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Threat bias interacts with combat, gene to boost PTSD risk

Israeli soldiers tracked through deployment to ID predictors -- NIH study

Threat bias interacts with combat, gene to boost PTSD risk
2013-02-14
(Press-News.org) Soldiers preoccupied with threat at the time of enlistment or with avoiding it just before deployment were more likely to develop post-traumatic stress disorder (PTSD), in a study of Israeli infantrymen. Such pre-deployment threat vigilance and avoidance, interacting with combat experience and an emotion-related gene, accounted for more than a third of PTSD symptoms that emerged later, say National Institutes of Health scientists, who conducted the study in collaboration with American and Israeli colleagues.

"Since biased attention predicted future risk for PTSD, computerized training that helps modify such attention biases might help protect soldiers from the disorder," said Daniel Pine, M.D., of the NIH's National Institute of Mental Health (NIMH).

Pine, Yair Bar-Haim, Ph.D., of Tel Aviv University, and colleagues, report their findings, Feb. 13, 2013, in the journal JAMA Psychiatry.

Bar-Haim's team tracked 1085 male Israeli soldiers from recruitment through combat deployment during 2008-2010, to pinpoint how shifting attitudes toward threat interact with other factors to predict symptoms that develop after exposure to dangers. They expected that the more soldiers paid attention to avoiding threats just before and during deployment, the more they would suffer PTSD symptoms.

Researchers measured threat attention biases over the course of soldiers' first year of service: at the time of recruitment, about six months later – just before deployment to combat – and six months after deployment. Data from all three time points was collected for 487 of the soldiers.

Soldiers performed a computerized task that required paying attention to locations of neutral words, such as "data" or threatening words, such as "dead." A faster reaction time for identifying the location of threat words indicated increased threat vigilance. Slower reaction times to such word locations indicated attention away from threat, or threat avoidance.

The study also examined how threat attention bias vulnerability might be moderated by other factors, including the gene that codes for the protein on neurons that recycles the brain chemical messenger serotonin from the synapse. Versions of this serotonin transporter gene had been previously linked to PTSD risk. Evidence suggests that people with gene versions that result in less efficient recycling may be overly vigilant toward threats under normal circumstances. Yet there is also evidence that having these low-efficiency versions may help people cope with dangerous conditions, when such heightened vigilance may be adaptive.

As expected, soldiers who experienced higher combat exposure – e.g., served in units operating outside Israel's security fence – tended to show more threat vigilance than those with less stressful assignments. Compared to soldiers who were neither vigilant nor avoidant, soldiers with greater vigilance at recruitment or avoidance at six months – on the eve of deployment – had more PTSD symptoms at the end of their first year of service.

Although serotonin gene type had no direct effect on symptoms, the low efficiency gene version, combined with high threat vigilance, appeared to confer some protection to soldiers who experienced high combat exposure.

"Their natural tendency to attend to threats may lead to less adaptive emotional responses and elevated anxiety when environmental conditions are safe and stable, but to perfectly normal and adaptive responses in combat, where vigilance toward minor threats is crucial for survival," explained Pine.

Bias toward threats showed no such association with PTSD symptoms in those with the high efficiency version of the gene. Nor did gene type interact with threat bias to predict PTSD in solders with low combat exposure. Similarly, among the low combat exposure group, a history of traumatic experiences, self-reported combat experience, threat bias or gene type had no bearing on PTSD symptoms.

Higher pre-deployment PTSD symptoms and failure to complete high school also predicted higher post-deployment PTSD risk.

"Extreme adaptation challenges, such as those arising from soldiers' shifting exposures to relatively safe and acutely hostile environments, may produce shifting psychological and behavioral symptoms of hyper-vigilance and avoidance," explained the researchers.

They propose that computer-based attention bias modification techniques (see below) be tested in both soldiers prior to deployment as well as in PTSD patients, in combination with evidence-based cognitive therapies.



INFORMATION:

Reference:

Wald I, Degnan KA, Gorodetsky E, Charney DS, Fox NA, Fruchter E, Goldman D, Lubin G, Pine DS, Bar-Haim Y. Attention to Threats and Combat-Related Post-Traumatic Stress Symptoms: Prospective Associations and Moderation by the Serotonin Transporter Gene. JAMA Psychiatry, Feb. 13, 2013.

VIDEO:

NIMH's Dr. Daniel Pine explains how the study in Israeli soldiers helps to identify factors involved in stress resilience to PTSD. http://www.youtube.com/watch?v=7jdYj6_-OG0

The mission of the NIMH is to transform the understanding and treatment of mental illnesses through basic and clinical research, paving the way for prevention, recovery and cure. For more information, visit http://www.nimh.nih.gov.

About the National Institutes of Health (NIH): NIH, the nation's medical research agency, includes 27 Institutes and Centers and is a component of the U.S. Department of Health and Human Services. NIH is the primary federal agency conducting and supporting basic, clinical, and translational medical research, and is investigating the causes, treatments, and cures for both common and rare diseases. For more information about NIH and its programs, visit http://www.nih.gov.


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Threat bias interacts with combat, gene to boost PTSD risk

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[Press-News.org] Threat bias interacts with combat, gene to boost PTSD risk
Israeli soldiers tracked through deployment to ID predictors -- NIH study