Magic mushrooms may 'reset' the brains of depressed patients

Authored by www3.imperial.ac.uk and submitted by ImperialCollege
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Patients taking psilocybin to treat depression show reduced symptoms weeks after treatment following a 'reset' of their brain activity.

The findings come from a study in which researchers from Imperial College London used psilocybin – the psychoactive compound that occurs naturally in magic mushrooms – to treat a small number of patients with depression in whom conventional treatment had failed.

In a paper, published in the journal Scientific Reports, the researchers describe patient-reported benefits lasting up to five weeks after treatment, and believe the psychedelic compound may effectively reset the activity of key brain circuits known to play a role in depression.

Comparison of images of patients’ brains before and one day after they received the drug treatment revealed changes in brain activity that were associated with marked and lasting reductions in depressive symptoms.

The authors note that while the initial results of the experimental therapy are exciting, they are limited by the small sample size as well as the absence of a control group – such as a placebo group – to directly contrast with the patients.

Dr Robin Carhart-Harris, Head of Psychedelic Research at Imperial, who led the study, said: “We have shown for the first time clear changes in brain activity in depressed people treated with psilocybin after failing to respond to conventional treatments.

“Several of our patients described feeling ‘reset’ after the treatment and often used computer analogies. For example, one said he felt like his brain had been ‘defragged’ like a computer hard drive, and another said he felt ‘rebooted’.

"Psilocybin may be giving these individuals the temporary ‘kick start’ they need to break out of their depressive states and these imaging results do tentatively support a ‘reset’ analogy. Similar brain effects to these have been seen with electroconvulsive therapy.”

Over the last decade or so, a number of clinical trials have been conducted into the safety and effectiveness of psychedelics in patients with conditions such as depression and addictions, yielding promising results.

In the recent Imperial trial, the first with psilocybin in depression, 20 patients with treatment-resistant form of the disorder were given two doses of psilocybin (10 mg and 25 mg), with the second dose a week after the first. Nineteen of these underwent initial brain imaging and then a second scan one day after the high dose treatment.

Carhart-Harris and team used two main brain imaging methods to measure changes in blood flow and the crosstalk between brain regions, with patients reporting their depressive symptoms through completing clinical questionnaires.

Immediately following treatment with psilocybin, patients reported a decrease in depressive symptoms – corresponding with anecdotal reports of an ‘after-glow’ effect characterised by improvements in mood and stress relief.

Functional MRI imaging revealed reduced blood flow in areas of the brain, including the amygdala, a small, almond-shaped region of the brain known to be involved in processing emotional responses, stress and fear. They also found increased stability in another brain network, previously linked to psilocybin’s immediate effects as well as to depression itself.

Psilocybin may be giving these individuals the temporary ‘kick start’ they need to break out of their depressive states – Dr Robin Carhart-Harris Lead author

These findings provide a new window into what happens in the brains of people after they have ‘come down’ from a psychedelic, where an initial disintegration of brain networks during the drug ‘trip’, is followed by a re-integration afterwards.

Dr Carhart-Harris explained: “Through collecting these imaging data we have been able to provide a window into the after effects of psilocybin treatment in the brains of patients with chronic depression.

"Based on what we know from various brain imaging studies with psychedelics, as well as taking heed of what people say about their experiences, it may be that psychedelics do indeed ‘reset’ the brain networks associated with depression, effectively enabling them to be lifted from the depressed state."

The authors warn that while the initial findings are encouraging, the research is at an early stage and that patients with depression should not attempt to self-medicate, as the team provided a special therapeutic context for the drug experience and things may go awry if the extensive psychological component of the treatment is neglected.

They add that future studies will include more robust designs and currently plan to test psilocybin against a leading antidepressant in a trial set to start early next year.

Professor David Nutt, Edmond J. Safra Professor of Neuropsychopharmacology and director of the Neuropsychopharmacology Unit in the Division of Brain Sciences, and senior author of the paper, added: “Larger studies are needed to see if this positive effect can be reproduced in more patients. But these initial findings are exciting and provide another treatment avenue to explore.”

The research was supported by the Medical Research Council, the Alex Mosley Charitable Trust and the Safra Foundation.

‘Psilocybin for treatment-resistant depression: fMRI-measured brain mechanisms’ by Carhart-Harris, R, et al. is published in the journal Scientific Reports.

Main article image: Carhart-Harris, R, et al. Scientific Reports.

Image two: Robin Carhart-Harris (Imperial College London / Thomas Angus)

Kossimer on October 13rd, 2017 at 21:33 UTC »

How much my problems and loneliness were really hurting me were only made clear by my first trip on shrooms. I became overwhelmed with the desire to run, or dance, or climb, and climb onto the roof of a park bathroom I did (staying still was simply not an option, very different to how I am normally), where I layed for hours and had a much needed cry. The obviousness of how I simply needed to change my behavior was revealed, and it felt so easy to do. I felt more sober than I had my entire life (besides watching the moon smear across the sky. Is okay though, it stopped whenever I told it to hush).

I found an impressive staff-looking stick up there and I just twirled it and thought. Shrooms guide pathways of thought forward that you've intentionally or unintentionally buried deep down and ignored. You can't choose to not think about what's on your mind when you're on shrooms. I'm very introverted and it changed something inside me; I felt an abundance of true extrovertism for the first time, instead of just feigning it for the sake of my social life. I actually wanted to dance. I'm jealous of you guys btw, being an extrovert is fun as hell.

Anyway, all of my unhealthy inhibitions were gone. While I still have them, they're better, and shrooms unapologetically made it so clear that they were me and not the world around me. I could choose to keep behaving this way if I wanted. None of this is experienced in words, just pure understanding inside your own mind, so all these words don't do it justice at all. It's been over a year and I feel like I've slumped back into my usual self more than I should have. I think I'm due for another treatment, which is exactly what it can be when used responsibly. Speaking of, I did have an experienced friend with me. He was just cold and wanted to stay in his sleeping bag while I had this experience. Please don't take them alone, especially the first time.

Tr3v3336 on October 13rd, 2017 at 20:16 UTC »

Is there any evidence that there is a decrease in depression when using lower doses? I have dealt with depression for a long time and I would like to try this, but I don't necessarily want to trip the hell out. 10-25g is a pretty large amount.

Edit: I was thinking grams didn't see the article said mg.

ImperialCollege on October 13rd, 2017 at 12:24 UTC »

If you’re interested, the full journal article (‘Psilocybin for treatment-resistant depression: fMRI-measured brain mechanisms’) can be read here: https://www.nature.com/articles/s41598-017-13282-7