Increased amygdala responses to emotional faces after psilocybin for treatment-resistant depression

Psychedelics work differently than SSRIs and are hypothesized to treat the underlying disconnect with emotions, getting someone in touch with them again. This analysis of an open-label study (n=20) supports this argument with fMRI studies that showed increased amygdala responses to emotional stimuli.

Abstract of Increased amygdala responses to emotional faces after psilocybin for treatment-resistant depression

“Recent evidence indicates that psilocybin with psychological support may be effective for treating depression. Some studies have found that patients with depression show heightened amygdala responses to fearful faces and there is reliable evidence that treatment with SSRIs attenuates amygdala responses (Ma, 2015). We hypothesised that amygdala responses to emotional faces would be altered post-treatment with psilocybin. In this open-label study, 20 individuals diagnosed with moderate to severe, treatment-resistant depression, underwent two separate dosing sessions with psilocybin. Psychological support was provided before, during and after these sessions and 19 completed fMRI scans one week prior to the first session and one day after the second and last. Neutral, fearful and happy faces were presented in the scanner and analyses focused on the amygdala. Group results revealed rapid and enduring improvements in depressive symptoms post-psilocybin. Increased responses to fearful and happy faces were observed in the right amygdala post-treatment, and right amygdala increases to fearful versus neutral faces were predictive of clinical improvements at 1-week. Psilocybin with psychological support was associated with increased amygdala responses to emotional stimuli, an opposite effect to previous findings with SSRIs. This suggests fundamental differences in these treatments’ therapeutic actions, with SSRIs mitigating negative emotions and psilocybin allowing patients to confront and work through them. Based on the present results, we propose that psilocybin with psychological support is a treatment approach that potentially revives emotional responsiveness in depression, enabling patients to reconnect with their emotions.:

Authors: Leor Roseman, Lysia Demetriou, Matthew B. Wall, David J. Nutt & Robin L. Carhart-Harris

Notes on Increased amygdala responses to emotional faces after psilocybin for treatment-resistant depression

This paper is a follow-up/further analysis of Carhart-Harris and colleagues (2016).

  • Opposite amygdala response between psychedelics (increased) and SSRIs (decreased)
  • Hypothesized to show patients (with unipolar depression) reconnecting with their emotions
  • Right amygdala responses (after treatment) were predictive of clinical improvements at 1-week later

“Increased post-treatment BOLD responses were observed in the right amygdala for fearful (p=.001) and happy faces (p=.022), with a trend effect for neutral faces (p=.066). After correcting for 10 tests (5 contrasts X 2 ROIs), only the increased responses to fearful faces remained significant.”

The researchers note that all these changes are in the right amygdala and no significant change is found in the left amygdala.

The amygdala is a complex subcortical structure that is sensitive to emotional stimuli. Functional MRI studies of untreated clinically depressed patients have found amygdala hyper-sensitivity to negative emotional stimuli, and treatment with SSRIs has been found to attenuate this; both with chronic SSRI-use as well as early in treatment, prior to the appearance of clinical improvements.”

SSRIs seem to dampen these hyper-sensitive responses. They found that psychedelics didn’t have this effect, but in some cases even enhanced the responsitivity (fearful faces, right amygdala). What they challenge with this finding is the hypothesis that a lower response is indicative of lower depression scores. There may be different ways/methods to lowering depression scores, one in which amygdala responses are lowered (SSRIs, and affect in general is lowered), and another in which it’s raised (partly, psychedelics, connect with emotions).

“…SSRIs and related antidepressants have a more generalised muting influence on amygdala responses to emotionally salient stimuli. Relatedly, negative stimuli may be processed as especially salient, and thus be associated with greater amygdala responses which are subsequently hyper-sensitive to intervention-led change.

“Since the majority of patients reported improvements with the treatment, most answered in the affirmative and described a greater willingness to accept all emotions post-treatment (including negative ones). These effects were often contrasted with those of their previous depression treatments which they described as working to reinforce emotional avoidance and disconnection.”

This further supports the above point of connecting patients to their emotions.

In the final part of the discussion, the authors point out various limitations and future directions for research. These include suggestions for more fMRI moments (during, 1 week after, 1 month after) and comparisons with other subject groups (e.g. healthy normals) and with a placebo.

Summary of Increased amygdala responses to emotional faces after psilocybin for treatment-resistant depression

Psychedelic therapy is a re-emerging paradigm in psychiatry that seeks to treat core psychological issues via a small number of profound and potentially transformative psychological experiences. It has shown promising results in treating treatment-resistant depression.

The amygdala is a complex subcortical structure that is sensitive to emotional stimuli. Treatment with SSRIs has been found to attenuate amygdala hyper-sensitivity to negative emotional stimuli.

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Find this paper

Increased amygdala responses to emotional faces after psilocybin for treatment-resistant depression

https://doi.org/10.1016/j.neuropharm.2017.12.041

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Cite this paper (APA)

Roseman, L., Demetriou, L., Wall, M. B., Nutt, D. J., & Carhart-Harris, R. L. (2018). Increased amygdala responses to emotional faces after psilocybin for treatment-resistant depression. Neuropharmacology142, 263-269.

Study details

Compounds studied
Psilocybin

Topics studied
Neuroscience Depression Treatment-Resistant Depression

Study characteristics
Original Re-analysis Open-Label Re-analysis

Participants
20 Humans

Authors

Authors associated with this publication with profiles on Blossom

Leor Roseman
Leor Roseman is a researcher at the Centre for Psychedelic Research, Imperial College London. His work focussed on psilocybin for depression, but is now related to peace-building through psychedelics.

David Nutt
David John Nutt is a great advocate for looking at drugs and their harm objectively and scientifically. This got him dismissed as ACMD (Advisory Council on the Misuse of Drugs) chairman.

Jeronimo Beccar
Jeronimo Beccar is Co-Founder and CEO at Hyka.

Institutes

Institutes associated with this publication

Imperial College London
The Centre for Psychedelic Research studies the action (in the brain) and clinical use of psychedelics, with a focus on depression.

Compound Details

The psychedelics given at which dose and how many times

Psilocybin 10 - 25
mg | 2x

Linked Research Papers

Notable research papers that build on or are influenced by this paper

Psilocybin with psychological support for treatment-resistant depression: an open-label feasibility study
This is the first modern study (n=12) on psilocybin and its effects on treatment-resistant depression (TRD). It shows that two sessions with psilocybin (10mg and 25mg) in combination with psychological support can reduce depressive symptoms over periods of one week to three months after treatment. Psilocybin was well tolerated by all of the patients, and no serious or unexpected adverse events occurred.

Linked Clinical Trial

Assessing the subjective intensity of oral psilocybin in patients with treatment-resistant depression: A Pilot Study (PSILODEP-PILOT)
This open-label trial (n=12), also known as PSILODEP-PILOT is the first to test psilocybin in patients in the UK. The study found psilocybin (10-25mg, x2) to be well-tolerated.

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