16 results on '"Dedert, Eric A."'
Search Results
2. Multimodal smoking cessation treatment combining repetitive transcranial magnetic stimulation, cognitive behavioral therapy, and nicotine replacement in veterans with posttraumatic stress disorder: A feasibility randomized controlled trial protocol.
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Young, Jonathan R., Polick, Carri S., Michael, Andrew M., Dannhauer, Moritz, Galla, Jeffrey T., Evans, Mariah K., Troutman, Addison, Kirby, Angela C., Dennis, Michelle F., Papanikolas, Claire W., Deng, Zhi-De, Moore, Scott D., Dedert, Eric A., Addicott, Merideth A., Appelbaum, Lawrence G., and Beckham, Jean C.
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NICOTINE replacement therapy ,COGNITIVE therapy ,SMOKING cessation ,POST-traumatic stress disorder ,TOBACCO use ,TRANSCRANIAL magnetic stimulation - Abstract
Tobacco-related deaths remain the leading cause of preventable death in the United States. Veterans suffering from posttraumatic stress disorder (PTSD)—about 11% of those receiving care from the Department of Veterans Affairs (VA)—have triple the risk of developing tobacco use disorder (TUD). The most efficacious strategies being used at the VA for smoking cessation only result in a 23% abstinence rate, and veterans with PTSD only achieve a 4.5% abstinence rate. Therefore, there is a critical need to develop more effective treatments for smoking cessation. Recent studies suggest the insula is integrally involved in the neurocircuitry of TUD. Thus, we propose a feasibility phase II randomized controlled trial (RCT) to study a form of repetitive transcranial magnetic stimulation (rTMS) called intermittent theta burst stimulation (iTBS). iTBS has the advantage of allowing for a patterned form of stimulation delivery that we will administer at 90% of the subject's resting motor threshold (rMT) applied over a region in the right post-central gyrus most functionally connected to the right posterior insula. We hypothesize that by increasing functional connectivity between the right post-central gyrus and the right posterior insula, withdrawal symptoms and short-term smoking cessation outcomes will improve. Fifty eligible veterans with comorbid TUD and PTSD will be randomly assigned to active-iTBS + cognitive behavioral therapy (CBT) + nicotine replacement therapy (NRT) (n = 25) or sham-iTBS + CBT + NRT (n = 25). The primary outcome, feasibility, will be determined by achieving a recruitment of 50 participants and retention rate of 80%. The success of iTBS will be evaluated through self-reported nicotine use, cravings, withdrawal symptoms, and abstinence following quit date (confirmed by bioverification) along with evaluation for target engagement through neuroimaging changes, specifically connectivity differences between the insula and other regions of interest. [ABSTRACT FROM AUTHOR]
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- 2024
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3. Posttraumatic stress disorder, trauma, and accelerated biological aging among post-9/11 veterans.
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Bourassa, Kyle J., Garrett, Melanie E., Caspi, Avshalom, Dennis, Michelle, Hall, Katherine S., Moffitt, Terrie E., Taylor, Gregory A., VA Mid Atlantic MIRECC Workgroup, Beckham, Jean C., Calhoun, Patrick S., Dedert, Eric, Elbogen, Eric B., Hurley, Robin A., Kilts, Jason D., Kimbrel, Nathan A., Kirby, Angela, Martindale, Sarah L., Marx, Christine E., McDonald, Scott D., and Moore, Scott D.
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- 2024
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4. Telehealth Interventions Designed for Women: an Evidence Map
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Goldstein, Karen M., Zullig, Leah L., Dedert, Eric A., Alishahi Tabriz, Amir, Brearly, Timothy W., Raitz, Giselle, Sata, Suchita Shah, Whited, John D., Bosworth, Hayden B., Gordon, Adelaide M., Nagi, Avishek, Williams, Jr, John W., and Gierisch, Jennifer M.
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- 2018
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5. Validation of Veterans Affairs Electronic Medical Record Smoking Data Among Iraq- and Afghanistan-Era Veterans
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Calhoun, Patrick S., Wilson, Sarah M., Hertzberg, Jeffrey S., Kirby, Angela C., McDonald, Scott D., Dennis, Paul A., Bastian, Lori A., Dedert, Eric A., The VA Mid-Atlantic MIRECC Workgroup, and Beckham, Jean C.
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- 2017
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6. Epigenome-wide meta-analysis of PTSD across 10 military and civilian cohorts identifies methylation changes in AHRR
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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 P.F., Stein, Murray B., Ursano, Robert J., Vermetten, Eric, Vinkers, Christiaan H., Wang, Lin, Youssef, Nagy A., Marx, Christine, Grant, Gerry, Stein, Murray, Qin, Xue Jun, Jain, Sonia, McAllister, Thomas W., Zafonte, Ross, Lang, Ariel, Coimbra, Raul, Andaluz, Norberto, Shutter, Lori, George, Mark S., Brancu, Mira, Calhoun, Patrick S., Dedert, Eric, Elbogen, Eric B., Fairbank, John A., Hurley, Robin A., Kilts, Jason D., Kirby, Angela, Marx, Christine E., McDonald, Scott D., Moore, Scott D., Morey, Rajendra A., Naylor, Jennifer C., Rowland, Jared A., Swinkels, Cindy, Szabo, Steven T., Taber, Katherine H., Tupler, Larry A., Van Voorhees, Elizabeth E., Yoash-Gantz, Ruth E., Basu, Archana, Brick, Leslie A., Dalvie, Shareefa, Daskalakis, Nikolaos P., Ensink, Judith B.M., Hemmings, Sian M.J., Herringa, Ryan, Ikiyo, Sylvanus, Koen, Nastassja, Montalvo-Ortiz, Janitza, Nispeling, Danny, Pfeiffer, John, Schijven, Dick, Seedat, Soraya, Shinozaki, Gen, Sumner, Jennifer A., Swart, Patricia, Tyrka, Audrey, Van Zuiden, Mirjam, Wani, Agaz, Wolf, Erika J., Zannas, Anthony, Uddin, Monica, Nievergelt, Caroline M., ACS - Pulmonary hypertension & thrombosis, Graduate School, Adult Psychiatry, ARD - Amsterdam Reproduction and Development, Child Psychiatry, APH - Mental Health, ANS - Mood, Anxiety, Psychosis, Stress & Sleep, APH - Global Health, Psychiatry, Amsterdam Neuroscience - Mood, Anxiety, Psychosis, Stress & Sleep, Anatomy and neurosciences, MUMC+: MA Psychiatrie (3), Psychiatrie & Neuropsychologie, and RS: MHeNs - R3 - Neuroscience
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Male ,0301 basic medicine ,Oncology ,VA Mid-Atlantic MIRECC Workgroup ,General Physics and Astronomy ,medicine.disease_cause ,IMMUNOLOGY ,Epigenesis, Genetic ,Stress Disorders, Post-Traumatic ,Cohort Studies ,Epigenome ,chemistry.chemical_compound ,POSTTRAUMATIC-STRESS-DISORDER ,0302 clinical medicine ,Basic Helix-Loop-Helix Transcription Factors ,Medicine ,DNA METHYLATION ,Kynurenine ,Stress Disorders ,Multidisciplinary ,ASSOCIATION ,Methylation ,Post-Traumatic Stress Disorder (PTSD) ,Anxiety Disorders ,Military Personnel ,Mental Health ,CpG site ,Meta-analysis ,DNA methylation ,Female ,ARYL-HYDROCARBON RECEPTOR ,medicine.medical_specialty ,Science ,behavioral disciplines and activities ,Article ,General Biochemistry, Genetics and Molecular Biology ,03 medical and health sciences ,AGE ,Genetic ,Clinical Research ,Internal medicine ,mental disorders ,Genetics ,Humans ,EXPOSURE ,Epigenetics ,Post-traumatic stress disorder ,PGC PTSD Epigenetics Workgroup ,business.industry ,PROFILES ,General Chemistry ,DNA Methylation ,Immune dysregulation ,Repressor Proteins ,030104 developmental biology ,chemistry ,Case-Control Studies ,Post-Traumatic ,Wounds and Injuries ,Epigenetics analysis ,business ,030217 neurology & neurosurgery ,INTRuST Clinical Consortium ,Epigenesis - 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., PTSD has been associated with DNA methylation of specific loci in the genome, but studies have been limited by small sample sizes. Here, the authors perform a meta-analysis of DNA methylation data from 10 different cohorts and identify CpGs in AHRR that are associated with PTSD.
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- 2020
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7. Self- and Other-Directed Violence as Outcomes of Deployment-Based Military Sexual Assault in Iraq/Afghanistan-era Veteran Men and Women
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Wilson, Laura C., Newins, Amie R., Wilson, Sarah M., Elbogen, Eric B., Dedert, Eric A., Calhoun, Patrick S., Beckham, Jean C., and Kimbrel, Nathan A.
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stomatognathic system ,parasitic diseases ,mental disorders ,Article ,nervous system diseases - Abstract
Although military sexual assault (MSA) has been well-established as a risk factor for psychopathology (e.g., PTSD, depression), little research has examined the association between MSA and self- and other-directed violence. Furthermore, there has been a growing empirical focus on potential gender differences in the effects of MSA, but few of these studies have examined gender differences in self- and other-directed violence. In a sample of 1571 Iraq/Afghanistan-era veterans (21.0% women), we examined the effect of MSA on difficulty controlling violent behavior and attempting suicide among veteran men and women, above and beyond the influence of childhood sexual abuse, combat trauma, PTSD, and major depressive disorder. Results of a logistic regression revealed that MSA increased risk of attempting suicide and difficulty controlling violence among women but not men. Thus, the results suggest that MSA may be a risk factor for both types of violence in women. Furthermore, because PTSD was associated with both types of violence in both men and women, MSA may also confer risk of violence via PTSD.
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- 2020
8. Threat-induced anxiety during goal pursuit disrupts amygdala-prefrontal cortex connectivity in posttraumatic stress disorder
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Sun, Delin, Gold, Andrea L., Swanson, Chelsea A., Haswell, Courtney C., Brown, Vanessa M., Stjepanovic, Daniel, LaBar, Kevin S., Morey, Rajendra A., Beckham, Jean C., Brancu, Mira, Calhoun, Patrick S., Dedert, Eric, Elbogen, Eric B., Green, Kimberly T., Kimbrel, Nathan, Kirby, Angela, McCarthy, Gregory, Moore, Scott D., Runnals, Jennifer J., Swinkels, Cindy, Tupler, Larry A., Van Voorhees, Elizabeth E., Weiner, Richard D., and Psychology
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0301 basic medicine ,Ventromedial prefrontal cortex ,Prefrontal Cortex ,Anxiety ,behavioral disciplines and activities ,Amygdala ,Article ,lcsh:RC321-571 ,Task (project management) ,Stress Disorders, Post-Traumatic ,03 medical and health sciences ,Cellular and Molecular Neuroscience ,0302 clinical medicine ,medicine ,Humans ,Prefrontal cortex ,lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry ,Biological Psychiatry ,030304 developmental biology ,0303 health sciences ,Brain Mapping ,medicine.diagnostic_test ,Psychophysiological Interaction ,Goal pursuit ,Magnetic Resonance Imaging ,Psychiatry and Mental health ,Posttraumatic stress ,030104 developmental biology ,medicine.anatomical_structure ,medicine.symptom ,Psychiatric disorders ,Psychology ,Functional magnetic resonance imaging ,Goals ,psychological phenomena and processes ,030217 neurology & neurosurgery ,Cognitive psychology ,Neuroscience ,Clinical psychology - Abstract
To investigate how unpredictable threat during goal pursuit impacts fronto-limbic activity and functional connectivity in posttraumatic stress disorder (PTSD), we compared military veterans with PTSD (n = 25) vs. trauma-exposed control (n = 25). Participants underwent functional magnetic resonance imaging (fMRI) while engaged in a computerized chase-and-capture game task that involved optimizing monetary rewards obtained from capturing virtual prey while simultaneously avoiding capture by virtual predators. The game was played under two alternating contexts-one involving exposure to unpredictable task-irrelevant threat from randomly occurring electrical shocks, and a nonthreat control condition. Activation in and functional connectivity between the amygdala and ventromedial prefrontal cortex (vmPFC) was tested across threat and nonthreat task contexts with generalized psychophysiological interaction (gPPI) analyses. PTSD patients reported higher anxiety than controls across contexts. Better task performance represented by successfully avoiding capture by predators under threat compared with nonthreat contexts was associated with stronger left amygdala-vmPFC functional connectivity in controls and greater vmPFC activation in PTSD patients. PTSD symptom severity was negatively correlated with vmPFC activation in trauma-exposed controls and with right amygdala-vmPFC functional connectivity across all participants in the threat relative to nonthreat contexts. The findings showed that veterans with PTSD have disrupted amygdala-vmPFC functional connectivity and greater localized vmPFC processing under threat modulation of goal-directed behavior, specifically related to successfully avoiding loss of monetary rewards. In contrast, trauma survivors without PTSD relied on stronger threat-modulated left amygdala-vmPFC functional connectivity during goal-directed behavior, which may represent a resilience-related functional adaptation. Department of Veterans Affairs' (VA) Mid-Atlantic Mental Illness Research, Education and Clinical Center (MIRECC) of the VA Office of Mental Health Services; Office of Research and Development (ORD) [5I01CX000748-01, 5I01CX000120-02]; National Institute for Neurological Disorders and StrokeUnited States Department of Health & Human ServicesNational Institutes of Health (NIH) - USANIH National Institute of Neurological Disorders & Stroke (NINDS) [R01NS086885-01A1]; VA Career Development Awards, from the Clinical Science Research and Development (CSRD) Service [IK2CX000525, IK2CX000718]; VA Career Development Award from the Rehabilitation Research and Development (RRD) [5IK2RX001298]; VA Research Career Scientist Award [11S-RCS-009]; Intramural Research Program at the National Institute of Mental HealthUnited States Department of Health & Human ServicesNational Institutes of Health (NIH) - USANIH National Institute of Mental Health (NIMH); Office of the Director, National Institutes of HealthUnited States Department of Health & Human ServicesNational Institutes of Health (NIH) - USA [S10 OD 021480]; Mid-Atlantic Healthcare Network This project was supported in part by the Department of Veterans Affairs' (VA) Mid-Atlantic Mental Illness Research, Education and Clinical Center (MIRECC) of the VA Office of Mental Health Services, the Mid-Atlantic Healthcare Network, and the Office of Research and Development (ORD; 5I01CX000748-01, 5I01CX000120-02). Additional financial support was provided by the National Institute for Neurological Disorders and Stroke (R01NS086885-01A1; R.A.M.). Work Group Members: Drs Kimbrel and Dedert were supported by VA Career Development Awards #IK2CX000525 and IK2CX000718, respectively, from the Clinical Science Research and Development (CSR&D) Service. Dr Van Voorhees was supported by a VA Career Development Award (#5IK2RX001298) from the Rehabilitation Research and Development (RR&D). Dr Beckham was supported by a VA Research Career Scientist Award (#11S-RCS-009). A.L.G. was supported by the Intramural Research Program at the National Institute of Mental Health. Research reported in this publication was supported by the Office of the Director, National Institutes of Health under Award Number S10 OD 021480.
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- 2020
9. Threat-induced anxiety during goal pursuit disrupts amygdala-prefrontal cortex connectivity in posttraumatic stress disorder
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Psychology, Sun, Delin, Gold, Andrea L., Swanson, Chelsea A., Haswell, Courtney C., Brown, Vanessa M., Stjepanovic, Daniel, LaBar, Kevin S., Morey, Rajendra A., Beckham, Jean C., Brancu, Mira, Calhoun, Patrick S., Dedert, Eric, Elbogen, Eric B., Green, Kimberly T., Kimbrel, Nathan, Kirby, Angela, McCarthy, Gregory, Moore, Scott D., Runnals, Jennifer J., Swinkels, Cindy, Tupler, Larry A., Van Voorhees, Elizabeth E., Weiner, Richard D., Psychology, Sun, Delin, Gold, Andrea L., Swanson, Chelsea A., Haswell, Courtney C., Brown, Vanessa M., Stjepanovic, Daniel, LaBar, Kevin S., Morey, Rajendra A., Beckham, Jean C., Brancu, Mira, Calhoun, Patrick S., Dedert, Eric, Elbogen, Eric B., Green, Kimberly T., Kimbrel, Nathan, Kirby, Angela, McCarthy, Gregory, Moore, Scott D., Runnals, Jennifer J., Swinkels, Cindy, Tupler, Larry A., Van Voorhees, Elizabeth E., and Weiner, Richard D.
- Abstract
To investigate how unpredictable threat during goal pursuit impacts fronto-limbic activity and functional connectivity in posttraumatic stress disorder (PTSD), we compared military veterans with PTSD (n = 25) vs. trauma-exposed control (n = 25). Participants underwent functional magnetic resonance imaging (fMRI) while engaged in a computerized chase-and-capture game task that involved optimizing monetary rewards obtained from capturing virtual prey while simultaneously avoiding capture by virtual predators. The game was played under two alternating contexts-one involving exposure to unpredictable task-irrelevant threat from randomly occurring electrical shocks, and a nonthreat control condition. Activation in and functional connectivity between the amygdala and ventromedial prefrontal cortex (vmPFC) was tested across threat and nonthreat task contexts with generalized psychophysiological interaction (gPPI) analyses. PTSD patients reported higher anxiety than controls across contexts. Better task performance represented by successfully avoiding capture by predators under threat compared with nonthreat contexts was associated with stronger left amygdala-vmPFC functional connectivity in controls and greater vmPFC activation in PTSD patients. PTSD symptom severity was negatively correlated with vmPFC activation in trauma-exposed controls and with right amygdala-vmPFC functional connectivity across all participants in the threat relative to nonthreat contexts. The findings showed that veterans with PTSD have disrupted amygdala-vmPFC functional connectivity and greater localized vmPFC processing under threat modulation of goal-directed behavior, specifically related to successfully avoiding loss of monetary rewards. In contrast, trauma survivors without PTSD relied on stronger threat-modulated left amygdala-vmPFC functional connectivity during goal-directed behavior, which may represent a resilience-related functional adaptation.
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- 2020
10. Pilot Cohorts for Development of Concurrent Mobile Treatment for Alcohol and Tobacco Use Disorders
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Medenblik, Alyssa M, primary, Calhoun, Patrick S, additional, Maisto, Stephen A, additional, Kivlahan, Daniel R, additional, Moore, Scott D, additional, Beckham, Jean C, additional, Wilson, Sarah M, additional, Blalock, Dan V, additional, and Dedert, Eric A, additional
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- 2021
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11. Gene Expression Analysis in Three Posttraumatic Stress Disorder Cohorts Implicates Inflammation and Innate Immunity Pathways and Uncovers Shared Genetic Risk With Major Depressive Disorder.
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Garrett, Melanie E., Qin, Xue Jun, Mehta, Divya, Dennis, Michelle F., Marx, Christine E., Grant, Gerald A., Stein, Murray B., Kimbrel, Nathan A., Beckham, Jean C., Hauser, Michael A., Ashley-Koch, Allison E., Brancu, Mira, Calhoun, Patrick S., Dedert, Eric, Elbogen, Eric B., Fairbank, John A., Hurley, Robin A., Kilts, Jason D., Kirby, Angela, and Martindale, Sara
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POST-traumatic stress disorder ,PSYCHIATRIC research ,GENE expression ,NATURAL immunity ,GENE regulatory networks ,GENE ontology ,BIOLOGICAL variation - Abstract
Posttraumatic stress disorder (PTSD) is a complex psychiatric disorder that can develop following exposure to traumatic events. The Psychiatric Genomics Consortium PTSD group (PGC-PTSD) has collected over 20,000 multi-ethnic PTSD cases and controls and has identified both genetic and epigenetic factors associated with PTSD risk. To further investigate biological correlates of PTSD risk, we examined three PGC-PTSD cohorts comprising 977 subjects to identify differentially expressed genes among PTSD cases and controls. Whole blood gene expression was quantified with the HumanHT-12 v4 Expression BeadChip for 726 OEF/OIF veterans from the Veterans Affairs (VA) Mental Illness Research Education and Clinical Center (MIRECC), 155 samples from the Injury and Traumatic Stress (INTRuST) Clinical Consortium, and 96 Australian Vietnam War veterans. Differential gene expression analysis was performed in each cohort separately followed by meta-analysis. In the largest cohort, we performed co-expression analysis to identify modules of genes that are associated with PTSD and MDD. We then conducted expression quantitative trait loci (eQTL) analysis and assessed the presence of eQTL interactions involving PTSD and major depressive disorder (MDD). Finally, we utilized PTSD and MDD GWAS summary statistics to identify regions that colocalize with eQTLs. Although not surpassing correction for multiple testing, the most differentially expressed genes in meta-analysis were interleukin-1 beta (IL1B), a pro-inflammatory cytokine previously associated with PTSD, and integrin-linked kinase (ILK), which is highly expressed in brain and can rescue dysregulated hippocampal neurogenesis and memory deficits. Pathway analysis revealed enrichment of toll-like receptor (TLR) and interleukin-1 receptor genes, which are integral to cellular innate immune response. Co-expression analysis identified four modules of genes associated with PTSD, two of which are also associated with MDD, demonstrating common biological pathways underlying the two conditions. Lastly, we identified four genes (UBA7 , HLA-F , HSPA1B , and RERE) with high probability of a shared causal eQTL variant with PTSD and/or MDD GWAS variants, thereby providing a potential mechanism by which the GWAS variant contributes to disease risk. In summary, we provide additional evidence for genes and pathways previously reported and identified plausible novel candidates for PTSD. These data provide further insight into genetic factors and pathways involved in PTSD, as well as potential regions of pleiotropy between PTSD and MDD. [ABSTRACT FROM AUTHOR]
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- 2021
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12. Examining the Crux of Autonomic Dysfunction in PTSD: Whether Chronic or Situational Distress Underlies Elevated Heart Rate and Attenuated Heart-Rate Variability
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Dennis, Paul A., Dedert, Eric A., Van Voorhees, Elizabeth E., Watkins, Lana L., Hayano, J., Calhoun, Patrick S., Sherwood, Andrew, Dennis, Michelle F., and Beckham, Jean C.
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Adult ,Stress Disorders, Post-Traumatic ,Young Adult ,Cross-Sectional Studies ,Adolescent ,Autonomic Nervous System Diseases ,Heart Rate ,Ecological Momentary Assessment ,Electrocardiography, Ambulatory ,Humans ,Severity of Illness Index ,Article ,Stress, Psychological - Abstract
Posttraumatic stress disorder (PTSD) has been linked to elevated heart rate (HR) and reduced heart rate variability (HRV) in cross-sectional research. Using ecological momentary assessment and minute-to-minute HRV/HR monitoring, we examined whether cross-sectional associations between PTSD symptom severity and HRV/HR were due to overall elevations in distress levels or to attenuated autonomic regulation during episodes of acute distress.Two hundred nineteen young adults (18-39 years old), 99 with PTSD, underwent 1 day of Holter monitoring and concurrently reported distress levels via ecological momentary assessment. Using multilevel modeling, we examined the associations between momentary distress and the 5-minute means for low-frequency (LF) and high-frequency (HF) HRV and HR immediately following distress ratings, and whether PTSD symptom severity moderated these associations.Compared with the controls, participants with PTSD recorded higher ambulatory distress (mean [standard deviation] = 1.7 [0.5] versus 1.2 [0.3], p.001) and HR (87.2 [11.8] versus 82.9 [12.6] beats/min, p = .011), and lower ambulatory LF HRV (36.9 [14.7] versus 43.7 [16.9 ms, p = .002) and HF HRV (22.6 [12.3] versus 26.4 [14.6] milliseconds, p = .043). Overall distress level was not predictive of HR or HRV (p values.27). However, baseline PTSD symptom severity was associated with elevated HR (t(1257) = 2.76, p = .006) and attenuated LF (t(1257) = -3.86, p.001) and HF (t(1257) = -2.62, p = .009) in response to acute momentary distress.Results suggest that PTSD is associated with heightened arousal after situational distress and could explain prior findings associating PTSD with HR/HRV. Implications for treatment and cardiovascular risk are discussed.
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- 2016
13. Posttraumatic Stress Disorder Symptom Network Analysis in U.S. Military Veterans: Examining the Impact of Combat Exposure.
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Phillips, Rachel D., Wilson, Sarah M., Sun, Delin, Morey, Rajendra, Van Voorhees, Elizabeth, Marx, Christine E., Calhoun, Patrick S., Fairbank, John A., Tupler, Larry A., Beckham, Jean C., Brancu, Mira, Swinkels, Cindy M., McDonald, Scott D., Yoash-Gantz, Ruth, Taber, Katherine H., Hurley, Robin, Dedert, Eric A., Elbogen, Eric B., Kilts, Jason, and Kirby, Angela C.
- Abstract
Recent work inspired by graph theory has begun to conceptualize mental disorders as networks of interacting symptoms. Posttraumatic stress disorder (PTSD) symptom networks have been investigated in clinical samples meeting full diagnostic criteria, including military veterans, natural disaster survivors, civilian survivors of war, and child sexual abuse survivors. Despite reliable associations across reported networks, more work is needed to compare central symptoms across trauma types. Additionally, individuals without a diagnosis who still experience symptoms, also referred to as subthreshold cases, have not been explored with network analysis in veterans. A sample of 1,050 Iraq/Afghanistan-era U.S. military veterans (851 males, mean age = 36.3, SD = 9.53) meeting current full-criteria PTSD (n = 912) and subthreshold PTSD (n = 138) were assessed with the Structured Clinical Interview for DSM-IV Disorders (SCID). Combat Exposure Scale (CES) scores were used to group the sample meeting full-criteria into high (n = 639) and low (n = 273) combat exposure subgroups. Networks were estimated using regularized partial correlation models in the R-package qgraph , and robustness tests were performed with bootnet. Frequently co-occurring symptom pairs (strong network connections) emerged between two avoidance symptoms, hypervigilance and startle response, loss of interest and detachment, as well as, detachment and restricted affect. These associations replicate findings reported across PTSD trauma types. A symptom network analysis of PTSD in a veteran population found significantly greater overall connectivity in the full-criteria PTSD group as compared to the subthreshold PTSD group. Additionally, novel findings indicate that the association between intrusive thoughts and irritability is a feature of the symptom network of veterans with high levels of combat exposure. Mean node predictability is high for PTSD symptom networks, averaging 51.5% shared variance. With the tools described here and by others, researchers can help refine diagnostic criteria for PTSD, develop more accurate measures for assessing PTSD, and eventually inform therapies that target symptoms with strong network connections to interrupt interconnected symptom complexes and promote functional recovery. [ABSTRACT FROM AUTHOR]
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- 2018
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14. Brain structural covariance network Topology in remitted Posttraumatic stress Disorder.
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Sun, Delin, Davis, Sarah L., Haswell, Courtney C., Swanson, Chelsea A., LaBar, Kevin S., Fairbank, John A., Morey, Rajendra A., Beckham, Jean C., Brancu, Mira, Calhoun, Patrick S., Dedert, Eric, Elbogen, Eric B., Green, Kimberly T., Hurley, Robin A., Kilts, Jason D., Kimbrel, Nathan, Kirby, Angela, Marx, Christine E., McCarthy, Gregory, and McDonald, Scott D.
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POST-traumatic stress disorder ,BRAIN anatomy - Abstract
Posttraumatic stress disorder (PTSD) is a prevalent, chronic disorder with high psychiatric morbidity; however, a substantial portion of affected individuals experience remission after onset. Alterations in brain network topology derived from cortical thickness correlations are associated with PTSD, but the effects of remitted symptoms on network topology remain essentially unexplored. In this cross-sectional study, US military veterans (N = 317) were partitioned into three diagnostic groups, current PTSD (CURR-PTSD, N = 101), remitted PTSD with lifetime but no current PTSD (REMIT-PTSD, N = 35), and trauma-exposed controls (CONTROL, n = 181). Cortical thickness was assessed for 148 cortical regions (nodes) and suprathreshold interregional partial correlations across subjects constituted connections (edges) in each group. Four centrality measures were compared with characterize between-group differences. The REMIT-PTSD and CONTROL groups showed greater centrality in left frontal pole than the CURR-PTSD group. The REMIT-PTSD group showed greater centrality in right subcallosal gyrus than the other two groups. Both REMIT-PTSD and CURR-PTSD groups showed greater centrality in right superior frontal sulcus than CONTROL group. The centrality in right subcallosal gyrus, left frontal pole, and right superior frontal sulcus may play a role in remission, current symptoms, and PTSD history, respectively. The network centrality changes in critical brain regions and structural networks are associated with remitted PTSD, which typically coincides with enhanced functional behaviors, better emotion regulation, and improved cognitive processing. These brain regions and associated networks may be candidates for developing novel therapies for PTSD. Longitudinal work is needed to characterize vulnerability to chronic PTSD, and resilience to unremitting PTSD. [ABSTRACT FROM AUTHOR]
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- 2018
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15. The Effect of Draft DSM-5 Criteria on Posttraumatic Stress Disorder Prevalence
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Calhoun, Patrick S., Hertzberg, Jeffrey S., Kirby, Angela C., Dennis, Michelle F., Hair, Lauren P., Dedert, Eric A., and Beckham, Jean C.
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Adult ,Diagnostic and Statistical Manual of Mental Disorders ,Male ,Stress Disorders, Post-Traumatic ,Area Under Curve ,Prevalence ,Humans ,Female ,Sensitivity and Specificity ,Article ,Southeastern United States - Abstract
This study was designed to examine the concordance of proposed DSM-V posttraumatic stress disorder (PTSD) criteria with DSM-IV classification rules and examine the impact of the proposed DSM-V PTSD criteria on prevalence.The sample (N = 185) included participants who were recruited for studies focused on trauma and health conducted at an academic medical center and VA medical center in the southeastern United States. The prevalence and concordance between DSM-IV and the proposed DSM-V classifications were calculated based on results from structured clinical interviews. Prevalence rates and diagnostic efficiency indices including sensitivity, specificity, area under the curve (AUC), and Kappa were calculated for each of the possible ways to define DSM-V PTSD.Ninety-five percent of the sample reported an event that met both DSM-IV PTSD Criterion A1 and A2, but only 89% reported a trauma that met Criterion A on DSM-V. Results examining concordance between DSM-IV and DSM-V algorithms indicated that several of the algorithms had AUCs above 0.90. The requirement of two symptoms from both Clusters D and E provided strong concordance to DSM-IV (AUC = 0.93; Kappa = 0.86) and a greater balance between sensitivity and specificity than requiring three symptoms in both Clusters D and E.Despite several significant changes to the diagnostic criteria for PTSD for DSM-V, several possible classification rules provided good concordance with DSM-IV. The magnitude of the impact of DSM-V decision rules on prevalence will be largely affected by the DSM-IV PTSD base rate in the population of interest.
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- 2012
16. Pilot Cohorts for Development of Concurrent Mobile Treatment for Alcohol and Tobacco Use Disorders.
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Medenblik AM, Calhoun PS, Maisto SA, Kivlahan DR, Moore SD, Beckham JC, Wilson SM, Blalock DV, and Dedert EA
- Abstract
Alcohol and tobacco are the 2 most frequently used drugs in the United States and represent the highest co-occurrence of polysubstance use. The objective of this study was to refine an intervention combining mobile contingency management with cognitive-behavioral telephone counseling for concurrent treatment of alcohol and tobacco use disorders. Two cohorts (n = 13 total, n = 5 women) of participants were enrolled, with 10/13 completing treatment and 7/13 completing the 6-month follow-up. At enrollment, participants were drinking a mean of 28.9 drinks per week (SD = 14.1), with a mean of 14.7 heavy drinking days in the past month (SD = 9.9), and a mean of 18.1 cigarettes per day (SD = 11.7). Treatment included a mobile application that participants used to record carbon monoxide and breath alcohol content readings to bioverify abstinence. Participants received up to 4 sessions of phone cognitive-behavioral therapy and monetary reinforcement contingent on abstinence. In cohort 1, 4/6 participants reported abstinent or low-risk drinking post-monitoring. Six weeks post quit-date, 2/6 participants were CO-bioverified abstinent from tobacco use, with 2/6 in dual remission. These results were maintained at 6-months. In cohort 2, 6/7 reported abstinent or low-risk drinking post-monitoring, 5 weeks post quit-date. At the post-monitoring visit, 5/7 were CO-bioverified abstinent from smoking, with 5/7 in dual remission. At 6-months, 3/7 reporting abstinent or low-risk drinking, 1/7 had bioverified abstinence from smoking, with 1/7 in dual remission. Observations suggest that it is possible to develop a concurrent mobile treatment for alcohol and tobacco use disorders., Competing Interests: Declaration of conflicting interests: The author(s) declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article., (© The Author(s) 2021.)
- Published
- 2021
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