Hostname: page-component-cc8bf7c57-xrnlw Total loading time: 0 Render date: 2024-12-11T23:06:05.595Z Has data issue: false hasContentIssue false
  • English
  • Français

Childhood trauma is associated with developmental trajectories of EEG coherence, alcohol-related outcomes, and PTSD symptoms

Published online by Cambridge University Press:  02 December 2024

Zoe E. Neale Open the ORCID record for Zoe E. Neale [Opens in a new window] ,
Kaitlin Bountress Open the ORCID record for Kaitlin Bountress [Opens in a new window] ,
Christina Sheerin Open the ORCID record for Christina Sheerin [Opens in a new window] ,
Stacey Saenz de Viteri ,
Shannon Cusack Open the ORCID record for Shannon Cusack [Opens in a new window] ,
David Chorlian ,
Peter B. Barr Open the ORCID record for Peter B. Barr [Opens in a new window] ,
Isabelle Kaplan Open the ORCID record for Isabelle Kaplan [Opens in a new window] ,
Gayathri Pandey Open the ORCID record for Gayathri Pandey [Opens in a new window]  and
Kristina A. Osipenko
...Show all authors
Zoe E. Neale*
Affiliation:
Department of Psychiatry and Behavioral Sciences, State University of New York Downstate Health Sciences University, Brooklyn, NY, USA VA New York Harbor Healthcare System, Brooklyn, NY, USA
Kaitlin Bountress
Affiliation:
Department of Psychiatry, Virginia Commonwealth University, Virginia Institute for Psychiatric and Behavior Genetics, Richmond, VA, USA
Christina Sheerin
Affiliation:
Department of Psychiatry, Virginia Commonwealth University, Virginia Institute for Psychiatric and Behavior Genetics, Richmond, VA, USA
Stacey Saenz de Viteri
Affiliation:
Department of Psychiatry and Behavioral Sciences, State University of New York Downstate Health Sciences University, Brooklyn, NY, USA
Shannon Cusack
Affiliation:
Department of Psychiatry, Virginia Commonwealth University, Virginia Institute for Psychiatric and Behavior Genetics, Richmond, VA, USA
David Chorlian
Affiliation:
Department of Psychiatry and Behavioral Sciences, State University of New York Downstate Health Sciences University, Brooklyn, NY, USA
Peter B. Barr
Affiliation:
Department of Psychiatry and Behavioral Sciences, State University of New York Downstate Health Sciences University, Brooklyn, NY, USA VA New York Harbor Healthcare System, Brooklyn, NY, USA
Isabelle Kaplan
Affiliation:
Department of Psychiatry and Behavioral Sciences, State University of New York Downstate Health Sciences University, Brooklyn, NY, USA
Gayathri Pandey
Affiliation:
Department of Psychiatry and Behavioral Sciences, State University of New York Downstate Health Sciences University, Brooklyn, NY, USA
Kristina A. Osipenko
Affiliation:
Department of Psychiatry and Behavioral Sciences, State University of New York Downstate Health Sciences University, Brooklyn, NY, USA
Vivia McCutcheon
Affiliation:
Department of Psychiatry, Washington University School of Medicine, St Louis, MO, USA
Sally I-Chun Kuo
Affiliation:
Department of Psychiatry, Rutgers University, Robert Wood Johnson Medical School, Piscataway, NJ, USA
Megan E. Cooke
Affiliation:
Department of Psychiatry, Rutgers University, Robert Wood Johnson Medical School, Piscataway, NJ, USA
Sarah J. Brislin
Affiliation:
Department of Psychiatry, Rutgers University, Robert Wood Johnson Medical School, Piscataway, NJ, USA
Jessica E. Salvatore
Affiliation:
Department of Psychiatry, Rutgers University, Robert Wood Johnson Medical School, Piscataway, NJ, USA
Chella Kamarajan
Affiliation:
Department of Psychiatry and Behavioral Sciences, State University of New York Downstate Health Sciences University, Brooklyn, NY, USA
Bernice Porjesz
Affiliation:
Department of Psychiatry and Behavioral Sciences, State University of New York Downstate Health Sciences University, Brooklyn, NY, USA
Ananda B. Amstadter
Affiliation:
Department of Psychiatry, Virginia Commonwealth University, Virginia Institute for Psychiatric and Behavior Genetics, Richmond, VA, USA
Jacquelyn L. Meyers
Affiliation:
Department of Psychiatry and Behavioral Sciences, State University of New York Downstate Health Sciences University, Brooklyn, NY, USA
COGA Investigators
Affiliation:
The Collaborative Study on the Genetics of Alcoholism (COGA) funded by the NIAAA (U10AA008401)
*
Corresponding author: Zoe E. Neale; Email: [email protected]
Rights & Permissions [Opens in a new window]

Abstract

Background

Associations between childhood trauma, neurodevelopment, alcohol use disorder (AUD), and posttraumatic stress disorder (PTSD) are understudied during adolescence.

Methods

Using 1652 participants (51.75% female, baseline Mage = 14.3) from the Collaborative Study of the Genetics of Alcoholism, we employed latent growth curve models to (1) examine associations of childhood physical, sexual, and non-assaultive trauma (CPAT, CSAT, and CNAT) with repeated measures of alpha band EEG coherence (EEGc), and (2) assess whether EEGc trajectories were associated with AUD and PTSD symptoms. Sex-specific models accommodated sex differences in trauma exposure, AUD prevalence, and neural development.

Results

In females, CSAT was associated with higher mean levels of EEGc in left frontocentral (LFC, ß = 0.13, p = 0.01) and interhemispheric prefrontal (PFI, ß = 0.16, p < 0.01) regions, but diminished growth in LFC (ß = −0.07, p = 0.02) and PFI (ß = −0.07, p = 0.02). In males, CPAT was associated with lower mean levels (ß = −0.17, p = 0.01) and increased growth (ß = 0.11, p = 0.01) of LFC EEGc. Slope of LFC EEGc was inversely associated with AUD symptoms in females (ß = −1.81, p = 0.01). Intercept of right frontocentral and PFI EEGc were associated with AUD symptoms in males, but in opposite directions. Significant associations between EEGc and PTSD symptoms were also observed in trauma-exposed individuals.

Conclusions

Childhood assaultive trauma is associated with changes in frontal alpha EEGc and subsequent AUD and PTSD symptoms, though patterns differ by sex and trauma type. EEGc findings may inform emerging treatments for PTSD and AUD.

Keywords

alcohol use disorderchildhood traumaEEG coherenceneurodevelopmentposttraumatic stress disorder
Type
Original Article
Information
Psychological Medicine , First View , pp. 1 - 14
Check for updates
Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution and reproduction, provided the original article is properly cited.
Copyright
Copyright © The Author(s), 2024. Published by Cambridge University Press

Introduction

Childhood trauma is common, with an estimated ~20–66% of individuals in the United States experiencing at least one traumatic event before adulthood (Blaustein, Reference Blaustein, Rossen and Hull2013; Finkelhor, Turner, Ormrod, & Hamby, Reference Finkelhor, Turner, Ormrod and Hamby2009; Read, Ouimette, White, Colder, & Farrow, Reference Read, Ouimette, White, Colder and Farrow2011). Childhood trauma encompasses interpersonal victimization (e.g. physical, sexual abuse/violence) as well as non-interpersonal events (e.g. accidents, illness, loss; Briggs-Gowan, Carter, & Ford, Reference Briggs-Gowan, Carter and Ford2012; Mongillo, Briggs-Gowan, Ford, & Carter, Reference Mongillo, Briggs-Gowan, Ford and Carter2009). Exposure to childhood trauma is thought to disrupt ‘normative’ stages of childhood development, including cognitive, emotional, and social skills development, and predisposes children to psychiatric sequelae (D'Andrea, Ford, Stolbach, Spinazzola, & van der Kolk, Reference D'Andrea, Ford, Stolbach, Spinazzola and van der Kolk2012; Mongillo et al., Reference Mongillo, Briggs-Gowan, Ford and Carter2009; Teicher & Samson, Reference Teicher and Samson2013), including posttraumatic stress disorder (PTSD) (Duncan, Saunders, Kilpatrick, Hanson, & Resnick, Reference Duncan, Saunders, Kilpatrick, Hanson and Resnick1996; Khoury, Tang, Bradley, Cubells, & Ressler, Reference Khoury, Tang, Bradley, Cubells and Ressler2010) and alcohol use disorder (AUD) (Schückher, Sellin, Fahlke, & Engström, Reference Schückher, Sellin, Fahlke and Engström2018). Experiencing childhood trauma yields PTSD and AUD hazard ratios of ~1.4–3.5 (Sartor et al., Reference Sartor, McCutcheon, Pommer, Nelson, Grant, Duncan and Heath2011, Reference Sartor, McCutcheon, Nelson, Duncan, Bucholz and Heath2012) thus, it is important to improve our understanding of the mechanisms by which exposure to trauma may impact development and psychiatric outcomes.

Epidemiologic studies report high co-occurrence between PTSD and both problematic alcohol use and AUD (Brown, Stout, & Mueller, Reference Brown, Stout and Mueller1999; Debell et al., Reference Debell, Fear, Head, Batt-Rawden, Greenberg, Wessely and Goodwin2014; Kessler, Chiu, Demler, Walters, & Walters, Reference Kessler, Chiu, Demler, Walters and Walters2005; Mills, Teesson, Ross, & Peters, Reference Mills, Teesson, Ross and Peters2006; Pietrzak, Goldstein, Southwick, & Grant, Reference Pietrzak, Goldstein, Southwick and Grant2011). One model for understanding this comorbidity is the shared liability model, which suggests that shared, common factors (e.g. trauma, genetics, physiological, and psychological traits) contribute to increased risk for alcohol use behaviors, AUD, and PTSD (Danovitch, Reference Danovitch2016). Indeed, twin and molecular studies suggest correlated genetic risk (Bountress et al., Reference Bountress, Bustamante, Subbie-Saenz de Viteri, Chatzinakos, Sheerin, Daskalakis and Amstadter2022; Sartor et al., Reference Sartor, McCutcheon, Pommer, Nelson, Grant, Duncan and Heath2011; Sheerin et al., Reference Sheerin, Bountress, Meyers, Saenz de Viteri, Shen, Maihofer and Amstadter2020; Xian et al., Reference Xian, Chantarujikapong, Scherrer, Eisen, Lyons, Goldberg and True2000). Growing research has begun to explore the role of shared neurobiological mechanisms (Brady & Sinha, Reference Brady and Sinha2005; Gilpin & Weiner, Reference Gilpin and Weiner2017). Neurophysiological and neuropsychological measurement can further our understanding of shared risk beyond self-report data (Davis et al., Reference Davis, Jovanovic, Norrholm, Glover, Swanson, Spann and Bradley2013). Some work has focused on the role of early stress in producing a cascade of neurobiological changes, such as reduced functional activity and/or structural alterations in key brain areas, that may act to increase risk for psychiatric disorders (Teicher et al., Reference Teicher, Andersen, Polcari, Anderson, Navalta and Kim2003). More research is needed to uncover possible mechanisms by which early trauma may influence neuropsychological development.

Electroencephalogram (EEG) has long been used to examine individual differences in brain function and neuropsychiatric health (Smit et al., Reference Smit, Andreassen, Boomsma, Burwell, Chorlian, de Geus and Wright2021). EEG coherence (EEGc) is a heritable measure of neural functional connectivity, which measures the degree of synchrony in brain oscillatory activity between two regions (Chorlian, Rangaswamy, & Porjesz, Reference Chorlian, Rangaswamy and Porjesz2009; Chorlian et al., Reference Chorlian, Tang, Rangaswamy, O'Connor, Rohrbaugh, Taylor and Porjesz2007; Markovska-Simoska, Pop-Jordanova, & Pop-Jordanov, Reference Markovska-Simoska, Pop-Jordanova and Pop-Jordanov2018). The human central nervous system has a prolonged developmental course, with critical periods in early life and adolescence, especially in prefrontal regions (Larsen & Luna, Reference Larsen and Luna2018; Silbereis, Pochareddy, Zhu, Li, & Sestan, Reference Silbereis, Pochareddy, Zhu, Li and Sestan2016). Childhood stress can harm neural development during these sensitive periods (Andersen et al., Reference Andersen, Tomada, Vincow, Valente, Polcari and Teicher2008). Increased neural functional connectivity, measured via EEG, has been observed in cross-sectional studies of childhood trauma (Cook, Ciorciari, Varker, & Devilly, Reference Cook, Ciorciari, Varker and Devilly2009), and adults with AUD and PTSD (Almli et al., Reference Almli, Lori, Meyers, Shin, Fani, Maihofer and Ressler2018; Dunkley et al., Reference Dunkley, Sedge, Doesburg, Grodecki, Jetly, Shek and Pang2015; Huang, Mohan, De Ridder, Sunaert, & Vanneste, Reference Huang, Mohan, De Ridder, Sunaert and Vanneste2018; Park et al., Reference Park, Lee, Kim, Lee, Jung, Sohn and Choi2017), suggesting that increased functional connectivity may be a shared pathway of risk for AUD and PTSD. Associations between EEGc and neuropsychiatric conditions are complex, but better characterized in schizophrenia (Maran, Grent-; -Jong, & Uhlhaas, Reference Maran, Grent-’t-Jong and Uhlhaas2016), where greater connectivity in lower frequency bands (delta and theta) corresponds to lower cognitive performance and abnormal cortical organization (Di Lorenzo et al., Reference Di Lorenzo, Daverio, Ferrentino, Santarnecchi, Ciabattini, Monaco and Siracusano2015; Lehmann et al., Reference Lehmann, Faber, Pascual-Marqui, Milz, Herrmann, Koukkou and Kochi2014). However, increased coherence is not always adverse – frontal alpha connectivity, involved in information processing and attention (Foxe & Snyder, Reference Foxe and Snyder2011), is lower in schizophrenia compared to controls (e.g. Di Lorenzo et al., Reference Di Lorenzo, Daverio, Ferrentino, Santarnecchi, Ciabattini, Monaco and Siracusano2015; Lehmann et al. Reference Lehmann, Faber, Pascual-Marqui, Milz, Herrmann, Koukkou and Kochi2014; Tauscher, Fischer, Neumeister, Rappelsberger, & Kasper, Reference Tauscher, Fischer, Neumeister, Rappelsberger and Kasper1998). Prior research from the Collaborative Study on the Genetics of Alcoholism (COGA) indicates that AUD manifests as increased resting EEG interhemispheric theta and alpha coherence in fronto-central, fronto-temporal, temporo-parietal, centroparietal and parietal-occipital regions (Meyers et al., Reference Meyers, Zhang, Chorlian, Pandey, Kamarajan, Wang and Porjesz2021; Porjesz & Rangaswamy, Reference Porjesz and Rangaswamy2007; Rangaswamy & Porjesz, Reference Rangaswamy and Porjesz2008). Another COGA study indicated that AD polygenic scores were associated with increased fronto-central, temporo-parietal, centroparietal, and parietal-occipital interhemispheric theta and alpha connectivity in males (Meyers et al., Reference Meyers, Chorlian, Johnson, Pandey, Kamarajan, Salvatore and Porjesz2019a). This research on EEGc could be useful in investigating a possible shared pathway of risk for AUD and PTSD.

Research on the relationship between trauma and neural functional connectivity has focused almost exclusively on adults, ignoring periods of rapid EEGc development in adolescence and young adulthood (Cook et al., Reference Cook, Ciorciari, Varker and Devilly2009; Thatcher, North, & Biver, Reference Thatcher, North and Biver2008). Normative developmental trajectories of EEGc in adolescence have not been comprehensively characterized to our knowledge (Segalowitz, Santesso, & Jetha, Reference Segalowitz, Santesso and Jetha2010) as there are only a few studies with smaller samples; however, emerging literature from COGA suggests alpha coherence tends to increase throughout adolescence, flatten around mid-twenties, and then slowly decline (Chorlian et al., Reference Chorlian, Kamarajan, Meyers, Pandey, Zhang, Kinreich and Porjesz2024). Disrupted alpha rhythm, power, and frontal asymmetry have also been detected in individuals with a range of psychiatric conditions (Eidelman-Rothman, Levy, & Feldman, Reference Eidelman-Rothman, Levy and Feldman2016; Ippolito et al., Reference Ippolito, Bertaccini, Tarasi, Di Gregorio, Trajkovic, Battaglia and Romei2022; Périard et al., Reference Périard, Dierolf, Lutz, Vögele, Voderholzer, Koch and Schulz2024), including PTSD in adults (Badura-Brack et al., Reference Badura-Brack, Becker, McDermott, Ryan, Becker, Hearley and Wilson2015; Huang et al., Reference Huang, Yurgil, Robb, Angeles, Diwakar, Risbrough and Baker2014; Kemp et al., Reference Kemp, Griffiths, Felmingham, Shankman, Drinkenburg, Arns and Bryant2010; Meyer et al., Reference Meyer, Smeets, Giesbrecht, Quaedflieg, Smulders, Meijer and Merckelbach2015; Popescu et al., Reference Popescu, Popescu, DeGraba, Fernandez-Fidalgo, Riedy and Hughes2019). Alpha frequency EEGc is of particular interest as alpha activity has been implicated in studies of impaired memory and cognitive decline in older adults (Babiloni et al., Reference Babiloni, Del Percio, Lizio, Noce, Lopez, Soricelli and Stocchi2018; Blinowska et al., Reference Blinowska, Rakowski, Kaminski, De Vico Fallani, Del Percio, Lizio and Babiloni2017; Hogan, Swanwick, Kaiser, Rowan, & Lawlor, Reference Hogan, Swanwick, Kaiser, Rowan and Lawlor2003; Zhang et al., Reference Zhang, Geng, Wang, Guo, Gao, Zhang and Wang2021), and is hypothesized to be related to acetylcholine levels in the brain (Babiloni et al., Reference Babiloni, Del Percio, Bordet, Bourriez, Bentivoglio, Payoux and Rossini2013; Sharma & Nadkarni, Reference Sharma and Nadkarni2020). Childhood trauma is associated with increased right alpha EEG asymmetry (Meiers, Nooner, De Bellis, Debnath, & Tang, Reference Meiers, Nooner, De Bellis, Debnath and Tang2020), which has also been linked to low mood and social withdrawal in adolescence (Stewart, Towers, Coan, & Allen, Reference Stewart, Towers, Coan and Allen2011). Yet, only a single, small study of EEG functional connectivity and trauma in adolescence has been published (Cook et al., Reference Cook, Ciorciari, Varker and Devilly2009). Correlations of brain connectivity measures with attention and psychopathology suggest that increased EEG functional connectivity contributes to deficits in cognitive functioning and psychopathology (Canuet et al., Reference Canuet, Ishii, Pascual-Marqui, Iwase, Kurimoto, Aoki and Takeda2011; Imperatori et al., Reference Imperatori, Fabbricatore, Innamorati, Farina, Quintiliani, Lamis and Della Marca2015; Kamarajan et al., Reference Kamarajan, Ardekani, Pandey, Chorlian, Kinreich, Pandey and Porjesz2020; Zinn, Zinn, & Jason, Reference Zinn, Zinn and Jason2016), but without longitudinal data, cannot be definitively tested. To the best of our knowledge, EEGc specifically has not yet been examined longitudinally as a biological marker that may link trauma exposure to alcohol-related outcomes and PTSD in adolescents.

The purpose of this study is to investigate the relations among childhood trauma, trajectories of EEG functional connectivity, and risk for AUD and PTSD in adolescence and young adulthood. Using data from COGA, a multi-site study of extended families densely affected with alcohol-related problems (Agrawal et al., Reference Agrawal, Brislin, Bucholz, Dick, Hart, Johnson and Porjesz2023; Meyers et al., Reference Meyers, Brislin, Kamarajan, Plawecki, Chorlian, Anohkin and Porjesz2023), we examined associations between childhood trauma, longitudinal EEGc trajectories, and downstream associations between EEGc and alcohol and trauma-related outcomes (i.e. PTSD symptoms) in COGA's prospective study of adolescent and young adult offspring. We hypothesized that childhood trauma would be associated with differences in frontal alpha EEGc, with the most robust effects observed for those individuals with history of childhood sexual assault. We also expected that these differences in functional connectivity would be associated with increased AUD and PTSD symptoms. We hope findings increase understanding of long-term effects of childhood trauma on neural functioning and psychiatric and behavioral outcomes, enhance knowledge of biological mechanisms by which trauma influences outcomes, and advance work towards novel opportunities for intervention targets.

Methods

Sample

The Collaborative Study on the Genetics of Alcoholism (COGA)'s prospective study began its multi-site data collection in 2004 and ended in 2019. Details on data collection and procedures have been published previously (Dick et al., Reference Dick, Balcke, McCutcheon, Francis, Kuo, Salvatore and Bucholz2023). Briefly, 3715 offspring (14 495 total assessments) from families densely affected with AUD and community comparison families who had at least one parent interviewed in an earlier phase of the COGA study, were enrolled when they were between the ages of 12–22, with new participants added as they reached the age of 12. The COGA study re-assessed participants approximately every two years. A comprehensive battery was administered that included the adult Semi-Structured Assessment for the Genetics of Alcoholism (SSAGA) or the age-appropriate adolescent SSAGA (cSSAGA-A) and parent version (cSSAGA-P) if participants were under age 18. The SSAGA and cSSAGA-A covered substance use problems as well as other psychiatric disorders, including PTSD. As previously detailed (Meyers et al., Reference Meyers, Brislin, Kamarajan, Plawecki, Chorlian, Anohkin and Porjesz2023), a brain function battery was administered at each assessment. These included neurophysiological measures during resting state. Figure 1 shows available data and which assessments are used in the present study. Due to differences in EEG functional connectivity during adolescence compared to adulthood (Segalowitz et al., Reference Segalowitz, Santesso and Jetha2010), and to account for the mean age of onset of regular drinking for the sample (17.48 for males and 17.85 for females), the analytic sample was limited to adolescents age 12–16 at baseline with three or more EEG assessments (n = 1652).

Figure 1. This flowchart illustrates the COGA assessments used in the present study. Gray bars represent data collected in COGA, and black bars and white ‘X’ represent assessment waves used in the current study. The analytic sample was limited to individuals aged 12–16 at baseline.

Assessment of primary constructs

Lifetime history of 21 potentially traumatic events (DSM-IV Criterion A) were based on cSSAGA-A baseline assessments. Although the SSAGA or cSSAGA-A was given at all assessment timepoints, participants were asked to report lifetime maximum DSM-5 AUD symptom count (AUDsx; range 0–11) and, for those who endorsed a Criterion A event, lifetime maximum DSM-IV PTSD Criterion B-D symptom count scores (PTSDsx; range 0–20) at each wave. Therefore, in this study we used lifetime symptom counts ascertained at follow-up 3 (M age = 22) to allow sufficient opportunity for AUDsx to present in late adolescence/young adulthood. Based on evidence that interpersonal assaultive events are more ‘potent’ than non-assaultive events, that traumatic events cluster together, and to remain consistent with prior studies (Meyers et al., Reference Meyers, McCutcheon, Pandey, Kamarajan, Subbie, Chorlian and Porjesz2019b; Subbie-Saenz de Viteri et al., Reference Subbie-Saenz de Viteri, Pandey, Pandey, Kamarajan, Smith, Anokhin and Meyers2020), we constructed three non-mutually exclusive variables representing report of (1) one or more childhood physical assaultive traumas (CPAT; stabbed, shot, mugged, threatened with a weapon, robbed, kidnapped, held captive), (2) childhood sexual assaultive traumas (CSAT; rape or molestation), and (3) childhood non-assaultive traumas (CNAT; life-threatening accident, disaster, witnessing someone seriously injured or killed, unexpectedly finding a dead body), experienced prior to age 13, to ensure that traumatic exposure occurred prior to longitudinal EEGc measures. CPAT, CSAT, and CNAT were endorsed by 8.65%, 43.93%, and 25.24% of the sample, respectively. Based on literature that suggests socioeconomic status (SES) can impact brain development (Hackman, Farah, & Meaney, Reference Hackman, Farah and Meaney2010), we covaried for family SES as indexed by parental report of highest education in COGA Phase 1–3.

EEG Recording and Data Processing procedures have been detailed previously (Meyers et al., Reference Meyers, Brislin, Kamarajan, Plawecki, Chorlian, Anohkin and Porjesz2023) and are summarized in the Supplementary materials.

Statistical analyses

All analyses were stratified by sex and clustered by family to account for relatedness. Primary analyses examined discrete childhood trauma variables (CPAT, CSAT, CNAT) as predictors of intercept and slope of EEGc (alpha EEG inter- and intra-hemispheric coherence) during adolescence and young adulthood using latent growth curve models (LGCM) for those with three or more EEG assessments. We ran the LGCM models in Mplus version 8.9 (Muthén & Muthén, Reference Muthén and Muthén1998-2017), which employs full information maximum likelihood to account for missing data. A non-response analysis indicated that individuals who did not return for follow-up were younger (OR: 2.1, p < 0.001) and less likely to report a prior non-assaultive trauma (OR: 1.3, p < 0.001). No significant differences regarding sex, race/ethnicity, sexual and assaultive trauma exposure, or EEGc were observed. EEGc from bipolar pairs at three frontal sites (Fig. 2), left intra-hemispheric frontal-central (LFC: FZ-CZ--F3-C3), right intra-hemispheric frontal-central (RFC: FZ-CZ--F4-C4), and prefrontal inter-hemispheric (PFI: F8-F4--F7-F3) were examined in separate models. We modeled both linear and quadratic growth components for EEGc. The models that included the quadratic term did not converge, thus we moved ahead with a linear slope term. Any mention of slope in the following sections refer to linear slope.

Figure 2. This figure displays a schematic of bipolar electrode pairs (indicated by black dotted lines) and coherence pairs (indicated by black solid lines) derived between bipolar electrode pairs.

Next, we examined the association between childhood trauma exposure and the intercepts and slopes of EEGc. The intercept estimates individual variation in starting values, which may reflect different types of exposures prior to the measurement period, as well as other trait differences. The slope reflects how change in EEGc occurs over time, on average. Given the known co-occurrence of different types of trauma exposures, the models allowed for simultaneous testing of associations between trauma exposure types and EEGc intercept and slope. The models also evaluated whether intercept and growth parameters in EEGc were associated with AUDsx in the full sample. In a subset of the sample that endorsed exposure to a potentially traumatic event (i.e. met Criterion A for PTSD diagnosis) at any point from baseline to follow-up 3, we added PTSDsx as an additional dependent variable to account for the co-occurrence of AUD and PTSD. Figure 3 is an illustration of the path diagram for the analytic model.

Figure 3. This figure displays a path diagram of the latent growth curve model used to evaluate the association between childhood trauma and intercept and slope of EEG coherence, as well as associations between EEG coherence intercept and slope with AUD symptoms. In the trauma-exposed subsample, PTSD symptoms were also examined as a dependent variable, with the correlation between AUD and PTSD symptoms accounted for by the model. Growth curves were estimated based on individually varying age at the time of each EEG coherence observation. Parental education was included as a covariate. Note: CNAT, Childhood non-assaultive trauma; CSAT, Childhood sexual assaultive trauma; CPAT, Childhood physical assaultive trauma; EEGc, EEG coherence.

Results

Descriptive characteristics of the sample, stratified by sex

Demographic, alcohol and trauma-related characteristics of the sex-stratified sample are provided in Table 1. The overall sample (N = 1652) was 51.75% female. There were no sex differences among race/ethnic groups or participation rates. At baseline, females were significantly younger than males, but mean age did not significantly differ at the three follow-up assessments. Male participants reported significantly more lifetime maximum drinks, and AUD symptoms. Although male and female participants did not differ on rates of childhood trauma exposure, male participants were more likely to report CPAT, whereas female participants were more likely to report CSAT. Among participants exposed to any traumatic event prior to follow-up 3, mean PTSD symptoms 0.75 in males and 1.56 in females, and the modal response for both males and females was zero symptoms. Female participants reported significantly more PTSD symptoms and significantly fewer AUD symptoms compared to male participants.

Table 1. Descriptive information for demographic, alcohol-related, and trauma-related characteristics of the sample

Note: AUD, alcohol use disorder, and PTSD, post-traumatic stress disorder. PTSD symptoms were assessed only in those who reported a history of trauma. Maximum drinks, AUD symptoms, PTSD symptoms were lifetime measures assessed at follow-up 3. *These items (PTSD and AUD symptoms) were calculated among individuals who reported any trauma exposure by follow-up 3. Bold text indicates p-value less than 0.05. Bold italic text indicates p-value less than 0.01.

EEG functional connectivity patterns and associations with childhood trauma

Results of LGCMs estimating the unconditional mean intercept and linear slope of EEGc over time are displayed in Table 2. There was significant positive mean intercept and slope of all three frontal alpha EEGc pairs, indicating that overall, coherence tended to increase over time. The association of CPAT, CSAT, and CNAT with intercept and slope of frontal alpha EEGc, and the association between slope and intercept with AUD symptoms in male and female participants are displayed in Table 3. In the male-only model, we observed a significant association between CPAT and intercept (ß = −0.17, p = 0.010) and slope (ß = 0.11, p = 0.006) of LFC alpha EEGc (FZ-CZ--F3-C3). This suggests that males who reported CPAT had lower values at baseline, but a faster rate of change in EEGc over time. This association was not observed in male RFC or PFI alpha EEGc (FZ-CZ--F4-C4 and F8-F4--F7-F3, respectively). In contrast, in female participants, we observed a significant association between CSAT and intercept (ß = 0.13, p = 0.008) and slope (ß = −0.07, p = 0.016) of LFC alpha EEGc (FZ-CZ--F3-C3), as well as the intercept (ß = 0.16, p = 0.002) and slope (ß = −0.07, p = 0.024) of PFI alpha EEGc (F8-F4--F7-F3). This indicates that female participants who reported CSAT had higher initial values of LFC and PFI alpha EEGc, and a decreased rate of change in LFC and PFI alpha EEGc over time. We observed no significant associations between CNAT and EEGc, and no associations between CSAT or CPAT on our measure of RFC alpha EEGc (FZ-CZ--F4-C4). Greater parental education was associated with decreased intercept (ß = −0.02, p = 0.003) of LFC alpha EEGc in males but had no association with intercept or slope in females.

Table 2. Results of the unconditional linear growth model for repeated measures of three frontal alpha EEG coherence Pairs in adolescent male and female COGA participants

Note: Bold text indicates p-value less than 0.05. Bold italic text indicates p-value less than 0.01.

Table 3. Linear growth model results for the effect of childhood trauma exposure on slope and intercept of three frontal alpha EEG coherence Pairs and subsequent AUD symptoms in adolescent male and female COGA participants

Note: CNAT, Childhood non-assaultive trauma; CSAT, Childhood sexual assaultive trauma; CPAT, Childhood physical assaultive trauma. Bold text indicates p-value less than 0.05. Bold italic text indicates p-value less than 0.01.

Associations between EEG functional connectivity and AUD symptoms

Results of LGCMs estimating the association between intercept and slope of frontal alpha EEGc at three frontal bipolar pairs with AUDsx in male and female participants are displayed in the lower half of Table 3. In males, we observed a significant positive association between intercept and AUDsx in RFC alpha EEGc (ß = 0.36, p = 0.04), and a negative association between intercept and AUDsx in PFI alpha EEGc (ß = −3.33, p < 0.001). EEGc These results suggest that both higher initial values in LFC alpha EEGc, but greater initial values PFI alpha EEGc were associated with increased AUDsx. In female participants, we observed a significant negative association with slope of LFC alpha EEGc (ß = −1.81, p = 0.013), which suggests steeper decline in LFC alpha EEGc over time was associated with increased AUDsx. We observed no associations between intercept and EEGc on AUDsx in females, and no association between slope and AUDsx in males.

Association between EEG functional connectivity and AUD and PTSD symptoms in trauma-exposed participants

Results of LGCMs estimating the associations between intercept and slope of alpha EEGc and subsequent AUDsx and PTSDsx in male and female trauma-exposed participants are displayed in Table 4. We found that intercept of LFC alpha EEGc (FZ-CZ--F3-C3) was positively associated with both AUDsx (ß = 0.53, p < 0.001) and PTSDsx (ß = 2.65, p < 0.001) in trauma-exposed females, suggesting that greater initial values of EEGc were associated with higher levels of PTSD and AUD symptoms. There were no FZ-CZ--F3-C3 intercept or slope associations with AUDsx or PTSDsx observed in trauma-exposed males. For our measure of RFC alpha EEGc (FZ-CZ--F4-C4), we found that intercept was significantly positively associated with both AUDsx (ß = 4.10, p < 0.001) and PTSDsx (ß = 2.47, p < 0.001) in males. In females, slope of RFC alpha EEGc (FZ-CZ--F4-C4) was negatively associated with AUDsx (ß = −3.16, p = 0.002) and PTSDsx (ß = −5.19, p = 0.001), suggesting that diminished growth of EEGc was associated with greater AUDsx and PTSDsx. For PFI alpha EEGc (F8-F4--F7-F3), intercept was significantly positively associated with PTSD symptoms in males (ß = 1.05, p < 0.001), and females (ß = 1.69, p < 0.001). Slope of the same coherence pair (F8-F4--F7-F3), was negatively associated with PTSDsx (ß = −2.02, p = 0.0231) in trauma-exposed males, suggesting that higher initial values and diminished growth of PFI alpha EEGc associated with increased PTSDsx.

Table 4. Linear growth model results measuring associations between slope and intercept of three frontal alpha EEG coherence pairs and subsequent AUD symptoms in the trauma-exposed subsample of adolescent male and female COGA participants

Note: Analyses were limited to individuals who reported at least one traumatic experience during any assessment from baseline to the third follow-up. PTSD symptoms and AUD symptoms represent the lifetime maximum symptoms as reported at the third follow-up assessment. Models account for childhood trauma variables and parental education associations with intercept and slope of EEG coherence. Bold text indicates p-value less than 0.05. Bold italic text indicates p-value less than 0.01.

Discussion

This is the first study, to our knowledge, to examine the association between childhood trauma and longitudinal EEG coherence (EEGc) across adolescence and its role as a potential biological mechanism linking trauma exposure to AUD and PTSD symptoms in young adulthood. We observed differences in trajectories of left frontocentral alpha EEGc related to childhood sexual and physical assaultive trauma in females and childhood physical assaultive trauma in males. The left frontotemporal region of the brain is associated with language, learning, and memory, and has been implicated in studies of the effect of traumatic stress on the brain (Bremner, Reference Bremner2006; Carrion, Weems, Richert, Hoffman, & Reiss, Reference Carrion, Weems, Richert, Hoffman and Reiss2010; Carrion & Wong, Reference Carrion and Wong2012; Stark et al., Reference Stark, Parsons, Van Hartevelt, Charquero-Ballester, McManners, Ehlers and Kringelbach2015). EEG interhemispheric alpha coherence in the prefrontal region also showed increased intercept but diminished growth in females with history of childhood sexual assaultive trauma, suggesting differences in executive function in these individuals. EEGc was associated with subsequent AUD and PTSD symptoms in trauma-exposed participants, with patterns indicating that trauma exposure was associated with worse AUD/PTSD outcomes.

As hypothesized, we found different patterns of EEGc over time related to childhood trauma exposure before age 13. Results demonstrating differences in both intercept and slope of EEGc are associated with childhood assaultive trauma and psychopathology extend the largely cross-sectional, adult-focused literature (Cardenas, Price, & Fein, Reference Cardenas, Price and Fein2018; Cook et al., Reference Cook, Ciorciari, Varker and Devilly2009; Park et al., Reference Park, Lee, Kim, Lee, Jung, Sohn and Choi2017; Tcheslavski & Gonen, Reference Tcheslavski and Gonen2012). Our models indicated higher baseline left frontocentral EEGc in females with CSAT, consistent with a small (n = 30) cross-sectional study by Ito, Teicher, Glod, and Ackerman (Reference Ito, Teicher, Glod and Ackerman1998), which observed higher alpha EEGc in the left hemisphere of children with severe sexual or physical abuse histories. The present study extends this literature by demonstrating nuanced trajectories: decreased alpha EEGc growth in females with CSAT and increased growth in males with CPAT. One explanation for these findings is that childhood trauma may lead to extended hyperarousal and mesolimbic system overactivation, disrupting typical neural network development (Teicher et al., Reference Teicher, Ito, Glod, Andersen, Dumont and Ackerman1997; Teicher & Samson, Reference Teicher and Samson2016). Notably, no associations between CNAT and EEGc were observed, consistent with literature indicating assaultive trauma poses higher risk for PTSD (Breslau et al., Reference Breslau, Kessler, Chilcoat, Schultz, Davis and Andreski1998), depression (McCutcheon et al., Reference McCutcheon, Heath, Nelson, Bucholz, Madden and Martin2009), and more pronounced changes in brain development (De Bellis & Zisk, Reference De Bellis and Zisk2014; Meyers et al., Reference Meyers, McCutcheon, Pandey, Kamarajan, Subbie, Chorlian and Porjesz2019b). Additionally, this study extends literature on functional connectivity and shared liability for AUD and PTSD. Differences in frontal functional connectivity were associated with AUD and PTSD symptoms, but to varying degrees across sexes. Importantly, findings demonstrated associations with both slope and intercept, offering insights potentially missed in prior cross-sectional studies. Together, these findings on trauma, AUD, and EEGc offer some of the first longitudinal evidence of associations between childhood trauma and frontal neural connectivity, with implications for understanding development of psychopathology.

The present study observed significant associations between childhood trauma and alpha EEGc in only the left hemisphere for both males and females, regardless of trauma type. Previous studies have reported differences between hemispheres in individuals with childhood trauma, such as smaller left dorsolateral prefrontal cortex volume in those with childhood trauma (Carballedo et al., Reference Carballedo, Lisiecka, Fagan, Saleh, Ferguson, Connolly and Frodl2012; Lu et al., Reference Lu, Xu, Cao, Yin, Gao, Wang and Xu2019; Paquola, Bennett, & Lagopoulos, Reference Paquola, Bennett and Lagopoulos2016). While our study investigated connectivity in the frontal and central regions of the brain, other studies have seen lateral differences in the temporal region, such as smaller left hippocampal volume compared to controls (Bremner et al., Reference Bremner, Randall, Vermetten, Staib, Bronen, Mazure and Charney1997; Shu et al., Reference Shu, Xue, Liu, Chen, Zhu, Sun and Zhao2013; Stein, Koverola, Hanna, Torchia, & McCLARTY, Reference Stein, Koverola, Hanna, Torchia and McCLARTY1997). Further, less hippocampal activation is associated with increased PTSD symptoms (van Rooij et al., Reference van Rooij, Stevens, Ely, Hinrichs, Michopoulos, Winters and Jovanovic2018). Another study observed abnormal connectivity between the left PFC and anterior hippocampus in children with PTSD (Heyn et al., Reference Heyn, Keding, Ross, Cisler, Mumford and Herringa2019). Given the findings from the present study and previous connectivity and imaging studies, future studies should investigate the associations between sex differences and trauma type with connectivity between the PFC and hippocampus in individuals reporting childhood trauma.

Sex differences in trauma type, PTSD, and AUD, are well documented by previous research (Beals et al., Reference Beals, Belcourt-Dittloff, Garroutte, Croy, Jervis and Whitesell2013; Boudoukha, Ouagazzal, & Goutaudier, Reference Boudoukha, Ouagazzal and Goutaudier2017; Chung & Breslau, Reference Chung and Breslau2008; Erol & Karpyak, Reference Erol and Karpyak2015; Kessler, Sonnega, Bromet, Hughes, & Nelson, Reference Kessler, Sonnega, Bromet, Hughes and Nelson1995). Men are more likely to experience trauma, but less likely to be diagnosed with PTSD compared to women (Beals et al., Reference Beals, Belcourt-Dittloff, Garroutte, Croy, Jervis and Whitesell2013; Kessler et al., Reference Kessler, Sonnega, Bromet, Hughes and Nelson1995). Women are more likely to have co-morbid PTSD and AUD (Peltier et al., Reference Peltier, Roberts, Verplaetse, Zakiniaeiz, Burke, Moore and McKee2022), potentially due to higher risk of recurring, high impact trauma (Beals et al., Reference Beals, Belcourt-Dittloff, Garroutte, Croy, Jervis and Whitesell2013; Hien, Cohen, & Campbell, Reference Hien, Cohen and Campbell2005). In our sample, CSAT was more prevalent in females, and CPAT more prevalent in males. Females also reported significantly higher PTSD symptoms, which may be related to their higher rates of CSAT. Moreover, sex may play also influence the relationship between trauma and neurocognitive development (Helpman et al., Reference Helpman, Zhu, Suarez-Jimenez, Lazarov, Monk and Neria2017). Prior research in COGA (Meyers et al., Reference Meyers, McCutcheon, Pandey, Kamarajan, Subbie, Chorlian and Porjesz2019b) found that females reporting sexual assault had a decreased rate of change in frontal theta oscillations during response inhibition. Structural and functional neuroimaging studies also demonstrate interactions among sex, type, and timing of trauma exposure (for review, see Helpman et al., Reference Helpman, Zhu, Suarez-Jimenez, Lazarov, Monk and Neria2017). In the present study, we observed sex differences dependent on trauma type: in males, CPAT was linked to lower baseline left frontocentral alpha EEGc and a faster rate of change, while in females, CSAT was linked to higher starting values and a slower rate of change. While the observed sex differences may relate to the variation in physical v. assaultive trauma prevalence, the differences in direction of these associations may also suggest true sex-specific effects.

The findings from this study have important implications. First, these results suggest that traumatic experiences in childhood have lasting impacts on brain function, as evidenced by the fact that sexual/physical abuse was associated with both concurrent influences on EEGc and on changes across development. Additionally, type of trauma experienced may have differential associations with EEGc across sexes. Females with childhood sexual assault exposure and males with childhood physical assault exposure may be particularly high-risk groups on whom prevention and intervention efforts should be prioritized. Although links between trauma and PTSD and AUD have been well-established, these study results begin to suggest that atypical changes in alpha EEGc across development may be one factor by which certain traumatic experiences confer risk for AUD and PTSD. This study joins other emerging work (e.g. Kummar, Correia, and Fujiyama, Reference Kummar, Correia and Fujiyama2019) in suggesting that there may be some clinical value in integrating EEG measures into treatment for trauma-exposed individuals, as such biological markers may enable earlier diagnoses and/or an avenue through which to provide neurofeedback over the course of treatment.

Limitations and future directions

Limitations

Missing data – LGCM requires at least three timepoints, which were present in ~85% of COGA's prospective study sample overall, but only 59% of the analytic sample in the present analyses. Childhood Trauma Measures – While some traumatic events would have occurred during the study period (baseline through follow-up 3), many of the childhood traumatic events assessed relied on retrospective self-reports. Retrospective reports may be unstable over time, typically underestimating trauma exposure prevalence, potentially biasing this study's findings towards the null, especially for the individuals who were older at baseline. This may also account in part for the relatively small effect sizes observed for the effect of trauma on EEGc. Additionally, participants’ perceptions of how stressful they found the traumatic event, experiences of prolonged/repeated traumas, and childhood maltreatment (e.g. neglect) were not measured. Although our models accounted for the effect of different types of trauma, we did not present the effect of multiple types of trauma exposure (e.g. CPAT*CSAT) due to power limitations, despite evidence that children often experience multiple types of childhood abuse (Chiu et al., Reference Chiu, Lutfey, Litman, Link, Hall and McKinlay2013). Future analyses that account for ‘dose’ effects (e.g. an individual who has been stabbed, shot, and mugged would have a CPAT dose of 3) and interactive effects would add further insight into our understanding of the effects of complex trauma on the developing brain. Additionally, as symptom counts reflected lifetime problems, it is unknown whether the symptoms reported reflect participants’ current state or whether they had recovered by the time of assessment. Confounding variables – This was an observational study, so we caution against any causal inferences based on the significant associations in our findings, as these associations could be attributed to third variables. There are several factors unaccounted for in the present analyses that may impact the neurodevelopmental processes examined, such as parental factors, sociodemographic factors, fetal alcohol exposure, and individual factors, including genetics and family history of alcohol problems (Pandey et al., Reference Pandey, Seay, Meyers, Chorlian, Pandey, Kamarajan and Porjesz2020). Additional research that more comprehensively integrates the range of important factors is needed.

Future directions

This study focused on alpha EEGc, which is just one of several potentially informative EEG phenotypes. The number of EEG phenotypes available is so vast that future research would likely benefit from integrating machine learning and other methods for the management of big data (Golmohammadi, Harati Nejad Torbati, Lopez de Diego, Obeid, & Picone, Reference Golmohammadi, Harati Nejad Torbati, Lopez de Diego, Obeid and Picone2019; Pawan & Dhiman, Reference Pawan and Dhiman2023) while maintaining a focus on clinical relevance when executing these techniques. In addition, studies that more comprehensively assess childhood trauma (e.g. repeated/prolonged trauma), maltreatment (e.g. neglect), and other stressful life experiences (e.g. discrimination, neighborhood violence) are needed to better understand the way that adverse experiences in childhood may impact neural connectivity and subsequent psychopathology. Another important future direction for this research is the integration of genetic and other biological factors (e.g. family history) associated with trauma, PTSD, and alcohol-related outcomes (e.g. consumption, problems, AUD) and EEG connectivity. Including these informative measures may shed further light on the shared neurobiological mechanisms of risk between PTSD and AUD, as well as increase our ability to better identify individuals who may benefit most from intervention.

Conclusions

This novel study explored associations between childhood trauma and longitudinal alpha EEG coherence in frontal brain regions in children and adolescents, and their association with subsequent AUD and PTSD in young adulthood. Our findings suggest that childhood assaultive trauma is associated with changes in neural connectivity patterns, and the nature of these associations differs by sex and trauma exposure type. Further, trajectories of neural connectivity were associated with subsequent AUD and PTSD symptoms. These findings contribute valuable insights into the neurodevelopmental consequences of childhood trauma, extending beyond the predominantly cross-sectional adult literature. Importantly, sex-specific variations in neural connectivity underscore the need for a comprehensive understanding of trauma's impact on brain functioning. The relevance of EEG coherence as a potential biomarker for early diagnosis and targeted interventions is also emphasized. Moving forward, integrating machine learning techniques and exploring other genetic and biological factors could enhance our understanding of the shared neurobiological mechanisms underlying PTSD, AUD, and trauma-related EEG coherence, with the goal to guide targeted interventions for high-risk groups.

Supplementary material

The supplementary material for this article can be found at https://doi.org/10.1017/S0033291724002599.

Acknowledgements

The Collaborative Study on the Genetics of Alcoholism (COGA), Principal Investigators B. Porjesz, V. Hesselbrock, T. Foroud; Scientific Director, A. Agrawal; Translational Director, D. Dick, includes ten different centers: University of Connecticut (V. Hesselbrock); Indiana University (H.J. Edenberg, T. Foroud, Y. Liu, M.H. Plawecki); University of Iowa Carver College of Medicine (S. Kuperman, J. Kramer); SUNY Downstate Health Sciences University (B. Porjesz, J. Meyers, C. Kamarajan, A. Pandey); Washington University in St. Louis (L. Bierut, J. Rice, K. Bucholz, A. Agrawal); University of California at San Diego (M. Schuckit); Rutgers University (J. Tischfield, D. Dick, R. Hart, J. Salvatore); The Children's Hospital of Philadelphia, University of Pennsylvania (L. Almasy); Icahn School of Medicine at Mount Sinai (A. Goate, P. Slesinger); and Howard University (D. Scott). Other COGA collaborators include: L. Bauer (University of Connecticut); J. Nurnberger Jr., L. Wetherill, X., Xuei, D. Lai, S. O'Connor, (Indiana University); G. Chan (University of Iowa; University of Connecticut); D.B. Chorlian, J. Zhang, P. Barr, S. Kinreich, Z. Neale, G. Pandey (SUNY Downstate); N. Mullins (Icahn School of Medicine at Mount Sinai); A. Anokhin, S. Hartz, E. Johnson, V. McCutcheon, S. Saccone (Washington University); J. Moore, F. Aliev, Z. Pang, S. Kuo (Rutgers University); A. Merikangas (The Children's Hospital of Philadelphia and University of Pennsylvania); H. Chin and A. Parsian are the NIAAA Staff Collaborators. We continue to be inspired by our memories of Henri Begleiter and Theodore Reich, founding PI and Co-PI of COGA, and also owe a debt of gratitude to other past organizers of COGA, including Ting- Kai Li, P. Michael Conneally, Raymond Crowe, and Wendy Reich, for their critical contributions. This national collaborative study is supported by NIH Grant U10AA008401 from the National Institute on Alcohol Abuse and Alcoholism (NIAAA) and the National Institute on Drug Abuse (NIDA).

Funding statement

This research was funded by the National Institute on Alcohol Abuse and Alcoholism (U10AA008401 to BP, and R01AA030010 to JM and AA).

Competing interests

The authors declare that they have no competing interests.

Ethical standards

The authors assert that all procedures contributing to this work comply with the ethical standards of the relevant national and institutional committees on human experimentation and with the Helsinki Declaration of 1975, as revised in 2008.

Footnotes

*

These authors contributed equally to this work and share senior authorship.

References

Agrawal, A., Brislin, S. J., Bucholz, K. K., Dick, D., Hart, R. P., Johnson, E. C., … Porjesz, B. (2023). The collaborative study on the genetics of alcoholism: Overview. Genes, Brain and Behavior, 22(5), e12864. https://doi.org/10.1111/gbb.12864Google Scholar
Almli, L. M., Lori, A., Meyers, J. L., Shin, J., Fani, N., Maihofer, A. X., … Ressler, K. J. (2018). Problematic alcohol use associates with sodium channel and clathrin linker 1 (SCLT1) in trauma-exposed populations. Addiction Biology, 23(5), 11451159. https://doi.org/10.1111/adb.12569CrossRefGoogle ScholarPubMed
Andersen, S. L., Tomada, A., Vincow, E. S., Valente, E., Polcari, A., & Teicher, M. H. (2008). Preliminary evidence for sensitive periods in the effect of childhood sexual abuse on regional brain development. The Journal of Neuropsychiatry and Clinical Neurosciences, 20(3), 292301. https://doi.org/10.1176/jnp.2008.20.3.292CrossRefGoogle ScholarPubMed
Babiloni, C., Del Percio, C., Bordet, R., Bourriez, J.-L., Bentivoglio, M., Payoux, P., … Rossini, P. M. (2013). Effects of acetylcholinesterase inhibitors and memantine on resting-state electroencephalographic rhythms in Alzheimer's disease patients. Clinical Neurophysiology: Official Journal of the International Federation of Clinical Neurophysiology, 124(5), 837850. https://doi.org/10.1016/j.clinph.2012.09.017CrossRefGoogle ScholarPubMed
Babiloni, C., Del Percio, C., Lizio, R., Noce, G., Lopez, S., Soricelli, A., … Stocchi, F. (2018). Functional cortical source connectivity of resting state electroencephalographic alpha rhythms shows similar abnormalities in patients with mild cognitive impairment due to Alzheimer's and Parkinson's diseases. Clinical Neurophysiology: Official Journal of the International Federation of Clinical Neurophysiology, 129(4), 766782. https://doi.org/10.1016/j.clinph.2018.01.009CrossRefGoogle ScholarPubMed
Badura-Brack, A. S., Becker, K. M., McDermott, T. J., Ryan, T. J., Becker, M. M., Hearley, A. R., … Wilson, T. W. (2015). Decreased somatosensory activity to non-threatening touch in combat veterans with posttraumatic stress disorder. Psychiatry Research, 233(2), 194200. https://doi.org/10.1016/j.pscychresns.2015.06.012CrossRefGoogle ScholarPubMed
Beals, J., Belcourt-Dittloff, A., Garroutte, E. M., Croy, C., Jervis, L. L., Whitesell, N. R., … The AI-SUPERPFP team. (2013). Trauma and conditional risk of posttraumatic stress disorder in two American Indian reservation communities. Social Psychiatry and Psychiatric Epidemiology, 48(6), 895905. https://doi.org/10.1007/s00127-012-0615-5CrossRefGoogle ScholarPubMed
Blaustein, M. E. (2013). Childhood trauma and a framework for intervention. In Rossen, E. A. & Hull, R. V. (Eds.), Supporting and educating traumatized students: A guide for school-based professionals (pp. 321). USA: OUP.Google Scholar
Blinowska, K. J., Rakowski, F., Kaminski, M., De Vico Fallani, F., Del Percio, C., Lizio, R., & Babiloni, C. (2017). Functional and effective brain connectivity for discrimination between Alzheimer's patients and healthy individuals: A study on resting state EEG rhythms. Clinical Neurophysiology: Official Journal of the International Federation of Clinical Neurophysiology, 128(4), 667680. https://doi.org/10.1016/j.clinph.2016.10.002CrossRefGoogle Scholar
Boudoukha, A. H., Ouagazzal, O., & Goutaudier, N. (2017). When traumatic event exposure characteristics matter: Impact of traumatic event exposure characteristics on posttraumatic and dissociative symptoms. Psychological Trauma: Theory, Research, Practice, and Policy, 9(5), 561566. https://doi.org/10.1037/tra0000243CrossRefGoogle ScholarPubMed
Bountress, K. E., Bustamante, D., Subbie-Saenz de Viteri, S., Chatzinakos, C., Sheerin, C., Daskalakis, N. P., … Amstadter, A. (2022). Differences in genetic correlations between posttraumatic stress disorder and alcohol-related problems phenotypes compared to alcohol consumption-related phenotypes. Psychological Medicine, 53(12), 57675777. https://doi.org/10.1017/S0033291722002999CrossRefGoogle ScholarPubMed
Brady, K. T., & Sinha, R. (2005). Co-occurring mental and substance use disorders: The neurobiological effects of chronic stress. The American Journal of Psychiatry, 162(8), 14831493. https://doi.org/10.1176/appi.ajp.162.8.1483CrossRefGoogle ScholarPubMed
Bremner, J. D. (2006). Traumatic stress: Effects on the brain. Dialogues in Clinical Neuroscience, 8(4), 445461.CrossRefGoogle ScholarPubMed
Bremner, J. D., Randall, P., Vermetten, E., Staib, L., Bronen, R. A., Mazure, C., … Charney, D. S. (1997). Magnetic resonance imaging-based measurement of hippocampal volume in posttraumatic stress disorder related to childhood physical and sexual abuse—A preliminary report. Biological Psychiatry, 41(1), 2332. https://doi.org/10.1016/S0006-3223(96)00162-XCrossRefGoogle ScholarPubMed
Breslau, N., Kessler, R. C., Chilcoat, H. D., Schultz, L. R., Davis, G. C., & Andreski, P. (1998). Trauma and posttraumatic stress disorder in the community: The 1996 Detroit area survey of trauma. Archives of General Psychiatry, 55(7), 626632. https://doi.org/10.1001/archpsyc.55.7.626CrossRefGoogle ScholarPubMed
Briggs-Gowan, M. J., Carter, A. S., & Ford, J. D. (2012). Parsing the effects violence exposure in early childhood: Modeling developmental pathways. Journal of Pediatric Psychology, 37(1), 1122. https://doi.org/10.1093/jpepsy/jsr063CrossRefGoogle ScholarPubMed
Brown, P. J., Stout, R. L., & Mueller, T. (1999). Substance use disorder and posttraumatic stress disorder comorbidity: Addiction and psychiatric treatment rates. Psychology of Addictive Behaviors, 13(2), 115122. https://doi.org/10.1037/0893-164X.13.2.115CrossRefGoogle Scholar
Canuet, L., Ishii, R., Pascual-Marqui, R. D., Iwase, M., Kurimoto, R., Aoki, Y., … Takeda, M. (2011). Resting-state EEG source localization and functional connectivity in schizophrenia-like psychosis of epilepsy. PloS One, 6(11), e27863. https://doi.org/10.1371/journal.pone.0027863CrossRefGoogle ScholarPubMed
Carballedo, A., Lisiecka, D., Fagan, A., Saleh, K., Ferguson, Y., Connolly, G., … Frodl, T. (2012). Early life adversity is associated with brain changes in subjects at family risk for depression. The World Journal of Biological Psychiatry, 13(8), 569578. https://doi.org/10.3109/15622975.2012.661079CrossRefGoogle ScholarPubMed
Cardenas, V. A., Price, M., & Fein, G. (2018). EEG coherence related to fMRI resting state synchrony in long-term abstinent alcoholics. NeuroImage. Clinical, 17, 481490. https://doi.org/10.1016/j.nicl.2017.11.008CrossRefGoogle ScholarPubMed
Carrion, V. G., Weems, C. F., Richert, K., Hoffman, B. C., & Reiss, A. L. (2010). Decreased prefrontal cortical volume associated with increased bedtime cortisol in traumatized youth. Biological Psychiatry, 68(5), 491493. https://doi.org/10.1016/j.biopsych.2010.05.010CrossRefGoogle ScholarPubMed
Carrion, V. G., & Wong, S. S. (2012). Can traumatic stress alter the brain? Understanding the implications of early trauma on brain development and learning. Journal of Adolescent Health, 51(2, Supplement), S23S28. https://doi.org/10.1016/j.jadohealth.2012.04.010CrossRefGoogle ScholarPubMed
Chiu, G. R., Lutfey, K. E., Litman, H. J., Link, C. L., Hall, S. A., & McKinlay, J. B. (2013). Prevalence and overlap of childhood and adult physical, sexual, and emotional abuse: A descriptive analysis of results from the Boston area community health (BACH) survey. Violence and Victims, 28(3), 381402.CrossRefGoogle ScholarPubMed
Chorlian, D. B., Kamarajan, C., Meyers, J. L., Pandey, A. K., Zhang, J., Kinreich, S., & Porjesz, B. (2024). Non-linear development of EEG coherence in adolescents and young adults shown by the analysis of neurophysiological trajectories and their covariance. bioRxiv, 2024.03.13.584867. https://doi.org/10.1101/2024.03.13.584867Google Scholar
Chorlian, D. B., Rangaswamy, M., & Porjesz, B. (2009). EEG coherence: Topography and frequency structure. Experimental Brain Research, 198(1), 5983. https://doi.org/10.1007/s00221-009-1936-9CrossRefGoogle ScholarPubMed
Chorlian, D. B., Tang, Y., Rangaswamy, M., O'Connor, S., Rohrbaugh, J., Taylor, R., & Porjesz, B. (2007). Heritability of EEG coherence in a large sib-pair population. Biological Psychology, 75(3), 260266. https://doi.org/10.1016/j.biopsycho.2007.03.006CrossRefGoogle Scholar
Chung, H., & Breslau, N. (2008). The latent structure of post-traumatic stress disorder: Tests of invariance by gender and trauma type. Psychological Medicine, 38(4), 563573. https://doi.org/10.1017/S0033291707002589CrossRefGoogle ScholarPubMed
Cook, F., Ciorciari, J., Varker, T., & Devilly, G. J. (2009). Changes in long term neural connectivity following psychological trauma. Clinical Neurophysiology: Official Journal of the International Federation of Clinical Neurophysiology, 120(2), 309314. https://doi.org/10.1016/j.clinph.2008.11.021CrossRefGoogle ScholarPubMed
D'Andrea, W., Ford, J., Stolbach, B., Spinazzola, J., & van der Kolk, B. A. (2012). Understanding interpersonal trauma in children: Why we need a developmentally appropriate trauma diagnosis. The American Journal of Orthopsychiatry, 82(2), 187200. https://doi.org/10.1111/j.1939-0025.2012.01154.xCrossRefGoogle Scholar
Danovitch, I. (2016). Post-traumatic stress disorder and opioid use disorder: A narrative review of conceptual models. Journal of Addictive Diseases, 35(3), 169179. https://doi.org/10.1080/10550887.2016.1168212CrossRefGoogle ScholarPubMed
Davis, T. A., Jovanovic, T., Norrholm, S. D., Glover, E. M., Swanson, M., Spann, S., & Bradley, B. (2013). Substance use attenuates physiological responses associated with PTSD among individuals with co-morbid PTSD and SUDs. Journal of Psychology & Psychotherapy, Suppl 7, 006. https://doi.org/10.4172/2161-0487.S7-006Google ScholarPubMed
Debell, F., Fear, N. T., Head, M., Batt-Rawden, S., Greenberg, N., Wessely, S., & Goodwin, L. (2014). A systematic review of the comorbidity between PTSD and alcohol misuse. Social Psychiatry and Psychiatric Epidemiology, 49(9), 14011425. https://doi.org/10.1007/s00127-014-0855-7CrossRefGoogle ScholarPubMed
De Bellis, M. D., & Zisk, A. (2014). The biological effects of childhood trauma. Child and Adolescent Psychiatric Clinics of North America, 23(2), 185222. https://doi.org/10.1016/j.chc.2014.01.002CrossRefGoogle ScholarPubMed
Di Lorenzo, G., Daverio, A., Ferrentino, F., Santarnecchi, E., Ciabattini, F., Monaco, L., … Siracusano, A. (2015). Altered resting-state EEG source functional connectivity in schizophrenia: The effect of illness duration. Frontiers in Human Neuroscience, 9, 234. https://doi.org/10.3389/fnhum.2015.00234CrossRefGoogle ScholarPubMed
Dick, D. M., Balcke, E., McCutcheon, V., Francis, M., Kuo, S., Salvatore, J., … Bucholz, K. (2023). The collaborative study on the genetics of alcoholism: Sample and clinical data. Genes, Brain and Behavior, 22(5), e12860.CrossRefGoogle Scholar
Duncan, R. D., Saunders, B. E., Kilpatrick, D. G., Hanson, R. F., & Resnick, H. S. (1996). Childhood physical assault as a risk factor for PTSD, depression, and substance abuse: Findings from a national survey. The American Journal of Orthopsychiatry, 66(3), 437448. https://doi.org/10.1037/h0080194CrossRefGoogle ScholarPubMed
Dunkley, B. T., Sedge, P. A., Doesburg, S. M., Grodecki, R. J., Jetly, R., Shek, P. N., … Pang, E. W. (2015). Theta, mental flexibility, and post-traumatic stress disorder: Connecting in the parietal cortex. PloS One, 10(4), e0123541. https://doi.org/10.1371/journal.pone.0123541CrossRefGoogle ScholarPubMed
Eidelman-Rothman, M., Levy, J., & Feldman, R. (2016). Alpha oscillations and their impairment in affective and post-traumatic stress disorders. Neuroscience & Biobehavioral Reviews, 68, 794815. https://doi.org/10.1016/j.neubiorev.2016.07.005CrossRefGoogle ScholarPubMed
Erol, A., & Karpyak, V. M. (2015). Sex and gender-related differences in alcohol use and its consequences: Contemporary knowledge and future research considerations. Drug and Alcohol Dependence, 156, 113. https://doi.org/10.1016/j.drugalcdep.2015.08.023CrossRefGoogle ScholarPubMed
Finkelhor, D., Turner, H., Ormrod, R., & Hamby, S. L. (2009). Violence, abuse, and crime exposure in a national sample of children and youth. Pediatrics, 124(5), 14111423. https://doi.org/10.1542/peds.2009-0467CrossRefGoogle Scholar
Foxe, J. J., & Snyder, A. C. (2011). The role of alpha-band brain oscillations as a sensory suppression mechanism during selective attention. Frontiers in Psychology, 2, 154. https://doi.org/10.3389/fpsyg.2011.00154CrossRefGoogle ScholarPubMed
Gilpin, N. W., & Weiner, J. L. (2017). Neurobiology of comorbid post-traumatic stress disorder and alcohol-use disorder. Genes, Brain, and Behavior, 16(1), 1543. https://doi.org/10.1111/gbb.12349CrossRefGoogle ScholarPubMed
Golmohammadi, M., Harati Nejad Torbati, A. H., Lopez de Diego, S., Obeid, I., & Picone, J. (2019). Automatic analysis of EEGs using big data and hybrid deep learning architectures. Frontiers in Human Neuroscience, 13, 76. Retrieved from https://www.frontiersin.org/articles/10.3389/fnhum.2019.00076CrossRefGoogle ScholarPubMed
Hackman, D. A., Farah, M. J., & Meaney, M. J. (2010). Socioeconomic status and the brain: Mechanistic insights from human and animal research. Nature Reviews. Neuroscience, 11(9), 651659. https://doi.org/10.1038/nrn2897CrossRefGoogle ScholarPubMed
Helpman, L., Zhu, X., Suarez-Jimenez, B., Lazarov, A., Monk, C., & Neria, Y. (2017). Sex differences in trauma-related psychopathology: A critical review of neuroimaging literature (2014–2017). Current Psychiatry Reports, 19(12), 104. https://doi.org/10.1007/s11920-017-0854-yCrossRefGoogle ScholarPubMed
Heyn, S. A., Keding, T. J., Ross, M. C., Cisler, J. M., Mumford, J. A., & Herringa, R. J. (2019). Abnormal prefrontal development in pediatric posttraumatic stress disorder: A longitudinal structural and functional magnetic resonance imaging study. Biological Psychiatry. Cognitive Neuroscience and Neuroimaging, 4(2), 171179. https://doi.org/10.1016/j.bpsc.2018.07.013CrossRefGoogle ScholarPubMed
Hien, D., Cohen, L., & Campbell, A. (2005). Is traumatic stress a vulnerability factor for women with substance use disorders? Clinical Psychology Review, 25(6), 813823. https://doi.org/10.1016/j.cpr.2005.05.006CrossRefGoogle Scholar
Hogan, M. J., Swanwick, G. R. J., Kaiser, J., Rowan, M., & Lawlor, B. (2003). Memory-related EEG power and coherence reductions in mild Alzheimer's disease. International Journal of Psychophysiology, 49(2), 147163. https://doi.org/10.1016/S0167-8760(03)00118-1CrossRefGoogle ScholarPubMed
Huang, M.-X., Yurgil, K. A., Robb, A., Angeles, A., Diwakar, M., Risbrough, V. B., … Baker, D. G. (2014). Voxel-wise resting-state MEG source magnitude imaging study reveals neurocircuitry abnormality in active-duty service members and veterans with PTSD. NeuroImag : Clinical, 5, 408419. https://doi.org/10.1016/j.nicl.2014.08.004CrossRefGoogle ScholarPubMed
Huang, Y., Mohan, A., De Ridder, D., Sunaert, S., & Vanneste, S. (2018). The neural correlates of the unified percept of alcohol-related craving: A fMRI and EEG study. Scientific Reports, 8(1), 923. https://doi.org/10.1038/s41598-017-18471-yCrossRefGoogle ScholarPubMed
Imperatori, C., Fabbricatore, M., Innamorati, M., Farina, B., Quintiliani, M. I., Lamis, D. A., … Della Marca, G. (2015). Modification of EEG functional connectivity and EEG power spectra in overweight and obese patients with food addiction: An eLORETA study. Brain Imaging and Behavior, 9(4), 703716. https://doi.org/10.1007/s11682-014-9324-xCrossRefGoogle ScholarPubMed
Ippolito, G., Bertaccini, R., Tarasi, L., Di Gregorio, F., Trajkovic, J., Battaglia, S., & Romei, V. (2022). The role of alpha oscillations among the main neuropsychiatric disorders in the adult and developing human brain: Evidence from the last 10 years of research. Biomedicines, 10(12), 3189. https://doi.org/10.3390/biomedicines10123189CrossRefGoogle ScholarPubMed
Ito, Y., Teicher, M. H., Glod, C. A., & Ackerman, E. (1998). Preliminary evidence for aberrant cortical development in abused children. The Journal of Neuropsychiatry and Clinical Neurosciences, 10(3), 298307. https://doi.org/10.1176/jnp.10.3.298CrossRefGoogle ScholarPubMed
Kamarajan, C., Ardekani, B. A., Pandey, A. K., Chorlian, D. B., Kinreich, S., Pandey, G., … Porjesz, B. (2020). Random forest classification of alcohol use disorder using EEG source functional connectivity, neuropsychological functioning, and impulsivity measures. Behavioral Sciences (Basel, Switzerland), 10(3), 62. https://doi.org/10.3390/bs10030062Google ScholarPubMed
Kemp, A. H., Griffiths, K., Felmingham, K. L., Shankman, S. A., Drinkenburg, W., Arns, M., … Bryant, R. A. (2010). Disorder specificity despite comorbidity: Resting EEG alpha asymmetry in major depressive disorder and post-traumatic stress disorder. Biological Psychology, 85(2), 350354. https://doi.org/10.1016/j.biopsycho.2010.08.001CrossRefGoogle ScholarPubMed
Kessler, R. C., Chiu, W. T., Demler, O., Walters, E. E., & Walters, E. E. (2005). Prevalence, severity, and comorbidity of 12–month DSM-IV disorders in the national comorbidity survey replication. Archives of General Psychiatry, 62(6), 617. https://doi.org/10.1001/archpsyc.62.6.617CrossRefGoogle ScholarPubMed
Kessler, R. C., Sonnega, A., Bromet, E., Hughes, M., & Nelson, C. B. (1995). Posttraumatic stress disorder in the National Comorbidity Survey. Archives of General Psychiatry, 52(12), 10481060. https://doi.org/10.1001/archpsyc.1995.03950240066012CrossRefGoogle ScholarPubMed
Khoury, L., Tang, Y. L., Bradley, B., Cubells, J. F., & Ressler, K. J. (2010). Substance use, childhood traumatic experience, and Posttraumatic Stress Disorder in an urban civilian population. Depression and Anxiety, 27(12), 10771086. https://doi.org/10.1002/da.20751CrossRefGoogle Scholar
Kummar, A. S., Correia, H., & Fujiyama, H. (2019). A brief review of the EEG literature on mindfulness and fear extinction and its potential implications for posttraumatic stress symptoms (PTSS). Brain Sciences, 9(10), 258. https://doi.org/10.3390/brainsci9100258CrossRefGoogle ScholarPubMed
Larsen, B., & Luna, B. (2018). Adolescence as a neurobiological critical period for the development of higher-order cognition. Neuroscience and Biobehavioral Reviews, 94, 179195. https://doi.org/10.1016/j.neubiorev.2018.09.005CrossRefGoogle ScholarPubMed
Lehmann, D., Faber, P. L., Pascual-Marqui, R. D., Milz, P., Herrmann, W. M., Koukkou, M., … Kochi, K. (2014). Functionally aberrant electrophysiological cortical connectivities in first episode medication-naive schizophrenics from three psychiatry centers. Frontiers in Human Neuroscience, 8, 635. https://doi.org/10.3389/fnhum.2014.00635CrossRefGoogle ScholarPubMed
Lu, S., Xu, R., Cao, J., Yin, Y., Gao, W., Wang, D., … Xu, Y. (2019). The left dorsolateral prefrontal cortex volume is reduced in adults reporting childhood trauma independent of depression diagnosis. Journal of Psychiatric Research, 112, 1217. https://doi.org/10.1016/j.jpsychires.2019.02.014CrossRefGoogle ScholarPubMed
Maran, M., Grent-’t-Jong, T., & Uhlhaas, P. J. (2016). Electrophysiological insights into connectivity anomalies in schizophrenia: A systematic review. Neuropsychiatric Electrophysiology, 2(1), 6. https://doi.org/10.1186/s40810-016-0020-5CrossRefGoogle Scholar
Markovska-Simoska, S., Pop-Jordanova, N., & Pop-Jordanov, J. (2018). Inter- and intra-hemispheric EEG coherence study in adults with neuropsychiatric disorders. Prilozi (Makedonska Akademija Na Naukite I Umetnostite. Oddelenie Za Medicinski Nauki), 39(2–3), 519. https://doi.org/10.2478/prilozi-2018-0037Google ScholarPubMed
McCutcheon, V. V., Heath, A. C., Nelson, E. C., Bucholz, K. K., Madden, P. a. F., & Martin, N. G. (2009). Accumulation of trauma over time and risk for depression in a twin sample. Psychological Medicine, 39(3), 431441. https://doi.org/10.1017/S0033291708003759CrossRefGoogle Scholar
Meiers, G., Nooner, K., De Bellis, M. D., Debnath, R., & Tang, A. (2020). Alpha EEG asymmetry, childhood maltreatment, and problem behaviors: A pilot home-based study. Child Abuse & Neglect, 101, 104358. https://doi.org/10.1016/j.chiabu.2020.104358CrossRefGoogle ScholarPubMed
Meyer, T., Smeets, T., Giesbrecht, T., Quaedflieg, C. W. E. M., Smulders, F. T. Y., Meijer, E. H., & Merckelbach, H. L. G. J. (2015). The role of frontal EEG asymmetry in post-traumatic stress disorder. Biological Psychology, 108, 6277. https://doi.org/10.1016/j.biopsycho.2015.03.018CrossRefGoogle ScholarPubMed
Meyers, J. L., Brislin, S. J., Kamarajan, C., Plawecki, M. H., Chorlian, D., Anohkin, A., … Porjesz, B. (2023). The collaborative study on the genetics of alcoholism: Brain function. Genes, Brain and Behavior, 22(5), e12862. https://doi.org/10.1111/gbb.12862CrossRefGoogle Scholar
Meyers, J. L., Chorlian, D. B., Johnson, E. C., Pandey, A. K., Kamarajan, C., Salvatore, J. E., … Porjesz, B. (2019a). Association of polygenic liability for alcohol dependence and EEG connectivity in adolescence and young adulthood. Brain Sciences, 9(10), 280. https://doi.org/10.3390/brainsci9100280CrossRefGoogle ScholarPubMed
Meyers, J. L., McCutcheon, V. V., Pandey, A. K., Kamarajan, C., Subbie, S., Chorlian, D., … Porjesz, B. (2019b). Early sexual trauma exposure and neural response inhibition in adolescence and young adults: Trajectories of frontal theta oscillations during a go/no-go task. Journal of the American Academy of Child and Adolescent Psychiatry, 58(2), 242255.e2. https://doi.org/10.1016/j.jaac.2018.07.905CrossRefGoogle Scholar
Meyers, J. L., Zhang, J., Chorlian, D. B., Pandey, A. K., Kamarajan, C., Wang, J.-C., … Porjesz, B. (2021). A genome-wide association study of interhemispheric theta EEG coherence: Implications for neural connectivity and alcohol use behavior. Molecular Psychiatry, 26(9), 50405052. https://doi.org/10.1038/s41380-020-0777-6CrossRefGoogle ScholarPubMed
Mills, K. L., Teesson, M., Ross, J., & Peters, L. (2006). Trauma, PTSD, and substance use disorders: Findings from the Australian national survey of mental health and well-being. American Journal of Psychiatry, 163(4), 652658. https://doi.org/10.1176/ajp.2006.163.4.652CrossRefGoogle ScholarPubMed
Mongillo, E. A., Briggs-Gowan, M., Ford, J. D., & Carter, A. S. (2009). Impact of traumatic life events in a community sample of toddlers. Journal of Abnormal Child Psychology, 37(4), 455468. https://doi.org/10.1007/s10802-008-9283-zCrossRefGoogle Scholar
Muthén, L. K., & Muthén, B. O. (1998). Mplus user's guide. Los Angeles, CA: Muthén & Muthén.Google Scholar
Pandey, G., Seay, M. J., Meyers, J. L., Chorlian, D. B., Pandey, A. K., Kamarajan, C., … Porjesz, B. (2020). Density and dichotomous family history measures of alcohol use disorder as predictors of behavioral and neural phenotypes: A comparative study across gender and race/ethnicity. Alcoholism, Clinical and Experimental Research, 44(3), 697710. https://doi.org/10.1111/acer.14280CrossRefGoogle ScholarPubMed
Paquola, C., Bennett, M. R., & Lagopoulos, J. (2016). Understanding heterogeneity in grey matter research of adults with childhood maltreatment—A meta-analysis and review. Neuroscience & Biobehavioral Reviews, 69, 299312. https://doi.org/10.1016/j.neubiorev.2016.08.011CrossRefGoogle ScholarPubMed
Park, S. M., Lee, J. Y., Kim, Y. J., Lee, J.-Y., Jung, H. Y., Sohn, B. K., … Choi, J.-S. (2017). Neural connectivity in internet gaming disorder and alcohol use disorder: A resting-state EEG coherence study. Scientific Reports, 7(1), 1333. https://doi.org/10.1038/s41598-017-01419-7CrossRefGoogle ScholarPubMed
Pawan, , & Dhiman, R. (2023). Machine learning techniques for electroencephalogram based brain-computer interface: A systematic literature review. Measurement: Sensors, 28, 100823. https://doi.org/10.1016/j.measen.2023.100823Google Scholar
Peltier, M. R., Roberts, W., Verplaetse, T. L., Zakiniaeiz, Y., Burke, C., Moore, K. E., & McKee, S. A. (2022). Sex differences across retrospective transitions in posttraumatic stress and substance use disorders. Journal of Dual Diagnosis, 18(1), 1120. https://doi.org/10.1080/15504263.2021.2016027CrossRefGoogle ScholarPubMed
Périard, I. A.-C., Dierolf, A. M., Lutz, A., Vögele, C., Voderholzer, U., Koch, S., … Schulz, A. (2024). Frontal alpha asymmetry is associated with chronic stress and depression, but not with somatoform disorders. International Journal of Psychophysiology, 200, 112342. https://doi.org/10.1016/j.ijpsycho.2024.112342CrossRefGoogle Scholar
Pietrzak, R. H., Goldstein, R. B., Southwick, S. M., & Grant, B. F. (2011). Prevalence and axis I comorbidity of full and partial posttraumatic stress disorder in the United States: Results from wave 2 of the national epidemiologic survey on alcohol and related conditions. Journal of Anxiety Disorders, 25(3), 456465. https://doi.org/10.1016/j.janxdis.2010.11.010CrossRefGoogle ScholarPubMed
Popescu, M., Popescu, E.-A., DeGraba, T. J., Fernandez-Fidalgo, D. J., Riedy, G., & Hughes, J. D. (2019). Post-traumatic stress disorder is associated with altered modulation of prefrontal alpha band oscillations during working memory. Clinical Neurophysiology, 130(10), 18691881. https://doi.org/10.1016/j.clinph.2019.06.227CrossRefGoogle ScholarPubMed
Porjesz, B., & Rangaswamy, M. (2007). Neurophysiological endophenotypes, CNS disinhibition, and risk for alcohol dependence and related disorders. TheScientificWorldJournal, 7, 131141. https://doi.org/10.1100/tsw.2007.203CrossRefGoogle ScholarPubMed
Rangaswamy, M., & Porjesz, B. (2008). Uncovering genes for cognitive (dys)function and predisposition for alcoholism spectrum disorders: A review of human brain oscillations as effective endophenotypes. Brain Research, 1235, 153171. https://doi.org/10.1016/j.brainres.2008.06.053CrossRefGoogle ScholarPubMed
Read, J. P., Ouimette, P., White, J., Colder, C., & Farrow, S. (2011). Rates of DSM-IV-TR trauma exposure and posttraumatic stress disorder among newly matriculated college students. Psychological Trauma: Theory, Research, Practice and Policy, 3(2), 148156. https://doi.org/10.1037/a0021260CrossRefGoogle ScholarPubMed
Sartor, C. E., McCutcheon, V. V., Nelson, E. C., Duncan, A. E., Bucholz, K. K., & Heath, A. C. (2012). Investigating the association between childhood sexual abuse and alcohol use disorders in women: Does it matter how we ask about sexual abuse? Journal of Studies on Alcohol and Drugs, 73(5), 740748. https://doi.org/10.15288/jsad.2012.73.740CrossRefGoogle ScholarPubMed
Sartor, C. E., McCutcheon, V. V., Pommer, N. E., Nelson, E. C., Grant, J. D., Duncan, A. E., … Heath, A. C. (2011). Common genetic and environmental contributions to post-traumatic stress disorder and alcohol dependence in young women. Psychological Medicine, 41(7), 14971505. https://doi.org/10.1017/S0033291710002072CrossRefGoogle ScholarPubMed
Schückher, F., Sellin, T., Fahlke, C., & Engström, I. (2018). The impact of childhood maltreatment on age of onset of alcohol use disorder in women. European Addiction Research, 24(6), 278285. https://doi.org/10.1159/000494766CrossRefGoogle ScholarPubMed
Segalowitz, S. J., Santesso, D. L., & Jetha, M. K. (2010). Electrophysiological changes during adolescence: A review. Brain and Cognition, 72(1), 86100. https://doi.org/10.1016/j.bandc.2009.10.003CrossRefGoogle ScholarPubMed
Sharma, R., & Nadkarni, S. (2020). Biophysical basis of alpha rhythm disruption in Alzheimer's disease. eNeuro, 7(2), ENEURO.0293-19.2020. https://doi.org/10.1523/ENEURO.0293-19.2020CrossRefGoogle ScholarPubMed
Sheerin, C. M., Bountress, K. E., Meyers, J. L., Saenz de Viteri, S. S., Shen, H., Maihofer, A. X., … Amstadter, A. B. (2020). Shared molecular genetic risk of alcohol dependence and posttraumatic stress disorder (PTSD). Psychology of Addictive Behaviors, 34(5), 613619. https://doi.org/10.1037/adb0000568CrossRefGoogle ScholarPubMed
Shu, X.-J., Xue, L., Liu, W., Chen, F.-Y., Zhu, C., Sun, X.-H., … Zhao, H. (2013). More vulnerability of left than right hippocampal damage in right-handed patients with post-traumatic stress disorder. Psychiatry Research: Neuroimaging, 212(3), 237244. https://doi.org/10.1016/j.pscychresns.2012.04.009CrossRefGoogle ScholarPubMed
Silbereis, J. C., Pochareddy, S., Zhu, Y., Li, M., & Sestan, N. (2016). The cellular and molecular landscapes of the developing human central nervous system. Neuron, 89(2), 248268. https://doi.org/10.1016/j.neuron.2015.12.008CrossRefGoogle ScholarPubMed
Smit, D. J. A., Andreassen, O. A., Boomsma, D. I., Burwell, S. J., Chorlian, D. B., de Geus, E. J. C., … Wright, M. J. (2021). Large-scale collaboration in ENIGMA-EEG: A perspective on the meta-analytic approach to link neurological and psychiatric liability genes to electrophysiological brain activity. Brain and Behavior, 11(8), e02188. https://doi.org/10.1002/brb3.2188CrossRefGoogle ScholarPubMed
Stark, E. A., Parsons, C. E., Van Hartevelt, T. J., Charquero-Ballester, M., McManners, H., Ehlers, A., … Kringelbach, M. L. (2015). Post-traumatic stress influences the brain even in the absence of symptoms: A systematic, quantitative meta-analysis of neuroimaging studies. Neuroscience & Biobehavioral Reviews, 56, 207221. https://doi.org/10.1016/j.neubiorev.2015.07.007CrossRefGoogle ScholarPubMed
Stein, M. B., Koverola, C., Hanna, C., Torchia, M. G., & McCLARTY, B. (1997). Hippocampal volume in women victimized by childhood sexual abuse. Psychological Medicine, 27(4), 951959. https://doi.org/10.1017/S0033291797005242CrossRefGoogle ScholarPubMed
Stewart, J. L., Towers, D. N., Coan, J. A., & Allen, J. J. B. (2011). The oft-neglected role of parietal EEG asymmetry and risk for major depressive disorder. Psychophysiology, 48(1), 8295. https://doi.org/10.1111/j.1469-8986.2010.01035.xCrossRefGoogle ScholarPubMed
Subbie-Saenz de Viteri, S., Pandey, A., Pandey, G., Kamarajan, C., Smith, R., Anokhin, A., … Meyers, J. L. (2020). Pathways to post-traumatic stress disorder and alcohol dependence: Trauma, executive functioning, and family history of alcoholism in adolescents and young adults. Brain and Behavior, 10(11), e01789. https://doi.org/10.1002/brb3.1789CrossRefGoogle ScholarPubMed
Tauscher, J., Fischer, P., Neumeister, A., Rappelsberger, P., & Kasper, S. (1998). Low frontal electroencephalographic coherence in neuroleptic-free schizophrenic patients. Biological Psychiatry, 44(6), 438447. https://doi.org/10.1016/s0006-3223(97)00428-9CrossRefGoogle ScholarPubMed
Tcheslavski, G. V., & Gonen, F. F. (2012). Alcoholism-related alterations in spectrum, coherence, and phase synchrony of topical electroencephalogram. Computers in Biology and Medicine, 42(4), 394401. https://doi.org/10.1016/j.compbiomed.2011.12.006CrossRefGoogle ScholarPubMed
Teicher, M. H., Andersen, S. L., Polcari, A., Anderson, C. M., Navalta, C. P., & Kim, D. M. (2003). The neurobiological consequences of early stress and childhood maltreatment. Neuroscience and Biobehavioral Reviews, 27(1–2), 3344. https://doi.org/10.1016/s0149-7634(03)00007-1CrossRefGoogle ScholarPubMed
Teicher, M. H., Ito, Y., Glod, C. A., Andersen, S. L., Dumont, N., & Ackerman, E. (1997). Preliminary evidence for abnormal cortical development in physically and sexually abused children using EEG coherence and MRIa. Annals of the New York Academy of Sciences, 821(1), 160175. https://doi.org/10.1111/j.1749-6632.1997.tb48277.xCrossRefGoogle Scholar
Teicher, M. H., & Samson, J. A. (2013). Childhood maltreatment and psychopathology: A case for ecophenotypic variants as clinically and neurobiologically distinct subtypes. The American Journal of Psychiatry, 170(10), 11141133. https://doi.org/10.1176/appi.ajp.2013.12070957CrossRefGoogle ScholarPubMed
Teicher, M. H., & Samson, J. A. (2016). Annual research review: Enduring neurobiological effects of childhood abuse and neglect. Journal of Child Psychology and Psychiatry, and Allied Disciplines, 57(3), 241266. https://doi.org/10.1111/jcpp.12507CrossRefGoogle ScholarPubMed
Thatcher, R. W., North, D. M., & Biver, C. J. (2008). Development of cortical connections as measured by EEG coherence and phase delays. Human Brain Mapping, 29(12), 14001415. https://doi.org/10.1002/hbm.20474CrossRefGoogle ScholarPubMed
van Rooij, S. J. H., Stevens, J. S., Ely, T. D., Hinrichs, R. C., Michopoulos, V., Winters, S. J., … Jovanovic, T. (2018). The role of the hippocampus in predicting future PTSD symptoms in recently traumatized civilians. Biological Psychiatry, 84(2), 106115. https://doi.org/10.1016/j.biopsych.2017.09.005CrossRefGoogle ScholarPubMed
Xian, H., Chantarujikapong, S. I., Scherrer, J. F., Eisen, S. A., Lyons, M. J., Goldberg, J., … True, W. R. (2000). Genetic and environmental influences on posttraumatic stress disorder, alcohol and drug dependence in twin pairs. Drug and Alcohol Dependence, 61(1), 95102. https://doi.org/10.1016/S0376-8716(00)00127-7CrossRefGoogle ScholarPubMed
Zhang, H., Geng, X., Wang, Y., Guo, Y., Gao, Y., Zhang, S., … Wang, L. (2021). The significance of EEG alpha oscillation spectral power and beta oscillation phase synchronization for diagnosing probable Alzheimer disease. Frontiers in Aging Neuroscience, 13, 631587. https://doi.org/10.3389/fnagi.2021.631587CrossRefGoogle ScholarPubMed
Zinn, M. L., Zinn, M. A., & Jason, L. A. (2016). Intrinsic functional hypoconnectivity in core neurocognitive networks suggests central nervous system pathology in patients with myalgic encephalomyelitis: A pilot study. Applied Psychophysiology and Biofeedback, 41(3), 283300. https://doi.org/10.1007/s10484-016-9331-3CrossRefGoogle ScholarPubMed
Figure 0

Figure 1. This flowchart illustrates the COGA assessments used in the present study. Gray bars represent data collected in COGA, and black bars and white ‘X’ represent assessment waves used in the current study. The analytic sample was limited to individuals aged 12–16 at baseline.

Figure 1

Figure 2. This figure displays a schematic of bipolar electrode pairs (indicated by black dotted lines) and coherence pairs (indicated by black solid lines) derived between bipolar electrode pairs.

Figure 2

Figure 3. This figure displays a path diagram of the latent growth curve model used to evaluate the association between childhood trauma and intercept and slope of EEG coherence, as well as associations between EEG coherence intercept and slope with AUD symptoms. In the trauma-exposed subsample, PTSD symptoms were also examined as a dependent variable, with the correlation between AUD and PTSD symptoms accounted for by the model. Growth curves were estimated based on individually varying age at the time of each EEG coherence observation. Parental education was included as a covariate. Note: CNAT, Childhood non-assaultive trauma; CSAT, Childhood sexual assaultive trauma; CPAT, Childhood physical assaultive trauma; EEGc, EEG coherence.

Figure 3

Table 1. Descriptive information for demographic, alcohol-related, and trauma-related characteristics of the sample

Figure 4

Table 2. Results of the unconditional linear growth model for repeated measures of three frontal alpha EEG coherence Pairs in adolescent male and female COGA participants

Figure 5

Table 3. Linear growth model results for the effect of childhood trauma exposure on slope and intercept of three frontal alpha EEG coherence Pairs and subsequent AUD symptoms in adolescent male and female COGA participants

Figure 6

Table 4. Linear growth model results measuring associations between slope and intercept of three frontal alpha EEG coherence pairs and subsequent AUD symptoms in the trauma-exposed subsample of adolescent male and female COGA participants

Supplementary material: File

Neale et al. supplementary material

Neale et al. supplementary material
Download Neale et al. supplementary material(File)
File 13.9 KB