcker Pedersen, Carsten, Bøen, Erlend, Boks, Marco P., Bosch, Rosa, Brum, Murielle, Brumpton, Ben M., Brunkhorst-Kanaan, Nathalie, Budde, Monika, Bybjerg-Grauholm, Jonas, Byerley, William, Cairns, Murray, Casas, Miquel, Cervantes, Pablo, Clarke, Toni-Kim, Cruceanu, Cristiana, Cuellar-Barboza, Alfredo, Cunningham, Julie, Curtis, David, Czerski, Piotr M., Dale, Anders M., Dalkner, Nina, David, Friederike S., Degenhardt, Franziska, Djurovic, Srdjan, Dobbyn, Amanda L., Douzenis, Athanassios, Elvsåshagen, Torbjørn, Escott-Price, Valentina, Ferrier, I. Nicol, Fiorentino, Alessia, Foroud, Tatiana M., Forty, Liz, Frank, Josef, Frei, Oleksandr, Freimer, Nelson B., Frisén, Louise, Gade, Katrin, Garnham, Julie, Gelernter, Joel, Giørtz Pedersen, Marianne, Gizer, Ian R., Gordon, Scott D., Gordon-Smith, Katherine, Greenwood, Tiffany A., Grove, Jakob, Guzman-Parra, José, Ha, Kyooseob, Haraldsson, Magnus, Hautzinger, Martin, Heilbronner, Urs, Hellgren, Dennis, Herms, Stefan, Hoffmann, Per, Holmans, Peter A., Huckins, Laura, Jamain, Stéphane, Johnson, Jessica S., Kalman, Janos L., Kamatani, Yoichiro, Kennedy, James L., Kittel-Schneider, Sarah, Knowles, James A., Kogevinas, Manolis, Koromina, Maria, Kranz, Thorsten M., Kranzler, Henry R., Kubo, Michiaki, Kupka, Ralph, Kushner, Steven A., Lavebratt, Catharina, Lawrence, Jacob, Leber, Markus, Lee, Heon-Jeong, Lee, Phil H., Levy, Shawn E., Lewis, Catrin, Liao, Calwing, Lucae, Susanne, Lundberg, Martin, MacIntyre, Donald J., Magnusson, Sigurdur H., Maier, Wolfgang, Maihofer, Adam, Malaspina, Dolores, Maratou, Eirini, Martinsson, Lina, Mattheisen, Manuel, McCarroll, Steven A., McGregor, Nathaniel W., McGuffin, Peter, McKay, James D., Medeiros, Helena, Medland, Sarah E., Millischer, Vincent, Montgomery, Grant W., Moran, Jennifer L., Morris, Derek W., Mühleisen, Thomas W., O’Brien, Niamh, O’Donovan, Claire, Olde Loohuis, Loes M., Oruc, Lilijana, Papiol, Sergi, Pardiñas, Antonio F., Perry, Amy, Pfennig, Andrea, Porichi, Evgenia, Potash, James B., Quested, Digby, Raj, Towfique, Rapaport, Mark H., DePaulo, J. Raymond, Regeer, Eline J., Rice, John P., Rivas, Fabio, Rivera, Margarita, Roth, Julian, Roussos, Panos, Ruderfer, Douglas M., Sánchez-Mora, Cristina, Schulte, Eva C., Senner, Fanny, Sharp, Sally, Shilling, Paul D., Sigurdsson, Engilbert, Sirignano, Lea, Slaney, Claire, Smeland, Olav B., Smith, Daniel J., Sobell, Janet L., Søholm Hansen, Christine, Soler Artigas, Maria, Spijker, Anne T., Stein, Dan J., Strauss, John S., Świątkowska, Beata, Terao, Chikashi, Thorgeirsson, Thorgeir E., Toma, Claudio, Tooney, Paul, Tsermpini, Evangelia-Eirini, Vawter, Marquis P., Vedder, Helmut, Walters, James T. R., Witt, Stephanie H., Xi, Simon, Xu, Wei, Yang, Jessica Mei Kay, Young, Allan H., Young, Hannah, Zandi, Peter P., Zhou, Hang, Zillich, Lea, Adolfsson, Rolf, Agartz, Ingrid, Alda, Martin, Alfredsson, Lars, Babadjanova, Gulja, Backlund, Lena, Baune, Bernhard T., Bellivier, Frank, Bengesser, Susanne, Berrettini, Wade H., Blackwood, Douglas H. R., Boehnke, Michael, Børglum, Anders D., Breen, Gerome, Carr, Vaughan J., Catts, Stanley, Corvin, Aiden, Craddock, Nicholas, Dannlowski, Udo, Dikeos, Dimitris, Esko, Tõnu, Etain, Bruno, Ferentinos, Panagiotis, Frye, Mark, Fullerton, Janice M., Gawlik, Micha, Gershon, Elliot S., Goes, Fernando S., Green, Melissa J., Grigoroiu-Serbanescu, Maria, Hauser, Joanna, Henskens, Frans, Hillert, Jan, Hong, Kyung Sue, Hougaard, David M., Hultman, Christina M., Hveem, Kristian, Iwata, Nakao, Jablensky, Assen V., Jones, Ian, Jones, Lisa A., Kahn, René S., Kelsoe, John R., Kirov, George, Landén, Mikael, Leboyer, Marion, Lewis, Cathryn M., Li, Qingqin S., Lissowska, Jolanta, Lochner, Christine, Loughland, Carmel, Martin, Nicholas G., Mathews, Carol A., Mayoral, Fermin, McElroy, Susan L., McIntosh, Andrew M., McMahon, Francis J., Melle, Ingrid, Michie, Patricia, Milani, Lili, Mitchell, Philip B., Morken, Gunnar, Mors, Ole, Mortensen, Preben Bo, Mowry, Bryan, Müller-Myhsok, Bertram, Myers, Richard M., Neale, Benjamin M., Nievergelt, Caroline M., Nordentoft, Merete, Nöthen, Markus M., O’Donovan, Michael C., Oedegaard, Ketil J., Olsson, Tomas, Owen, Michael J., Paciga, Sara A., Pantelis, Chris, Pato, Carlos, Pato, Michele T., Patrinos, George P., Perlis, Roy H., Posthuma, Danielle, Ramos-Quiroga, Josep Antoni, Reif, Andreas, Reininghaus, Eva Z., Ribasés, Marta, Rietschel, Marcella, Ripke, Stephan, Rouleau, Guy A., Saito, Takeo, Schall, Ulrich, Schalling, Martin, Schofield, Peter R., Schulze, Thomas G., Scott, Laura J., Scott, Rodney J., Serretti, Alessandro, Shannon Weickert, Cynthia, Smoller, Jordan W., Stefansson, Hreinn, Stefansson, Kari, Stordal, Eystein, Streit, Fabian, Sullivan, Patrick F., Turecki, Gustavo, Vaaler, Arne E., Vieta, Eduard, Vincent, John B., Waldman, Irwin D., Weickert, Thomas W., Werge, Thomas, Wray, Naomi R., Zwart, John-Anker, Biernacka, Joanna M., Nurnberger, John I., Cichon, Sven, Edenberg, Howard J., Stahl, Eli A., McQuillin, Andrew, Di Florio, Arianna, Ophoff, Roel A., and Andreassen, Ole A.

Published

2021

50. The Pharmacogenomics of Bipolar Disorder study (PGBD): identification of genes for lithium response in a prospective sample

Author

Oedegaard, Ketil J, Alda, Martin, Anand, Anit, Andreassen, Ole A, Balaraman, Yokesh, Berrettini, Wade H, Bhattacharjee, Abesh, Brennand, Kristen J, Burdick, Katherine E, Calabrese, Joseph R, Calkin, Cynthia V, Claasen, Ana, Coryell, William H, Craig, David, DeModena, Anna, Frye, Mark, Gage, Fred H, Gao, Keming, Garnham, Julie, Gershon, Elliot, Jakobsen, Petter, Leckband, Susan G, McCarthy, Michael J, McInnis, Melvin G, Maihofer, Adam X, Mertens, Jerome, Morken, Gunnar, Nievergelt, Caroline M, Nurnberger, John, Pham, Son, Schoeyen, Helle, Shekhtman, Tatyana, Shilling, Paul D, Szelinger, Szabolcs, Tarwater, Bruce, Yao, Jun, Zandi, Peter P, and Kelsoe, John R

Subjects

Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Health Sciences, Brain Disorders, Human Genome, Genetics, Depression, Mental Health, Clinical Research, Prevention, Behavioral and Social Science, Detection, screening and diagnosis, Evaluation of treatments and therapeutic interventions, 4.2 Evaluation of markers and technologies, 6.1 Pharmaceuticals, Mental health, Aged, Antidepressive Agents, Bipolar Disorder, Diagnostic and Statistical Manual of Mental Disorders, Female, Follow-Up Studies, Genome-Wide Association Study, Humans, Lithium Compounds, Male, Middle Aged, Pharmacogenetics, Prospective Studies, Retrospective Studies, Secondary Prevention, Valproic Acid, Bipolar disorder, Lithium, Mood stabilizer, GWAS, Prospective trial, Personalized medicine, Precision medicine, Clinical Sciences, Public Health and Health Services, Psychology, Psychiatry, Clinical sciences, Epidemiology, Clinical and health psychology

Abstract

BackgroundBipolar disorder is a serious and common psychiatric disorder characterized by manic and depressive mood switches and a relapsing and remitting course. The cornerstone of clinical management is stabilization and prophylaxis using mood-stabilizing medications to reduce both manic and depressive symptoms. Lithium remains the gold standard of treatment with the strongest data for both efficacy and suicide prevention. However, many patients do not respond to this medication, and clinically there is a great need for tools to aid the clinician in selecting the correct treatment. Large genome wide association studies (GWAS) investigating retrospectively the effect of lithium response are in the pipeline; however, few large prospective studies on genetic predictors to of lithium response have yet been conducted. The purpose of this project is to identify genes that are associated with lithium response in a large prospective cohort of bipolar patients and to better understand the mechanism of action of lithium and the variation in the genome that influences clinical response.Methods/designThis study is an 11-site prospective non-randomized open trial of lithium designed to ascertain a cohort of 700 subjects with bipolar I disorder who experience protocol-defined relapse prevention as a result of treatment with lithium monotherapy. All patients will be diagnosed using the Diagnostic Interview for Genetic Studies (DIGS) and will then enter a 2-year follow-up period on lithium monotherapy if and when they exhibit a score of 1 (normal, not ill), 2 (minimally ill) or 3 (mildly ill) on the Clinical Global Impressions of Severity Scale for Bipolar Disorder (CGI-S-BP Overall Bipolar Illness) for 4 of the 5 preceding weeks. Lithium will be titrated as clinically appropriate, not to exceed serum levels of 1.2 mEq/L. The sample will be evaluated longitudinally using a wide range of clinical scales, cognitive assessments and laboratory tests. On relapse, patients will be discontinued or crossed-over to treatment with valproic acid (VPA) or treatment as usual (TAU). Relapse is defined as a DSM-IV manic, major depressive or mixed episode or if the treating physician decides a change in medication is clinically necessary. The sample will be genotyped for GWAS. The outcome for lithium response will be analyzed as a time to event, where the event is defined as clinical relapse, using a Cox Proportional Hazards model. Positive single nucleotide polymorphisms (SNPs) from past genetic retrospective studies of lithium response, the Consortium on Lithium Genetics (ConLiGen), will be tested in this prospective study sample; a meta-analysis of these samples will then be performed. Finally, neurons will be derived from pluripotent stem cells from lithium responders and non-responders and tested in vivo for response to lithium by gene expression studies. SNPs in genes identified in these cellular studies will also be tested for association to response.DiscussionLithium is an extraordinarily important therapeutic drug in the clinical management of patients suffering from bipolar disorder. However, a significant proportion of patients, 30-40 %, fail to respond, and there is currently no method to identify the good lithium responders before initiation of treatment. Converging evidence suggests that genetic factors play a strong role in the variation of response to lithium, but only a few genes have been tested and the samples have largely been retrospective or quite small. The current study will collect an entirely unique sample of 700 patients with bipolar disorder to be stabilized on lithium monotherapy and followed for up to 2 years. This study will produce useful information to improve the understanding of the mechanism of action of lithium and will add to the development of a method to predict individual response to lithium, thereby accelerating recovery and reducing suffering and cost.Trial registrationClinicalTrials.gov Identifier: NCT01272531 Registered: January 6, 2011.

Published

2016