Overcoming Long-Term Trauma Can Be Facilitated

Summary: Researchers facilitated the extinction of long-term traumatic memories in mice by enhancing activity in the nucleus reuniens.

Source: EPFL

How the brain deals with trauma is complex, and it’s intuitive to say that we, as humans, get over trauma differently depending on if it happened a long time ago or if it was recent. But what scientific evidence do we have about the way the brain deals with short-term versus long-term traumatic memories?

EPFL scientists have identified the specific regions in the brains of mice responsible for reprograming traumatic experiences towards safety, and the brain regions are indeed different and depend on whether the trauma happened recently or a long time ago. They found that they could facilitate the extinction of long-lasting traumatic memories by enhancing the activity of a primitive region of the brain called the nucleus reuniens.

The results are published today in Nature Neuroscience.

“Traumatic memories are so emotionally charged that they are difficult to ‘erase’ or extinguish. Despite this fact, surprisingly little is known about these long-term traumatic memories,” explains EPFL’s Nestlé Chair Johannes Gräff, principal investigator of the study. “In our study, it’s the first time someone has researched fear extinction at the brain circuit level for long-lasting traumatic memories.”

In 2018, Gräff and his team identified the cells in the brain responsible for reprogramming long-term trauma towards safety, also in mice. The same cell that was activated during a traumatizing experience was also activated after therapy, indicating that the traumatized cell itself was reprogrammed towards safety, giving insight into how the brain deals with trauma at the cellular level.

But Gräff and his team wanted understand how traumatized brain cells were reprogrammed towards safety and if other regions of the brain facilitated this reprogramming. What they found was that the canonical extinction pathway for recent memories is not involved for the extinction of so-called remote or long-term traumatic memories.

The nucleus reuniens facilitates recovery

In the experiment, the mice underwent ‘Pavlovian fear conditioning’, in which they received an electric shock from the ground. A traumatized mouse expresses its fear by freezing, but after the therapy, the mouse regains confidence and normal mobility. One group of mice received therapy 1 day after the trauma, while another group received therapy 30 days later.

The scientists determined which brain circuits were active in both groups of mice. They found that a direct cortico-amygdalar pathway was active 1 day following the trauma, but after 30 days, an indirect pathway was active, one that was rooted in the nucleus reuniens.

This shows a sad looking lady sitting on a bench
They found that they could facilitate the extinction of long-lasting traumatic memories by enhancing the activity of a primitive region of the brain called the nucleus reuniens. Image is in the public domain

“Interestingly, the activity in the reuniens peaked shortly before the mouse ceased to express fear. It’s as if the activity in the reuniens anticipates the end of freezing,” continues Gräff. “When we manipulated the activity of the reuniens, time-locked to these peaks, we saw that it was indeed important for regulating fear. So when we boosted the activity, the mice froze less. When we inhibited it, the mice froze more.”

“That anticipation of when freezing ends is actually probably the most enlightening finding of our research from a purely technical perspective.”

The results provide insight at the brain-circuit level as to why traumatic memories are persistent and harder to extinguish. They shed light on the brain mechanisms involved for recovering from long-term traumatic memories.

Turning this recent discovery into therapy for people suffering from post-traumatic stress disorder or other long-term traumatic experiences that affect mental health remains a challenge. In collaboration with a partner institute in the Netherlands, the scientists currently have approval to study similar brain mechanisms in humans.

About this PTSD research news

Source: EPFL
Contact: Hillary Sanctuary – EPFL
Image: Image is in the public domain

Original Research: Closed access.
A thalamo-amygdalar circuit underlying the extinction of remote fear memories” by Bianca A. Silva, Simone Astori, Allison M. Burns, Hendrik Heiser, Lukas van den Heuvel, Giulia Santoni, Maria Fernanda Martinez-Reza, Carmen Sandi & Johannes Gräff. Nature Neuroscience


Abstract

A thalamo-amygdalar circuit underlying the extinction of remote fear memories

Fear and trauma generate some of the longest-lived memories. Despite the corresponding need to understand how such memories can be attenuated, the underlying brain circuits remain unknown.

Here, combining viral tracing, neuronal activity mapping, fiber photometry, chemogenetic and closed-loop optogenetic manipulations in mice, we show that the extinction of remote (30-day-old) fear memories depends on thalamic nucleus reuniens (NRe) inputs to the basolateral amygdala (BLA). We found that remote, but not recent (1-day-old), fear extinction activates NRe-to-BLA inputs, which become potentiated upon fear reduction.

Furthermore, both monosynaptic NRe-to-BLA and total NRe activity increase shortly before freezing cessation, suggesting that the NRe registers and transmits safety signals to the BLA. Accordingly, pan-NRe and pathway-specific NRe-to-BLA inhibition impairs, whereas their activation facilitates, remote fear extinction.

These findings identify the NRe as a crucial BLA regulator for extinction and provide the first functional description of the circuits underlying the attenuation of consolidated fear memories.

Join our Newsletter
I agree to have my personal information transferred to AWeber for Neuroscience Newsletter ( more information )
Sign up to receive our recent neuroscience headlines and summaries sent to your email once a day, totally free.
We hate spam and only use your email to contact you about newsletters. You can cancel your subscription any time.