Huberman Lab - How Psilocybin Can Rewire Our Brain, Its Therapeutic Benefits & Its Risks
Episode Date: May 8, 2023In this episode, I discuss what psilocybin is (chemically) and how it works at the cellular and neural circuit level to trigger neuroplasticity, which is our brain’s ability to rewire itself in ways... that lead to long-lasting shifts in our emotional, cognitive and behavioral patterns and abilities. I discuss the emerging clinical trial evidence for the use of psilocybin in the treatment of depression, addictions and other psychiatric challenges. I explain the typical duration and phases of a psilocybin journey, the different categories of dosages often used and I explain the importance of set, setting and support when using psychedelics. I explain which groups of people place themselves at great risk by taking psilocybin as well as groups that could benefit, and I highlight the rapidly changing legal and medical landscape around psilocybin. This episode is a thorough exploration of psilocybin from the scientific and clinical literature perspective and ought to be of interest to anyone curious about psilocybin, mental health, neuroplasticity and/or psychedelics more generally. 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 ROKA: https://roka.com/huberman HVMN: https://hvmn.com/huberman LMNT: https://drinklmnt.com/huberman Supplements from Momentous https://www.livemomentous.com/huberman Timestamps (00:00:00) Psilocybin, Legal Considerations (00:08:32) Sponsors: Eight Sleep, ROKA, HVMN (00:12:00) Psilocybin Becomes Psilocin in the Gut, Serotonin (00:17:00) The Serotonin 2A Receptor, Therapeutic Outcomes SSRIs vs. Psilocybin (00:21:40) Serotonin Receptor Expression; Visual Hallucinations & Eyes Closed (00:27:21) Safety & Cautions for Specific Patient Populations (00:29:13) Sponsor: AG1 (00:30:28) Psilocybin, “Magic Mushrooms” Dosing, Micro-Dosing, “Heroic Doses” (00:36:21) Psychedelic Journey: Set, Setting & Support (00:43:43) Music & the Psilocybin Journey; Duration of Effects (00:48:58) Psilocybin & the Brain: Subjective Experiences, Perception (00:58:36) Sponsor: LMNT (00:59:48) Brain Networks & Therapeutic Outcomes (01:05:23) Creativity; Music, Emotionality & Psychedelic Journeys (01:12:39) Depression & Psychedelics as Neuroplasticity “Wedge” (01:16:53) Positive Psychedelic Journeys, Unity, “Oceanic Boundlessness” (01:25:23) “Bad Trips”, Anxiety & Physiological Sighs (01:32:57) Therapeutic Use of Psilocybin (01:36:11) Neuroplasticity, Structural Brain Changes & Psilocybin (01:48:08) Psychedelics: Therapeutic Breakthroughs & Depression (01:56:37) Combining Psilocybin Therapy & Talk Therapy, Antidepressant Effects (02:03:11) Psilocybin Experience & Mental Health (2:06:42) Zero-Cost Support, YouTube Feedback, Spotify & Apple Reviews, Sponsors, Momentous, Neural Network Newsletter, Social Media Title Card Photo Credit: Mike Blabac Disclaimer
Transcript
Discussion (0)
Welcome to the Huberman Lab podcast where we discuss science and science-based tools for everyday life.
I'm Andrew Huberman and I'm a professor of neurobiology and
Ophthalmology at Stanford School of Medicine. Today, we are discussing
psilocybin.
psilocybin is a psychedelic meaning it modifies the psyche and in doing so, it changes our level of consciousness.
Psychedelics, such as
psilocybin, change the way that we perceive the outside world and our internal world, our
memories, our thoughts, our feelings, etc. Not just while one is under the influence of psilocybin,
but it can also fundamentally change all of those things afterwards and for a very long period
of time afterwards as well, which is one of the reasons why there's growing excitement about the application of psilocybin and another psychedelics for the treatment
of various mental health issues such as depression, alcohol abuse disorder, and addictions of various
kinds, as well as things like OCD and eating disorders. Today, we will discuss psilocybin,
talking about what it is. In fact, you may be surprised to learn that psilocybin basically
is serotonin. Now, for those of you that are familiar with psilocybin and serotonin, you
might think, wait, that's not true. But in fact, psilocybin's main effect is to mimic
serotonin. But it does it in a very specific way because it activates a subset of serotonin
receptors in a very strong fashion, leading to neuroplasticity at the level of
the neural circuits, that is the brain areas and connections that serve things like memory
and perception.
So, if any of that is confusing at this point, I promise to make it all clear in just a
few minutes.
Silicibin is one of many psychedelics, of course.
There are things like LSD, DMT, 5MEO, DMT, even MDMA will not consider to classic psychedelic
is considered a psychedelic in the general sense.
Today's episode is going to focus on psilocybin in particular.
I will tell you what psilocybin is,
how it works at the molecular and cellular level.
I'll talk about how it changes brain circuitry.
I'll talk about the clinical effects,
what's been demonstrated in controlled laboratory studies. I'll talk about how it changes brain circuitry. I'll talk about the clinical effects, what's been demonstrated in controlled laboratory studies.
I'll talk about dosages and translating from psilocybin mushrooms to actual psilocybin.
And the compound that actually exerts the effects of psilocybin, which it turns out is not psilocybin,
but something called psilocybin.
Sylocybin is the actual compound that goes into the brain to create all the changes in consciousness
and all the rewiring effects that we associate with psilocybin.
So understanding how psilocybin is converted to psilocybin has tremendous impact on the
duration of a psilocybin journey, whether or not that psilocybin journey is going to lead
to a short or longer window for neuroplasticity.
In fact, many people don't realize this, but much of the positive changes that are possible
with proper, and I do want to underscore,
proper psilocybin therapeutic approaches,
takes place after the session
in which one feels all the typical,
or typically associated effects of psilocybin,
like hallucinations and changes in thought patterns, et cetera.
So today, we are going to talk a little bit about chemistry,
but I promise to make it accessible to anyone
and everyone regardless of whether or not
you have a background in chemistry or biology.
We're going to talk about some cell biology,
the actual neural changes that occur
when one takes psilocybin.
And we're going to talk about how neural circuits
change over time and how all of that impacts the changes
that most people are interested in when they go on a psilocybin journey.
Things such as longstanding improvements in mood, things such as tremendous insight
into themselves and to others, into their past, their present, and their future, and even
changes in their levels of creativity or their ability to experience joy from music
or their ability to dissociate in a positive way
from things that formerly were depressing
or triggers for depression.
In fact, we're going to talk quite a lot
about the conditions inside of a psilocybin journey
that make it actually positive and therapeutic.
This is a very important point
that I'll make several times throughout today's episode, which is that just because something invokes neuroplasticity changes
in brain circuitry does not mean that it's therapeutic, or I should say does not necessarily
mean that it's therapeutic. For neuroplasticity to be therapeutic, it has to be adaptive,
it has to allow someone to function better in life than they did previously.
So today we will talk about how the conditions of a psilocybin journey, including whether or not it's
done with eyes closed or eyes open or whether or not people alternate between eyes closed and eyes open
phases of that journey, as well as whether or not music is played during that journey and even what
types of music are played, will dictate whether or not somebody will feel better or worse
in the days and weeks and years following that psilocybin journey, as well as the dosage level,
because as you'll soon learn as well, there are clinical studies showing that just one psilocybin
journey can improve mood in a longstanding way, but most clinical trials involve two dosages, spaced in very precise
ways from one another with appropriate follow-up.
But in both of those particular journeys, the structure of the journey, who's present,
who's not present, eyes open or eyes closed, the particular music that's played, all of
those features make up part of a larger neuroplasticity trigger of which psilocybin is critical, but
psilocybin is not the only variable. So whether or not you're interested in participating in a
clinical study or whether or not you're interested in psilocybin for other reasons, this is critical
information to understand. So today we're going to talk about nearly every feature of psilocybin
possible, including what psilocybin is, how it works at the level of chemistry, cell
biology, and neural networks, and neuroplasticity.
We will talk about the clinical studies, we'll talk about dosages, we will talk about conditions
of clinical studies, and we will talk about the post psilocybin journey period in which
neuroplasticity and the various activities, including therapy or perhaps not therapy, can contribute
to positive therapeutic changes from psilocybin.
Now, as we go into this discussion, I do want to underscore the fact that at the time of
recording this episode, meaning now, May 2023, psilocybin is still a schedule one drug.
It is considered illegal in the United States.
There's perhaps just one exception
to that, maybe a few others, but the main exception is in the state of Oregon.
Silasibon has been approved in particular therapeutic settings for use in particular conditions,
namely depression and some forms of addiction. So in Oregon, it's more or less in the domain of decriminalized as opposed to actually legal.
In other areas of the country, including Oakland, California, there's some areas in which
it has been decriminalized and perhaps there are a few others that I'm not aware of.
But in general, psilocybin and other psychedelics are still considered illegal.
This is very important, not just saying this to protect me, I'm saying this to protect
you, possessing or certainly selling psilocybin, except for rare instances such as clinical studies and
these decriminalized areas that I talked about a moment ago, is still very much not allowed under
the law. Today, I'll also discuss safety issues. I'll talk about whether or not young people,
meaning people 25 or younger, should consider psilocybin given that their
brain is still in a rampant period of naturally occurring neuroplasticity.
I will also talk about dosages as it relates to people who have formerly been on or may
currently be on different forms of antidepressants.
And I will talk about people who are at risk for psychotic episodes, either because they know they themselves have a propensity for psychosis, or they have close family members who
have psychosis, which includes things like schizophrenia, bipolar depression, as well
as things like borderline personality and some related psychiatric conditions.
So today's episode really will be a deep dive into psilocybin.
So whether or not you think you're already familiar with psilocybin in its effects or
whether or not you're just curious about them, I do encourage, if you're willing, to try
and ratchet through some of the understanding of how psilocybin works and what it is, leading
up to some of the therapeutic applications and different patterns of dosing, spacing
of different sessions, et cetera.
Because I do believe that with that knowledge in hand,
you will be able to make far better, much more informed decisions
about whether or not psilocybin is right for you.
Before we begin, I'd like to emphasize that this podcast
is separate from my teaching and research roles at Stanford.
It is, however, part of my desire and effort
to bring zero cost to consumer information about science
and science-related tools to the general public.
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Let's talk about psilocybin.
And again, today we're going to focus specifically on psilocybin
and we're going to set aside all
the other psychedelics for future episodes.
psilocybin is what's called a tripdomine.
That refers to its chemical composition, not to the so-called psychedelic trip.
In fact, it's spelled differently.
Tripdomine is TRYP.
Trip, TRYP, of course.
Tripdomines include psilocybin, but also things like DMT and 5M and EO DMT.
The trip to mean psychedelics very closely resemble serotonin itself.
That's right, most of you have probably heard of the chemical serotonin, and serotonin
is what's called a neuromodulator, which means your brain embodies naturally make it,
and that it modifies or changes the activity of other neurons and neural circuits.
And it does that generally by either increasing or decreasing the activity of those neural circuits.
If I were to show you a picture of the chemical structure of psilocybin or its active derivative, silosin,
and I were to also put right alongside it an image of the chemical structure of serotonin
provided that you weren't a chemist who really likes to focus on the detailed differences between
things. You would say those look very similar. And indeed psilocybin and its active form Silasin
are very similar structurally and chemically to serotonin itself. Now as I mentioned before,
serotonin is something that you naturally make.
And yes, it's true that about 90% of the serotonin in your brain and body is
manufactured in your gut. However, contrary to popular belief,
the serotonin in your brain is not
manufactured from the serotonin in your gut. You have separate independent sources of serotonin.
That is, you have particular neurons that make serotonin in your gut. You have separate independent sources of serotonin. That is, you have particular neurons
that make serotonin in your brain. You also have serotonin in your gut and those work more
less in parallel separately. Now, what does serotonin do? This is really important to understand
because of the similarity between psilocybin and its actin-form silicin and serotonin.
Serotonin, in that it's a neuromodulator,
changes the activity of other neurons,
and the net effects of those changes
are things that you're familiar with.
For instance, satiety,
or the feeling that we've had enough of various things,
such as food, or a social interaction, or sex,
or pleasure of any kind.
Serotonin is involved in all of that and an enormous number of other things, such as mood
regulation, such as our sense of pleasure itself or lack of pleasure, such as whether or
not we feel motivated or not motivated, it works in concert with other neuromodulators, such
as dopamine and epinephrine and norepinephrine.
In fact, if this were an episode about serotonin, which it is not, you would soon realize that
serotonin is involved in so many different functions that impact our daily life.
And that is one reason why certain antidepressant medications, which alter either increase
or decrease the amount of serotonin transmission in the brain will often have a lot of side effects
related to things like mood, libido, appetite, sleep, etc. It's because serotonin is involved
in so many different things. And serotonin is involved in so many different things because
there are a lot of different so-called serotonin receptors. Serotonin is a chemical that we
call a ligand, and the chemical ligand is simply the thing that plugs into
the receptor for that chemical or ligand.
The receptors, in this case serotonin receptors, have the opportunity to do all sorts of different
things.
They can change the activity of neurons, making them more active or less active.
They can cause growth factors to be released, making sure that those neurons reinforce or
even build up stronger connections so that they're more likely to be active
in the future.
Serotonin binding to particular receptors
can even change the gene expression in particular cells,
making those cells proliferate, so make more of them,
making those cells more robust, making those cells
interact with new elements of the brain embody.
Basically serotonin and all these different receptors
that it binds to has dozens if not hundreds
and maybe even thousands of different functions. So the fact that psilocybin so closely resembles serotonin
leads to a very important question that we should all be asking ourselves, which is why is it that
psilocybin, which looks so much like serotonin, when one takes it in the form of magic mushrooms or some other
form, maybe the synthetic form of psilocybin itself, which nowadays is manufactured in laboratories
and placed in different psilocybin containing foods and pills, etc. Why that leads to complex yet
fairly circumscribed sets of experience, like visual and auditory hallucinations, changes
in particular, thought patterns, and neuroplasticity that, in many cases, in the clinical setting,
provided things are done correctly, improvements in mood, relief from depression, relief from
various compulsive disorders, etc.
This is really what you need to understand, if you want to understand psilocybin and how
it works, and how to make it work optimally for a given condition or goal.
You have to understand what it's actually doing and what allows psilocybin to do fairly
specific things in comparison to serotonin, even though psilocybin and serotonin are so
similar, is that psilocybin mainly binds to and activates the so-called serotonin 2A receptor.
The serotonin 2A receptor is one of, again many different serotonin receptors,
but serotonin 2A is expressed in particular areas of the brain,
and even on particular areas of neurons in the brain,
that allow for very specific types of changes in neural circuitry to take place,
not just when one is under the influence of psilocybin, but afterwards as well. So really in order to have a
useful discussion about psilocybin, we need to talk a lot about the serotonin 2A receptor. But, you know,
fortunately for you, unless you're somebody really interested in structural biology or cell biology,
that discussion is not going to be about the binding pocket for serotonin on serotonin
to a receptor or a lot of the downstream signaling of the serotonin to a receptor.
We'll talk a little bit about that where it's relevant.
But more importantly, at least for sake of today's discussion, we're going to talk about
how the serotonin to a receptor is really the one responsible for triggering all the changes in neural circuitry that lead to the changes that is the improvements in mood, the relief from
compulsive disorders in many cases.
But really it's the serotonin 2A receptor selectivity of psilocybin that is leading to all the
excitement that you hear about in terms of psilocybin as a therapeutic tool.
Let me say that from a slightly different angle. that you hear about in terms of psilocybin as a therapeutic tool.
Let me say that from a slightly different angle.
There are data that I'll talk about today
which show that one, although in most cases,
two psilocybin journeys done with particular dosages
of psilocybin lead to maximal binding or occupancy
of those serotonin-2A receptors
in ways that lead to significant and unprecedented
relief for major depression. In fact, you'll soon learn that the clinical trials for psilocybin
are outperforming standard therapy and outperforming so-called SSRIs and various other antidepressants
in terms of providing depression relief in ways that are frankly staggering, not just to me, but to the psychiatric
community at large.
And this is what so much of the excitement is coming from.
Now, that statement could be taken one way, which is to just say, okay, well, here's a
compound psilocybin that outperforms SSRIs.
And therefore, all the attention should be on psilocybin.
But SSRI stands for selective serotonin reuptake inhibitor. In other words,
the SSRIs of which there's now a lot of controversy, things like prozac, zooloft, etc.
I'm sure you've heard some of this controversy. There are people who are very pro SSRIs,
although they're a growing number of people who really feel that the SSRIs are probably
most appropriate for things like obsessive compulsive disorder where they, in fact, can be very beneficial.
But there's a lot of kind of leaning back from SSRIs as the B-All end-all for the treatment
of depression nowadays because of the side effect profiles.
And the fact that it's not even really clear that serotonin deficiencies are the major
cause of depression in the first place.
Now, again, we're talking about psilocybin, not about SSRIs, but you should be thinking,
wait, how is it that two molecules, psilocybin and some particular SSRI, both of which look
like end-or-increased serotonin transmission in the brain, are leading to either incredibly
positive and interesting outcomes or to kind of troubling side effect riddled outcomes.
And again, it all boils back down to the selectivity of psilocybin
to bind that serotonin 2A receptor.
And so, in order to understand how psilocybin works,
and in order to understand proper dosing profiles
and spacing of sessions, aka journeys,
we really need to talk a little bit more about the serotonin two-ay receptor, where it is in the brain, what sorts of things happen when psilocybin binds
the serotonin two-ay receptor, and how those things set in motion, the various changes,
the neuroplasticity that allows people to feel better in terms of their mood, and as you'll
soon learn, can experience more pleasure and joy from things like music
and enhanced creativity. All the things that I do believe, whether or not people are thinking about
or maybe even exploring psilocybin for recreational or therapeutic purposes,
all the things that people want and are really talking about and perhaps even doing psilocybin
in order to obtain. So before going any further, I just want to place an image in your mind.
You can place an image in your mind whereby when serotonin is released in the brain naturally,
not having taken any compound, any drug, anything, it's getting released at a lot of different
sites, binding to a lot of different serotonin receptors, doing a lot of different things.
When somebody takes an SSRI, the net effect of that selective serotonin re-uptake inhibitor
is that there's more serotonin
around to exert its effects.
Because it's a reuptake inhibitor at the synapse,
the connections between neurons,
the serotonin can do its thing more extensively
and for longer periods of time.
But it's doing it kind of non-specifically.
So when you think about standard
anti-diprescent treatments,
at least for sake of this discussion,
you kind of think of a sprinkling or a kind of
spraying of serotonin at different locations in the brain and binding to lots of different
receptors.
Whereas when you think about psilocybin, even though the subjective effects are pretty
diverse, we'll talk about those in a few moments, what you're really talking about is a molecule,
psilocybin that looks a lot like serotonin that is
selectively and very strongly binding to and activating
that serotonin 2A receptor. So that's the image I'd like you to
embed in your mind. And then the next image I'd like you to
embed in your mind is where these serotonin 2A receptors
are located in the brain. Well, the serotonin-2A receptors are located in the brain. The serotonin-2A receptors are located
in multiple brain regions,
but they have a tremendous amount of expression
in the so-called neocortex, the outside of the brain,
that includes things like our prefrontal cortex,
which is involved in understanding context,
which behaviors, thoughts, and speech patterns
are appropriate for certain circumstances,
how to switch context and category switch
when you go from playing sports to hanging out with friends
to being in a professional setting.
You change your behavior in the way that you speak
and perhaps even the way that you think.
You might think some things that are out of context
but you probably keep those to yourself
and your ability to keep those to yourself
are dependent on a functional prefrontal cortex.
There are a lot of 5HT2A and by the the way 5HT is the abbreviation for serotonin.
So there are a lot of serotonin to A receptors in the prefrontal cortex, also in other areas
of the cortex that are associated with sensation and perception, that is hearing of sounds,
that is seeing of particular things, and in, there is a very, very, very high
expression of serotonin 2A receptors in the visual cortex.
And that is one of the reasons why psilocybin triggers visual hallucinations.
And provided psilocybin is present at sufficient enough concentration, that is, taken at a
sufficient dosage.
One will experience profound visual hallucinations regardless of whether or not their eyes are
open or their eyes are closed.
Now that's an important fact because it explains one of the major effects of psilocybin that
people experience while they are on the drug.
Now as I'll talk about a little bit later in terms of what constitutes a useful
psilocybin session, useful meaning that it's leading to adaptive improvements in mood, adaptive
improvements in creativity and cognition, et cetera, is that people not have their eyes open
for at least the majority of the psilocybin session. This is something I've discussed with several experts
who are running clinical studies on psilocybin
in their laboratories, some of whom are going to be guests
on the human lab podcast and upcoming episodes.
And I can't underscore this enough.
Because your visual cortex contains so many
of these serotonin-2A receptors,
and because psilocybin binds so strongly
to that serotonin to a receptor, you're
going to experience a lot of visual hallucinations when you are under the influence of psilocybin.
There's no surprise there. This has been known for hundreds, if not thousands of years. It's
one of the main reasons why people take psilocybin. However, as I mentioned earlier, these hallucinations
occur even when the eyes are closed.
And it's now fairly well established that if people are to take psilocybin and have their
eyes open, much of their cognition, much of their thinking, much of the time spent in that
psilocybin journey is focused on the altered perceptions of things in the outside environment. Sometimes this looks like a sort of a fracturing of the outside world
into kind of geometric shapes.
Sometimes it appears as a kind of melting of things in the visual environment,
including people's faces or a morphing of people's faces.
All of that has a strong, let's just call it a draw for a lot of people
who are looking for a highly unusual experience inside of the psilocybin journey.
But I think if one's goal is to derive long-lasting benefit from the psilocybin experience, it's
very clear that having an eye mask or some other eye covering or something that ensures
that one's eyes are closed for the majority
if not the entire psilocybin session is going to be very useful because it's going to limit
the extent to which one is focused on those outside changes in visual perception, aka hallucinations.
And rather, we'll allow the person to go inward to combine whatever it is that they happen
to be seen in their mind's eye with the different thoughts and memories and changes in their emotions that are occurring.
And that going inward by staying in the eye mask, at least for the majority of the time,
seems to be a very, if not the critical feature of making the psilocybin journey effective
in the therapeutic sense.
Now once again, I want to cue to some of the safety precautions here.
I'm going to say this at least three times throughout today's episode. in the therapeutic sense. Now, once again, I want to cue to some of the safety precautions here.
I'm going to say this at least three times throughout today's episode.
As I'm talking now, and various other times throughout today's episode, you may get the
impression that I'm all for everybody doing psilocybin, and that is simply not the case.
In order for psilocybin journey to be therapeutically useful, it does require certain conditions
and supports, and there are certain people for which psilocybin use is going to be contraindicated, meaning
they should not do psilocybin.
In particular, people who have existing or have a predisposition to psychotic episodes
or bipolar episodes, even having a first relative who has bipolar or schizophrenic or schizophrenic type of issues can be a rule out
condition that is can get someone eliminated from a clinical study on psilocybin for fear of
triggering psychotic episodes not just during the psilocybin journey but potentially in a long
standing way. So again, that's really critical. The other thing is that everything I'm talking about
today unless I say otherwise is really focused on adults, meaning people who are 25 years old or older, that is their basic
wiring and rewiring of the brain that we call developmental neuroplasticity is completed.
All right. Most of the studies today that I'll talk about involve subjects ranging from 25 years of
age, out to about 70 years of age, but no one younger. So again, psilocybin and its use is certainly not
for everybody, it's still illegal. It's being used in the clinical setting and research setting,
there are these pockets of decriminalized areas and potentially soon legalization of psilocybin,
but again only in the proper clinical setting. Okay, again, I say that not just to protect
myself, but I say that also to protect all of you. Silicibin is a powerful, powerful drug,
not just to be under the influence of,
but also in terms of its longstanding changes
after the effects of psilocybin have worn off.
I'd like to take a quick break
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year supply of vitamin D3K2. Let's talk a little bit about dosing of
psilocybin and also about micro dosing of psilocybin. Now, this is an area that I wouldn't
say is controversial, but that there's just how should we say this. There's a lot of
loose thinking around this in the non-clinical, non-research communities,
but within the clinical and research communities,
there's a lot of data that's come out
indicating what effective and safe doses
provided all other things are considered safe.
Safe doses of psilocybin actually are.
And here we really can go back to our discussion
of psilocybin as quote unquote magic mushrooms or mushrooms
and if one were to translate from the mushroom form of psilocybin to
the psilocybin that's actually used in various studies because
frankly in these studies people aren't eating mushrooms. They're typically taking synthetic psilocybin either
intravenously injected into a vein or orally and
either intravenously injected into a vein or orally. And that's how the researchers are able to tightly control the amount of psilocybin.
And the typical dosage that's used in clinical studies ranges from one milligram often
given repeatedly from day to day over long periods of time, so called microdosing.
And really that one milligram per day, or even
up to 3 milligrams per day, repeatedly over time, is what people generally think of as microdosing,
as compared to, say, a 10 milligram dose given once, maybe twice, in two separate sessions,
or a 25 to 30 milligram dosage that's given once or twice. Now, those amounts of one to three milligrams,
or 10 milligrams, or 25 to 30 milligrams, might not mean much to those of you that don't think
about these things in the research terms. Perhaps you've heard of microdosing and you've also heard
of macro or, quote unquote, heroic dosing, okay? That's sort common, or I was just a popular nomenclature
for psychedelics, and I'll circle back to that
in a few minutes.
But I think one of the questions that I hear a lot
is how much psilocybin is present
in a given amount of mushrooms.
And so the way this typically works is that mushrooms
are often discussed in terms of grams or ounces.
So in eighth of mushrooms,
we're first doing eighth of an ounce of mushrooms or X number of grams or ounces, so an eighth of mushrooms, refers to an eighth of an ounce of mushrooms,
or x number of grams of mushrooms.
The breakdown is actually quite simple.
1,000 milligrams equals one gram.
And the concentration of psilocybin
in most so-called magic mushrooms
is about 1%.
So one gram of mushrooms, 1000 milligrams means that it contains
approximately, and again, it's approximately 10 milligrams of psilocybin. And then most
of the clinical studies, it's been shown that the dosage of 25 to 30 milligrams given,
or I should say, taken once or twice, we'll talk about the spacing of sessions
a little bit later, taken once or twice is what's leading to the most pronounced therapeutic
outcomes.
But of course, with enhanced therapeutic outcomes, one also observes enhanced side effect
profiles, or what are called adverse events.
So there's an important nuanced conversation that has to take place.
But right now, we're talking about the conversion of grams of mushrooms to psilocybin.
So one gram of mushrooms being 1,000 milligrams containing 1% psilocybin means that it contains
10 milligrams of psilocybin.
Now the so-called heroic doses that you've heard about, and this is something that's discussed
more with the,
let's call them traditional or classic psychonauts.
These are people that may have an advanced degree,
but typically are not running laboratories,
exploring the effects of psilocybin
and controlled clinical trials.
These are people who have been long time explorers
and often writers and people who have been spokespeople
for psilocybin and other
psychedelics.
And they will often refer to the so-called heroic doses.
It's a little bit hard to translate from that informal community to the scientific data,
but in discussing that topic with various researchers who run laboratories at major universities
focused on psychedelic therapies.
What I was told is that the quote-unquote heroic dose that's often discussed really refers to a
5 gram or so dose of mushrooms. So what that translates to is 50 milligrams of psilocybin.
So when you hear someone talk about a quote-unquote heroic dose, they're probably referring to
ingestion of 50 milligrams or so of psilocybin, but in its mushroom form.
So about five grams of mushrooms.
And again, it's important to point out that the concentration of psilocybin in different
strains of mushrooms and in different batches, depending on the age of those mushrooms and
how they've been stored, et cetera, can vary tremendously from batch to batch.
In fact, there are some laboratories that have explored the range of psilocybin concentration in different mushroom strains, and different so-called magic
mushrooms. And that range is pretty broad. It's anywhere from a half percent all the way
up to 2 percent. What that means is that someone might get a hold of one gram of mushrooms
thinking that they're taking 10 milligrams of psilocybin in those mushrooms, when in fact
they're actually taking 20. Or somebody could take three grams of
mushrooms thinking they're taking 30 grams of psilocybin, and in fact they're
only taking 10 or 15 milligrams of psilocybin. So the sourcing is really key,
obviously, as things become more legal and more regulated and more used in the
therapeutic setting. Or, and this is what's happening more and more, or as people start to rely on synthetically made
psilocybin as opposed to using mushrooms
to ingest psilocybin, then certainly the dosaging
is going to be more consistent from batch to batch
because we're not saying about batches
and mushrooms we're talking about batches
of psilocybin itself.
So now I'd like to take a step back
from all this chemistry and cell biology and talk a little bit about the structure of a psilocybin itself. So now I'd like to take a step back from all this chemistry and cell biology
and talk a little bit about the structure
of a psilocybin journey itself.
And relate that to what we now know
about what's happening in the brain
during the psilocybin journey.
And then a little bit later,
we will return to that serotonin 2A receptor
when we talk about some of the more lasting changes
in brain chemistry and brain wiring
that occur after the
psilocybin journey is over.
So let's take a couple of minutes and just discuss the various components of an effective
therapeutic psilocybin journey.
And here I'm not detailing a menu of things that people should do in order to pretend that
they are a psilocybin assisted therapy coach or to do self-administered psilocybin therapy.
That is not what I'm doing. What I am trying to do is to share with you the consistent components
that are present in the clinical trials that have demonstrated the effectiveness of psilocybin
for the treatment of depression and for other compulsive and addictive disorders. And those data,
meaning the specific data related to those trials and the references themselves
will get into a little bit later.
But we can't really have a conversation about psilocybin and what it does without talking
about the so-called set and setting, as it's often referred to, that is known to at least
bias the probability of the journey
being beneficial and not a so-called bad trip.
So what are the variables that make up
an effective and safe psilocybin journey?
And again, when we say safe,
we're referring to people who are not prone
to psychotic episodes.
They don't even have a first relative
that's prone to psychotic episodes.
We're talking about people that are 25 years or older.
We're talking about people that, for instance, are not taking
antidepressants that impact the serotonin system.
This is very important to understand.
I think a lot of people don't know this, but as far as I know,
all of the studies that have explored psilocybin for its ability to
positively impact brain chemistry and mood and function have
required that people either not beyond or abstain from antidepressants in the weeks leading
up to the psilocybin journey.
Now that is not to say that if you are currently taking SSRIs or something similar that you
should cease taking them and do psilocybin, I am absolutely not saying that.
That could be very, very, very dangerous, if not catastrophic.
Anytime you're gonna take anything
or stop taking anything for that matter,
you do need to consult with your physician.
Let's get to the psychiatrist as well.
So let's talk about psilocybin journeys
from the subjective side and from the structural side.
And when I say the structural side,
what I mean is what does a psychedelic journey actually include?
And here are the words set and setting become extremely important.
Some of you may have heard that set and setting are the foundation of a well-done or even
therapeutically beneficial psychedelic journey.
And all of that really hinges on safety and outcomes.
So set refers to mindset, the mindset of the person taking the psychedelic
and setting refers to, as the name suggests, the setting in which they're taking it in and the people
that are present there. So let's talk about setting first. The setting for a psychedelic journey
needs to be one in which the person under the influence of the psilocybin or other psychedelic
is safe. That means no windows they can jump out of. That means no streets of moving cars they can run out into.
That means no opportunity for getting lost. That means no opportunity for getting into bodies of water.
In other words, it requires that there be at least one and perhaps even two or more other individuals who are not also taking psychedelics, right, who are not also taking psychedelics present
in that setting to ensure that the person taking the psilocybin is not going to harm themselves or others.
I say this not to sound like a school teacher, even though technically I'm a school teacher,
but because of course I don't want anyone to get harmed and I'm also aware that there's a lot of interest nowadays in
get harmed. And I'm also aware that there's a lot of interest nowadays in psychedelics such as psilocybin becoming legal or decriminalized for their therapeutic applications. And
if we look back to the late 1960s and early 1970s when the Control Substances Act was invoked
to make psychedelics like psilocybin illegal, one of the bases for that was not just the
geopolitical unrest at the time,
and things like the Vietnam War, but also some highlighted instances in which people did not take
set in setting into consideration, took things like LSD, stared at the sun, when blind, or took
Silasibon, went out, and harmed somebody else. Again, these are very, very isolated instances, but these
are the exact sort of instances that lead to criminalization or the fact that things
like psilocybin and LSD and MDMA for that matter are considered illegal. Again, I completely
acknowledge that there are a number of different factors making them illegal. We can have a whole
discussion about that. We talk about the drug trade, the war on drugs, but right now is such a critical time in the history
and the use of psychedelics for therapeutic
and other reasons.
And getting setting correct, meaning making it
absolutely as safe as possible for the person
taking the psychedelic is absolutely key.
And one of the best ways to ensure that it's safe
is to have responsible individuals
who are not under the influence of psychedelics
present in that environment.
So that's one component of setting.
The other component of setting that we talked about earlier,
which turns out to be very important,
is the opportunity and perhaps even the bias
toward the person on the psychedelic being seated
or ideally lying down and being in the eye mask
or at least having their eyes covered
so that they can combine any spontaneous visual hallucinations that occur with the various
thought processes that are occurring while under the influence of psychedelics.
This is far and away different than, quote-unquote, taking mushrooms and going into the woods or
taking mushrooms and going to the beach.
What we're talking about today is the use of psychedelics for particular brain
rewiring outcomes that, yes, can involve things like changing one's relationship to nature,
or changing one's relationship to somebody else by interacting with nature or somebody
else. And while I'm not trying to diminish the potential value of those sorts of psychedelic
journeys, if we look at the scientific data, the vast majority of it, not just in the clinical setting,
but in terms of understanding the safety and efficacy and positive rewiring of brain
circuitry that allows people to feel better, to understand themselves better, and to interact
with life in more adaptive ways, going forward out of the psychedelic journey, involve
these very, let's say, you know, subdued settings that are typically in one room,
a closed environment with one or two other individuals, acting as sort of guides or helping
the individual by talking to them from time to time if they feel like they have to sort
through a particular aspect of the psychedelic journey that's creating anxiety.
And we'll talk about the contour of the psychedelic journey that almost everyone who takes psilocybin
at somewhere between 20 and 30 milligram dosages
tends to experience.
But the setting that I'm describing
is not just a list of things to, you know,
make sure you're safe, but they're really the list of things
that also ensure that one can get the maximum benefit
out of the psilocybin journey.
Now, other things included in setting that are known, again, from scientific literature, to be very influential in terms of the psilocybin journey. Now other things included in setting that are known, again from
scientific literature, to be very influential in terms of the experience that one has and to
bias things towards a positive experience are, again, safety, I'm asked, but also the presence of music.
Now when I first heard about this from one of the premiere researchers on psilocybin and other
psychedelics, which is Robin Cardard Harris. He's a professor at University of California, San Francisco, who's
one of the major pioneers in the studies of psychedelics. And when he first started telling
you about the critical role that music plays, I thought, okay, that makes sense. You know,
music can impact our emotion, impact the way that we think, and could therefore impact
what one experience is during the psychedelic
journey. But he really underscored for me the extent to which music is not just a sort of
incidental feature of the setting in psychedelic setting, but that it is one of the, but that it is
one of the major drivers of the actual cognitive and emotional experience that somebody has on
something like psilocybin that allows the psilocybin journey to be looked at or viewed,
not just as beneficial, but, and this is quoted in the scientific literature as one of the
most profound and important positive experiences that one ever experienced in their life.
So let's talk about the sorts of music that have been used in these clinical studies.
Well, first of all, we need to think about
how long the psilocybin journey itself is going to be.
And the typical duration of the psilocybin journey
is anywhere from four to six hours.
It's going to depend somewhat on dose.
It's going to depend somewhat on variability in people's
liver metabolism
and it's also going to depend somewhat
on how much food people have in their gut.
In all the clinical studies that I read,
it was advised that people not have any food in their gut
at the time in which they ingest or injected
with the psilocybin.
It's particularly true of people are going to be taking
psilocybin mushrooms in order to get their psilocybin.
And that has been done in a few studies.
So most studies, however, use synthetic psilocybin taken orally.
Again, that's converted to psilocybin in the gut by the acidity of the gut.
And the acidity of the gut is going to be impacted by the various foods that people eat.
And so that's one of the major reasons why people are advised to not eat for at least
four hours prior to
the psilocybin journey.
So, here we've got this six hour, what we're calling journey, because that's what everyone
calls it, or trip, that people start experiencing about 30 to 45 minutes after ingesting psilocybin
or taking psilocybin.
There's a peak component in which there's a maximal intensity of emotion and often that's
also associated with anxiety.
And this is very important to understand.
The anxiety component is part of what in the therapeutic setting they refer to as ego
dissolution and that anxiety around the peak.
And I think most people would probably hear peak experience and think, oh, we're talking
about a peak positive experience. But no, we're referring to a peak experience and anxiety
that people stay with and then come down from gradually as one goes from the second or
third hour after taking psilocybin. And that tapers off slowly toward the six hour mark, what sometimes people refer
to as parachuting back in. Of course, they're not, hopefully, I would very much hope people aren't
actually parachuting back in while on psilocybin, but I think you get the idea. The music that's
typically played in the clinical studies using psilocybin for the treatment of depression or for compulsive disorders or addiction,
tends to have a particular contour
that matches with and can also drive
that contour of the psilocybin journey that I just described.
Again, we're talking about people wearing an eye mask
with guides present, so people who are not taking psilocybin
there as well to ensure that the person feels supported and is safe.
The person is typically lying down, sometimes sitting down, but more often,
not lying down, wearing an eye mask.
And the music that's played at the beginning of the psilocybin session
tends to be music that doesn't have a lot of vocalizations.
It tends to be things like classical music.
It tends to be fairly low volume, but then transitions into music that has a lot of percussion.
So often drums, that tends to be higher volume, that has a lot of intensity.
At about the time, that one would be experiencing the peak in emotion and in perception, the so-called peak of the journey.
That intense music tends to be played for about 45 minutes to 90 minutes, depending on the study one looks at,
and then tends to transition into softer music again, sometimes choral type or more melodic music,
often female voices in particular, and then
transition into nature sounds and things that are more or less mimic the outside natural
world and less so synthetic things like drums or instruments and vocalizations and things
of that sort.
So why would it be so important that music match and even contribute to the subjective experience
that people have on psychedelics.
And here we should probably take a couple of moments and just talk about what those subjective
experiences are like. So for people that haven't done psilocybin or any psychedelics,
it's a little hard to describe. But one way to describe it is that there's a lot of so-called
perceptual blending. So for instance, people in the eye mask will report seeing some geometric
shapes and colors, but perhaps the music they're listening to will then start to change the
intensity or the movement of whatever it is that they're seeing hallucinating inside
of the eye mask in ways that are linked. This is referred to as synesthesia or the merging
of different senses that are not ordinarily merged. In addition, people under the influence of psilocybin or other psychedelics for that matter
often will report that their pattern of breathing becomes linked to the perceptions of things that they
are hearing or seeing or feeling. So for instance, if they take a big deep breath in and then a long
exhale out, they may find that during the long exhale out, that the notes
of music that they're hearing in those moments are also drawn out for the duration of the
breath, and they'll inhale, and that they're getting at least what they perceive as control
over the music, which of course they are not actually controlling by using their breath.
And that perhaps their visual perceptions are also being merged with that.
So those are just a couple of examples of how perceptual blending, aka synesthesia, can occur while under the influence of psilocybin.
And this really is highly individual from one person to the next. Some people, for instance,
will find that if they take their fingertips and rub them across the couch or the chair
that they happen to be lying down or sitting on, that they will experience a change in the
music. Maybe even if they move their hand up that they will experience a change in the music,
maybe even if they move their hand up, they hear an increase in frequency of sound,
they move their hand down, they hear a decrease in frequency of sound, and that all of this is linked
to their emotional state at the same time, and vice versa. We're talking about a lot of perceptual
and emotional blending and some sense of control over one's perceptions and emotions in a way that's very
unordinary, even extraordinary.
Now we can step back from all of this very subjective description of the psychedelic journey and ask
what is going on that would allow these sorts of things to occur and there you are already equipped with an understanding of the
cell biology and the chemistry that makes all of this possible.
And that is that when psilocybin is ingested and then converted to silicin, it's the
silicin that crosses the blood brain barrier.
And then even though silicin looks a lot like serotonin, silicin has this incredible ability
to predominantly activate the serotonin 2A receptor.
Well, we can understand much of what's happening at a
subjective level during the psychedelic journey, even right down to the sorts of emotions and
perceptual blending the synesthesia. We can understand a lot of that by understanding
where the serotonin 2A receptors are expressed on neurons and what those particular neurons
are doing. And the simplest way to describe this is that there's a category of neurons that we call pyramidal neurons.
Pramidal neurons are found lots of places in the brain,
but they're called pyramidal neurons
because they're shaped like a pyramid.
They have a cell body, which is the part of the cell
that has the DNA in it.
A lot of other important things like the organelles
might have conduit, et cetera.
And then they also have what are called dendrites.
Dendrites are the little branches or processes
that reach out both from the bottom of these cells.
And then these pyramidal cells are interesting
because they also grow a branch up, up, up, up, up, up,
into layers of neural tissue above them.
And they have what's called an apical branch.
That's the part that grows up.
And then they fan out at the top. And that fanning out at the top allows them to communicate with
other neurons in their environment. Okay. So if you're not getting a good picture of this
in your mind for my description, I apologize, but simply think about putting your arms out
to the side. And by doing that, you're able to interact with things that are some distance
from your body. It's sort of an obvious thing in that case. These cells are effectively doing the same thing by extending little processes out into layers
above them and to the sides. And this is really important because much of the serotonin
two A receptors that are present on neurons in the brain are present in those apical
dendrites, those branches of these pyramidal neurons that are above and that extend out to the side of those neurons.
And so when somebody is under the influence of psilocybin, that means that psilocybin has bound
to the receptors on those apical dendrites and it's increasing lateral communication across brain areas.
In fact, this is perhaps one of the most well-documented effects of psilocybin and
other psychedelics, which is that there's a shift from the brain being more modular, meaning
more segmented, like auditory neurons are communicating electrically and chemically, largely
with other auditory neurons. Of course, they'll communicate with other types of neurons,
too, right? When I hear something off to my right, you know, like a snap of fingers off
the right, I'll turn my head, and my ability to do that depends on my auditory neurons
being linked up with things like my motor system and my visual system. But the key thing
to understand is that when there is psilocybin present in one system, that the communication
of any of these pyramidal neurons, the ones involved in hearing, the ones involved in thinking,
the ones involved in memory, the ones involved in visual perception or in the generation of visual
hallucinations with eyes closed, those are all talking to many, many more other neurons more
extensively. So what happens effectively is that there's a reduction in the modularity, the separateness
of function in the brain, and an increase in what's called integration of communication
across what would otherwise be disparate brain regions.
We can say that really simply by saying, psilocybin increases communication across the brain.
Now, in addition to that, there's a reduction in what's called the hierarchical organization of the brain. Now, in addition to that, there's a reduction in what's called the hierarchical
organization of the brain. Typically, sensory information comes in from the outside environment. So,
we hear something, we see something, we taste something, we smell something, and in what's called
bottom-up fashion, meaning bottom from the periphery, up, meaning it propagates up through the eyes, through the nose, through the ears, through
the skin, or the senses in those regions, I should say, up into areas of the brain that
sit deep to the cortex, like the thalamus.
And then the thalamus is sort of a way station.
It's like a switchboard that sends visual stuff to the visual centers and auditory stuff
to the auditory centers and touch stuff to the touch centers
and things that maybe trigger a memory
to off to the memory centers of the brain, et cetera.
That's the typical organization.
It's hierarchical because it goes from the periphery
up to the more complex processing regions of the brain
that make decisions, that link all of that stuff
to prior experience, maybe plans about the future.
When psilocybin is present in the system, there's a broadening of the flow of that information
from the bottom up as well. And that has to do with what's called the laminate gating. The thalamus is
a very interesting structure. We probably don't want to go into it in too much detail right now,
but it really is like a switchboard in a way station saying, hey, pay attention to the visual stuff.
Pay attention to the auditory stuff or just to the visual and auditory stuff and ignore,
you know, touch sensation for the time being.
We're vice versa.
When psilocybin is present in the system and when serotonin 2A receptors are activated
very strongly, there is a tremendous broadening of the flow of information up and through
the phalamus.
So not only is there more communication of so-called higher-order brain centers, we refer
to them as higher order because they're involved in thinking and decision-making and emotion,
et cetera, but there's also a shift in the flow of sensory information into the brain that
can generally be described as broader and including more blending of the different senses.
And when I say blending of the senses, I'm also referring to blending of the sense of interoception,
of our sense of our body and what's happening inside of our body. And this, without question,
at least partially explains why when under the influence of psilocybin, one's breathing can be linked to a sound,
and then suddenly the sound, one thinks,
is being controlled by one's breathing,
or that the sound itself can be linked
to something that we see in our mind's eye,
while in the eye mask.
Essentially what I'm describing here is
that serotonin to a receptor activation
allows for more broad, less precise, and less hierarchical activation
of brain circuitry.
And when I say hierarchical, what I mean is that normally things go from periphery, from
eyes to thalamus to visual cortex.
However, when under the influence of psilocybin, as I mentioned before, even in the eye mask,
the visual cortex is going to be very activated, even in the absence of any visual input.
So then, if one hears a sound, perhaps from music, a particular motif or voice, and that's
linked to a particular emotional state, that is now being blended with visual phenomenon
occurring within the brain that have no external stimulus.
And so while the patterns of activation in the brain while under the influence of psilocybin aren't random, they are far less channeled, far less modular, and far less hierarchical
than would ever be the case when not under the influence of psilocybin.
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Huberman. Now in all fairness to the scientific literature,
there are not one, not two, not three, but four prominent
theories of which brain networks are most activated
during a psilocybin or other psychedelic journey.
And so for those of you that are interested in those different models,
first of all, please know that they are not competing models.
While some of them disagree about some of the details, it's very likely that all of these
models are true.
They include things like changes in the so-called default mode network.
There's a lot of interest in this.
I've talked about it before on this podcast, the default mode network because the network
in the brain that's thought to be responsible for spontaneous imagination, for day dreaming, and that reflects sort of the base activation
state of the brain when there's no drugs in our system.
And the default mode network is one of the systems
or networks rather that is thought to be
rewired under conditions of psilocybin or other psychedelics.
Again, if you're interested in these models
in comparing and contrasting them,
there's a very nice review from Brian Rothslab at Duke entitled the Neural Basis of Psychedelic Action
will provide a link to this in the show note captions. And again, I just want to emphasize that
all of these models have been shown to be true in different studies. And what they all point to
is more extensive communication between areas of the brain that normally are not as active
at the same time while under the influence of psychedelics such as psilocybin.
The controversy in the field relates to which of these networks is the one that changes
the most to explain the therapeutic outcomes that have been discovered in recent years.
So again, check out that review if you're interested in that sort of thing.
In the meantime, we can cut a broad swath through all of those models and just say that
psilocybin expands the functional connectivity of the brain while one is under the influence
of psilocybin. And it does seem that some of that expanded functional connectivity persists
after the effects of psilocybin have worn off. And that statement about the functional
connectivity of the brain being more expanded, not just during the psilocybin session, but after as well has been substantiated in a number
of papers. But one of the key papers in this area is one that I recommend people check out if
they're interested in this sort of thing is entitled the effects of psilocybin and MDMA on
between network resting state functional connectivity and healthy volunteers. And I like this paper
for a number of reasons. First of all, it's a very high quality paper carried out
in the laboratory of Robin Carter at Harris at UCSF.
Again, one of the premier researchers
in this area of psychedelics and their function,
what they do in the brain,
and also their therapeutic applications,
but also because it focused on healthy volunteers.
They explored using brain imaging,
what brain areas are active in a resting state,
so things like default mode network,
then they had people take psilocybin or MDMA, and then they looked at the connectivity between those
brain areas in those same individuals when they were not under the influence of these drugs and
found more extensive connectivity, all of which pointed to an enhanced lateral connectivity, less hierarchical organization,
effectively more interconnection and communication
between different brain areas.
I think not only is the fact that they looked at healthy volunteers
very interesting and important,
but also that they looked at this resting state of the brain.
They weren't providing a particular auditory or visual stimulus
for people to hear or look at while they were in the brain imaging scanner,
as it's called
Rather they were simply looking at how the brain was behaving at rest
And so it's very clear that for people that do too or even just one of these psilocybin journeys and a particular dose
That the brain is actually getting rewired. You know, we hear this a lot
psilocybin or other psychedelics lead to plasticity. They rewire your brain. Let's
go back to what we said at the beginning. Rewiring of the brain is not the goal. Adaptive
rewiring of the brain is the goal, right? Rewiring that leads to new ideas that are interesting
that are accessible after the psychedelic journey. New ideas and new ways of thinking or
feeling that allow people to function better in their
lives, that's the goal of effective psychedelic therapies, not simply rewiring of the brain.
You know, a brain injury for that matter will lead to rewiring of the brain, but that's
maladaptive rewiring.
The use of things like amphetamines or methamphetamines in particular will lead to rewiring of
the brain, but that is strongly maladaptive rewiring.
So now there are really dozens of studies conducted inhumans using brain imaging and other
techniques have evaluated how things like psilocybin change connectivity in the brain.
And I think the take home message is it expands that connectivity.
However, it seems to do so in ways that still allow people to function in their daily lives.
One of the key things that I gleaned from the literature on the therapeutic use of
psilocybin for the treatment of depression is that very seldom do people who take psilocybin
experience long-term issues with memory.
Why is that so critical?
Well, you could imagine that increasing connectivity in the brain, reducing modularity,
reducing hierarchical organization in the brain would lead to disruptions in memory,
right?
It's as if you're shuffling books on the bookshelf, so to speak, but that doesn't seem to
be the case.
Rather, it seems that the increase in connectivity is leading provided setting, setting are
correct, provided safety protocols are followed to positive rewiring or adaptive rewiring of
neural tissues.
That's one of the things that makes psychedelics and psilocybin in particular very exciting
from the therapeutic standpoint.
And of course, we have to acknowledge it's also what has a lot of people excited about
psychedelics, not just for the treatment of depression, but for expanding the brain's
capabilities more generally.
So along those lines, I want to touch on the issues of creativity and the experience of
life outside of psychedelic journeys is impacted by psychedelic journeys.
And here this relates to a question that I heard a lot when I put the call out on social
media that I was going to do this episode.
And I asked people, what do you want to know about psilocybin?
And one of the more common questions that I got was, does it increase creativity? Does it increase our experience of life in ways that are beneficial,
aside from its now documented positive effects in treating depression and compulsive disorders and
addiction? And the short answer to this is yes, but that the positive effects of psychedelics,
psilocybin in particular, on creativity and our experience of life,
have only been explored in a fairly narrow set of dimensions.
However, where it's been explored, there's some really interesting findings.
So one of the more interesting findings, I think,
is a paper entitled, Increase Low Frequency Brain Responses to Music
after psilocybin therapy for depression.
I think this is a really interesting paper, because what the authors did is they took advantage of the fact that in these therapeutic psilocybin sessions
that were carried out for the treatment of depression, music is being played and there are prior
studies showing that when music is played, you activate different brain areas depending on what
sort of music is being played. That's somewhat obvious, perhaps. You know, sad music versus, you know, intense, you know,
you could think about heavy metal versus choir music versus
Gregorian Chants versus punk rock music and on and on.
It makes sense that different brain areas would be activated
when different patterns of music are played.
However, the do seem to be some universal features of brain activation in response to music.
This should probably be the topic of an entire episode
of the Hewerman lab podcast,
and indeed it will be, for instance,
there are areas of the auditory cortex
that are activated, no surprise there,
and areas of the brain's reward circuitry,
the so-called ventral striatum,
and the so-called mesolimbic reward pathway.
I talked a lot about these in the episodes about dopamine that I've done previously.
These are brain areas that lead to the release of dopamine in other brain areas and that
reinforce certain experiences and that tend to give us the subjective feeling of, yes,
I like this, I want more.
So in this particular paper, what the authors did is they took advantage of the fact that people are in the clinic,
they're on psilocybin, they're listening to music.
And as you recall, the music played at different stages of the psilocybin journey are different.
They have a different emotional component.
And music is a really nice stimulus in the laboratory, as we say, because like with
visual stimuli, you can break it down into high frequency, low frequency.
All right, sounds like doon doon or these kinds of things.
I was my attempt at low frequency versus high frequency,
auditory stimuli, or at the spatial frequency,
or what in the auditory domain would be called
the temporal frequency, is it boom, boom, boom,
or is it boom, boom, boom, boom, boom, boom,
all we've changed there is the temporal frequency.
The sound was somewhat the same, but the distance between those sounds was different.
You get the idea.
So they have access to these people and these different conditions, and they can put them
in the brain scanner, and they can do that before and after having taken psilocybin.
And the long and short of this study is that psilocybin
changes one's experience of music,
not just during the psilocybin journey itself,
but thereafter.
And in fact, it changes one's emotional response to music
in very interesting ways.
For instance, one of the more common features
of major depression is that people don't derive as much pleasure from different types of experiences, whether or not it's food
or sex or social experiences, to the point where sometimes they just stop trying to seek
out those experiences.
People with depression often feel as if music no longer has the same impact.
It just doesn't really lift them up very much.
This study found that people who have taken psilocybin, according to the parameters we talked about earlier, can get a return of
the elevated emotionality, the positive emotions associated with music that formerly made them
feel good. In other words, they can feel music again. They can feel good in response to
music again. Now, this is interesting because in theory,
it could be that psilocybin simply allowed them
to access the emotions around music again more generally,
but that's actually not with this paper
and some other papers that have been published report.
Rather, it seems that taking psilocybin
can increase one's positive perception of music that one likes
and can tone down or reduce the depressiveness or the sadness of music that tends to make one
sad, even after the psilocybin has worn off and for a long period of time afterwards,
maybe even forever, although no study, of course, can be carried out forever because forever,
it's forever.
What we do know, however, is that psilocybin can rewire the connections between the emotion
centers in the brain and the networks that control auditory perception of music and leads
to this condition in which people who felt like, I was depressed or I couldn't feel the
music, I just wasn't getting the same lift and joy from it again, they can start to experience more joy from that music again and that music
that made them feel sad and depressed has a diminished capacity to make them feel sad
and depressed.
And there's a lot of neuroimaging data in this paper that point to the specific brain
areas that include areas like the ventral tegmental area that can explain why these sorts of effects
were the curse.
So this isn't just subjective reports of people saying, oh yeah, you know, I was depressed
and then music didn't feel really good.
And now it feels great.
Or that used to make me feel so sad.
And now I feel like I have a capacity to listen to that without being, you know, crushed by
feelings of sadness.
The paper included some subjective reports of that sort, but then was able to link those
to changes in brain circuitry and brain activation
in response to music using neuroimaging. So in that way, it really points to both the subjective
and structural and functional changes that psilocybin can bring about through that expanded
connectivity between brain errors. Because remember during the psilocybin session, it's not as if
music or the perception of music is specifically being looked at or
focused on in these studies, rather music is playing. People are in the eye mass, they're
feeling all sorts of things, they're breathing, they're hearing, they're touch, it's all happening
all at once, there's a peak, it's long, there's a long taper, the music's changing. Okay, all of that
took place in this study as well, but it is after the session when comparing
brain activation states to music of our particular type, sad or happy, and comparing that to
the patterns of brain activation that occurred before the psilocybin journey, that they discover
that people's brains have rewired during the psilocybin session in a way that allows them
to experience joy and response to music again.
So that's one of the more rigorous studies I was able to find that addresses this question of whether or not
psilocybin really does rewire the brain in ways that allows us to be more creative and experience life differently
after the psilocybin session. Now that paper didn't focus specifically on creativity. I did an entire episode on creativity
that talked about different types of meditation,
like open monitoring meditation.
It talked about different patterns of thinking
that one can actually practice to increase creativity.
We had arguably one of the most creative people
on the planet, Rick Rubin.
Came on this podcast, talked about the creative process
from the perspective of music and his role
in producing music.
So you can check out those episodes if you're interested in the neural circuitry related to
creativity. At least at the time of recording this episode, there haven't been a lot of studies
looking specifically at the brain networks that we think are involved in creativity and how those
change in response to psilocybin and other psychedelics. I imagine those studies are either
happening now or will happen in the future. But the studies I just described, referring to the changes in emotionality and responses to music,
I think provide a nice template for what's likely happening, both during psilocybin
journeys and after those psilocybin journeys. When we talk about less hierarchical organization,
more connectivity between brain areas, what it's pointing to is the fact that during the psilocybin journey,
people have the opportunity to learn new relationships between different sensory and emotional states.
And those new relationships seem to persist long after the psychedelic journey has been finished.
And a lot of people researching psilocybin in the clinical setting think that that's one of the
major reasons why psilocybin in other psychedelics
can rewire our relationship to things more broadly.
It allows for new learning, new contingencies.
And when we look at depression,
we often think, you know,
diminished mood, people now have an appetite,
they're not interested in social relationships
or romantic relationships, they're really struggling.
And all of that, of course, is true.
But another lens to look at depression through is that a lot of that thinking and a lot of those emotional states that are negative
are somewhat habitual. They relate to a sort of implicit understanding and living out
of the idea that A leads to B leads to C. Okay, you seek out a relationship, it doesn't
work out. Try a new job, you don't get the job, you get the job, it's no good. All these
negative outcomes of if A then B then C. And it does seem that psilocybin can
have this effect of invoking new patterns of learning, new considerations about what might
be possible. And indeed, may even lead to actual rewiring of the emotion centers in the brain
with these other brain areas and vice versa in ways that eject people from the psilocybin
session thinking, oh, you know, yeah, I used to feel this way
about something, work, relationships myself, et cetera.
But I'm willing to consider this other possibility
or this other possibility seems at least partially true
to the extent that I'm willing to go out
and evaluate that.
Now here I'm speaking very subjectively,
but remember, we have to tie back the subjective experiences
and changes of things
like music and emotion and our relationship to life and jobs and relationships back to the
cell biology and chemistry of psilocybin because ultimately it really is just a chemical
activating receptors, those receptors changing networks in the brain and the journey itself
seems to be the time when all of those changes are put in motion. It's like a boulder that gets rolling.
In fact, I think the best way to think about
psilocybin and other psychedelics is that they initiate
the neuroplasticity process, but they are not the neuroplasticity process itself.
And the journey itself is not where all the neuroplasticity occurs.
We know that for sure.
In fact, if you want to imagine how
psilocybin and other psychedelics work to change the brain, think about them as a wedge that gets
underneath the boulder that is the neuroplasticity that gets rolling forward. And then think about
whether or not the plasticity is adaptive or maladaptive, whether or not it actually serves you in
your life on a daily basis or not, depending on whether or not you're using your conscious brain to move that boulder in a particular
direction, not just bulldozing through things and destroying them, but clearing a path
through old, ineffective, maybe even destructive patterns of thoughts or emotions, etc.
I give you that analogy because I think it more accurately captures what psychedelics,
like psilocybin are doing,
rather than the typical discussion around psychedelics
that we tend to hear, which is that,
oh, it creates plasticity and plasticity is what you want.
The next couple of minutes, I'd like to focus
on some of the key and stereotype
that is characteristic experiences that people tend to have
during a psilocybin journey,
because there's some really interesting research on this.
These are phrases that perhaps you've heard before, things like letting go,
ego dissolution, feelings of connectedness. While all of that is very subjective on the one hand,
those words are heard often enough and repeatedly enough in psilocybin sessions and after psilocybin sessions,
along with this description of this psilocybin
experience as one of the most profound of one's life, or one of the most positive in the ideal case
of one's life, that they are worth exploring. We should also, of course, explore the so-called
bad trip, the possibility that someone will have a not good time or even very frightening time
while under the influence of psilocybin. So there have been some scientific studies that have explored what
sorts of subjective experiences that is thoughts and feelings, insights that
people have that relate to positive therapeutic outcomes, and more generally with
the sense that the psilocybin journey was positive or maybe even tremendously
positive in one's life. So while there's a century or more of writings about psychedelics that describe things like
enhanced feelings of connectedness or dissolution of the ego, the loss of one sense of self,
and then the regaining of one sense of self, and so on, there's a particular paper that
describes some of those things in terms of rating scales, that is, the sorts of tests
that people can take in which they answer particular questions
and that link back to things like feelings
of connectedness and ego dissolution
that allows us to put some numbers to those experiences
and to look at some of the statistics
associated with those experiences.
And this is really what's important
about scientific studies,
whether or not a measure is subjective,
so if someone's self-reporting how they felt or feel,
or whether or not it's measure of blood pressure
or of a chemical in the blood stream, etc.
It's the use of numbers and statistics that allows comparison between different groups and that can be compared between studies
that allows us to make some firm conclusions about what sorts of things
psilocybin may or may not be doing when it's effective or not.
So the paper I'd like to highlight is entitled, Quality of Acute Psychedelic Experience predicts therapeutic efficacy of
psilocybin for treatment-resistant depression. I'll put a link to this paper in
the show note captions, but the basic contour of this paper is that they looked at
subjects that underwent two different psilocybin sessions. One, at a relatively low-ish dose of 10
milligrams of psilocybin, again that would be equivalent to about one gram of psychedelic mushrooms, more or less.
And a second session involving subjects taking 25 milligrams of psilocybin, or what's roughly equivalent to somebody taking two and a half grams of psilocybin mushrooms. Those people then answered what's called the altered states of consciousness questionnaire,
which allow them to address, and here I'm paraphrasing, the quality of experiences in the 25
milligrams psilocybin session. So without going into too much detail, it's often the case in these
sorts of two session studies that subjects will take a slightly lower dose of psilocybin to familiarize
themselves with the experience, and then the higher dose that leads to the more intense experience, intense meaning a
bigger, more intense peak, a longer session overall, greater distortions and emotionality
and perceptual experience, all the stuff we talked about before.
So what this study found is that one of the key features, if not the key feature of a
positive quote unquote psychedelic experience
is this sense of oceanic boundlessness
occurring at some point during the psychedelic journey.
Now oceanic boundlessness doesn't necessarily mean
anything to any of us.
It probably means different things to different people.
It's this idea that one is experiencing something
extremely unusual, even mystical, and beyond this world
and one's normal experience, but that it's not aligned with any specific outcome in the
moment.
It's not directly attached to any one feeling or memory or thought process.
It's a little bit tough to describe because I can guarantee you, I'm not on psilocybin
or any psychedelics right now.
And I can only imagine that you're not, although some of you might be, I can guarantee you, I'm not on psilocybin or any psychedelics right now. And I can only imagine that you're not
to lose some of you might be.
I can't even imagine what this podcast would be like
for somebody on psilocybin at this moment.
But in any case, oceanic boundlessness,
a feeling of the experience being mystical
and not really heading in any one particular direction,
just a feeling of massive connectedness
with one's environment, both in the room and session, perhaps with the guides, with oneself, with
one's past, with one's present, people outside the room, with the entire world, maybe even
the universe, that sort of thing.
The intensity of that experience of oceanic boundlessness, the mystical experience, seems to be positively correlated
with positive therapeutic outcomes. That is relief from major depression.
During the psychedelic journey, as we talked about before, there are a number of steps that one
typically goes through. So there's the build up to first experiencing the effects of the drug
about maybe 20 to 45 minutes into the
journey or trip, then the peak.
And it is during that peak that people often feel the sense of oceanic boundlessness.
However, it's also often the case that it is during the peak, the maximum intensity
of emotion.
And we know based on direct measurements, also increases in blood pressure and heart rate often very significant increases in anxiety and fear as well.
That people will experience things like ego dissolution.
And the guides role at that point is of course to keep the person safe, make sure they don't run out of the room, jump out of a window, run into traffic.
to keep the person safe, make sure they don't run out of the room, jump out of a window, run into traffic.
Sadly, these are things that have happened outside of a strong, healthy, safe set and setting.
But the guide's role is to keep the person safe, but also to encourage them to let go and
move through that experience, to experience the anxiety, allow it to peak, allow them to
see that they're not going to die from that anxiety.
They're not going to dissolve.
They won't lose their sense of self completely, or they may temporarily feel as if they lose
their sense of self, but then they feel it restored at various intervals during the peak,
or as they exit that peak and move toward the, say, second, third, fourth, fifth hour of
the session.
So, when exactly these feelings of oceanic boundlessness
and ego dissolution occur varies from person to person, but typically it's during the peak that
the ego dissolution, the fear and the need to, quote unquote, let go is most typical. I think
perhaps the best way to describe the data in this paper in a way that's meaningful to everybody
is to refer you to figure two, which if you're
not looking at the paper, it won't mean anything to you, but I'll describe it.
And if you do want to take a look at figure two, again, you can access the paper in the
show note captions.
What they did is they looked at a number of different subjective measures, things like experience
of unity, the feeling that one is connected to others into the world. Things like spirituality, whether or not
the whole thing felt like a spiritual experience,
whether or not it was a blissful state,
whether or not there were insights,
whether or not somebody felt disembodied out of body,
whether or not somebody had a lot of anxiety,
whether or not they had these synesthesia,
these blending of visual auditory, touch, and breathing
and things of that sort.
And they addressed which of those measures
related to the positive clinical outcomes
that were observed later after the psilocybin were off. And while I'm not going to go point by point through each one of these measures,
there's a general feature to emerge from the study, which is that
the experience of unity, the sense that the psilocybin journey was spiritual,
an experience of bliss at some point inside of the psilocybin journey was spiritual and Experience of bliss at some point inside of the psilocybin journey
The sense that there were insights that there were learnings about one's life and oneself
When those things were experienced very strongly that correlated with the person being what was called a
Responder to the psilocybin treatment meaning they got relief from their depression
Whereas people who felt less of that, okay? so the non-responders, as they're called, the
people who do not benefit so much in the long run from the psilocybin treatment, tended
to report less of an experience of unity, less of a spiritual experience, less of a blissful
state, less insightfulness, and so on.
Whereas there were very few differences between the people that derogged benefit from the
psilocybin treatment and those did not, along the dimensions of syneshesia, this blending
of different perceptions that ordinarily doesn't occur for most people, or complex imagery,
right?
Put simply, everyone who took psilocybin in this study at 25 milligrams saw a complex
imagery. They saw a lot of hallucinations
But just seeing hallucinations did not lead to the positive clinical outcomes in terms of mood
Anxiety was a very interesting measure here because ordinarily we think of the ego dissolution the letting go is such a key component of the psychedelic journey
In terms of the positive therapeutic outcomes. This has been discussed quite a lot.
And in full disclosure, Robin Carter at Harris has already come on to record an episode
of the Hubert and Lab podcast.
That episode hasn't been released yet, but it will be released soon.
And he talks about the importance of this letting go in terms of the positive clinical outcomes
of the psilocybin journey.
And indeed, that is true.
And I should also mention that Dr. Matthew Johnson from Johns Hopkins, who also runs
a laboratory
exploring psychedelics and their role in treating things like eating disorders and depression,
etc.
Also doing incredible work.
Also talked about the importance of letting go during the psilocybin journey, this ego dissolution,
this ability to move through the anxiety.
And again, I can't underscore this enough because it's been told to me over and over again
by the top researchers in this area
that people head into that peaking phase
of the psilocybin journey.
And oftentimes it is not pleasant for them.
They're feeling like it's uncomfortable, it's scary,
and their heart rate is up, and their blood pressure is up,
and they're having a hard time calming down
than they want to calm down.
But it does seem that while the guides should not ramp them up
and get them more stressed, that the ability to move through that stressful period to somewhat guide oneself,
or to be encouraged to guide oneself through that peak, and that anxiety and the fear of losing
oneself and the so-called ego-disillusion that occurs, is an important feature for an effective
therapeutic session. In this study, anxiety itself was inversely correlated with a positive
therapeutic outcome. So this is important and somewhat nuanced. On the one hand, I'm telling you
that the letting go, the ego dissolution, does seem to be important in terms of reporting a psychedelic
experience as effective as having accomplished something and perhaps even explaining
some of the long-term positive effects to emerge from that psychedelic journey. In this case,
psilocybin journey. However, non-responders, that is, people who did psilocybin, but did not have
a positive therapeutic outcome in comparison to the responders. Those non-responders tended to have higher subjective
ratings of anxiety than did the responders. So this is important and what it speaks to is the fact
that, well, yes, letting go during the session, experiencing some anxiety, perhaps even the
ego dissolution of dissolving of self and then the return of self is important. It is also important, it seems, that anxiety not be so, so high or subjectively experienced
as so high that one does not experience the positive neuronal rewiring that leads to
a more pervasive elevated mood.
So I'm definitely saying two things at once because I'm trying to capture the data accurately.
It would not be fair for me to say, just let go, experience as much anxiety as is possible.
And that's part of the process.
Yes, letting go, again, an air quote seems to be important for one's experience of the
psychedelic journey in particular around the peak that occurs about two hours in or so.
However, extreme levels of anxiety seem inversely correlated or
negatively correlated would be the better way to put it with the positive therapeutic outcome
or relief from depression. So this takes us back to all of the things we've been talking
about thus far, not just the chemistry and biological action of psilocybin, but the key
importance of getting dosage right, the key importance of making sure that you're in
a safe environment,
but also one in which the guides really know what they're doing.
I think this is one of the biggest and most important reasons
for having well-trained guides who really understand
the contour of the psychedelic journey,
but are also trained in how to help somebody
with their anxiety in real time while they're
under the effects of psilocybin. And of course, to help somebody with their anxiety in real time while they're under the effects of
psilocybin.
And, of course, to help people integrate those feelings of high anxiety and maybe guide
them back down to a calmer state during the psychedelic session itself.
And here I can just mention some unpublished data and studies, and, again, this is very
preliminary, but through discussions with Dr. Matthew Johnson, who is running these psilocybin
and other sorts of psychedelic trials at Johns Hopkins.
He and I discussed the importance of having a real-time tool to adjust anxiety while under the influence of psychedelics like psilocybin.
And there he asked and they've started to incorporate is my understanding some of the real-time respiration tools, that is breathing tools, that we know based on work in my laboratory, Dr. David Speagles' laboratory,
can reduce anxiety very quickly in real time, and that involves the use of the so-called physiological sigh.
I've talked a lot about this before on previous podcasts, so rather than explain it to you again here now,
we'll put a link to the physiological sigh. I do a demonstration of it in the show note captions.
I'll also link to a recent paper that we published in cell reports medicine.
This was a collaborative work that my laboratory did with Dr. David Speagles Laboratory at Stanford
School of Medicine, showing that the physiological size among the different deliberate respiration
techniques, one of the fastest and most effective ways to reduce levels of autonomic arousal
aka anxiety or stress.
And Dr. Matthew Johnson's laboratory
has started to incorporate physiological size within these psychedelic sessions as a tool
that the guides can refer people to before the session begins, teaching it to them, so
they realize they can calm themselves down if necessary in real time. It works the first
time, it works every time. This is not because it's some magic breathing technique that
I created, it certainly is not. This is not because it's some magic breathing technique that I created.
It certainly is not.
This is a naturally occurring pattern of breathing that occurs in sleep and in waking, but that
when done deliberately leads to very rapid and quite significant decreases in stress and
anxiety.
And then when people are inside of the psychedelic session, if they feel their anxiety levels
are going too high, they're heading toward what might be called a quote-unquote bad trip.
They're starting to panic or really think they're going to have a panic attack or die.
Again, the subjective experience is going to be layered on top of the physiological
experience.
And one's heart rate being really elevated.
So stress and agitation.
By using the physiological sigh inside of the psychedelic session, Dr. Johnson's laboratory,
and I believe at least one other laboratory are starting to use
breathing techniques such as the physiological saw as a way for these people who are under
the influence of psilocybin to self-direct their own calm and to bring that level of anxiety
down so that they can continue to move through the peak and move through the other phases of
the psychedelic journey in ways that can be most beneficial for them.
So to close out the description of this really wonderful study, and by the way,
it's another one from the Card Heart Harris Laboratory about the subjective
experience of ego-disillusion or oceanic boundlessness, this mystical state,
as so key as a component of a positive psilocybin journey,
I'll just read for you the final sentence of this paper because it captures it so well.
of psilocybin journey, I'll just read for you the final sentence of this paper because it captures it so well.
Quote, it seems vital that appropriate consideration is paid to the importance of promoting a certain
kind of experience as the quality of that experience may be the critical determinant of therapeutic
success.
Now, before we move into what will be a very brief description of some of the other rewiring
phenomena that psilocybin can induce, and then into some of the other rewiring phenomena that psilocybin can induce.
And then into some of the therapeutic applications of psilocybin as they relate to these recent,
really exciting clinical trials for depression and addictive disorders and things of that sort.
I just want to cue everybody to a paper that I think many people will want to take a look at
in thinking about psilocybin.
And I'll provide a link to this paper as well in the show note captions.
This paper is entitled, Theor Use of Silicibin,
Practical Considerations for Dosing and Administration.
And this is a wonderful paper
because it really goes step by step
through the pharmacology of psilocybin,
of which you now understand a bit,
but it goes into a bit more detail.
But then it also really nicely describes
the contour of a psilocybin session
and what's happening at the level of chemistry, early, middle, peak,
and toward the end of the psilocybin session. And then also importantly gets into issues of
dosage and translating from mushrooms to psilocybin itself to psilocybin.
Things I talked about earlier, but in a bit more detail if you'd like to see that detail.
And then perhaps most importantly, there's a section on contraindications where it points
out that, of course, women who are pregnant or breastfeeding, people who have a predisposition
to psychosis, those people should really avoid the use of psilocybin in other psychedelics
entirely.
It also talks about where the evidence is strong, moderate, and weak for the use of
psilocybin for treatment of various disorders.
I can just summarize that very quickly because it's where we're going ahead in a few minutes,
which is that the most evidence for positive therapeutic outcomes responds to psilocybin,
taking and conducted in the manner that we've been describing today in terms of dosage and
journey, set, and setting is for cancer-related depression, cancer-related anxiety, and treatment-resistant depression.
That's where most of the evidence resides. There's also some evidence for the use of psilocybin
journeys, and again, this is typically one or two psilocybin journeys spaced in the cases of two
journeys anywhere from one to two weeks apart.
And again, with all of the same contour of supports
and setting that we've been talking about today.
And there there's some evidence for improvement
in terms of outcomes in alcohol use disorder independence
and tobacco addiction.
And then finally, there's the least amount of evidence
although there is clinical trial support
for relief
or partial relief, for obsessive compulsive disorder,
cluster headaches and migraines,
and demoralization due to AIDS diagnosis.
So this paper has a lot of really interesting information
in terms of different conditions, in terms of dosage,
and again, contraintegations, and what's called adverse events.
What sorts of bad things can and do happen
as a consequence of psilocybin and other types
of psychedelic journeys, both during and after
those psilocybin or psychedelic sessions.
We'll talk a bit more about this
when we go into some of those clinical studies
because adverse reactions is always a key measure
in any clinical study.
So very soon we'll get into the more recent clinical studies related to psilocybin for
the use of treating depression and some other conditions.
But before we do that, I'd be remiss if I didn't talk about how psilocybin does and does
not change the brain.
What is and what is not known about that?
In fact, when I put out the call for questions about psilocybin, many of the questions related
to these issues. The first thing to understand is that a psilocybin journey is really a way
to try and put that wedge under the boulder as I described it, to try and invoke neuroplasticity
of our particular kind. And in that way, it's kind of remarkable, if you think about it,
that everyone has different lives, different experiences, psychedelics, in this case, psilocybin, are activating these brain networks that each of us has more
broadly than they would normally be activated.
These are very abnormal patterns of thinking and perceiving and experiencing our emotional
and physical life, et cetera.
And yet, so often, the outcomes are positive, not always, but the outcomes are positive.
The experience is positive, even though it but the outcomes are positive, the experiences
positive, even though it might have these anxiety moments or components within them.
It's very important to understand that psilocybin and the journey, while important, are not
really what all of this is about.
It's really about neuroplasticity.
So researchers, in particular, neuroscientists, are very intensely interested in understanding
what sorts of neuroplasticity psilocybin creates.
Because it turns out there are lots of different types
where processes involved with neuroplasticity.
For instance, brain networks, behavior, thinking,
emotion, et cetera, can change.
Because of the addition of new neurons,
that's one form of neuroplasticity
that's referred to as neurogenesis, the production of new neurons,
most typically in the so-called dentate gyros or other subregions of the hippocampus, a brain area involved in learning and memory.
Neurogenesis in other regions of the adult human brain are exceedingly rare, and to be honest, it may not occur at all.
This is a debated area.
rare. And to be honest, it may not occur at all. This is a debated area. We could do an entire episode about this. But for the most part, neuroscientists don't really believe that your neocortex,
your striatum, your cerebellum, has that much neurogenesis that's related to learning and memory
of new things or new experiences. And we don't actually think that occurs as a consequence of
taking psilocybin either.
Now some of you who are familiar with, for instance, the cerebellum might be saying, wait,
what about granular cell proliferation in the cerebellum or what about the rostral migratory
stream from the subventricular zone where there are neuroblasts, you know, spitting out
little neurons that migrate into the nose to replenish the olfactory neuron population?
Yes, that's all true. That does occur. It's been observed in mice. It's been observed in monkeys.
And to some extent, it's been observed in humans. But it's not, again, I repeat, it is not a
prominent feature of learning and acquisition of new skills, new ideas or new emotional states.
Perhaps the best supported evidence for neurogenesis underlying new thoughts, experiences,
abilities, emotions, etc. is the production of new neurons in that dentate gyrosubregion
of the hippocampus.
And that probably does occur in humans.
But neurogenesis is not really the dominant mode of changing neural circuitry in adult humans.
It might be a player in adolescence, in young childhood.
It is certainly a player before we are born
when we are still in utero,
but then the brain is being wired up in many different ways,
including the addition of new neurons
and changing of connections.
All this is to say that while neurogenesis
is a really sticky idea and it makes great headlines,
the addition of new neurons is not really the way
that the brain changes.
Under psilocybin, other psychedelics, or just generally,
it's perhaps responsible for maybe one to two percent,
and I'm being generous there,
of the rewiring events that are going to be most important
for all of us.
So we need to set that down and cement that there
until further evidence comes out to the contrary.
That's certainly where I, and here I feel comfortable speaking,
for the majority of neuroscientists out there,
professional neuroscientists, that is.
The paper showing adult neurogenesis are interesting,
but they don't really explain most of the plasticity
that occurs in the adult human brain.
So if neurogenesis isn't it, what is? Well, it's very clear that psilocybin, other psychedelics, and
any sort of behavioral or drug intervention that can induce neuroplasticity
does so largely through the addition or strengthening of new neural
connections or through the elimination or weakening of other neural
connections.
And if you look at the data exploring the mechanistic basis for psilocybin-induced neuroplasticity,
it's mostly focused on animal brains, animal models, mice and rats in particular.
A little bit on primates, but mostly mice and rats because that's where the interventions
can be done of knockout animals, of imaging the brain in real time.
Of course, there are the beautiful studies of Robin Carter-Art Harris and others exploring
neuroplasticity at the level of brain imaging, at the level of ultrasound measurements of
how active or certain brain areas in humans, how extensive is the modularity or not extensive
is the modularity, etc.
The stuff we talked about earlier.
So in other words, there are neuroplasticity studies
with the effects of psilocybin in humans.
But in terms of underlying mechanisms of neuroplasticity,
I think the predominant theory is that
psilocybin induces neuroplasticity
through the addition of novel connections
in those pyramidal neurons of the frontal cortex,
elsewhere in the cortex,
and certainly also in the visual cortex,
probably also subcortically as well below the cerebral cortex.
In areas like the phalamus, maybe even in the brainstem as well, and that those neuroplasticity
events are structural and functional, and they involve a couple of basic events, the most
prominent of which is the growth of dendrites, dendrites, or those little branches or processes
that come out of the neurons,
not just the pyramidal neurons,
but other neurons as well.
But since we're talking mainly about pyramidal neurons today,
both the apical, those ones that top,
they're called the apical tufts,
they're the ones that reach laterally
to connect with other neurons,
communicate with other neurons
that we talked about before,
as well as the dendrites that come out
of the base of those pyramidal neurons.
Those processes grow in response to psilocybin,
as well as the addition of what are called dendritic spines. So the dendrites are the branches. The spines
are these little protrusions that grow out. Actually, here, I don't know if this is coincidence
or not. Again, I always say I wasn't in control of the design phase, but these little protrusions
actually look like little mushrooms. They have a little stalk and they have a little head,
a little spine head, and those little head, a little spine head and
those little spines. So think of these as like little tiny mushroom appearing. They aren't
actual mushrooms. The first person that puts in the comments, oh my goodness, I learned
today that mushrooms grow out of our neurons when we take magic mushrooms. That is not what
I'm saying. What I'm saying is that these little mushroom-shaped protrusions that we're calling dendritic spines do, in fact, grow out of dendritic branches of neurons when animals ingest psilocybin
or are injected with psilocybin, and that those little mushroom-shaped protrusions are
the sites of new excitatory connections, new locations for input from other neurons to activate those neurons
that have those little mushroom shape protrusions.
If you'd like to see examples of this, both movies and still shots, it's pretty remarkable.
There's a paper that I'll provide a link to in the show note captions.
This was published in the journal Neuron, Cell Press Journal, excellent journal entitled
Silicide and Induces Rapid and Persistent Growth of Dendritic Spines in the frontal
cortex in vivo.
So, these measurements were done in the mouse equivalent, more or less, of the prefrontal
cortex.
There's some interesting details in this paper, for instance, that those new connections
persist.
So, they don't just grow out during the psilocybin being active in the bloodstream and
brain of the animal.
They persist.
Okay, so this may, again, may explain some of the persistent changes that occur in people after
psilocybin journeys.
They may too grow new spines.
I should also mention that a reduction in the number of dendritic spines, these little
mushroom-shaped protrusions, in the frontal cortex neurons of humans occurs in depressed patients.
We know that from post-mortem tissue. And that drugs that relieve depression or that treatments, including behavioral treatments,
that provide some relief from depression, do seem to be correlated with increases in
spine growth in frontal cortex neurons as well.
So this raises a very interesting idea, which is perhaps it's the growth of new connections.
These new dendritic spines,ires in particular neurons that's created by administration of psilocybin
that explains the relief from depression
that people experience.
So this is just one paper,
but it's one paper of a growing body of work
showing that yes, indeed, psilocybin induces
both structural and functional plasticity
in the human and animal brain.
It does that in the human brain at therapeutic doses
of anywhere from 10 to 25, perhaps even 30 milligrams
per session, one or two sessions.
I should mention that the mouse studies
tended to use quite high doses of psilocybin.
I was actually, I wasn't shocked,
but I was somewhat wide-eyed for a moment
to realize that most of the studies looking at changes
in plasticity
in the mouse brain in responses to psilocybin use the equivalent of 1 milligram per kilogram of body weight
Which is if you do the math and you translate what we were talking about before in terms of dosages. I'll just spare you all the time
It's about double the sorts of dosages that are typically used in humans Maybe even triple in some cases. Now it's often the case in animal studies because of the metabolism of animals being different,
but also because seeing effects of drugs in animal studies can be difficult. They did use a
dose response anywhere from zero to 0.25 to half to one to two milligrams per kilogram of
psilocybin in the study, so they had a dose response curve, but focus mainly on this one milligram per kilogram dosage.
In any event, the point is that many of the studies that describe these pretty dramatic
structural changes in the animal brain, most typically the mouse brain in response to psilocybin,
use dosages of psilocybin that if translated to humans would be about double the human
therapeutic dose.
So that is something that we need to take into consideration.
Nonetheless, it's very clear that in both animal studies and humans, psilocybin is inducing
both structural and functional changes in brain circuitry, and that in humans, the network
connectivity is being changed dramatically.
We talked about those data earlier, and that the underlying basis for that might be, again,
might be.
We don't know for sure the The addition of new gendered expires
on these pyramidal neurons
that we've been talking about repeatedly throughout today
is episode, although neurogenesis, perhaps,
and other modes of neuroplasticity,
such as the elimination of certain connections,
perhaps related to unhealthy maladaptive thoughts
or feeling that a particular sad song is overwhelmingly sad.
It could be the case that those sorts of things change subjectively
because of the removal of neural connections.
If you're going to think like a neurobiologist or scientist for that matter,
you don't ever want to think that one mechanism can explain all the effects
of a given drug or a given experience is almost certainly likely to be the consequence
of multiple mechanisms acting in parallel.
And because I know there are people out there who would like to know even more about the
neuroplasticity induced by psychedelics, including psilocybin, there's a wonderful review that I
provide a link to in the show note captions entitled Psychedelics and Neuroplasticity,
a systematic review unraveling the biological underpinnings of psychedelics.
This review is great because it goes a step beyond
just psilocybin silicin, binding to the serotonin-2A receptor
and things like brain derived in a trophic factor.
It actually talks a lot about the intracellular signaling
and exactly how neurons change their excitability patterns
based on this activation of the serotonin-2A receptor.
It's probably more detailed than most of you out there
are interested in, but if you are interested
in that level of detail
This is a wonderful open access review. So a few minutes ago
I talked about where there is strong
Modest and somewhat weak or rather I should say minimal evidence for the therapeutic use of psilocybin to treat various disorders and
across the board it really appears that
major depression and so-called intractable
depression, in some cases, is where we're seeing the most exciting research to date.
Now, keep in mind that because of the Control Substance Act being invoked in 1970 in the
United States, and because it was only just a few years ago, really, only about five years
ago, that psychedelics, including psilocybin, received what's called
breakthrough status at the FDA, that there are now a lot of clinical trials exploring how
psilocybin can impact various things like mood disorders, addictive disorders, and so
on.
Prior to 2018, when that therapeutic breakthrough potential was established in the United
States, I think a lot of people in the so-called psychedelics community had the sense and really the belief
that these drugs had enormous potential, but they just weren't being explored that extensively.
So I do want to give a nod to the incredible researchers, such as Robin Cardard Harris,
but also Matthew Johnson, Roland Griffiths, Nolan Williams, and many others.
Okay, I'm certainly not listing off everybody.
That would take hours.
But those researchers have really pioneered both the legal efforts and the funding efforts
and most importantly, the research efforts defining the clinical data that I'm about to
describe.
And here, I'm going to summarize the clinical data in a bit of a top contour fashion, just
giving you the kind of highlights.
We will, of course, provide links to the papers if you'd like to look into it further.
But I'm only giving you the top contour because I've had the great fortune of having Matthew
Johnson on this podcast before.
You can find that episode at hubermanlab.com.
Just simply put Matt's name or psychedelics into the search function.
It'll take you to that episode in all formats, or links to all formats, rather.
I've also had the great fortune of sitting down recently
with Dr. Robert and Card Art Harris
to talk about his work at University of California, San Francisco
on psilocybin LSD, Iowaska, and DMT,
as it relates to depression and other disorders.
And that episode, which also will be released at hubermanlab.com
and on all platforms, YouTube, Apple, Spotify,
really goes in depth into these clinical studies
and what those studies really look like.
Who's in the room?
Whether or not people just get one dose or two doses,
how far apart those are separated.
All of that is covered in extensive detail
in that what I found to be wonderful discussion
with Dr. Robin Cardard Harris.
So if you're interested in all of the details as it relates to clinical application of psychedelics,
stay tuned for that episode soon.
Again, you can find that at hubermanlab.com and on all platforms.
In the meantime, I would be remiss if I didn't include a bit of discussion about what has
been observed in terms of using psilocybin journeys as a way
to treat depression because the data are just oh so exciting. Again, these data really
started to surface as the consequence of studies that were initiated around 2006 in just a
few select laboratories and then really picked up in terms of the number of laboratories
and number of studies between 2018 and now. So what you'll notice is in terms of the number of laboratories and number of studies between
2018 and now so what you'll notice is that most of the papers I'm about to describe were published in for instance
Phenomenal journals New England Journal of Medicine in
2021
New England Journal of Medicine
November 2022
Journal of the American Medical Association
Psychiatry just very recently, 2021.
So these are very recent papers.
Essentially, all of these clinical studies involve either one or two psilocybin sessions.
The dosages that were explored range from zero milligrams, oh, placebo, if you will.
Ten milligrams, in some cases, twenty- 25 milligrams, in some cases, 30 milligrams.
And most typically, people receive the same dosage for both sessions, if indeed they did
both sessions.
However, there's at least one study looking at just one single episode of psilocybin administration.
So this is the paper entitled No Surprise Single Dose Syllocybin for Treatment Resistant
Episode of major depression.
This is published in the New England Journal of Medicine
in November of 2022.
I'll just summarize the results of this single application
study.
They randomly assigned subjects who had treatment
resistant depression, so they'd resisted treatment
to other things to receive a single dose
of a synthetic formulation of psilocybin.
So they're not eating mushrooms,
they're getting a synthetic dose of psilocybin. So they're not eating mushrooms, they're getting a synthetic dose of psilocybin, but the dose is known of either 25 milligrams,
10 milligrams, or 1 milligram, which was the control. And they receive psychological support.
There were a number of different tests, subjective tests of depression,
taken before and after the psilocybin journey.
They had about 75 to 79 participants in each group,
again at the three different doses, 25, 10 or 1 milligram.
And they looked at the changes in these scores,
these depression-related scores on these tests.
There are many results from this paper one could summarize,
but among the most important results I can summarize
from the discussion, and here I'm paraphrasing that the change in baseline levels
of depression that is at week three following the psilocybin session was significantly better.
That is, people experienced more relief or more people experienced more relief from the
25 milligram dose than from the 1 milligram dose.
And this is important.
There was no significant difference between the 10 milligram dose and the 1 milligram dose than from the 1 milligram dose. And this is important. There was no significant
difference between the 10 milligram dose and the 1 milligram dose. This really points to
the fact that the 25 to 30 milligram dose that's used in the largest numbers of studies exploring
treatment resistant depression really seems to be, I don't want to say the best dose, but
the most effective dose at least in this clinical context, in this set and setting, and with this particular patient population.
So we want to be careful to say that so that one doesn't just translate the 25 milligrams
is better than 10 milligrams, although in this study, it was for sake of treatment, resistant,
depression, relief.
There were a number of other key aspects of this paper.
In particular, the exploration of so-called adverse events,
so things like headaches, propensity for self-harm,
actual self-harm, anxiety, and so on.
It's worth mentioning that there were adverse events
in essentially every group.
The number of adverse events was highest
in the 25 milligram dose group.
And this is observed in other studies as well.
With higher dosages, there tends to be greater relief from depressive symptoms, but also a
greater chance for adverse events.
Some of those adverse events can be quite severe, so feelings of suicidal ideation, etc.
Some of them one could consider a little less severe mild headache or severe headache
that was transient or anxiety that was transient. Again, highly individual responses. We could
go line by line and table by table through this paper which we won't because there's a lot
of data. Again, we'll provide a link to this paper if you'd like to cruise it yourself.
It's fairly straightforward to read. That's one thing that's nice about these clinical
trials is they tend to be written in fairly non-technical language,
although there's a little bit of technical language.
The important point is that a single dose
of 25 milligrams of psilocybin provided
significant relief from treatment of resistant depression
in this particular patient population,
but it is not the case that 100% of the people
who took 25 milligrams of psilocybin experience
that relief, however, the majority of them did.
Now, when you say majority in science, you really need to look to numbers.
And the reason I'm not telling you, oh, it was 75% or 60% or 50% is because it depends
on which time point people were analyzed.
People were asked about their level of depression relief immediately after, one week after, two
weeks after, two weeks after,
three weeks after, and the degree of relief
tended to change over time.
In fact, it tended to diminish over time,
but it was also stable, or remarkably stable,
I should say, at least by my read,
in the 25 milligram dose group.
And that is summarized nicely in figure two of the paper
because they explored these people's levels of depression
out to week 12, and they still saw a significant degree
of depression relief 12 weeks after the single 25 milligram
psilocybin dose session.
So as I mentioned earlier, there are now about a dozen
or so excellent studies.
Clinical trials exploring the use of single
or two session psilocybin treatment in that
25 to 30 milligram range, which seems to be the most effective dose for long-lasting
relief from depression.
Each one of those studies explored something different, as is important.
Replication is also important, of course, in order to validate previous studies. But for instance, there have been comparisons of psilocybin versus SSRIs or other antidepressants.
There have been comparisons of psilocybin plus psychoanalysis or cognitive behavioral therapy
versus cognitive behavioral therapy alone or psychoanalysis alone.
And so there's a lot of evaluation now of the clinical outcomes and the statistical
outcomes of these subjective measures and even some objective measures of neurochemistry
where that's possible in terms of trying to understand if and how psilocybin is effective
for the treatment of depression.
And the major takeaway is that indeed it does seem to be the case.
And the numbers that I feel comfortable not throwing out there, but putting out to you,
reflect my conversation with Robin Cardhard Harris.
Again, that will be released soon at HubermanLab.com, as well as takeaways from what I would
say are the six broadest studies, meaning they have the widest range of age groups, the
broadest demographic in terms of the subjects,
their backgrounds, their levels of education,
men, women, ethnicity, et cetera.
And a lot of that can be summarized
in the paper entitled,
Effects of Syllis I've An Assisted Therapy
on Major Depressive Disorder.
So it was a particular randomized clinical trial.
But in the discussion, I think they summarize it quite well,
which is that if you look at
the number of people who take this 25 milligram dose twice in session spaced about a week
apart, what you will find is that anywhere from 60 to 75% of the people who have major
depressive disorder, who do these psilocybin sessions in the proper setting, report a good experience with it, have minimal adverse events coming out of those sessions
and in the weeks following.
Those people experience substantial positive relief from major depression in ways that other
treatments that they've explored, including antidepressant drugs,
cognitive behavioral therapy,
and other types of therapy alone could not provide.
Now, it's a general feature of these clinical trials
focusing on psilocybin that people are asked
to stop taking their antidepressants
prior to participating in the trial.
It's also a general feature of these trials
that people are encouraged to not suddenly
start their antidepressant treatment
immediately afterwards because, of course, that could confound the results of the psilocybin
treatment.
However, and this is a very important thing to note, all subjects were encouraged not
to avoid taking those antidepressant medications.
If, in fact, their clinician felt that it was important for their immediate and long-term
survival. So, you know, no one should be reckless in thinking about what to add or delete from their drug
protocol when dealing with depression, right? The outcomes could be very severe in that case.
Nonetheless, we can paraphrase from the discussion of the paper I just mentioned
because it really highlights the incredible results that psilocybin applied in these particular therapeutic settings are providing.
And here again I'm paraphrasing. The present trial showed that psilocybin administered in the context of supportive psychotherapy,
consisting of approximately 11 hours of psychotherapy. So this is going to be two sessions of the psilocybin with proper therapeutic support, produced large rapid and sustained
antidepressant effects.
The effect sizes reported in the study were approximately 2.5 times greater than the
effects sizes found in psychotherapy.
And more than four times greater than the effect sizes found in psychopharmacologic depression
treatment studies.
In other words, four times the positive effect
observed with typical SSRIs or other pharmacology
of that sort.
These findings are consistent with the literature
that showed that combined pharmacotherapy
and psychotherapy were more efficacious
in the treatment of major depressive disorder
than either intervention alone.
So again, this points to the fact
that combining drug therapy with talk therapy, as it's often called,
is going to be more effective than the either treatment alone.
Here are the drug therapy, psilocybin therapy, and again, please don't take the fact that in these studies,
they tend to ask people to not take their antidepressant medication heading into the study
as a sign that one should stop taking their antidepressant medication.
Rather, I think this study and other studies like it, again, which will provide links to
in the show note captions that are discussed extensively in the episode with Dr. Carter
at Harris soon to come.
Really point to the incredible role that psilocybin can have in creating an experience inside
of the session, the journey or the trip as it's called, as well as initiating neuroplastic events.
Perhaps the addition of dendrit expands maybe even some new neurons, maybe, although I don't
think that's the predominant mode, but that leads to these more extensive conactivities in the brain,
you know, so-called reduction in modular networks, enhanced activity in brain areas that normally
wouldn't be talking to one another, but not doing that in any kind of haphazard way.
It really does seem that the one or two sessions of psilocybin that induce these feelings
of ego dissolution, that induce these feelings of oceanic boundlessness, right?
So mystical.
And in many ways, it's what I find so incredible about psilocybin and other psychedelics is
that despite the highly mystical, highly subjective and still
at this time somewhat top contour understanding of how they might exert their effects, you
can highlight bold face and underlying might there, right?
Because it hasn't really been firmly established what the exact cell biological rewiring events
are.
But there is now what I would refer to as a center of mass of data that point to the fact that psilocybin, when taken in the appropriate set and setting,
the appropriate dosages, can invoke the sorts of neuroplasticity and changes in emotionality
in perceptual experience, not just during the psychedelic session, but for long periods of time
after the psychedelic session that can provide really remarkable relief from things like major depression and perhaps other psychiatric
issues as well.
And of course, I realize that many of you are listening to and are watching this episode,
and you're not necessarily depressed or thinking about psychedelics like psilocybin in the
context of depression.
I hope today's discussion allowed you to better understand how psychedelics and
psilocybin in particular because that's what we've been talking about
Are able to exert these incredible effects that they seem to exert?
This is not a call for everyone to run out and do psilocybin. It is absolutely not that
It is however my attempt to really put a magnifying lens on this incredible area of research that's happening, not just in the context of clinical trials,
but in the context of trying to understand
how serotonin and how drugs like psilocybin,
which, in many ways, mimics serotonin,
and more particularly the activation of particular receptors
in the brain, like the serotonin 2A receptor.
I mean, just sit back and think about that,
the selective activation of this receptor,
which is, by the way, associated with the expansion
of the neocortex across evolution, didn't mention that before, but, which is, by the way, associated with the expansion of the neocortex across evolution,
didn't mention that before, but indeed it is, how that can lead to enhanced ways of thinking,
changed ways of thinking, actual learning inside of this short four hour or six hour session
that we call the psilocybin journey. So, as is often the case, perhaps, as is always the case,
here on the Hubertman Lab podcast, we did a deep dive into a topic today, into the topic of psilocybin journey. So as is often the case, perhaps, as is always the case, here on the Hubertman Lab podcast,
we did a deep dive into a topic today,
into the topic of psilocybin,
what it is, how it works,
the different ways in which it changes brain circuitry,
how it creates the experiences that we think of
as the psilocybin journey,
what the safety issues are,
what the so-called set and setting are
that can lend themselves to
positive therapeutic outcomes.
And in doing so, my goal was really to highlight several things.
First of all, I am very excited about the potential for psychedelics such as psilocybin to provide
relief for mental health issues that to date have been very hard for people to access.
In addition to that, I'm just fundamentally interested in the brain and how it works and how it can change this thing we call neuroplasticity. To me,
neuroplasticity is the holy grail of the human nervous system. As far as we know,
we are the animal that can have long-lasting neuroplasticity throughout the lifespan.
And if it requires the use of compounds in a safe and controlled way, such as psilocybin,
in order to achieve maximal plasticity in a short and controlled way, such as psilocybin,
in order to achieve maximum plasticity and a short amount of time, that's exciting.
But of course, that also needs to be considered with all of the safety precautions in mind
that we talked about earlier, including the fact that people who have a predisposition
or who have psychosis or bipolar disorder or a relative that has psychosis or bipolar disorder, younger people, meaning
people 25 years of age and younger, and really anyone who's not working with a dedicated
and highly trained physician needs to be very cautious about these compounds as well.
They're very exciting.
I think psilocybin isn't exciting and super interesting compound for basic and clinical
reasons and for other reasons as well.
But they are sharp blades, as we say. And with sharp blades, you can do incredible things, but they are sharp blades as we say.
And with sharp blades, you can do incredible things, but you can also cut yourself very badly.
So all those considerations need to be taken to mind.
So I consider the science and use of psilocybin to be an exciting, but still preliminary area
that I certainly am paying a lot of attention to.
And I know there's a lot of excitement about, so stay tuned for the episode with Dr. Robin Carter at Harris.
And we will probably revisit psilocybin
and we will certainly revisit the other psychedelics
and non-classical psychedelics, including LSD,
DMT, 5MEO, DMT, ketamine, MDMA, mescaline,
and all the rest in future episodes as well.
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Thank you once again for joining me for today's discussion all about psilocybin.
And last but certainly not least, thank you for your interest in science.
you