-
It's a real pleasure to be here
-
and to present the work I've been doing
-
over the last five years or so since my PhD.
-
Genuinely, I want you to try and understand
-
as much as you can
-
So it's not the easiest material,
-
And especially when you don't have a background in neuroscience.
-
It's not always that easy to get a handle on these processes.
-
But I'm going to do my absolute best
-
to try and help you understand, and
-
I'll provide some metaphors to try and
-
break things down to make things more accessible.
-
Also it would be useful to keep
-
some pens out because there will be
-
some references, so if you genuinely you do
-
want to understand how these drugs
-
work in the brain, then it does require
-
a bit of work on your parts as well, unfortunately.
-
So you'd have to go away and look up
-
some of these references and do some
-
background reading.
-
So I just want to start by saying
-
that this work is part of the
-
Beckley-Imperial psychedelic research programme,
-
which is an initiative between David Kotts
-
and Amanda Fielding of the Beckley Foundation.
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Amanda is a key collaborative partner in this work,
-
and David Nutts, the principal investigator on it.
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So we'll start with the science.
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We know that psilocybin is an ingredient
-
in magic mushrooms.
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Now, psilocybin is the [pro-drug] of psilocin,
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which is remarkably similar in its molecular structure
-
to the endogenous neurotransmitter
-
which is found throughout the brain, serotonin.
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So it is really quite striking how similar
-
it is in its molecular structure.
-
Just a subtle change in its structure
-
confers such profound effects of consciousness.
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So this already
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is a matter of great intrigue
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about how these drugs work in the brain.
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So what was found in the mid-1980s
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was a strong positive correlation
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between a psychedelic drug's affinity
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for the serotonin 2A receptor,
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a particular subtype of the serotonin receptor,
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and the drug's potency.
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So a good example to help illustrate
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it's principle is, LSD has a very high affinity
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for the serotonin 2A receptor --
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it's very sticky, and it's also incredibly potent.
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So that helps you understand.
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Also, Franz Vollenweider did an excellent study
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blocking the serotinin 2A receptor
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with ketanserin, a relatively selective
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serotonin 2A receptor blocker,
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and he found that pre-treatment
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with this drug blocked the psychedelic effects
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of psilocybin. So there's good evidence
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that these drugs trigger their effects
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on consciousness by initial effect on
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the serotonin 2A receptor.
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So already we have an important
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fundamental relationship that's been discovered
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between the serotonin system and how these drugs work
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in the brain.
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So where is the serotonin 2A receptor in the brain?
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Well, this is the largest serotonin 2A binding study
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that's been done by a colleague of ours,
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David Erritzoe.
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He used a radioactive tracer, or ligand,
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that sticks to serotonin 2A receptors in the brain.
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And then you can detect the signal
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where the ligand is stuck
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And so doing this, he found that
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the serotonin 2A receptor is
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very much a cortical receptor.
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So the outer layer of the brain, the cortex,
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(it's referred to as kind of like the bark of a tree)
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so this outer layer of the brain, that's where you find
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the serotonin 2A receptor.
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And it's especially prevalent,
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especially densely expressed,
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in high-level cortical regions.
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So these are regions that
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don't have a specific sensory function, like,
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for instance, the visual cortex, which is concerned
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with visual processing.
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The heteromodal regions so they have a more
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kind of divergent, and high-level, function
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and so the serotonin 2A receptor
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is especially densely expressed
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in these high-level cortical regions,
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such as the posterior cingulate cortex.
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You will hear this term referred to again
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throughout my talk
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because it's a key region of the brain,
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a very high-level region of the brain,
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and it seems to be especially implicated in
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the mechanistic action of these drugs,
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how they work in the brain.
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We also know that the serotonin 2A receptor
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is especially densely expressed
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in the particular layer of the cortex.
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So the cortex is organized in a kind of laminar
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way, and there's some large,
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what are referred to as pyramidal neurons
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in layer 5 of the cortex.
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That is... (pause)
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This is layer 5 here.
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So there's some large neurons there,
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and these are the principal output layer
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of the cortex,
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and there's also something else,
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which is especially important about
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this cellular group,
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in terms of how this drug works in the brain.
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So we know the serotonin 2A receptor is very important,
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We know where it is,
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in terms of its spatial distribution in the brain
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and also within the cortex itself,
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within its laminae organization. It's dense in the
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deep pyramidal cells in layer 5.
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We also know that if you stimulate
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the serotonin 2A receptor,
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you have an excitatory effect on the host cells.
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So the cell that expresses the receptor,
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if you stimulate it, then you're gonna make that cell
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more excitable.
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So these are all important principles that we know.
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These are kind of the bedrock findings so far
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about how psychedelics work in the brain.
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But these are all quite low level;
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my brain imaging work has been looking at
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a higher level,
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what's referred to as a macroscopic level.
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So, the level you can look at and see
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on a large scale in terms of
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brain networks, for instance,
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and regional brain activity.
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So let's start with our first study,
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our first fMRI study with psilocybin.
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This used the modality referred to as
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arterial spin labelling, which is
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a method which measures changes
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in blood flow in the brain.
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And generally there's quite a reliable relationship
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between blood flow in the brain and brain activity.
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So if blood flow increases,
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we generally infer
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that brain activity has increased.
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So this study had fifteen healthy volunteers,
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mean age of 34,
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the scans were 18 minutes in duration,
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there was a six-minute baseline,
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and then we looked at changes in blood flow
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after that baseline.
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There were two scans:
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a placebo scan followed by a drug scan.
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And volunteers just lay in the scanner.
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They were presented with a fixation cross:
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just a simple green cross that they looked at
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on a screen, and they just relaxed
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and were instructed really just to let their minds wander.
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And then we looked at how
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the drug affected blood flow
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during these conditions.
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We gave a dose of 2 mg of psilocybin--
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that compares to about 50 mg when given orally.
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We gave the drug intravenously,
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so 2 mg is equivalent to about 50 mg orally,
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so it's a moderate dose.
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Here's the design. Here's our 6-minute baseline.
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Infusion was given over 60 seconds.
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So it's a relatively rapid infusion.
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And then the onset of the effects is also rapid,
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so when the drug is given intravenously,
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really there is very little delay between
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delivery of the drug and the onset
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of the subjective effects.
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So the subjective effects actually begin,
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really, before the end of the 60-second adminstration,
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so the drug seems to really get in the brain
-
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very quickly and to change consciousness
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profoundly very quickly.
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So what was the first observation?
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Well, the first thing that we get
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before we analyze the results are people's
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descriptions of their experiences.
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So here's one of them:
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This volunteer said that "there was a definite
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sense of lubrication,
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of freedom,
-
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of the cogs being loosened and firing off
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in all sorts of unexpected directions."
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Now these subjective reports are really useful
-
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because they give you a sense of the
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mechanics that are going on in the brain,
-
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and the changes in the mechanics,
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which confer the subjective effect --
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what's going on in the brain on a mechanical level
-
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to produce the profound changes in consciousness.
-
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This volunteer said, "Everything became
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fragmented; things were all in bits
-
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and it was very hard to hold it all together
-
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in a coherent stream."
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So it's like I said, this stuff is really useful
-
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for understanding what is going on
-
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on a systems-level in the brain
-
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to produce these subjective effects.
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Now, the default mode network
-
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you've heard quite a lot about
-
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over the last two days.
-
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It is an incredibly important
-
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system that's been discovered in the brain.
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And one of its properties is that
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it has very dense connectivity,
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so if you look at the white matter
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tracks in the brain,
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so these are the fibers that connect
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different brain regions,
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then you'll find that there's a very dense
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coming together of connections within
-
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the default mode notwork.
-
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So there seems to be
-
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an incredibly important transit hub,
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a place where different regions
-
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can connect via,
-
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and information can be projected from,
-
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and also a very important integration center.
-
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So, to integrate brain function,
-
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information comes together at this common
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convergence zone, and then
-
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that gives a coherence to cognition, essentially.
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That's how it's understood so far.
-
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What else about the default mode network?
-
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So here's a metaphor to help you try and understand
-
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what people are thinking about its function.
-
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So a metaphor that could be used to explain
-
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what it does is a capital city in a country.
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It's a place where people come together,
-
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things come together,
-
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business gets done.
-
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And it's an incredibly important hub,
-
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and if ever
-
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God forbid, something were to happen to
-
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London, then, the country as a whole
-
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would be seriously effected,
-
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and not just Britain.
-
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So it's incredibly important
-
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integration hub, the default mode network.
-
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What else do we know about
-
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the default mode network?
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There's some evidences here.
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The default mode network undergoes
-
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significant ontogenetic development
-
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from infancy to adulthood.
-
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It undergoes maturation as cognition matures.
-
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It has also undergone significant
-
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evolutionary expansion
-
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so these regions have increased
-
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more than other regions
-
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from primates to humans.
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It's more metabolically active
-
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than elsewhere in the brain,
-
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so the posterior cingulate cortex,
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which is the region which is circled there,
-
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it actually accounts for 40% more
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blood flow than anywhere else
-
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in the brain.
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So it is a very metabolically hungry system
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and these regions that are part of it
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are incredibly metabolically hungry.
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It's doing something important.
-
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Now, a matter of intrigue in neuroscience
-
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is that people don't have a really good handle
-
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on what the default mode is
-
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and what it does,
-
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but of course, they enjoy speculating,
-
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and the researcher who really discovered
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the default mode network has referred
-
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to its very high energy levels
-
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as being like the brain's dark energy.
-
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So similar to dark energy in cosmology
-
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it is something that we know is there
-
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but we don't really know what it does.
-
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Really, we make inferences about it,
-
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based on its relative decrease in activity.
-
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So when you engage in a task,
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you see a decrease in activity
-
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in the default mode network,
-
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whereas otherwise
-
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it is incredibly active.
-
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So it's a mater of intrigue.
-
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What's going on here?
-
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What's all this energy for, and why
-
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is it consuming so much?
-
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We know that the default mode network
-
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is engaged during self-reflection,
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so that is a very staple finding.
-
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We also know that during
-
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complex mental imagery, such as
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spatial navigation or imagination,
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fantasy in one's mind eye,
-
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you'll also see increased activity
-
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in the default mode network.
-
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Mental time travel -- so that's being
-
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outside of the moment and
-
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daydreaming about future events
-
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or past biographical experiences.
-
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So whenever you come out of the moment
-
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and you daydream in this way,
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you see increased activity and connectivity
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in the default mode network.
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Also, theory of mind -- which is
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putting someone oneself
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in somebody else's shoes.
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You will also see increased activity
-
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in the default mode network during that function.
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And metacognition -- which thinking about thinking,
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that's also linked with
-
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default mode network activity.
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So Raichle, who I said is the guy who
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really discovered this network
-
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has also referred to it as
-
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the orchestrator of the self.
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So all these things
-
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led me to start thinking
-
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having a background in psychoanalysis
-
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and being interested in
-
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especially Freudian metapsychology
-
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instead of the more mechanistic
-
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ideas of Freud. There is remarkable overlap
-
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between his descriptions of the ego
-
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and the relationship between the ego
-
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and the unconscious mind, or the id,
-
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and what we're discovering in
-
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the default mode network.
-
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So in this paper, with Carhart-Harris & Friston,
-
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I submitted the idea that
-
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the default mode network is essentially
-
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the neural substrate source of the ego,
-
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which is an idea to be shot down
-
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if people find otherwise.
-
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But that's science. That's how we work.
-
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So what else is there about
-
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the default mode network?
-
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Well, what's it's relationship to depression?
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There's a very interesting relationship
-
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between default mode network parameters
-
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and depressive symptomatology.
-
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So we know that connectivity between
-
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the medial pre-frontal cortex
-
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of the default mode network
-
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and the posterior cingulate cortex
-
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which are
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(pause)
-
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the front bits and the back bits.
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So when connectivity between these regions
-
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is high,
-
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then scores in patients with depression
-
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on rumination (so these are scores in rumination.
-
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They are thinking over problems
-
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and ruminating on negative things),
-
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when this is high, connectivity
-
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betwen these regions is especially
-
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high. And we think this system,
-
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this overconnectivity, is really causing people to
-
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have a kind of stereotype style of thinking.
-
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So they are stuck in this system,
-
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they are stuck in their own heads,
-
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they are stuck on their sense of self.
-
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They are usually thinking very critically
-
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about themselves, and going over and over
-
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about how terrible they are.
-
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So this is a relationship we seem to be discovering
-
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about the default mode network
-
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and depressive symptomatology.
-
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This provides a useful background
-
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for what we're finding in terms of how
-
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psilocybin is affecting
-
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brain networks and brain systems.
-
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So in our ASL study, we found
-
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it was really quite surprising findings for us,
-
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given descriptions of consciousness
-
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being expanded by psychedelic drugs.
-
Not Synced
We are given some previous work,
-
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for instance, by Franz Vollenweider,
-
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we were thinking we were going to be seeing
-
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increases in brain activity or brain blood flow
-
Not Synced
with psilocybin.
-
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And despite dropping the threshold
-
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and a number of different things,
-
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we really didn't see this.
-
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All we were really seeing was
-
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the same pattern again and again,
-
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which was decreased blood flow
-
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in certain regions of the brain.
-
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What was intriguing was that
-
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the decreases that we were seeing were
-
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in these very same important hub strutures
-
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of the brain.
-
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So, for instance, the posterior cingulate cortex,
-
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this bit at the back,
-
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the thalamus,
-
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and the medial pre-frontal cortex --
-
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so these very reliably
-
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were coming up as being
-
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decreased under psilocybin.
-
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Here's just showing you again,
-
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the default mode network is this kind of
-
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hub, this connectivity hub, in the brain.
-
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We also found that
-
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there was a relationship between
-
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the magnitude of the decrease in blood flow
-
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and ratings of the intensity of the experience.
-
Not Synced
So, the larger the decrease in blood flow,
-
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particularly in the anterior cingulate cortex,
-
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the more intense people were describing
-
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their experiences.
-
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So whenever you find these relationships
-
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it kind of reinforces your inferences, really,
-
Not Synced
and provides some consolidation
-
Not Synced
for what you are finding
-
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and supports its functional meaning.
-
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So since our ASL study
-
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we did a [bold] study.
-
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This is kind of the classic [signal]
-
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of functional magnetic resonance imaging (fMRI).
-
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We really repeated the same protocol:
-
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15 healthy volunteers,
-
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infused with a drug over 60 seconds at 2 mg,
-
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and we found exactly the same thing.
-
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So this was really nice reinforcement
-
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for the initial finding that we had found
-
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with ASL.
-
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And these regions where there was a common
-
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overlap between the decreases in blood flow
-
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with ASL and the decreases in,
-
Not Synced
essentially venous oxygenation,
-
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or oxygenated blood with the BOLD signal
-
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of fMRI.
-
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So one of the merits of BOLD fMRI is
-
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that it allows you to do these
-
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functional connectivity analyses.
-
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So just to give you a feel for what that is,
-
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here is an image which shows
-
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the default mode network in orange
-
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and let's concentrate on the default
-
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mode network for a moment.
-
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So you can see that there are two regions in it,
-
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and there is one that has has yellow text,
-
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the PCC? and then you can see there is this
-
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time series underneath.
-
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So the PCC time series is in yellow
-
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and you can see that it overlaps with
-
Not Synced
anothertime series, and that is
-
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the medial prefontal cortex.
-
Not Synced
So it is by looking at correlations between
-
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fluctuations in the BOLD signal
-
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that we identify functionally coherent
-
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brain networks. We know these regions
-
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work together as a common network
-
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doing a common function.
