20.04.2024

Brain Biomarkers May Help Predict Risk of Severe PTSD

PTSD is a disorder that can sometimes develop after exposure to a traumatic event. People with PTSD may experience intrusive and frightening thoughts and memories of the event, experience sleep problems, feel detached or numb, or may be easily startled.

A new study suggests the severity of symptoms associated with post-traumatic stress disorder appears to be linked to individual brain wiring and the way the brain is tuned to respond to negative surprises.

In the study of combat veterans, researchers discovered distinct patterns for how the brain and body respond to learning danger and safety depending on the severity of PTSD symptoms. The findings of the study, funded in part by the National Institute of Mental Health, part of the National Institutes of Health, could help explain why symptoms of PTSD can be severe for some people but not others.

“Researchers have thought that the experience of PTSD, in many ways, is an overlearned response to survive a threatening experience,” said Susan Borja, Ph.D., chief of the National Institute of Mental Health Dimensional Traumatic Stress Research Program.

“This study clarifies that those who have the most severe symptoms may appear behaviorally similar to those with less severe symptoms, but are responding to cues in subtly different, but profound, ways.”

Insightfully, researchers explain that while almost half of all U.S. adults will experience a traumatic event in their life, most do not develop PTSD.

One theory explaining why some symptoms of PTSD develop suggests that during a traumatic event, a person may learn to view the people, locations, and objects that are present as being dangerous, if they become associated with the threatening situation.

While some of these things may be dangerous, some are safe. PTSD symptoms result when these safe stimuli continue to trigger fearful and defensive responses long after the trauma has occurred.

Despite the prominence of this theory, the way in which this learning occurs is not well understood.

In the new study, Ilan Harpaz-Rotem, Ph.D., associate professor of psychiatry at Yale University, Daniela Schiller, Ph.D., associate professor of psychiatry and neuroscience at the Icahn School of Medicine, and colleagues examined how mental adjustments performed during learning, and the way in which the brain tracks these adjustments, relate to PTSD symptom severity.

Combat veterans with varying levels of PTSD symptom severity completed a reversal learning task in which two mildly angry human faces were paired with a mildly aversive stimulus. During the first phase of this task, participants learned to associate one face with the mildly aversive stimulus.

During the second phase of this task this association was reversed, and participants learned to associate the second face with the mildly aversive stimulus.

Although all participants (those with minimal and severe symptoms) were able to perform the reversal learning, when the researchers took a closer look at the data, they found a difference response among highly symptomatic veterans.

This group responded with greater corrections in their physiological arousal (i.e., skin conductance responses) and brain region activity than what they had expected.

The amygdala, a brain area involved in associative learning, value encoding, and emotional responses, was particularly important. Both smaller amygdala volume and less precise tracking of the negative value of the face stimuli in the amygdala independently predicted PTSD symptom severity.

Differences in value tracking and associability were also found in other brain regions involved in computation related to threat learning, such as the striatum, the hippocampus, and the dorsal anterior cingulate cortex.

“What these results tell us is that PTSD symptom severity is reflected in how combat veterans respond to negative surprises in the environment —when predicted outcomes are not as expected — and the way in which the brain is attuned to these stimuli is different,” said Schiller.

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