The AURORA Study: a longitudinal, multimodal library of brain biology and function after traumatic stress exposure

McLean, Samuel A.; Ressler, Kerry J.; Koenen, Karestan C.; Neylan, Thomas C.; Germine, Laura; Jovanović, Tanja; Clifford, Gari D.; Zeng, Donglin; An, Xiuli; Linnstaedt, Sarah D.; Beaudoin, Francesca L.; House, Stacey L.; Bollen, Kenneth A.; Musey, Paul I.; Hendry, Phyllis L.; Jones, Christopher W.; Lewandowski, Christopher; Swor, Robert A.; Datner, Elizabeth M.; Mohiuddin, Kamran; Stevens, Jennifer; Storrow, Alan B.; Kurz, Michael C.; McGrath, Meghan E.; Fermann, Gregory J.; Hudak, Lauren A.; Gentile, Nina; Chang, Anna Marie; Peak, David A.; Pascual, José L.; Seamon, Mark J.; Sergot, Paulina; Peacock, W. Frank; Diercks, Deborah; Sánchez, León D.; Rathlev, Niels K.; Domeier, Robert M.; Haran, John P.; Pearson, Claire; Murty, Vishnu P.; Insel, Thomas R.; Dagum, Paul; Onnela, Jukka Pekka; Bruce, Steven E.; Gaynes, Bradley N.; Joormann, Jutta; Miller, Mark W.; Pietrzak, Robert H.; Buysse, Daniel J.; Pizzagalli, Diego A.; Rauch, Scott L.; Harte, Steven E.; Young, Larry J.; Deanna, M; Lebois, Lauren A. M.; Rooij, Sanne J.H. van; Luna, Beatríz; Smoller, Jordan W.; Dougherty, Robert F.; Pace, Thaddeus W.W.; Binder, Elisabeth B.; Sheridan, John F.; Elliott, James M.; Basu, Archana; Fromer, Menachem; Parlikar, T.A.; Zaslavsky, Alan M.; Kessler, Ronald C.

doi:10.1038/s41380-019-0581-3

Cited by 119 publications

(140 citation statements)

References 41 publications

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“… 141 These different symptom profiles may also have differences in their potential etiologies and biomarker profiles, thus examining PTSD and other APNS as single diagnostic categories may severely limit our ability to discover reliable biomarkers. However, as the field moves towards a more succinct definition of APNS outcomes that better characterize the full symptom profiles of trauma survivors (versus traditional syndromic classifications studied in isolation) 4 , we will increase our ability to identify accurate target groups to which blood-based risk biomarkers can more specifically identify vulnerable individuals.…”

Section: Challenges To the Discovery Of Circulating Risk Biomarkers Omentioning

confidence: 99%

“…Using this data, AURORA investigators and other individuals in the research community can improve outcome phenotypes, develop prediction tools, and improve understanding of molecular mechanisms driving APNS. For a more detailed description of the full study, please refer to the AURORA methods paper 4 .…”

Section: The Promise Of the Aurora Study To Identify Circulating Riskmentioning

confidence: 99%

“…While many individuals recover following trauma exposure, a substantial subset develop adverse posttraumatic neuropsychiatric sequelae (APNS). APNS, as previously defined 4 , can include a wide range of neuropsychiatric outcomes; three of the most common APNS are posttraumatic stress (PTS), major depression, and regional or widespread chronic musculoskeletal pain (CMP). These APNS cause tremendous suffering, functional impairment, high health care costs, and are a leading cause of disability among current and former members of the armed forces.…”

Section: Introductionmentioning

confidence: 99%

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Literature review and methodological considerations for understanding circulating risk biomarkers following trauma exposure

et al. 2019

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Exposure to traumatic events is common. While many individuals recover following trauma exposure, a substantial subset develop adverse posttraumatic neuropsychiatric sequelae (APNS) such as posttraumatic stress, major depression, and regional or widespread chronic musculoskeletal pain. APNS cause substantial burden to the individual and to society, causing functional impairment and physical disability, risk for suicide, lost workdays, and increased health care costs. Contemporary treatment is limited by an inability to identify individuals at high risk of APNS in the immediate aftermath of trauma, and an inability to identify optimal treatments for individual patients. Our purpose is to provide a comprehensive review describing candidate blood-based biomarkers that may help to identify those at high risk of APNS and/or guide individual intervention decision-making. Such blood-based biomarkers include circulating biological factors such as hormones, proteins, immune molecules, neuropeptides, neurotransmitters, mRNA and noncoding RNA expression signatures, while we do not review genetic and epigenetic biomarkers due to other recent reviews of this topic. The current state of the literature on circulating risk biomarkers of APNS is summarized, and key considerations and challenges for their discovery and translation are discussed. We also describe the AURORA study, a specific example of current scientific efforts to identify such circulating risk biomarkers and the largest study to date focused on identifying risk and prognostic factors in the aftermath of trauma exposure.

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Section: Challenges To the Discovery Of Circulating Risk Biomarkers Omentioning

confidence: 99%

Section: The Promise Of the Aurora Study To Identify Circulating Riskmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Literature review and methodological considerations for understanding circulating risk biomarkers following trauma exposure

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“…worry that I might be mentally ill") were selected to match those used in a large-scale U.S. National Institute of Mental Healthfunded study of trauma survivors (McLean et al, 2019). In the current study, the possible score range for the brief ASI was 0-12, with higher scores indicating higher levels of AS.…”

Section: Anxiety Sensitivitymentioning

confidence: 99%

Anxiety Sensitivity Prospectively Predicts Increased Acute Posttraumatic Stress and Related Symptoms After Sexual Assault

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et al. 2020

Journal of Traumatic Stress

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Anxiety sensitivity is a potential risk factor for posttraumatic stress symptoms (PTSS) and has been hypothesized to contribute to PTSS development. However, few prospective studies have evaluated whether anxiety sensitivity predicts PTSS. In a subsample of 48 women sexual assault survivors enrolled as part of a larger prospective observational study, elevated anxiety sensitivity measured via a brief assessment 1 week after experiencing a sexual assault was concurrently associated with PTSS at 1 week and prospectively predicted PTSS 6 weeks after the event, with small-to-medium effect sizes, η 2 p = .10, even after covarying for trauma history. Heightened anxiety sensitivity at 1-week postevent also interacted with time to predict anxiety and depression both before and after sexual assault, with medium-to-large effect sizes, η p 2 = .21-.24. This is consistent with research linking anxiety sensitivity to PTSS, but this was the first prospective study of which we are aware to demonstrate that anxiety sensitivity in the acute posttrauma period predicts PTSS among women who have recently experienced sexual assault. Future research should use the full Anxiety Sensitivity Index to replicate findings in a larger sample and explore whether targeting anxiety sensitivity could mitigate the development of PTSS in this vulnerable population. Nearly 100,000 women in the United States seek emergency care after sexual assault each year (Smith et al., 2018). More than half of women who experience sexual assault develop

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“…The discovery of noninvasive biomarkers for disease is a main goal in contemporary biomedicine 16 . A key emerging question is whether high-dimensional behavioral data can be used for clinical diagnosis 17,18 , particularly in the domain of mental health [19][20][21][22] . Instead of relying on the use of ratings by clinicians or selfreports from patients, the goal is to use objective and quantifiable behavioral data combined with artificial intelligence analyses to predict disease vulnerability or progression.…”

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confidence: 99%

Locomotion in virtual environments predicts cardiovascular responsiveness to subsequent stressful challenges

et al. 2020

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Individuals differ in their physiological responsiveness to stressful challenges, and stress potentiates the development of many diseases. Heart rate variability (HRV), a measure of cardiac vagal break, is emerging as a strong index of physiological stress vulnerability. Thus, it is important to develop tools that identify predictive markers of individual differences in HRV responsiveness without exposing subjects to high stress. Here, using machine learning approaches, we show the strong predictive power of high-dimensional locomotor responses during novelty exploration to predict HRV responsiveness during stress exposure. Locomotor responses are collected in two ecologically valid virtual reality scenarios inspired by the animal literature and stress is elicited and measured in a third threatening virtual scenario. Our model’s predictions generalize to other stressful challenges and outperforms other stress prediction instruments, such as anxiety questionnaires. Our study paves the way for the development of behavioral digital phenotyping tools for early detection of stress-vulnerable individuals.

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The AURORA Study: a longitudinal, multimodal library of brain biology and function after traumatic stress exposure

Cited by 119 publications

References 41 publications

Literature review and methodological considerations for understanding circulating risk biomarkers following trauma exposure

Literature review and methodological considerations for understanding circulating risk biomarkers following trauma exposure

Anxiety Sensitivity Prospectively Predicts Increased Acute Posttraumatic Stress and Related Symptoms After Sexual Assault

Locomotion in virtual environments predicts cardiovascular responsiveness to subsequent stressful challenges

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