Huberman Lab - Dr. Robin Carhart-Harris: The Science of Psychedelics for Mental Health
Episode Date: May 22, 2023In this episode, my guest is Robin Carhart-Harris, PhD, distinguished professor of neurology and psychiatry at the University of California, San Francisco. He is one of leading researchers in the stud...y of how psychedelics such as psilocybin, LSD and DMT can change the human brain and in doing so, be used to successfully treat various mental health challenges such as major depression, anorexia, obsessive-compulsive disorder (OCD) and addiction. He explains how psilocybin induces sustained changes in adaptive brain wiring and cognition. We discuss the key components of safe and effective psychedelic journeys, the role of hallucinations, the use of eye-masks to encourage people to “go internal,” and music, as well as what effective therapist support consists of before, during and after the session (also known as integration). We discuss micodosing vs. macrodosing and how researchers control for placebo effects in psychedelic research. We also discuss the current legal landscape around psychedelic therapies. Psychedelic therapies are fast emerging as powerful and soon-to-be mainstream treatments for medical health disorders, but they are not without their risks. As such, this episode ought to be of use to anyone interested in brain plasticity, mental health, psychology or neuroscience. For the full show notes, visit hubermanlab.com. Thank you to our sponsors AG1 (Athletic Greens): https://athleticgreens.com/huberman Eight Sleep: https://eightsleep.com/huberman Levels: https://levels.link/huberman HVMN: https://hvmn.com/huberman LMNT: https://drinklmnt.com/huberman Momentous: https://www.livemomentous.com/huberman The Brain Body Contract https://hubermanlab.com/tour Timestamps (00:00:00) Dr. Robin Carhart-Harris (00:02:12) Sponsors: Eight Sleep, Levels, HVMN (00:05:41) The Brain-Body Contract (00:06:31) Origin of the Word: “Psychedelics”; Pharmacology (00:12:05) Psychedelics & Revealing the Unconscious Mind, Psychotherapy (00:17:32) Microdosing (00:26:08) Psilocybin vs. Magic Mushroom Doses (00:28:28) “Psychedelic-Therapy”, Music (00:35:12) Sponsor: AG1 (00:36:26) Psychedelic Journey: “Trust, Let Go, Be Open” (00:43:01) Negative Emotions, Fear & Psychedelics (00:46:21) Global Functional Connectivity, Serotonin 2A Receptor; Subjective Experiences (00:52:33) Pharmacology: Therapeutics without Psychedelic Effects; SSRIs (00:58:45) Psilocybin & Depression; Long-Term Effects: Connectivity & Neuroplasticity (01:09:14) Sponsor: LMNT (01:10:26) Psilocybin Therapy & Anorexia (01:12:56) Integration Phase & Psychedelic-Therapy; Meditation (01:19:50) First-Time Psychedelic Use, “Entropic Brain Effect”, Neuroplasticity, Cognition (01:30:16) Fibromyalgia & Psychedelic Treatment; MDMA Therapy & “Inner Healer” (01:38:55) Placebo Response & Psychedelic Therapy (01:41:39) LSD & Psychedelic-Therapy, Micro-Dose (01:48:19) Combination Psilocybin-MDMA Therapy (01:56:06) DMT “Rocketship” & Serotonin 2A Receptors; Ibogaine (02:01:04) “Ego Dissolution”, Cocaine vs. Psychedelics; Relapses (02:12:26) Psychedelics & Legal Landscape; Decriminalization (02:17:54) MDMA, Trauma & Clinical Trials; Future Regulatory (FDA) Approval? (02:23:25) Psilocybin & Current Clinical Trials (02:28:41) Mental Health & Psychedelic Treatment, Safeguards, Paradigm Shift (02:34:39) Zero-Cost Support, YouTube Feedback, Spotify & Apple Reviews, Sponsors, Momentous, Social Media, Neural Network Newsletter Title Card Photo Credit: Mike Blabac Disclaimer
Transcript
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Welcome to the Uberman Lab podcast where we discuss science and science-based tools for everyday life.
I'm Andrew Uberman and I'm a professor of neurobiology and
Ophthalmology at Stanford School of Medicine. Today my guest is Dr. Robin Carrhart Harris.
Dr. Carrhart Harris is a distinguished professor of neurology and psychiatry at the University of California, San Francisco.
of neurology and psychiatry at the University of California, San Francisco. He is one of the leading researchers in the field of psychedelics and how they change
neural circuitry in the brain. His laboratory is responsible for understanding, for instance,
how psilocybin, also sometimes referred to as magic mushrooms, change neural circuitry in the brain,
such that new ideas and new forms of learning occur. His laboratory is also responsible for carrying out various
clinical trials, some of which have demonstrated that appropriate dosages of psilocybin can
alleviate major depression in more than 67% of people that take the drug. Now, this is not to say
that everybody should take psilocybin. And today's discussion describes both the clinical trials
and why treatments with psychedelics in some cases work and in some cases do not work in order to treat major depression.
As well as discussions around psilocybin, lysturgic acid diethylamide, sometimes also referred
to as LSD, as well as DMT, and how these change the brain and how those brain changes can
relate to changes in mental health as it relates to depression and other psychiatric challenges,
as well as how psychedelics are being applied in order to change general circuitry for sake of expanding
different aspects of the human mind, including creativity, intelligence, and much more.
During today's discussion, Dr. Carhartt Harris teaches us about the history of the study of psychedelics,
as well as how the legislature, that is the laws surrounding psychedelics,
are evolving in the United States and elsewhere for the laws surrounding psychedelics, are evolving in the United States
and elsewhere for the use of psychedelics to treat psychiatric challenges. By the end of
today's discussion, you will have a thorough understanding of how psychedelics work,
both in the short term during the actual journey or trip. In fact,
to much of my discussion today with Dr. Karl Harteris talks about the different aspects of
the psychedelic journey and how those relate to therapeutic outcomes.
And of course, by the end of today's discussion, you will also understand the long-term
effects of psychedelics, that is how they can actually rewire the brain.
Before we begin, I'd like to emphasize that this podcast is separate from my teaching
and research roles at Stanford.
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I hope to see you there. And now for my discussion with Dr. Robin Carhartt Harris. Dr. Carhartt
Harris, welcome. I've been wanting to talk to you for a long time. I certainly have known who you
are for quite a while because I place you in this very small, but very special and important category
of researchers who has been pioneering the use of psychedelics for the treatment of specific
clinical conditions and really carrying the torch for essentially the entire field.
So I want to start with a voice of gratitude and say thank you for doing this incredibly
important work.
Could you tell us a little bit about what psychedelics are?
In fact, I'm curious as to how the name psychedelic ever came to be.
And what do you think they potentially reveal about the workings of the brain?
And then we'll talk about the clinical applications.
Sure. Well, even that one is kind of hot one,
because opinions differ on how to define psychedelic,
but perhaps a good starting place
is to start with the etymology where did the word come from.
And it was a Brit, Xcomunicated,
living in Canada, Humphrey Osmond, who was due to present a paper at a National
Academy of Sciences meeting on psychotomometics, drugs that mimic aspects of psychosis in their and certain drugs like Meschillin, let's see 1956 and LSD, were on the bill, and he felt dissatisfied
with them being under this category of psychotomometics and felt that the signature psychological effects of
these compounds went beyond just mimicking psychotic symptoms. And so he wanted to find a more apt term
to speak to, in a sense, the principal component
of their action.
And he jotted down a few different possibilities
about it, doesn't know what so I think.
And one of them was psychodelic, actually,
it started as and ended up being psychod being psychedelic and he had a correspondence going on with another
Brit also living in the US all this Huxley
where they were playing with some
terms to refer to these compounds and
and in the end Osmond won with psychedelic and he had this little ditty of to fathom hell or saw angelic,
just take a pinch of psyche delic. That's what you put the disclaimer in. And so what does that mean? It's two ancient Greek words psyche means the human mind or if we're being
Actually true to the ancient Greek it means soul
And then the other component
means to make clear or to make visible or to make
Manifest or to. So all of those work and it's, it's a neologism,
it's a made-up word, but it does have that ancient Greek origin and it's speaking to this
principle that these compounds reveal aspects of the psyche, of the human mind, the soul, that are ordinarily not entirely visible.
And so that's yet emology, and it's wonderfully poetic, but I happen to think it's also very
accurate. It's a useful term because it's sort of, you might say, valence, non-specific.
It doesn't say you're going to have a great time or that you're going to go mad.
It's more that it reveals psyche and it could be hellish,
but it could be heavenly.
And so that's the etymology and also a bit of the psychology
and sort of pointing to the phenomenology,
the subjective experience.
But there's also a pharmacology here.
And quite recently there was put out a consensus statement about psychedelics that's really referring to what we call the classic psychedelics to say that
these are all compounds that work on a particular receptor in the brain, the serotonin
2A receptor, and that's another way that we could define these compounds. I said this one's a
little hot because I'm of the view that while the pharmacology is really useful, how the drugs
work chemically, you can't avoid the phenomenology. And if we're true to the etymology where the
term came from, then we must recognize and we cannot neglect the subjective experience.
Thank you for that beautiful description of what brought us to today in terms of
using the word psychedelics. And now it's thrown around all the time.
Yeah, too much.
Yeah, too much, and I'm guessing,
well, not guessing, I'm certain that it's also used
to describe many compounds that don't touch the 5-H-2-A,
the serotonin-2-A receptor.
So there is a broader categorization by most people,
and it'll be interesting to see where all the nomenclature
and naming goes.
For the time being, I'd love be interesting to see where all the nomenclature naming goes.
For the time being, I'd love for you to tell us
a bit more about this idea that psychedelics,
however one defines them, can reveal something
about the mind that can't be revealed otherwise.
Are you talking about the subconscious?
I mean, you know, psychologists and most famously Freud,
but also young and also neuroscientists, I think, think know, psychologists and most famously Freud, but also Jung and all also neuroscientists.
I think, think about subconscious processing.
I think perhaps the most salient example for me that's outside the realm of anything psychedelic
would be blind sight.
This phenomenon that you take people that are blind, but still have some connectivity in
their brain and you present them, you present them a board with a computer screen
with different number of dots on each side.
And you say, how many dots are on each side of the screen?
And they say, what do you mean?
I can't see the screen, I'm blind.
And you say, well, just guess.
And their guess rate is accurate, far more than chance
would predict.
So they have so-called blind sight.
And people have said, well, this is the subconscious
revealing itself.
There's no psychedelic drug involved, but what you're describing is a
pharmacologic-induced state that
reveals something that normally should we assume is masked or
that we are oblivious to
even though it's expressing itself. But what does it mean for these drugs to be revealing something
about the workings of the mind that would not be obvious
to us otherwise?
Yeah, so the example of blind sight is interesting,
but it's different.
Blind sight would be referring to non-conscious processing,
maybe implicit processing.
So stuff going on in the mind,
in perception, in a sense, that is below the threshold of conscious awareness, but yet is influencing you.
So it's sort of kind of related, but it's different.
So in depth psychology, psychoanalysis, psychodynamics, psychology, you know, could signal Freud, Carl Jung and so on.
We talk about the unconscious.
And there it's more about the kind of blood and guts of the human
condition, the human nature, both the personal unconscious,
so things that you might not want to necessarily be conscious of,
because it's painful, so that's the repression aspect pushing it out of conscious awareness.
Repressed memories in particular?
Yeah, like traumatic memories, difficult relationships, who could be complex trauma,
not necessarily just the specific, you know, index trauma, but a series of trauma.
And then you have the collective unconscious, which was really Carl Jung's contribution to say that
there's a transpersonal quality to the unconscious. There's aspects about humans, not just this individual human,
there's aspects to our minds, our psyches
that are not fully available to conscious awareness,
but can come up in certain states,
psychoanalysis, when crazy for dreaming
as their royal road to a knowledge of the unconscious,
that was Freud.
But we now know with psychedelics and this was what drew me into the area was discovering literature that was speaking to this particular action, the psychedelic action.
And we're saying that when these drugs, like LSD, cellosybin,
it found in magic mushrooms.
When they're used in psychotherapy material comes up
that maybe may have been repressed,
that is of therapeutic value and awareness
and insight of this material seems to catalyze the therapeutic
process with strong emotional release, these cathartic experiences and insights, whether
they're insights that are personal or whether they're transpersonal. But for me, this is really where the meat of it is
with psychedelics and classic psychedelics in particular,
the likes of compounds like LSD and Salasave.
And I would say that if it wasn't for this action
by classic psychedelics, we wouldn't be so interested
in psychedelics.
I think we only had compounds like ketamine,
NMDMA, cannabis.
That could be said broadly speaking to be psychedelic-like.
I don't think it necessarily would have captured the world's attention
as psychedelics are right now.
I actually think it's a major gap to feel is this principle action of the classic psychedelics.
What does this mean that I'm referring to, psyche revealing? What is that?
And I suppose where I'm going with this is what is that in terms of the biology as well?
What's going on in the brain and the body when people become aware of things that previously they weren't fully aware of?
I'd like to talk about some of the clinical trials that you've been involved with.
In particular, looking at psilocybin, as you mentioned, the principal hallucinatory psychedelic agent in magic mushrooms.
I'd like to start with a kind of nuts and bolts question, just so that everyone's on the same page.
I've read the papers that you've published and that others have published in this area,
and typically the dosages used in these trials are 25 milligrams of psilocybin.
And we talk about one recent trial in particular
that compared 25 to 10 milligrams to more frequent use
of very small amounts, one milligram
over three weeks, for instance.
However, when people talk about magic mushrooms,
they often talk about gram doses of the mushroom
because I'm assuming
that they contain milligram dosages of psilocybin.
Here we're not encouraging use of any kind, these are clinical trials, but for clarity
of understanding, what is the conversion typically?
Like one gram of magic mushrooms will contain how many milligrams of psilocybin on average.
Because of what I'm trying to do here
is calibrate people to this idea of microdosing
versus macrodosing.
And that's fairly straightforward to do
with respect to the clinical trials,
but then in the, a lot of the lay discussion
around this, you hear about heroic doses
versus microdoses. And so I think there's a lot of the lay discussion around this, you hear about heroic doses versus microdoses.
And so I think there's a lot of confusion.
So if you would educate us on this idea of what's a microdose
and perhaps also how many milligrams of psilocybin
are contained in a gram of, quote unquote, magic mushrooms.
Sure.
Well, a microdose is neither of these are that simple,
but it's a fun challenge.
But microdose, one definition is that it's a dose of,
typically a classic psychedelic like LSD or psilocybin
that has subperceptible psychedelic effects like it doesn't put you
into a noticeable, altered state of consciousness that feels like you're tripping.
And if that was LSD, it looks as though the threshold is around about, let's see, 10,
11, 12 micrograms.
Micrograms, on the very clear here, micrograms.
So 10 micrograms of LSD, are you saying will not induce visual hallucinations in most people?
So it's that's threshold level.
That's about the level that some people who are sensitive could feel it. But if you were to
talk to the microdose in gurus, they might say that that's kind of the ballpark for an LSD dose
that you would consider a microdose and then you would take sort of semi-regulately. It's typically
something like one day on one day off or one day on two days off
this kind of thing. There's different protocols. And yeah, so you know, some like Jim Faderman,
one of the popularizers of microdosing, I think would say that a true microdose should be subperceptible.
You shouldn't feel it yet.
The assumption is it's going to change you in some way on a kind of trait level, more
than a state level, maybe behaviorally.
And the typical story goes it will improve well-being, and maybe, maybe, it could improve certain aspects
of cognition, say related to creative thinking. I emphasise the maybe there because that's
another angle with microdosing. We're kind of waiting for some compelling evidence.
As things stand right now, I'd say we lack that compelling evidence. There's some suggestive stuff, but often the study designs aren't that strong.
It's really hard to do a study with microdosing because you need to have permission
to give people a microdose that, you know, for practical reasons, they would go home with. And otherwise, you're requiring them to be in the lab, say three
times a week for X number of weeks to meet the criteria of a course of microdosing, which
might be, you know, two or three times a week for say a month. And that's a hard thing to do in a lab study.
It's expensive.
You'd need to do that against a suitable control,
so a placebo control.
And there is a study that's been done in New Zealand
that has some interesting preliminary data that did,
I think, kind of did the design right.
But it hasn't been published yet.
I've seen some positive findings presented around improvements in moved, but it's a bit
early to get too excited about that.
It needs to go through peer review and all that.
But as things stand, you know, the evidence is pretty thick.
And we have to be honest about that.
We did quite a creative study with my colleagues at Imperial,
the guy leading that Balash, Shigeti, Hungarian chap,
did a really creative design,
very much his brain childhood, instructed people to do their own blinding,
their own placebo controlled blinding
of their own microdosing.
So this was a classic citizen science study,
like do it yourself science, where they would get their LSD
tabs and chop them up, put them into gel capsules,
so fake, and have other capsules that are the
placebo, that they just close, empty capsule. And then there was a whole barcode scan technique
so that you kind of shuffle them up, you know, but they've got the barcode in the QR code,
so you can break the code later on, but once you've shuffled them up, you know longer now which ones have the microdocene and which ones are empty.
Was this LSD?
This was LSD.
You also tried it with mushrooms, but the issues with the mushrooms was people would burp
sometimes, they'd belch and then they'd have this mushroom taste.
So then the instructed people to get some non-psychoactive mushroom material to put in.
So it's really not an easy study.
Not an easy study.
And I love that kind of science, you know, real creative, first mover kind of science.
And the result is fascinating because the short story is that the microdosing didn't
compellingly beat the placebo.
It did not.
It didn't.
And he controlled, because he asked, he controlled for expectancy.
So people was positive expectancy, which is, in a sense, the vehicle that carries the
placebo response, that's why you have a placebo, is the positive expectancy can drive a therapeutic
effect to a large extent. So he measured that pre-trial and then used it to kind of
correct for the response and how did it work? Those who got a placebo, but thought they
got a microdose, did as well as those who thought they got in microdose
and did get in microdose.
So it was the bigger effect, the majority of the effect was in thinking that you got in
microdose.
So in a sense, it was a victory for the power of the placebo response.
And it's created all sorts of controversy.
People don't want to believe it, you know, that kind of thing.
Well, that kind of thing.
But that's the beauty of science, isn't it?
That science is not about what you want to believe.
That right there is the beauty of science, really.
I love that experiment of kudos to them.
I'm not going to attempt to say his last name correctly.
I tried, yeah, but you made a mess of it.
No, no, I think you got it.
You were involved in a clinical trial that was published last year comparing 25 milligrams
of psilocybin to 10 milligrams of psilocybin.
It was a very, to a drug called S-Kid telepram.
Yeah. Yeah. lexapro.
Yeah, lexapro.
And this one milligram over a three week dosage.
I'm wanting to discuss the results of that study a bit,
and some of the other trials that you've done involving
psilocybin for depression, the treatment of depression.
Could we calibrate ourselves?
25 milligrams of psilocybin is that what wouldn't,
it's gonna be a perceptible dose,
presumably hallucinations and all that.
And is that what one would find in,
I'm guessing here, if I'm accurate,
this does not mean that I have experience here,
but two grams of mushrooms.
It's more than that, we think.
Yeah, sorry, I missed that one. We're not
fond of tangent, but 25 milligrams of solar siphon would be, we don't know, and it's important
that I say that because I wouldn't want people to hear my answer here and then use it
to calibrate their own dosing of mushrooms and get it way off. So it's guesswork and I would love to see someone
do a proper study on it and you know look at the psilocybin content in a given mass of
psilocybin mushrooms, magic mushrooms. But to my knowledge that hasn't really been done.
Someone like Paul Stammeritz would give better answer here, but I think the percentage
within the mushroom mass is of psilocybin in the mushroom mass and psilocybin, which is the
metabolite of psilocybin, is something in the 1% a little bit higher, maybe range. Okay, so one gram, 1000 milligrams of magic mushroom,
would contain about 10 milligrams of psilocybin.
Is that right?
Broadly speaking.
Yeah, great.
That helps calibrate.
And I think, again, just allows the lay person to understand a bit more of where we're
headed with these psilocybin trials
and the results.
So we don't have to restrict our discussion
to just that one clinical trial,
but if we include that one
and compare to some of the other trials that you've done,
I mean, you're laboratory seeing phenomenal,
in my opinion, phenomenal results in the treatment
of otherwise intractable depression, major depression,
which so many people suffer from, from two, I suppose, there are two sessions of using
psilocybin in these ranges of 10 to 25 milligrams. Do I have that correct? Yes.
Could we talk a little bit about what people typically experience
during those sessions that allows this phenomenal transformation of mood and state and trait as well?
And I'm especially interested in whether or not it is the experience during those sessions that is
is the experience during those sessions that is the trigger that's necessary for the transformation from a depressed to a non-depressed state. Because the impulse is to think it is,
that what one thinks and sees and hallucinates is, and here is, is so vital. But of course,
these drugs can create neuroplasticity changes in our neurowiring, presumably for long periods of time.
So what are your thoughts on the experience itself?
And maybe for those who have not done these compounds
before, you can explain a little bit
about what's typical for people.
And what you think is leading to that incredible,
positive and pervasive change in mood, state, and trait.
I would say that it's more than impulse that is leading us to think
that the experience is important. It's really data and converging evidence now. So independent
teams, independent studies are converging on the magnitude of certain kinds of experience, rated yes with subjective rating scales,
is predicting therapy to outcomes,
pretty, pretty strongly and very reliably.
And so that's guiding us.
Now, could you say, well, maybe those experiences
are some kind of epiphenominant of, say,
a central brain action?
Well, absolutely, but then all experiences and
epiphenomenon by that principle. And yet we care about it, you know, and it matters to
us and in our human relations with each other. So I think it does matter to a human being
when they're in a, say, a psilocybin therapy therapy session and as the drug effects begin to come on and the body starts
to feel a little strange and tingly and there's some initial anxiety and then in their minds I
they start to notice patterns and maybe colours and then maybe those patterns deeper and their dynamic, and they
have this fascinating organic quality.
Are the patients in your studies typically using an eye mask, or so they're in the eye
mask, so eyes close?
That's what you said, minds eye, as opposed to looking out into the clinical side.
Yes, and that's one of the major differences to psychedelic therapy versus taking a psychedelic
because you shut your eyes, you know.
And it's a world away from taking a psychedelic, yeah, a rave or something, you know, in a
sense, good luck with that.
But in psychedelic therapy, yeah, it's, you know, settled conditions, there's music playing and what I'm describing here is very much the default.
There's actually very little variability between the different sites that have done this work on these conditions.
Typically, it's two people. Ideally, mental health professionals, at least one who's a psychiatrist,
a clinical psychologist,
or some other kind of psychotherapist,
or psychiatric nurse.
But ideally, two who meet those criteria
with an individual who's ingested the drug,
and music playing throughout,
kind of run way into taking the drug
and then throughout, so there's continuity,
music with lyrics or without lyrics.
Without lyrics to begin with and the music
typically is spacious to begin with
and then builds and becomes atmospheric.
There might be, I don't know, some tribal drums in the distance and then builds and becomes atmospheric.
There might be, I don't know, some tribal drums in the distance
or something as it develops
or like the sound of a bird in the distance,
you know, a bird's call.
And then as it gets into more stronger drug effects,
the music starts to coax emotion and very intentionally, you know,
strings, for example, would come in. And it would be an interesting experiment, one that
we'd love to do, actually, to see whether if you were to pull that out,
whether the psychedelic experience would be as emotionally intense as it is in psychedelic therapy
when you have music there as a default. And across the board, people should find this remarkable
because it kind of is. All of the published studies that are now having such an impact on psychiatry and beyond
have music there as a staple component.
And we just take it as assumption that it needs to be.
I tend to share that assumption, but it's remarkable that it hasn't been tested properly.
But it's that.
And if you were to run with that, and if you were, you know, had a kind of critical agenda, you would say, well, this is music therapy,
you know, why are you making all this fuss about psychedelics? Where did it, it's music
that's there in all of these trials, with all these fantastic findings. So there is something
to that, you know, and this will team me up probably to talk about
psychedelic therapy being a combination treatment.
We have a hyphen between the two because I share
the hypothesis, the assumption that should be tested better,
that there is a positive interaction between the two,
that there's a synergy between the two.
That's why it's psychedelic therapy for the hyphen,
just like heart, heart, herif.
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This is extremely useful to hear because I think most people think, okay, psychedelic, whether
or not they have experience with psychedelics or not, it's a visual hallucination, some
auditory hallucination, some synesthesia, some visual auditory blending, some medicine
station, rubbing a surface and being able to elicit the sounds
in one's mind, of course, et cetera.
But so seldom do we actually hear about the specifics
of these clinical trials in a way that, for instance,
points to music as one of the perhaps key variables.
Now, you mentioned that as people enter these psychedelics
states that there's a little bit of initial anxiety.
Out a year and a half ago, I had a discussion with Dr. Matthew Johnson, who's running some
psilocybin trials at Johns Hopkins, as you know.
And he mentioned the critical importance, at least in his mind, to this idea of the patient,
quote unquote, letting go or allowing the experience
to take them someplace mentally,
as opposed to trying to constrain their sensory
and cognitive experience.
I'm curious what your reflections are on that idea
and why it might be so valuable clinically. And this ties back to this earlier
discussion we were having about the unconscious or about psychedelics revealing something that's
there all the time, but that we don't have access to. And again, I'm struggling to find the right
language for this because we don't really have a neural mechanism like, you know, top down inhibition or something like that to explain how this,
you know, unconscious might be uncorked in the psychedelic experience.
But to make it quite simple and direct, how important do you think it really is for the
patient to feel like they are, quote unquote, letting go and what in the world is letting
go in biological terms.
Yeah, yeah.
Well, I think we'll get there in terms of having the neuro correlates of the mind revealing
itself to itself, you know, the emergence of unconscious, the unconscious into consciousness
or unconscious material into conscious awareness.
It's a wonderful challenge, it's a huge challenge, but it's a challenge to embrace.
And letting go very much is again a staple component of how the different teams do this work in terms of encouraging a willingness to let go.
And when we started out doing our depression work and did that first trials, the first trial of
a psychedelic in formerly diagnosed depression, you know, where that was the target population and depressed population. It was the
first modern study to do that. And we visited Hopkins, our friends there and were
mentored on how to do the guiding, Bill Richards, Mary Kossimano. They were just so
that's Mary Cosimano, they were just so brilliant and you know, wise in there, in their guidance to us as to how to do the guiding in our trial. And so this phrase of trust, let go be open,
you'll hear a lot. I don't know who fairly it should be attributed to, but I would attribute it to Bill
Bill Richards. Yeah, everything's borrowed. You've probably got it from someone else, but it's
such a key principle. It's almost like a mantra that you're trying to instill in people's trust.
Let go be open. And those different components where the trust is about
the therapeutic rapport, that again, you know, this goes beyond just intuition now, we've
formally measured therapeutic rapport. We do it, even with just a single item, a visual analogue
scale item, a subjective rating scale item, on the morning of dosing,
and we find that it's a significant predictor of the quality of the experience that you
have under the drug in the psychedelic therapy, and then the therapeutic outcomes, X weeks
or months later. So very powerful kind of chain of sort of predictive components there, but trust
essentially important and again not just intuition but the data pointing to that.
Let go, there's a readiness, a readiness to surrender to let go, to not resist. We do measure that too and see that it's predictive of response.
And then the being open is about a willingness to go there, to confront, to be inquisitive.
Something that's easier said than done can be terrifying, you know. When you're dealing with a very vulnerable population,
it's probably more the rule than the exception that they're carrying some significant adversity,
life adversity, or frank trauma that they've suffered. And so that message of the open, be willing to confront and to go there, it's really, you know,
it's really powerful. And that's how it plays out. And often there is struggle. There's something going
on that is I don't want to be feeling this, make it stop, that can be nightmare-ish at times,
but it's very, very strong. And with these big doses that we give, it's very strong.
And actually, a student that I've worked with,
I think now doing a PhD, Ari Brower,
is working on a fantastic project, characterizing the different phases
of the psychedelic experience,
where the early phase is dominated by negative emotions and negative, negative,
the evalanced feelings of anxiety and struggle, and then it's a different story in the latter half.
Could I ask about that? First of all, I think that's fascinating and important to analyze the different phases.
And again, I'm delighted here because people typically hear
about a psychedelic journey,
but we never really hear about the kind of stereotypic components
of the beginning, middle, and end of that journey.
We know that there's a peak
and that there's a kind of a parachuting down and et cetera.
But when you say that typically there's an anxiety,
maybe some negative valence in the early stage,
do you mean about the sensations people are experiencing
or about some prior event that's being called to mind
that they're remembering?
Likewise, for the positive phase of the psychedelic journey
or trip, are people, do they still call it a trip?
Yeah.
All right, I guess we'll use trip.
For the psychedelic trip, are people feeling positive about the experience like, ah, like
there's been some sort of breakthrough or they're in a, in a calmer state or is it that
they tend to be focusing on prior events that were positive?
So in other words, is there a threading through of some concept that
comes to mind for people, maybe about an earlier trauma or maybe about a sense of self or a
sense of other forgiveness, you know, it could be any of these things. But what do we know about
the kind of finer details of all that? I would say the initial struggle is more against the general drug effects than pinning it on something specific.
It's more that normal waking consciousness, we have a sense generally speaking if we're well or well enough,
a sense of assurredness about what's what, you know, as a tail ear and so on. And we have that, sure, to an extent,
about ourselves as well.
It might be a losery, but we have it.
And what the drug's doing is it's breaking down all of that.
And it's scary as hell, you know?
And if it's a big dose, it's just like human nature
to rage against that a bit.
And a bit like dying, you dying, I don't want this.
It feels like I could be dying.
I might lose my mind.
Yeah, that's true.
I never come back.
Those two of the classics is,
but I might know that I've taken a psychedelic,
and I might even know a bit about psychedelics,
but I still fear that I'm gonna go mad,
or that I know that generally speaking,
these drugs don't have a high fertility risk.
I still think I'm gonna die, you know?
And it's just, it's very palpable and that comes up.
So, yeah, that's, I mean, those are the core fears that those two,
and very reliably, that comes up.
And it's really like a basic drug action.
It's dose-dependent, but it's a basic drug action that is forcing something
about the nature of the mind and the way it's made up,
that makes it feel that way.
But it feels like I'm losing my mind, or it feels like I could lose my mind, or that
I could go insane, or that maybe I'm dying here and this is bad.
You've talked many times before and have done really wonderful work, looking at the changes
in communication between different brain areas while people are under the influence of psychedelics.
And I think the gestalt of those data correct me if I'm wrong is that compared to the non-psychedelic
state that under psychedelic influence, there is far more, let's just call it interconnactivity
or communication between
a brain areas that typically aren't communicating, which probably is not surprising to people
given the subjective effects of these drugs.
What is the evidence that after the psychedelic journey is over that some or perhaps all of
that enhanced communication across brain areas is maintained.
And if so, what role do you feel that could play
in these incredible positive therapeutic outcomes?
Yeah.
So we've had some recent findings in that direction
where yes, it's true.
And the picture that says a thousand words,
that some people might be familiar with
are these two circles, a project that we did in collaboration
with some researchers, where,
ordinarily, the communication is going on within systems.
Like other regions of the visual system
will be speaking mostly within the visual system.
There'll be a kind of clikishness or a modularity
to the quality of the communication in the brain.
And then the cool finding with Salasibim
was the first paper is the communication, yes.
It sort of transcends these modules
and becomes much more intermodular crossing
different modalities and that effect correlated
with the magnitude of the subjective effects
and then we replicated it with LSD using different methods
and new paper will come out soon with We're DMT showing a similar effect.
It's a bit of a debate about what regions are most implicated,
but the general effect of an increase in global functional connectivity
is what we call it, or global communication in the brain.
And this is while under the influence of these drugs.
It's putting people into a brain scanner
while they are under the influence of the drug.
That itself must be quite an experience given that these scanners are small tubes.
You're in a bite bar, you've got a bite bar in your mouth.
That's quite a study.
You don't always have a bite bar.
At least with the psychedelics, but yeah, you've got to keep your heads still.
And you have the loud MR scanner noise going. But because it's regular,
there aren't too many surprises. So it's actually surprisingly tolerable.
And you're in a hospital setting, so you're not worried about what would happen if you had a
cardiac event. You've got professionals around and most people generally tolerate that setting quite well, surprisingly
well. But yeah, we do all that and yes, we do see that opening up of the communication
across systems in the brain. And it does speak to kind of intuition about the subjective
experience that different modalities might be blending with each other.
Sorry for interrupting, but I have to ask, is it thought that the activation of the
serotonin 2A receptor is what's responsible for the increased communication between brain
areas that under normal circumstances would not be communicated?
Yes, so there's a few reasons why some modeling work, the computational modeling work,
that first identifies whether to a receptor is and then looks at models, its basic effects on
neural activity will recapitulate the or recreate the effect that we see actually in the data with the scanning. So doing the computational modeling, you can see the same effect by knowing whether to
where the key receptors are and then making them do a certain thing that we know psychedelics.
I can imagine two possibilities and I think it's important to distinguish between these two.
One possibility is that the activation of
this serotonin 2A receptor leads to increased connectivity and thereby auditorium visual hallucinations
emerge, changed patterns of thinking emerge, etc. That's sort of the obvious interpretation. But
the scientist in me has to ask, is it possible that all of that increased connectivity is occurring,
and yet that is a distinct phenomenon layered on top of some other effect of the psychedelic drugs,
impacting access to the unconscious hallucinations? In other words, is it the increased connectivity
that's leading to the subjective experience, or are those two things happening in parallel?
Well, they happen in parallel and they map to each other.
But the question of causality, what causes what is the tricky thing where I would suggest that the
causality is circular, that they influence each other. And this gets a bit philosophical, but it kind of matters because otherwise,
you know, there's a trap that it's easy to fall into
where you're thinking that it's all about the brain action causing the subject of experience.
And that's typically what we do in cognitive neuroscience.
experience and that's typically what we do in cognitive neuroscience. It's kind of like the sort of first port of call kind of materialist approach. But one can be a materialist essentially, but
still appreciate that circular causality that mind also interacts with brain. And it's so hard to
pick the two apart. And there is a kind of essential dualism where subjective experience is the thing in and of itself.
But that's not to divorce it from what's going on
on the biological level.
The reason I ask is because as I understand it nowadays,
there's a bit of a movement within the scientific community
that studies psychedelics to develop drugs that can essentially cure,
or alleviate many of the symptoms of depression or trauma,
that are built off our understanding of how psychedelics
like psilocybin and here I'll throw MDMA in there,
although classically non-psychedelic,
it kind of gets lumped in when we get back to that later.
But that do not produce hallucinations
or massive changes in subjective experience.
Actually, I think this is what initially got us
into conversation on Twitter.
As I had learned about this paper
published out of a group at UC Davis
that essentially modifying psychedelics
so that they have potential therapeutic application
for the treatment of depression,
but zero hallucinogenic properties.
And I thought, wow, this is going to be
a very controversial thing in the world, right?
Because the history of psychedelics, as you pointed out,
has been one of people accessing different modes
of thinking, feeling, seeing things,
these in letting go, trust, et cetera,
a therapeutic relationship. And here we have, I don't want to say pharma because it's not really pharma,
but we have laboratories who are trying to tease apart the activation of receptors, independent
of all that subjective experience in order to essentially treat the same conditions.
I'd love for you to comment on this where you think it might be going and you
know whether or not you think that's the right or the wrong approach if it has any validity at all.
It is farmer, it's just smaller farmer, sort of start up farmer. Okay, so because farmer would like
to have drugs that can cure depression but don't make people hallucinate. Is that called?
They would and patients might and the system would love it because the system is used to it.
It's medicine. Right, and it doesn't give this this mental imagery of the summer of love in San
Francisco or of kaleidoscopies. It's more you could imagine the more to be careful with my wording here, those who would not be
inclined toward that might embrace a therapeutic, that is strictly effective at treating depression
with no hallucinations.
Yeah, and it doesn't look like an individual lying on a sofa, crying their eyes out about the life that they've lived,
and that deep catharsis being life transforming.
It's very different from that model.
I'm skeptical of it, for a few reasons.
One is that I can't see the logic.
I can't see the pieces fit in a way that's compelling.
And I'm also skeptical because I think
it could easily be wishful thinking
because of that point that patients would like it
and the system would like it.
And you've got to bear that in mind as well.
So, wouldn't it be convenient, you know, if it were true and you could get the therapy to action
without the psychedelic effects? Well, in a way, that's a little bit of what microdosing seems
to be designed to do. Like you said, take dosages there below that perceptual or awareness
of some effect threshold over a longer period of time in an attempt to ping the circuits
or alter the circuits, but not hallucinate, not have a catharsis.
So if microdosing can do that, and it's subperceptible, and microdosing isn't psychedelic action because where's
the psychedelic action? When psychedelic, when defined, means psyche revealing, you're
not getting that effect. You might be getting the pharmacology, you might be getting some
direct serotonin to a receptor agonism that could be driving a therapeutic response,
but you can get that with SSRIs as well.
And so my point is, what's new?
OK, maybe it's a bit new, and people are now developing direct-to-a agonists,
rather than indirect through a serotonin release.
They're like the selective serotonin reuptake inhibitors, the SSRIs like lexapro.
Are there any SSRIs that selectively agonize, which folks, by the way, means activate in
a good way.
Agony sounds terrible to those non-formed might think that mean that disrupt, but that
can activate the serotonin 2A receptor.
Are there any drugs that will do that that are not psychedelic? I'm not aware of any but then again, I'm not a cyclophonicologist.
There are.
I mean, are there any that are licensed and used as medicines in psychiatry?
I actually had this debate recently on social media and I couldn't see,
I couldn't see a compelling example.
I saw two A-Agnist that we use for other things.
You have a compound like Lissaride, used in treating Parkinson's, but actually it's more
of a dopamine agonist. Right. And they're always hitting other things, right?
Yeah. Yeah.
And I say tapping other neurodegenerative.
All there being is for other things.
So is there a selective serotonin to a receptor stimulator, an agonist?
That it isn't psychedelic, that is therapeutic in psychiatry and the answer firmly is no.
I haven't seen it yet.
Will they develop one?
Well, for patients, say, I hope so, because it would be great.
Let's wait and see.
If they do, I doubt it will be psychedelic, and I doubt it would have much to do with psychedelic therapy.
And it would be much more like the system we're used to
of chronic pharmacotherapy.
Take your drug every day.
Let's hope they find it and it works for patients' sake.
But as things stand right now, I'm a little skeptical. Now, some of the findings
that are being seen that are really exciting, fantastic work being done, showing things
like increases in the communication components of neurons, dendritic growth, spine growth,
synaptic spine growth.
Yeah, by the way folks, just to all interrupt for the data,
necessarily spine, the bone, you know,
the not the cerebral column,
but spines are these little like little tiny twigs
with bulbs on the end of neurons
that allow for communication points between neurons.
So neuroplasticity is often associated with growth
of dendrites and spines and so forth, which is what Robyn's referring to. That reminds me, and I just want to make
sure that we close the hatch on the earlier answer because I interrupted you, is the increased
connectivity between, or communication between brain areas that's observed while people are under
the influence of the psychedelic, also observed later after the effects of the drug
wear off. And then I'll just throw in another question there because we're onto this topic now.
To what extent do we think that neuroplasticity, structural changes in neurons, functional changes in
neurons are responsible for that? And how long does that last? Let's say I take, let's say I come
into your clinic,
subject in your experiment, I take do come in in the morning,
I do my psychedelic journey five or six hours later,
parachuting back to reality as we call it.
And then I go home, increase connectivity lasts for how long
and how long are the structural brain changes occurring?
Well, you're asking fantastic questions and partly because we don't have the answer yet, but we do
have some data and so we have looked, first of all, in a sense the functional plasticity
or what we assume it to be or at least the functional changes, the increase in communication
across systems, that increase in global connectivity,
functional connectivity, do we see it after the trip?
We know we see it during the trip,
pretty well replicated, correlating with intense
drug effects, do we see it after the trip?
Well, the answer is we've seen it in two
different depression cohorts,
Salasibian therapy for depression.
In one study where we look the next day, we saw it,
a kind of residual effect,
similar to what you see acutely,
being seen the next day.
And then in a subsequent study, we saw it also three weeks later.
So we've seen it in two independent datasets.
This decrease in modularity is how we measure it.
It's the same thing.
Essentially, broadly speaking, it's the same thing.
An increase in global connectivity,
functional connectivity.
And actually, unpublished, we've seen it
in healthy volunteers on a correlational level,
not on an absolute change level, but if you look
at its relationship to a mental health outcome, and this is an important thing to stress with
the depression work, we saw a relationship between the magnitude of that change, the decrease in
modularity or increase in global connectivity and the improvement in symptom severity. So interesting. Yeah.
I mean, and just a state of a different way.
So what Robyn's referring to is when you say modularity is neuroscientists,
we think of the different modular networks of the brain that, you know,
the eye talks to a region of the thalamus involved in vision, which talks to the visual cortex,
which, you know, eventually converges with auditory information, of course.
But there's a separation or modularity of function.
This increased connectivity is cross-modular during the trip, but afterwards as well.
And you're saying that that correlates very strongly with the strength of the therapeutic
outcome for depression.
I mean, the logical extension of that is that extreme modularity of brain
function is depressive in some way. Now, we don't want to go too far, but what does that mean
that increasing crosstalk between different modules of the brain is so strongly correlated
with a positive therapeutic outcome? We don't know other than that there's a relationship.
I mean, this is this is the thing.
We need to be a little careful not to run with it too far.
I mean, there's some things that it suggests.
I think it suggests a more flexible mode of brain functioning.
If you're not getting stuck in modules or the modules aren't
excessively cut off from each other. But you see different things with different presentations
if you were to look at cognition, sharper cognition is actually associated with more modularity.
So it's a rule that's a little slippery and we need to be careful with it.
I just, again, I'll forgive me for interrupting, but I think I have friends who are, I would
say, are on the spectrum who are very linear in their thinking and extremely intelligent
in the kind of classic sense of being able to ratchet through hard problems to arrive
in a solution.
And then I have friends who are, let's just call them, they are from the creative communities
outside of science that are very expansive.
They see connections between many different things, but sometimes you have to, not all of
them, you have to catch their ideas with a butterfly net.
And oftentimes what they're saying doesn't, sometimes just doesn't make any sense.
Now they also produce incredible creative works. But to have a conversation with
them is anything but a linear experience. They're not random thought generators. But there's
a non-linearity or randomness to their processing that's distinct from these other folks that
I'm describing as on the spectrum. And of course, it's a spectrum. There's a whole range in between.
Yeah.
It sounds to me like there is some therapeutic value to being able to move along this continuum
from the more linear to the non-linear.
Is that, is that correct?
Well, I think so.
Yeah, it's resonating what you're saying.
It's speaking to my intuition that, you know, you could be very passy, passy, passing things up, chopping things
up like an analytical scientist.
A splitter, as we say inside, you're either a lumber or a splitter.
Or the way I'm being very particular about what went to call something psychedelic, that
kind of passy analytical way of thinking you might associate with a more modular system, you know. Whereas the system
that's more globally interconnected and open, yeah, might be more flexible and creative
and divergent in the associations and so on. So yes, that's speaking to my intuition
too, how you're describing it. And I imagine if you take severe psychopathology, severe mental illness, like a depression,
I've always thought that there's something intuitive about the term itself, like a depression
in a landscape, you know, which is a whole physical depression.
A physical depression that it's easy to fall into and if you do, it's hard to get out of.
So almost, if I understand what you're saying correctly, almost like getting stuck at
one location on this continuum, because most people don't reside at one extreme or the
other full time and kind of migrate back and forth between expansive states and more linear
states.
Like you do with low mood, you know, if you're healthy and inverted commas, you can feel you low mood, you're disappointment, but you can spring back.
But someone with you know, you can spring back. Right.
Residus suicidal depressive person or to a cytolid depressed person.
Somehow, at least in my understanding, there's something about the extreme depressive states
and extreme anxiety states, something my laboratory is a bit more familiar with anxiety,
which alters the perception of time such that people feel like that negative state is
going to go on forever, or that if it goes away that it's going to return at random,
kind of a vulnerability to the time domain.
Yeah, yeah, that's it.
And it's so tragic, but that cognitive bias in depression,
that everything's hopeless and that there is no light
at the end of the tunnel.
Yeah, so, you know, if you were to get stuck in that rut
and have that bias, then you're
cut off from other things, other sensory modalities or modules, you know, cut off from the world,
cut off from other people, stuck in your inner rut.
And so, yes, I think we're sharing this intuition that a decrease in modularity or an opening
up of the system, the brain, could relate to an opening up of the mind that is kind of
enduring after the psychedelic dosing session.
And the third replication was to see in healthys an improvement in well-being because that
healthy, we don't look at depression.
So these are people that are healthy walking into the trial.
Take psilocybin twice.
Well, actually they do, but the first dose is 1 milligram, which they don't feel.
It's a placebo dose.
What a quote, micro.
Yeah, we stick EG on the heads to measure their brain waves during each dose and one milligram, you see no change.
So we, I think that you, microdose,
or, you know, I'm just kidding that.
I mean, I think again, the microdose,
as I've always just been a little bit skeptical
based on my conversations with the scientists
actually doing the work with psychedelics,
it seems like the answer keeps coming back. Do one or two, maybe three macrodosis
in a controlled safe setting? Well, that's compelling. The evidence for that is compelling,
and that's what's making all the difference right now. And microdosing is just appealing,
but again, you know, science isn't about what we want to believe.
It's about what's actually coming through and what seems to hold up, you know, to testing.
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Would you say that's right?
The one or two or three sessions and how far apart
are those typically spaced in time?
Yeah, typically one, two, three weeks across the sites
is the way people are doing the psychedelic therapy
dosing sessions, two sessions, Hopkins Imperial, NYU, that's been a kind of default to,
we actually used three in a current anorexia trial,
psilocybin therapy for anorexia,
two patients left to see after 19 who've gone through the trial,
very exciting results there.
You're seeing a alleviation of the obsessive thought about food and
willingness to consume healthier amounts of food. Yeah, even improved weight
at the long follow-up. So critical, when we didn't episode on eating disorders
and I learned that anorexia nervosa, which by the way,
folks, the rates of are not increasing. It's been pretty stable through time, despite what's
said about social media and et cetera. But anorexia nervosa being the most deadly of all psychiatric illnesses,
which is a big statement because, you know, manic depression, so-called bipolar depression
has a 20 to 30 times the typical suicide rate.
Basically, many anorexia, people with anorexia,
I think is how it's now, is what one says, not anorexics,
but people with anorexia often die.
Many of them die.
Yeah, so tragic, so often young people as well, and similarly
with suicide in terms of premature death. So the tragedy with psychiatry is so strong and
there. So it's so rewarding to be doing that trial and to be seeing good results. I have to
check myself a little bit that I'm reporting on it in this
really promissory way and the trial isn't yet publicly released and published so
it's still ongoing as well. But that was three sessions.
It is three sessions and I can't say what the dosage is because we still have
there is a blinding component but there are three dosing sessions in there. Let's see now, I think there are
two weeks apart. And we do the follow up. Yes.
I'd like to close out this description of the journey and
the trip by extending past the day when people actually take the drug
into this, what I've heard described
is the integration phase.
You know, you have to reintegrate, right?
All this increased connectivity
during the session hallucinations, insights, anxiety,
letting go, maybe revelation, maybe epiphany, okay, great.
At what point is that consolidated?
Meaning are these patients or subjects and studies
having daily conversation with their therapist?
Are they journaling every day?
And I want to keep in mind that most people
are not going to be part of a clinical trial.
And of course, here, we're not suggesting
what people do or not do.
But let's just put it this way not suggesting what people do or not do. But let's
just put it this way. We're people to use psychedelics. What is the way that people can maximize
on the neuroplasticity and the brain changes in a positive way in the days and weeks afterwards?
In other words, how long does this so-called integration last? And, you know, how far can we take this?
I mean, I could imagine that how often one chooses to think about the insights could also
have an impact.
Right?
Because clearly people went to raves.
Clearly people did psychedelics in the 60s.
We don't know if clearly people do psychedelics now, but we don't have data on those people.
You have access to the understanding
of how they're spending their time
and the therapeutic outcomes,
which we haven't gotten to the numbers yet,
but again, are incredibly impressive.
You know, in upwards of, as I understand it,
60% or more people getting relief from depression.
Yeah, 70% incredible,
especially when compared to the typical
Intiduppressant treatments and so on so
What is this business of integration? How is it done properly? Yeah, yeah gosh well how long does it last as well?
a lifetime
You know life is a journey like a trip is a journey, and there's always work
to do, you know, as Jack Cornfield says after the ecstasy, the laundry.
And yeah, there'll be other good ones as well, but I forget them.
But yeah, so the work's ongoing and there, yeah.
But this gives you a foot up.
It enables people to do the work more easily.
And that's true.
The classic psychedelics is also true, very true of MDMA therapy for post-traumatic stress
disorder.
It's really giving you a leg up, making it easier to do very, very difficult work,
going back to a trauma,
trying to digest it, process it, integrate it.
So it's such an essential component of the treatment model.
But one has to be realistic as well.
So, you know, by saying our integration lasts a lifetime well,
people delivering a service can't be there for a lifetime.
So what's the answer there?
And people are wrestling with that issue right now.
And I think one of the solutions might be
that it's in a sense on you to a point, you know,
the therapeutic team can treat you to a point and then it becomes what you might call practice.
In a similar way, that meditation is a practice.
It's something that you have to keep up and if it slips, then things could slip and that's the way it is. Or you have another
psychedelic treatment, you know, so people have even used this term of practice in relation
to psychedelics where there's a psychedelic practice, like there's, you know, a meditation meditation practice. But I'm using meditation intentionally here because they actually think that
meditative practice, spiritual practice, elements of spiritual practice could be a very
important complement to psychedelic therapy. And I think it's probably doing something similar in terms of promoting
an ability to sit with. A former colleague of mine said it quite well in relation to psychedelic
therapy versus chronic pharmacotherapy or like SSRI being on them all the time. So psychedelic therapy allows you to sit with rather than sit on.
I thought that's quite good. So the meditation, the mindfulness, the ability to
yes, be present-centred but also present-centred and accepting. So if things come up,
you can watch and process and then let go.
That holy grail of mindfulness, you know, awareness without reactivity,
respond. I grew up in the Bay Area and you'd hear this language, right? And I'm not being disparaging
this, I friends that are on the board of Estiline and work down there, and I've gone there.
And yet you hear these terms, right?
Be responsive, not reactive, which to a neuroscientist is like, greats on me, which probably just
means I have issues.
But then surely I do.
But it is like, what does that mean?
It's sort of saying, like, oh, to be the observer, but not be drawn into the experience.
And again, I don't want to be overly reductionist, but what I find so compelling about the emerging
data, because it really is data, on psychedelics as treatments for depression and trauma, namely
psilocybin and MDMA, is that it really seems to allow people this space that is so commonly thrown around,
giving space between stimulus and reaction.
I mean, Victor Frankl talked about this,
but I've been reading a wonderful book
called The Prince of Medicine,
that good dates back to the origins of medicine,
very dense book.
People have been talking about this stuff
and thinking about this stuff for thousands of years.
Psychedelic seem to give people access
to that better version of self, which is remarkable.
What's also remarkable, and it's perhaps worth pointing out, is that five years ago,
I never would have been comfortable having this conversation.
I would have been afraid to lose my job.
Stanford magazine this week just published an entire issue about psychedelics with how
ketamine works, MDMA, psilocybin, with the appropriate cautionary notes in there, but clearly times are changing.
Speaking of which, I know you're doing a trial on first time use of psychedelics.
What inspired that and what are you observing?
And as you tell us that, please give us a few of the key contours.
What's the dose? How old are these subjects? I'm assuming it's men, women, are they
suffering from depression or not? What's the landscape of that study? And I
I realized this is still early days of the study, or maybe it's close to completion. It's not yet
published, however, correct? It's not published, it's not submitted, it is completed.
So this was one of another one of our COVID studies, in a sense, meaning COVID hit and we had
to finish the study and it was hard to finish the study because of COVID.
That was true about psilocybin therapy versus esitalopram, lexapro trial, which is published,
New England Journal of Medicine. But the...
This was 20, that paper, by the way,
folks will provide a link to in the show note captions,
as well as some of Robyn's other papers.
I think that 2022 New England Journal paper
is really fabulous given it's the different dosages
and the comparison to essentially what is micro-dosing
and the comparison to Citalopra.
Yeah, that's interesting that you link the way we go small doses of salicybin to microdosing.
We didn't think of it that way.
We thought it was just a necessary placebo for the big, big dose, the 25 milligrams.
Yeah, so that we could say to everyone we're giving you salicybin and not be lying.
Yeah, for those who got a telepram,
lexin pro for six weeks,
they got a very, very low dose of psilocybin.
But it allowed us to standardize all the psychotherapy
and so on.
But the other study that you're referring to
was in healthy volunteers, middle-aged, average age,
I think was 40, so not your typical student study that is
so often the case in psychology research, all the undercreds and volunteering for your study.
So this is more of an age range and also I think it was an equal proportion of male and female.
All the staff actually were female, which the staff were
very proud of. Although it produces its own potential confound, right, to have all one
sex of staff. Possibly. Yeah. They did a good job in the sense that we saw significant
improvements in well-being at the end of the trial. So let me describe the design.
It was a repeated measures design meaning.
People come in, you collect your baseline data
and do a brain scan.
And you give people a placebo.
We gave people a placebo.
And actually let me rewind a little bit.
Everyone's healthy volunteers middle-aged,
never taken a psychedelic in their life.
None of them entirely fresh, virgin people coming in.
And the plan is to give them their first ever psychedelic experience, so that's what
we did in the study.
But to do it, we have this repeated measures designed where they'll first get a placebo.
And we have the placebo so that we can do all the procedures, all the therapy, all the
music listening, but not give a whopping dose of psilocybin. We again, we gave them a placebo
dose of psilocybin, 1 milligram. We stick EEG headsets on during the experience to record
the brain activity from the scalp, the oscillating electrical activity.
And we do the MRI scanning before and after to see deeper into the brain.
And we can look at the functional connectivity that we were referring to earlier and also
properties of brain anatomy, which we did in this study.
So the short story is that all of the changes that we saw both psychologically and
neurobiologically were seen with the 25 milligrams.
It all happened with that big, whopping dose.
And what did we see?
Well, we did see significant improvements in psychological well-being.
We saw what I call the entropic brain effect, which is actually
formally quite accurate. We see an increase in the informational complexity of
ongoing brain activity recorded with EEG on the dose of psilocybin. The
activity becomes more complex. It's harder to predict across time. It's more
informationally rich.
And that effect correlates as it does very reliably with the magnitude of the subjective
effect. So the bigger the trip, the bigger the centropic brain effect, now pretty well replicated
finding. But then the MRI, seeing deep into the brain, was probably our most exciting result, where
we didn't just see some functional brain changes, but we've seen some anatomical brain
changes as well.
We used a technique called diffusion tensor imaging that looks at the cabling of the brain,
the white matter tracks. And we saw a change in major tracks,
so we sort of limited our search space to really thick tracks,
really thick fibers.
And the fibers that came through as changing were ones that traveled
between the prefrontal cortex and the thalamus and the striatum. There were two tracks, two prefrontal tracks
that changed, and they changed in the direction of a decrease in axial diffusivity, which
could be interpreted as tracked integrity, where a decrease would be an increase in
tracked integrity. It is something that you see in the developing
brain that axial diffusivity decreases as a brain goes from being a baby to being an adult,
axial diffusivity goes down, and then in aging and pathologies of aging, axial diffusivity goes
up. So this is in the opposite direction of the results you talked about earlier in terms
of brain connectivity of a sort of increased communication across areas.
If I understand correctly, and I'm perfectly happy to be wrong, by the way, that this
decrease in axial diffusivity is translates to a higher fidelity of communication between
the prefrontal cortex and the thalamus
and stride as opposed to less.
And your description of this is somewhat like the transition
from babyhood and childhood to adulthood speaks to the same
where we know that there's a massive calling of connections
as opposed to growth of connections.
So in other words, as we get older,
we get better at doing certain things and less good at doing potentially most everything else.
Is that right?
Ish, because the change was anatomical and not functional. So the other stuff is really measuring
communication in the brain by looking at how the activity fluctuates across time
and whether those fluctuations in activity are synchronous between regions.
And if they are, we say they're functionally connected and we infer that they're talking
to each other because they go up and down in synchrony.
But when it comes to anatomy, we're talking about the justatic material
stuff. And so we're seeing the fibers in a property of the fibers change. At least that's
what we think. And recently we had an independent person come in and re-analyzed the data, because one of those things, incredible finding requires,
credible evidence, really strong evidence.
And I would say the evidence at the moment's one study,
so we need to be cautious on that.
But we did re-analyze it and use this correction,
procedure free water correction, to be more sure that it was a change
in the actual microstructure rather than something to do with the extracellular space, the water surrounding
the fibers, and it came through. In fact, the change was strengthened by doing this correction step. So these are, this is neuroplasticity as the consequence of one first time session
with 25 milligrams of psilocybin.
Yeah, yeah.
So we're excited and the two different, you know, the second analyst coming in,
wasn't sure she believed it and then she, you know, thought this correction technique
might kind of kill the result and then it came through and she's like, okay, now I'm excited too. So we'll see,
we don't know what it means, what does it mean functionally? We don't know, how did
the people change? Well, psychologically, as I said, well being improved, we did look
at their cognition and we used a cognitive flexibility paradigm that looks at
people's ability to notice a rule change and then flexibly adapt their behaviour based
on noticing this rule change, and people improved after the 25 milligrams and didn't significantly
improve after the placebo dose. There weren't correlations with the DTI change,
the cabling change and these psychological outcomes,
but with these studies in smaller sample sizes,
you don't always see those correlations come through.
So it's something, we don't know what it means,
but it's a change in brain anatomy that's in the opposite direction
to what you see in an aging brain or with pathology of aging.
And it's what you see in a healthy brain as it goes from normal, neurodevelopment into
adulthood.
Very, very exciting and intriguing.
And I appreciate that you highlighted that it's just one study, although from everything you said, it sounds like it's been done with immense rigor. So we will eagerly
await the publication of that study. And so we can peruse all the data and the subsequent studies.
I want to hear a bit about the study that you have been carrying out on the use of psilocybin
for the treatment of fibromyalgia.
I'm intrigued by fibromyalgia
because I have a good friend who also,
I won't reveal who it is.
And no, it's not me, this isn't, I have a friend thing
who also is a scientist who's
sits at a fairly high position
in the National Institutes of Health
who quietly has expressed to me
that they are incredibly frustrated with the fact that
the standard medical community has largely ignored fibromyalgia, and that for many years
it was kind of lumped with things like chronic fatigue syndrome and other so-called, again
so-called, I'm not saying this, but people offer them for these as, oh, it's psychosomatic,
that's all in your head, which is a neuroscientist, is a ridiculous statement to hear,
because it's all in your head, your brain is in your head
after all, your physiology and your psychology
are influencing each other, of course.
And the world is starting to appreciate that more.
But first of all, maybe you could tell people
what fibromyalgia is, what inspired you to do a study
on fibromyalgia using psilocybin of all things,
because that's surprising to me. And if you are allowed to or if you have access to the data
in mind, share with us a little bit about what you're discovering in that study.
Sure, yeah, happy to. So again, it's psilocybin therapy and the population is fibromyalgia syndrome.
So this is people presenting with a generalized chronic pain. So unlike some other pain disorders,
where the pain is focused, you can say it's my lower back, which is very common, chronic lower back pain. This is more generalized. And for that reason, it's hard to sort of know what it is.
And that's why it's been a controversial space in medicine. And it's been, yeah, it's had that charge thrown at it.
That maybe it's psychosomatic. And just to your point, is anything ever, you know, independent of the mind anyway.
But this is actually a fascinating space for how
subjective experience, the lived experience,
and the mind can influence the body.
Because there's some really interesting literature
around the etiology,
like how the pain has come about. in a sense, like, what caused the pain?
What's the story there?
And ahead of the trial, I would say to my colleagues, let's just be careful, because there is some
fascinating literature around things like a background of trauma and how that can relate to issues related to inflammation and how
that can express into things like fibromyalgia syndrome. I just said, be very careful there
because if you go in with an assumption that there's some very trauma, for example, then
there's that whole other side of psychoanalysis that massively
tripped it up around false memory and so on. And so please don't hold prior assumptions
that you're going to uncover very trauma in every case. Now, the team are treated, I think
eight people and it's going, it is going very well. Again, I just want to be careful with how I describe it to manage
expectations and not get too carried away. But I check in with the team every week and they're
still based in London doing the work. And it's remarkable what I hear about the profound experiences that people have
under the drug. In this study, we only give one dose. It's a very mechanistic study. We
actually have the EEG cap on in the sessions, like in the Healthy Volunteer Study, but this
time now taking into a clinical population.
And so they're in the, they're, they are wearing an eye mask under the influence of 25
milligrams of psilocybin.
Most of them probably have not done psilocybin before.
So it's a little bit like the first time study in some sense.
They have fibromyalgia that's debilitating in some way. They don't want it,
obviously. And during the session, are they thinking about their pain? Are they being told to
think about their pain? They're not being told to think about the pain. In fact, as I understand it, while there is a therapeutic model around acceptance of the
pain, it isn't, unlike some of the PTSD work, you aren't encouraging them to focus on
the index trauma and then work through it and try and digest it.
We don't do that with the pain.
So the pain's there, but there isn't an invitation to focus on it.
And that's probably one of the differences with classic psychedelic therapy versus MDMA therapy,
arguably MDMA therapy is more like a bit closer to traditional talk therapy,
where there is more dialogue. People are able to talk on MDMA.
whether there is more dialogue, people are able to talk on MDMA. In the MDMA trials, do you know whether or not they used eye masks?
Or because it seems to be an important distinction between, as you describe,
the therapeutic trip versus the trip that one does, you know, going into the woods
and taking, you know, take a cell, you know,
take a cell, you know, I've been in the woods or at a party or while staring at a poster or a leaf. Again, I'm not trying to trivialize those
experiences. I mean, obviously they can be profound, but so I'm told. But the MDMA trials
seem to involve, as you said, more directed dialogue and sometimes even kind of
empathic connection between people by their actually looking at one another, the eyes and eye contact
being such a key part of the human social cognitive connective networks. So do you know if they put I'm asked on people during the
third people? I'm pretty sure that they have the I musks there.
Right. Because a lot of the MDMA work, and I was part of an MDMA trial, it was, as I
understand, geared toward developing, because it's an empathogen empathy toward
the self. Yeah. I'm pretty sure they have the, I'm asked there, but they probably, and it's a great
question because you can formally test this.
It probably don't use them as much.
The thing is, with the classic psychedelics, if you're looking at your guides, your facilitators
and their faces are melting or whatever.
No, no, no.
On MDMA, you just might really start to feel more connected to that.
Yeah, it might just be especially beautiful.
Sure.
And yeah, there's that fascinating effect of loving the people that you're with.
And so I imagine they talk more and use the eye shades less.
And it is more interpersonal rather than like intra-personal going inside.
They do use a fascinating terminology
that some people have critiqued,
but it is a very interesting phenomenon
and it's this notion of the inner healer.
They use that language a lot.
It's been critiqued because it sounds very suggestive,
you know, and that's probably one of the
vehicles here driving the therapeutic process is suggestion.
I think we have to be honest about that.
But so when they go inside, that's another term that we use very much in the classic psychedelic
therapy work, you go inside, you know, you put the ice shades on and people are encouraged
to go inside, you know, you put the eye shades on and people are encouraged to go inside,
you know. But when they do that in the MDMA work especially, they might be told explicitly
and listen to the inner heglla, you know, and that kind of language. So you could see how a
cynic or a skeptic could come in and see that as some kind of like suggestive priming or biasing.
could come in and see that as some kind of like suggestive priming or biasing. I think they have points, skeptics often do, but I don't think it's all of the story. And just
briefly, because it's an interesting point, speaking to that point a bit, in our Salas
Ibn therapy versus S Teleprank trial, we measured pre-trial expectancy and we did it for both conditions.
So, you know, what kind of improvement do you expect with the lexapro, the S-tallopran at the end of the trial, and what kind of improvement if you go into the cellosybin arm and get a big two big doses of cellosybin, what kind of improvement do you think you'll see in that?
And of course it was a coin flip as to what people went into
and there was no crossover.
And what we found was that it was true that we had a sample bias
so most people had higher expectations on average
there were higher expectations for
psilocybin and its efficacy or effectiveness versus the SSRI, the lexapro. However, when we looked
at the correlation or the predictive relationship between pretrial expectancy and response, we saw the pre-trial expectancy for the acetalapram
predicted response to acetalapram across virtually every single measure, all these different
measures of depression and anxiety and well-being. And I think none of the scales, I'm pretty
sure it was none of about 12 or so mental health rating scales was there
a relationship between pretrial expectancy. Even though it was high, it didn't predict
pretrial expectancy, didn't predict response to the psilocybin therapy. So that was a bit
of a, you know, smash on the head for the idea that the classic psychedelic therapy is some kind of placebo response.
And I think it's so important to address that question because if it doesn't come through as it didn't come through,
then it opens up even more intrigue about, well, what is it then?
If it's not just a placebo response
or a super placebo response,
like an amplification of the placebo response,
then it must be something else.
And how intriguing it has a direct therapeutic action,
it must be something.
And we don't yet know what it is.
I talked about the residual, you know,
increasing global connectivity.
That's one possibility.
But the truth is we're just scratching the surface.
And yet the therapeutic outcomes are again
just so marvelously impressive.
I'm curious as to why, as well, there are that many labs,
but the laboratories that are focused
on classic psychedelics for the treatment of depression
and now as you mentioned, promising results
for anorexia and fibromyalgia as well,
although preliminary, very promising.
Why the lack of attention toward LSD,
is it that the LSD trips are just too long?
Is it that they are qualitatively different?
Are there any data on non-microdosis of LSD?
And here I wanna be very careful
because I learned through my interactions on social media
that this term microdosis, very misleading.
And in some cases can be dangerously misleading
because as you mentioned earlier, the effective
psychedelic dose or the effective meaning that can induce a real trip with hallucinations,
et cetera, of LSD is actually in the microgram range.
So some people hear microdose and they think microgram of LSD is a micrograms, is a microdose,
when in fact a macrodose of LSD can be measured in micrograms. So this is where in the absence of
scientific training, people can really go astray. Or even in lack of understanding of the metric system. And since now you're a recent rival to the US.
Fortunately for us, sorry, England's loss is the US
is gained by a Robin's lab move from England
to the United States recently.
So score one for us.
But why isn't there more use of LSD in these trials?
I think it probably is the duration of the trip,
but used to be stigma,
and it was easier to get your psilocybin study through
because others were, they were getting that through,
so there was still like, France,
Volonvider, in Zurich, in Switzerland,
and then Roland Griffiths coming along
and doing the psilibian work at Hopkins.
So you could appeal to that president and say, well, they're doing it over there, you know,
can we not do it in little England? So that's how it worked for us. We did actually go on and
do an LSD study once we kind of laid the foundations for doing this kind of work. And it was a brain
imaging study. It was a really extensive one actually, where we use both MRI and another
modality called MEG, sort of super EEG, in a sense. But, you know, why didn't we, why
didn't that turn our heads to think, oh, should we not be doing our trials with LSD?
It does have something to do with the pragmatics, like a study day with psilocybin is long enough.
So four to six hour trip?
Yeah, and the FDA asked us to have the people in the lab until eight hours post dose,
with personally, I think, could be quite excessive,
especially if it's a low dose.
And if you have that in the placebo condition as well,
it becomes impractical.
Scientists are not paid nearly enough to warrant the,
there's no such thing as overtime
in for the graduate students and postdocs.
Yeah, and it's often that there's more junior members that are doing that really hard work.
It was described very well to me by a student when I was a graduate student said to me,
they really can't afford to pay us by the hour.
Because we used to work. He was an electrophysiologist, so he would run experiments. No joke, folks.
Three to five day experiments,
sleeping in bouts of two hours here or there in a dark room with a bunch of equipment and
recording. So these are long, long acute physiological, electrophysiological recordings. So,
yeah, no, no scientists does it for the money. I promise you that there is money in pharma, there is not money in
personal income, it's not lucrative for the basic scientist. So, yeah, LSD is what,
anywhere from 8 to 15 hours? Yeah, 15 would be a little long, you'd be a bit worried if you
were still tripping at that time, maybe with a really big text. No, just kidding.
worried a few are still tripping at that time. Maybe we're the really big types.
No, just kidding.
But yeah, eight hours plus.
And dose dependent, yeah, if it's a bigger dose,
it's a longer experience.
But if you're gonna dose, say, 10 a.m. in the morning,
which is more or less how it often goes,
then that's six p.m. still feeling the effects.
And then how long do you wait now to kind of close
things out before they can go home. Even with solar cyber, you have people still at work
into the evening and the staff are always there later of course because they've got to pack up and
yeah, so these are long days and it's just it's too much, you know.
That makes sense.
You know, practicals and constraints.
I learned from a recent guest on this podcast that we recorded with Dr.
Sachin Pandu, who was a colleague of mine when I was down at the Salt Institute,
has pioneered a lot of the studies on so-called intermittent fasting,
that the reason the intermittent fat, that the eating period in these studies
in animals and now on humans is eight hours, the sort of feeding window in these studies is because
the graduate student was going to otherwise lose their relationship because their significant
other says, listen, you can be in the lab for 12 hours.
That meant some hours before the experiment, then eight hours and then some hours afterwards,
but you can't stay in there longer.
And many people use the eight hour feeding window as a consequence.
So the science has to exist and be carried out in real world frame.
It does.
It does.
MTMA is a little bit shorter, right?
It's about a four to...
It's also about four to seven.
Yeah, it's kind of similar to Salasai bin.
Yeah, it is.
And actually in the maps work, they reduce after a certain point.
So the boost, the boost, they have a boost. There are optional boosts there, yeah. So, so there is
that. And now people are thinking, well, even these Salas-Ibane sessions are long and expensive.
And if you have to have two staff members there all the time, that's expensive, that's where most of the expense is, is
in the staffing. So can we abridge the experience, make it shorter, and get away with it, and
get similar kind of therapies to outcomes? So there's a lot of interest in that direction.
They ask about, sorry to interrupt, but I want to make sure I don't forget to,
I ask about combination, psilocybin MDMA therapies.
The reason I ask about this is, um, and here truly not me,
but I know people who, um, do self administered, um, combination psilocybin
and MDMA, um, I think I have this right.
I think it's called a hippie flip.
Um, there's another one that involves LSD to again,
I'm not suggesting people do these kind
of drug combinations, but the way it was described to me was that the psilocybin, because it's so serotonergic,
sometimes can be not a downer, but can have a bit of a kind of a murky feel to it, some really
deep introspection, sometimes in the darker realms of one's psyche, depressive
thoughts, et cetera, not that it necessarily stays that way throughout the trip, but
that the MDMA, because it has a very strongly search and ergic, but also dopamine ergic,
I mean, so it has an emphetamine component, a cocaine-like, in fact.
If you've ever seen someone on an MDMA, their pupils are about the size of quarters.
For a reason, they're in extremely,
extreme autonomic arousal compared to a sedative,
which by the way, would constrict the pupils.
So they describe the use of MDMA
to kind of balance out the kind of affect component of it.
What are your thoughts on combination,
psilocybin, MDMA?
Does this hold any therapeutic potential?
This is obviously a backyard chemistry
in the sense that people are,
or kind of cow-boying the stuff on their own,
which again, I don't really recommend.
I like to see the science go first,
but I understand this is how it works in the real world.
Yeah, what are your thoughts on combining compounds?
Yeah, well, I guess they're cowboying it
in recreational contexts,
but also underground therapists do work with this combo.
That's what I'm referring to.
So I'm not talking about people parting with this stuff.
I'm talking about, there are thousands now of therapists
that offer psychedelic therapies illegally, really, because it's not
legally, at least not in the US to possess or sell, but that are doing this. So that's really why I'm
asking. Yeah, and you know, I think there's something to be said for when I have to be careful with
this as a scientist, but you know, if they're doing it, are they using some kind of trial and error?
The same is true, of course, with the longer history of psychedelic plant medicine use
by plants.
We include the fungi as well, so in the extended sense plants.
There will have been trial and error there.
It might not be as systematic as the science we do today, but maybe there's been a learning
process and maybe what they do, they've come to because
they found it works. So by that principle, I'm interested in that combination and whether
it does offer some advantages, maybe in certain patients, you know, if we, one of the buzz
terms in medicine these days is precision medicine, a precision medicine and personalized medicine. So maybe there are certain
cases where, you know, introducing, say, Solaceibin after the MDMA or the other way around could offer
some advantages. And the differences are interesting, you know, Solaceibin can get you to deep places, maybe, you know, the kernel of your suffering
and major life experiences and complexes that are causally linked to whatever the pathology
that you're presenting with.
But it can do it sometimes quite aggressively, you know?
And if it's, say, post-traumatic stress disorder, it can be overwhelming.
And you can fight it. And really it's that. It's that, you know, the resistance is a really
challenged, and they fight back. And the therapeutic breakthrough and the progress
isn't happening because you've agitated the defense mechanisms.
Whereas what MDMA offers is something arguably more directionally reliable in terms of the valence.
Like it's more directionally positive generally an MDMA experience.
Hard to have a bad time on that. Yeah.
To be quite blunt.
I mean, one of the concerns I had with MDMA, I've never done it recreation.
I have had not and have not ever done it recreationally.
But when it was done in this therapeutic setting, I realized because there was music
on at the beginning, I actually asked them to turn it off because I realized that the
music was becoming such an attractor to my attention that I suddenly asked them to turn it off because I realized that the music was becoming such an attractor to my attention
That I suddenly was starting to think about music and my love of music
Which was not the focus of the session that I
Was there you know for and I'm glad that they did turn the music off because the moment they did
I was able to drop in within the I'm asked to this to the sort of go inward and address some certain issues that at least to me felt key and productive.
So that seems to be the kind of hazard with MDMA
is that it's such an empathogen that one could start to,
you could go down any number of different rabbit holes.
Yeah, but it's also, it's a strength because you,
well, you know, the classics like Solaceibing can take you there very reliably, but maybe a bit aggressively
MDMA
makes it easier to go there and and that's it strength and that's why that
Marriage of MDMA therapy for PTSD in particular is
A good combo it works because you are going to go there,
in a sense you have to really make the therapeutic progress.
You're going to have to go back there.
But we're going to set it up so that you can go back there
and feel safer, more trusting, and be able to go back there,
whereas you've never otherwise been able to go back there without,
you know, dissociating or having, you know, horrible flashbacks and so on.
So that's the strength that it offers. I guess the limitation would be that maybe it doesn't take
you as deep as the classic psychedelics. And I tend to think I'm biased on this one that there's a kind of honesty to the classics in that it is, it is hell as well as heaven, you know, and that's the psyche. It is
in all roses. I really appreciate that you bring that up because I think that there's such a fear of
so-called bad trips. There's such a fear in non-psychedelic states
to avoid the painful.
And everything, everything we know
from trauma and the treatment of trauma.
We've had several guests on here.
My close colleague, close, close colleague at Stanford,
Dr. David Spiegel, our associate chair of psychiatry,
clinical hypnotist, amazing, amazing human being
and scientist and clinician, as really just, you know, like embedded this in my mind that
the only way to deal with trauma is to get right up next to that trauma to the point where
some relief is experienced. There is no other real way. And so I really appreciate that you're
saying that the classic psychedelics may offer
the, with a very strong nudge, perhaps, the opportunity to get into the uncomfortable
in a way that MDMA or some non-classical psychedelics, perhaps, do not. We're talking about timeframes
or duration of trips and these different compounds and how they differ and how they're similar.
I'd love for you to educate me on DMT
and some of the work that you're doing with DMT.
My understanding is that it's a very brief trip, minutes.
People I know who have done this,
again, therapeutically, actually,
I'll just point to one very exciting,
I think, group and initiative, which is the Veteran
Solutions Initiative, which is a group, this is carried out in Mexico, but in conjunction
with laboratories at Stanford and elsewhere who are evaluating the neural changes.
And this involves IBegin, which is Ibogo, which is a very long durations psychedelic, 22
hours or more, followed by, I think, one or two doses of DMT. This is for
veterans to deal with any number of issues. It appears to be working with great success,
and I've spoken to several of people who've gone through this, and the way that they described DMT,
almost across the board, was quote, here I'm just pulling quotes, right, anic data.
The most profound experience of my entire life,
even greater than the birth of my children,
quote, like being attached to the shock wave
of an atom bomb, quote, there's no way I would do another dose
because the first one was so unbelievable.
Interesting, by the way.
I think most of us, including me, would think, why wouldn't you want to do it again, then? But this idea that that was just beyond
anything. So these are significant, excuse me, these are significant statements coming
from individuals who have existed at the extremes of human experience to begin with, right?
These are so-called tier one operators within the special operations who exit and may or may not have trauma, but
DMT sounds like a
big deal
Yeah, short duration really big deal. What do we know about its chemistry?
What do we know about how it's impacting brain networks and what in the world is going on that people are describing it as
The ways I just mentioned a few moments ago.
Yeah, it's a rocket ship. If the Salah Sybin is like a ship leaving port, then yeah,
this is a rocket ship into craziness. Is it serotonin 2A?
It is. Yeah, so it is a classic psychedelic.
It's a direct agonist, a direct stimulator
of the serotonin 2A receptor.
It's an order of magnitude less potent than psilocybin,
but potent sees a funny thing because it's dose-dependent.
So that doesn't mean that the experience with DMT
is less than that of psilocybin. It's just that you give more of the drug. But it has, let's match by its
stickiness for the serotonin-to-a receptor, which is this kind of golden rule in psychedelic
sciences that it was discovered in the mid-1980s, this tight relationship between the affinity
or the stickiness or the binding potential
of a psychedelic for the two-ay receptor in particular, serotonin two-ay, and its potency,
and the sticky of the drug, the more potent. So LSD really sticky, very, very potent, you only need
those tiny microgram doses. So DMT, by its affinity, is a little less potent, but by its effects when you give a standard dose,
it's just wild. And DMT, because there's another compound called five-methodxy DMT, which is a
bit different pharmacologically and subjectively. It's similar in terms of its kinetics, it's
another rocket ship. Both compounds in the wild, so to speak, are smoked often, TMT and 5MEO,
people are vaping both actually now. There are vappe pens had been developed for people to administer this,
but more traditionally it's been a smoking thing.
This is clinically not recreationally, or both.
Both now.
I mean, you know, underground practitioners are using the vape pens, they like them because
people titrate the dosage, they get a feel for what it is
to be going into this state so that they feel
they can let go and go into it.
But actually, I think some of the veterans work
might be giving five MEO after the eye began.
Phenomenologically, if there's a difference between DMT
and five MEO, people might put it on 5MEO
being more of a reliable ego dissolution experience, less visual and more kind of all-round
immersion in the greater whole loss of self-identity and just immersion in everything.
Yeah, maybe we could just talk about ego dissolution for a second,
because it's such a sticky, interesting idea.
I can take a step back as a neuroscientist and say,
OK, ego dissolution, this idea that from a very early age,
we have a concept of self.
And that I wake up every morning and I know I'm me and not somebody else.
And presumably you do the same. And most people do the same, I would hope. But that and that
there are objects in the world and people in the world beyond us. But every time I hear about
ego dissolution, it sounds like it's a kind of a temporary elimination of the idea that things stop and start and stop between us and everything else.
Almost like, you know, in a kind of a, here I'm not trying to sound philosophical or metaphysical,
but they're sort of the molecular continuity of life, right? We're all at all just little bits.
Which is true, which is true, right? Not a functional way to go through the day, right?
Because you want to make a cup of coffee,
you don't really want to get lost in that
if your goal is to make a cup of coffee.
But, you know, what is the power of ego dissolution?
Is it the idea that we belong?
Is it a sense of meaning?
Is it the sense that we're not as important as we think,
which of course could be a wonderfully useful way
to go through life, to think that we're not as,
and we're vitally important, but we're not the only thing,
because I do believe connection is vital,
as most people do.
What is ego dissolution?
And why would this serotonin 2A activation cause that?
That's remarkable.
Yeah. Great questions.
I mean, what is it you alluded to it with the start stop,
I think, you know, because you could define it by boundaries
in a sense, what isn't me, is as valid here as a developing sense
of what is me that a child develops at whatever age.
And so a major characteristic of the ego dissolution experience rather than just a negative, a thing going away, my sense of
self going away, is the positive, oh, now I feel interconnected with other people in the world
at large and I realize, you know, that there is that molecular continuity and actually that's a
ground truth. And, oh, maybe the ego thing is somewhat illusory or at least the construction of my mind.
And indeed it is, right?
Well, it is.
Yeah, I mean, there's no transcendentalism about that.
It's just like logic.
I think about it a little bit like family.
I mean, we all know what immediate family is,
but sort of like, forgive me for interrupting myself.
I do it all the time anyway.
When I teach neuroanatomy, some clever student always figures out, okay, well, that's connected
to that and that's connected.
But ultimately, everything in the brain is connected to everything else.
There's just no way around that.
That's a true statement.
And so you really just have to decide where you draw the boundaries between.
Where are the modules? What are the modules? You could say the brain is just one big macro module.
And then you also want to include the body. And now, fortunately, people are starting to embrace
this idea that it's not mind-body. It's both because the nervous system extends through both,
of course. So as the same could be said said of family, like we're related, right?
Not just by virtue of the fact that we're human beings, if we did our genealogical charts,
we would find a convergence at some point.
And of course, you know, this becomes a bit of a game, but then one realizes that where
you draw the boundaries, and if you draw them at brother, sister, parents, biological parents, etc.
That's a game too.
And so it is just a construct.
Yeah, I mean, it is a fun game, you know, where do you draw the line and when to pass and
when to collapse?
It's also a classic consideration in science, when to pass.
And when...
The lumber versus the slitter.
It's brilliant.
Yeah. But you asked this question, like, well, why do psychedelics do it? And
there we think psychedelics do it because the target receptors, at least, you know, classic psychedelics
do it. And that's important to stress. So MDMA doesn't really do it in the same way. Might
soften the ego a bit, but yeah, that's debatable.
My experience with MDMA is that it's such a strong in pathogen. Yeah.
And that it can cause empathy for others. Yeah. Certainly you could imagine situations where one
in MDMA journey and afterwards says, you know, oh, these, these my oppressors, you know,
are the people that harm to me.
They, and here I'm not referring to my experience,
but, you know, they did the best with what they have.
Actually have empathy for them, forgiveness,
but also for oneself, that there's an empathy for self.
I know I said this earlier, that is very hard for most people
to access.
Perhaps it's not the narcissist out there listening.
They'll be like, of course, everybody for self.
But everyone else, I think,
all the other healthy people, or the healthy people,
other than narcissists and not picking on narcissists,
I have to imagine they suffer too.
In fact, I think that's the root of their narcissism.
That empathy for self is not something
that comes reflexively for most people.
And here I'm not talking about self-love or self-respect,
but this notion of being able to see the self
as not just deserving of love and care,
but actually holding that in place
while in confrontation with something challenging
in a way that allows more or not less access
to adaptive responses to that challenge. I think that's the way I kind of conceptualize it.
Yeah, yeah. But I mean, drugs offer a great, they offer great, they are great scientific tools
for tackling this question. What does ego dissolution and why do drugs modulate it? And what does that
tell you about the brain?
You know, because other drugs like cocaine,
releasing more of a different neurotransmitter dopamine,
more than serotonin, the opposite is the case with MDMA,
is more of an ego inflator, right?
Oh, absolutely.
People become hyperlinear, hyperlinked to their own desires and wishes, and future outcomes become an obsession.
It's the stuff of kind of American psycho and the kind of cliches and stereotypes of the 80s
cocaine culture. Yeah, yeah. We did a study once actually looking at dose-dependent relationship
with ego inflation on one axis,
an ego dissolution on the other, and saw that it just massively passed or differentiated between
cocaine and psychedelics. It's quite a neat study. So cocaine makes people's egos super-inflated
and so on and so on. It doesn't touch dissolution and the opposite is the case with psychedelics.
At least a key. Are you really imaging to explain how cocaine does that?
That would be a great study.
Yeah, great.
We should do that.
I have a sabbatical coming up.
I've got 12 months of sabbatical coming up.
Yeah.
I don't want to.
I'm going to show up in your lab.
Yeah, that's a really good one.
If it's right to finish the thread on why psychedelics and ego dissolution, we do know
some things, or we have some hypotheses
and it's that the target receptor is a serotonin to a receptor that the classic psychedelics hit.
I heavily expressed in what these days I like to call recent brain because evolutionarily it's recent brain.
It's cortex that humans have more than any other species. If you look at a mapping of cortical expansion
from say Macaq or Chimp to human, it's the very same map that you'll find the two-way
receptors in. So that's the target. And it's just easy to think that, oh, well, that could
be the egoic brain, you know, and the classic psychedelics
come in. They kind of, they scramble up the activity. That's the entropic brain action.
And in terms of, you know, the start stop, the boundaries, that entropic action sort
of spreads out the system. It doesn't shut it off, it sort of spreads it out, you know.
The solution. Yeah. And you know, that you were talking about the headspace as well.
So that fits, if it's more capacious, it sort of fits.
The big qualifier with psychedelic therapy that people rightly bring up is it doesn't last.
That's the paradox of it, the paradox of ego dissolution.
The ego might go away during the trip and you have these profound insights about the molecular continuity
and how we're all worn and interconnected, and then you come down, and however long later,
you know, the ego comes back,
but maybe with a vengeance,
and sadly, you know,
things can go right when people haven't done the work,
perhaps haven't done the integration work,
and maybe ego defenses come back,
and, you know,
and it's not a pretty picture.
How often do you see that in the trials that you do?
What percentage of the people coming through,
do you think end up with worse than they were
before the trial?
It's very rare in the trials that we've done.
Yeah, but you see defenses come back.
So you do see people relapse.
That's more, if you're pushing out to like three months plus
in something like treatment, resistant depression,
that's more the rule than the exception, sadly,
people relapse.
If their histories are, you know, histories of chronic depression, then while you
might give them a window of wellness, sadly, it doesn't last. It's not to say that it doesn't ever last.
It does, and we have people who are in our first treatment-resistant depression trial who are well to my
knowledge today, back at work doing fantastically well, but sadly, the majority of relapse to
my knowledge and need to do more psychedelic journeys.
Well, they can't because it's illegal. That's been the really difficult situation that we've
been up against is that we do a trial where all of a sudden this schedule one drug becomes
a medicine in the trial, or at least an experimental medicine. We give the treatment, it works fantastically well, gives people a remission that they've
never really had for however long, and then the trial ends and they deny that treatment
and worse still if they were to have that treatment, they would be committing a crime.
It's sort of a sick joke in a way, but that's the situation that we've been in.
And that's a perfect segue
for what I want to talk about now,
which is what is the current state of legality
in terms of the progression towards legality?
I'd also like to touch on the role of,
let's just say incoming big pharma.
There are a lot of startup companies now
trying to capitalize on these discoveries
that you and others have made.
The landscape out there is very unclear to me.
Maybe I'll just call out some silos as I see them.
And maybe we can draw some bridges between them
if they exist.
At the ground level, not the grassroots, but at the ground level, I look to laboratories
like yours, Matthew Johnson's, Rowling Griffiths, some laboratories at Stanford, Nolan Williams.
Lavaatories studying the effects of psychedelics in human beings, so not animal models, in terms of their clinical application
for the treatment of depression,
inorexia, I now know fibromyalgia, trauma,
let's lump MDMA in there as well,
assuming that it all works in an equivalent way
at the level of kind of where the legislature
is taking things.
Okay, so labs using government money, philanthropy, et cetera.
So labs using government money, philanthropy, etc. Then there are the therapists out there that are accessing what we believe are clean sources of MDMA, psilocybin, LSD to do this. They are
doing it illegally. This is in the US or other Western European countries because obviously it's gonna differ by country
who are administering these things.
Sort of on the basis of what they're reading
in these studies that you all are publishing,
but also expanding on and experimenting,
hippie flips and combination drugs and ketamine and et cetera,
but let's leave ketamine out right now
because it's legal, but there's that.
Then there's the, I don't wanna say,
it's sort of recreational slash open market, black market.
And here I wanna raise a flag to the fact that Dr. Peter Tia
did a terrific podcast on this recently
and his own podcast, The Drive,
the fact that a fentanyl,
lacing with fentanyl is now showing up in MDMA and psychedelics that
are purchased on the street.
So serious caution to those getting it from uncertain sources.
And then you've got pharma, and then as an umbrella for all of this, you've got the FDA
and law enforcement agencies, which currently say this stuff is illegal unless it's being
used in a clinical trial, selling it or possessing it can get you charged with a crime ranging
from, I don't want to say, because I don't know, but up to felonies, right?
Years in prison.
Okay.
So, can't take it through airports, can't, don't get caught with it, don't buy it, don't
sell it, Kind of thing. So where are we going from that picture of these silos?
I know things are in clinical trials now.
Most people, including myself, are not familiar
with how the different phases relate to the proximity
to legality.
Could you just kind of give us the landscape and touch on
how long you think it will be before the people
that come through your trials could
then go get a prescription for psilocybin or potentially buy it without the risk from a
reliable source one would hope but without the risk of getting thrown in jail.
I used to live in Oakland, California.
My understanding and please correct me if I'm wrong folks, don't trust this information
and get in trouble.
My understanding is that psilocybin is decriminalized in Oakland,
but that's not the same as being legal.
So what is going on out there?
Well, it was so much.
Yeah, I just asked 55 questions.
But feel free to answer just a subset of them if you like.
Yeah.
Well, Oakland's a funny one.
I live close to Oakland. There are head shops in Oakland.
You know, there might be selling cannabis and cannabis-related paraphernalia that are selling
mushrooms as well, psilocybin mushrooms. That's a fact. Opened it. Yeah. That's a fact. I can verify
that. I haven't purchased them, but I've gone in and kind of checked it. Yeah. That's a fact. I can verify that.
I haven't purchased them, but I've gone in and kind of checked it out like what's going
on here.
Yeah.
Yeah.
Yeah.
So, you know, the police aren't going to prioritize that activity, the purchasing of
of those mushrooms as a crime now in Oakland because of the decriminalization.
So those hedge-ops shouldn't strictly be selling,
well, they shouldn't be selling.
They won't have a license to be selling.
Licenses don't exist yet for that here.
But let's see whether they get shut down,
they probably will, I don't know.
But there's a church in
Oakland that say that they're selling and it's part of religious rights that they're using
that church model as a loophole. The way that Native Americans can use Pioté and they have a more genuine case, I think, because
there is a history there, but they're trying to kind of piggyback on that. Anyway, that's
sort of close to where we are right now, but federally, which is really the major inflection
point is the FDA and the licensing of psychedelics as medicines to be legally prescribed across
the country, across the US and beyond. That is close because the key phase, there are
different phases of clinical trials and the key one to know about is phase three. Phase
three trials are licensing trials. If they're successful
and typically you have to do at least two successful ones, show the results to the regulators who are
the FDA, the medicine regulators, and say, is this good enough now for you to give me a license so
that I can sell and provide this medicine that we've demonstrated is a medicine.
So that work has been done with MDMA therapy
for post-traumatic stress disorder maps
have led that work and done two face three trials.
I think they've already publicly announced
that the second trial had results consistent with the first.
We know the results of the first because they're published
and they were remarkably good, something like 67% remission rates. results consistent with the first, we know the results of the first because they're published
and they were remarkably good, something like 67% remission rates.
And long term, I understand me as some of those remission rates for trauma were years,
which is different than what you're describing for psilocybin, where people might need ongoing
dosing.
That's true.
Yeah, yeah.
But of course, just for trauma in those trials. My understanding is those
and the MA trials were not focused on depression. Yes, yes, focused on the trauma.
So that's something because that data is being filed now to my knowledge, like as we speak,
and they're anticipating a decision maybe this year
with rollout happening as early as next year. I mean, that's sort of best case, I think.
Could I ask you, when you say rollout,
who's, and it's the appropriate term for MDMA
because it's so-called rolling,
about 20% of my audience, maybe 50,
we'll understand that, not funny joke that I made.
Who's going to roll it out?
Is this where would one get the clean source of NDMA,
meaning not laced with fentanyl,
not laced with methamphetamine,
not undergone any chemical conversion to some other drug
which can happen with extended shelf life, et cetera.
Are people going to go to their psychiatrist to
get MDMA? And who's going to be providing it? Is it going to be some big major pharma?
This seems like a serious set of issues. It is. And I don't have all the answers. I do
know that maps would be providing because they've done the work and they have set themselves up in a sense to potentially become the provider
whether as a farmer company, which is the big question they're wrestling with at the moment.
It's very expensive to become a farmer company.
And yeah, they probably deserve to make the choice because they put in so many years of hard work when all of this stuff was considered like
rave culture party drug
They were the ones that
Spotted the
therapeutic potential that I mean we knew there was therapeutic potential based on work going back many decades
But I'm points to them and I think that I think in my opinion they should have the agency to make those decisions
Yeah, it's a remark such a remarkable thing that's been achieved and I think they've done it all on
philanthropic donations. I think so. Yeah, so there is this big question mark in the FDA
are also asking questions about,
to your question, you know, who can provide this? Because in the phase three work and up until this point,
there's been a maps training, a maps therapist training,
and you have to do this formal training in order to,
to be a practitioner within the trials.
But now there's a question from the FDA,
whether that maps training can be the training
that a clinician has to have to now be a provider.
And when I say rollout, it's like offering this
as a service, essentially.
And so where would the referral come from?
That's a good question that I'm not 100% on the answer, whether it would have to come
from a psychiatrist or whether someone's sort of general physician could do that referral,
but they will be going to a provider who is licensed and certified and will have done
some training.
And there will be a consensus on, you know, what constitutes good enough training to provide.
There will also be some stipulations on the basic underlying professionalism of the
clinician who provides.
So I imagine there'll have to be a mental health professional.
I don't think they would have to necessarily be a psychiatrist.
They could be a clinical psychologist.
For all the dosings, I think, without question,
there would have to be a physician present
or at least within ready access in case of an emergency.
Yes, especially with MDMA, because of the propensity for cardiac issues,
because of the emphetamine properties.
And where is psilocybin in terms of the phase trials?
Is it in phase two, phase three?
It's in phase three.
There's psilocybin therapy work being done
for treatment-resistant depression
by a company called Compass, those trials,
which are always multi-site, so there's always a bunch
of teams or labs, in a sense, geographically spread out that are each contributing to
data that then gets massed together and is then submitted as part of the Phase 3 trial
results.
So that's happening with Compass right now.
It's cellosubprety for treatment resistant depression
those trials have just started and I think the earliest estimate that I heard in a
in a journalistic article was because I don't think compass would say or they wouldn't say publicly
something like 2026
26. Wow, so MDMA is is ahead of
26. 26.
Wow.
So MDMA is ahead of Silicon.
Oh, yeah.
Yes.
Quite a few years ahead.
And it's more of a, not a certainty, but it's very, very strong position with MDMA, whereas
the work's only just begun with solar cyber in terms of the phase three trials.
But then you have this other situation of like however many psychedelic research centers there are now across the globe
It was nice to you know, we had the first one in London in 2019
First one in 2019 is 2023 now, and I don't know how many there are but so much has happened in such a small space of time
Yes, but you know, all these different indications
I've been able to tell you about anorexia
and fibromyalgia syndrome, trying to do a trial
with a colleague of mine at UCSF
in methamphetamine use disorder.
He's got a trial going on in Parkinson's disease
and chronic lower back pain and bipolar disorder. I mean,
there's so much going on, OCD, almost the full gamut of psychiatric disorders, not schizophrenia
to my knowledge of being looked at. So there's so much ground, ground, you know, ground
swell of activity. And I think these small investigators led studies, typically
they're small because trials are expensive, are going to be reporting positive results.
I know what we're seeing and it will be, you know, for, let's see now, at least four trials,
or with really positive results in very difficult to treat disorders.
And that's just us.
And I know there's so much elsewhere, addiction disorders as well.
You know, Matt Johnson's work obviously, Michael Boagin shoots.
So all this compelling groundswell, it's really something.
And yet, you know, the system to really make a big breakthrough in terms of licensing
is, of of course slow.
It's so that can frustrate people, but it has to be done properly.
Else, we revert back to what happened in the 70s, where there was a lot of interest in psychedelics.
It's kind of interesting to me. There was a close
juxtaposition of meditation and kind of behavioral approaches to self-directed state change and psychedelics.
Meditation kind of made it through the hatch. I mean, there were some years where it was considered
kind of counter-culture, whoo, magic carpet, weirdo stuff by Western science.
But now, I mean, there are tens of thousands
is not an overstatement of quality studies
exploring how meditation can provide advantages
for the mind and even for mental health.
And psychedelics are now catching up,
but they used to be close cousins
in the cultural framework.
But the problem was, I think, psychedelics were viewed as making people crazy.
And university professors lost their jobs for having discussions like the one that you
and I are having right now.
And some people went to jail, but mostly people either left academic institutions or lost
their jobs, whereas now these are some of the studies of the sort that you are doing
and that are taking place at Stanford and Hopkins and elsewhere are some of the greatest
magnetic pull for philanthropy for universities.
Donors are very interested in supporting these sorts of studies because they and their family members
and people they know suffer from psychiatric illness
for which the current big pharma approaches
simply have not worked.
So it's sort of interesting to me
that what once was seen as kind of poison
is now being viewed as a potential therapeutic.
It's not just interesting. I think it's hopefully it speaks to the evolution of the human species.
People seem to be coming more open-minded about becoming more open-minded.
That's right. That's a good one.
Yeah. And yet, yeah, there's so much that's happening so fast.
There are elements of, it's complexifying the space.
There is critique.
There's been some bad practice in psychedelic therapy boundary crossing issues that have
caused some scandals.
That's too bad, isn't it?
Yeah, well, I think to the gene therapy, right?
It just takes one bad incident.
Gene therapy was on a fast track three decades ago and then a sadly child died in a gene
therapy trial.
And it's like shut down gene therapy practically for half a decade and then it slowly started
ratcheting up again,
gene therapy broadly defined.
And now we're in the age of potential directed gene therapy
using CRISPR and things of that sort,
which makes people, some people cringe
and other people very excited.
If you have Huntington's in your family,
CRISPR is like the most exciting technology ever
because you could potentially eliminate it
from your family line going forward, of course.
So I just really hope that we can be balanced as this all plays out because it could go
similar way, given the stigma, given the history that people be very twitchy with
with some isolated incidents. And over generalise them perhaps.
In a sense, shining a light on them, I think, is important that that has happened recently,
is important because it really drills home how important it is that this work could be done right
and what the necessary safeguards and standards should be.
Yeah, it won't be an easy road forward, but we've got to hope that it succeeds,
because current treatments.
People talk about the mental health crisis and to your point earlier
about anorexia rates, it's not always actually the case when you look at the epidemiology,
when you look at the data that you see a big inflection in diagnoses or cases of psychiatric
illness, I would say it's more that the treatments haven't moved. They haven't really progressed. They haven't got any better since the 1950s more or less. And new drugs have been more of the same. So they
haven't been any paradigm shifts. And that's why I get a little impassioned when I talk about
psychedelic therapy and that point that this is something different. It's not a drug every day. That system is not cutting it.
Do we really want to keep on with that system? Sure, not everyone will want to trip, and that
will terrify some people so much that they'll just want to be on their lexapro or a non-psychedelic, psychedelic, or whatever. Of course, you should be allowed to have those options, of course,
and the more options are better.
But I think there is a great value in really understanding what psychedelic therapy is.
And I think when you do, you realize that it is a major paradigm challenge on many levels.
And the fact that it's different might be its greatest appeal at the moment, I think.
Well, I am certainly grateful for your passion, for the potential for psychedelics,
to be added to the array of potential treatments.
And I really also appreciate how much you put it
in there alongside the other treatments.
Maybe even combination with other treatments
as opposed to saying this is the thing
that's gonna cure everything.
And yet, the passion that you have
for this potential paradigm shift,
the one that really appears to be happening
at the level of clinical data now,
is so important.
So I want to extend a voice of gratitude for that and for the work that you're doing.
I mean, I've been outside of this field, but as a neuroscientist, I've been paying careful
attention to it.
Really for the last five, seven years or so.
And it's abundantly clear that it is a small group
of individuals who are really thinking in terms
of how the system works now and what needs to be done
in order to change the system for the better,
like yourself, that are really the driving force
behind this new movement or paradigm shift
that without question is going to lead to improvements in mental health
and physical health outcomes. So I just want to say thank you for that. Also thank you so much for
joining us today to share this immense knowledge set about the history of psychedelics, what they are,
what they aren't. They're clinical applications as seen in your laboratory and other laboratories.
I'm sure people already noticed this, but you're incredibly generous in terms of attribution.
And also in your caution about explaining how some of the results, in particular on anorexia,
fibromyalgia, are perhaps preliminary, but very exciting. They're not published yet anyway.
We wouldn't call them preliminary. And also for touching on mechanism, that is not just
about people feel better, but pointed to some potential underlying mechanisms in terms of
connectivity changes and on and on. So thank you so much for your time today. Thank you for the
work that you're doing. And thank you for the work that is sure to continue. We will provide
links to studies in your laboratory,
links to your laboratory so people can learn more and support in the ways that they deem
appropriate for them. But just thank you, thank you, thank you, such important work you're
doing, Robin. Thank you, Angie. It's been a pleasure.
Thank you for joining me today for my discussion with Dr. Robin, Carhartt Harris. I hope you found
it to be as informative about the science and clinical uses of psychedelics as I did.
If you'd like to learn more about Dr. Carrhart-Harris's research
or support that research,
or inquire into being a research subject
in one of his laboratory studies,
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