Could a drug prevent depression and PTSD?

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This is a tuberculosis ward,
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and at the time this picture was taken
in the late 1800s,
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one in seven of all people
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died from tuberculosis.
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We had no idea what was
causing this disease.
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The hypothesis was actually
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it was your constitution
that made you susceptible.
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And it was a highly romanticized disease.
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It was also called consumption,
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and it was the disorder of poets
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and artists and intellectuals,
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and some people actually thought
0:34 - 0:37

it gave you heightened sensitivity
0:37 - 0:40

and conferred creative genius.
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By the 1950s,
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we instead knew that tuberculosis
was caused by a highly contagious
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bacterial infection,
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which is slightly less romantic,
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but that had the upside of us
0:53 - 0:55

being able to maybe develop
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drugs to treat it.
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So doctors had discovered a new drug,
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Iproniazid, that they were optimistic
1:01 - 1:03

might cure tuberculosis,
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and they gave it to patients,
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and patients were elated.
1:07 - 1:10

They were more social, more energetic.
1:10 - 1:12

One medical report actually says
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they were dancing in the halls.
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And unfortunately this was not necessarily
because they were getting better.
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A lot of them were still dying.
1:24 - 1:26

Another medical report describes them
1:26 - 1:30

as being "inappropriately happy."
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And that is how the first
antidepressant was discovered.
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So accidental discovery
is not uncommon in science,
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but it requires more than just
a happy accident.
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You have to be able to recognize it
for discovery to occur.
1:47 - 1:50

As a neuroscientist, I'm going
to talk to you a little bit
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about my firsthand experience
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with what you want to call
the opposite of dumb luck,
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let's call it smart luck.
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But first a bit more background.
2:00 - 2:04

Thankfully, since the 1950s,
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we've developed some other drugs
and we can actually now cure tuberculosis.
2:07 - 2:11

And at least in the United States,
though not necessarily in other countries,
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we have closed our sanitoriums
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and probably most of you
are not too worried about TB.
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But a lot of what was true
in the early 1900s
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about infectious disease,
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we can say now
about psychiatric disorders.
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We are in the middle of an epidemic
of mood disorders
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like depression and post-traumatic
stress disorder, or PTSD.
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One in four of all adults
in the United States
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suffers from mental illness,
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which means that if you haven't
experienced personally
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or someone in your family hasn't,
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it's still very likely
that someone you know has,
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though they may not talk about it.
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Depression has actually now surpassed
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HIV/AIDS, malaria, diabetes, and war
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as the leading cause
of disability worldwide,
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and also, like tuberculosis in the 1950s,
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we don't know what causes it.
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Once it's developed, it's chronic,
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lasts a lifetime,
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and there are no known cures.
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The second antidepressant we discovered
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also by accident in the 1950s
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from an antihistamine
that was making people manic,
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Imipramine.
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And in both the case of the tuberculosis
ward an the antihistamine,
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someone had to be able to recognize
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that a drug that was designed
to do one thing --
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treat tuberculosis
or suppress allergies --
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could be used to do something
very different --
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treat depression.
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And this sort of repurposing
is actually quite challenging.
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When doctors first saw
this mood-enhancing effect of Iproniazid,
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they didn't really
recognize what they saw.
3:51 - 3:52

They were so used to thinking about it
3:52 - 3:56

from the framework
of being a tuberculosis drug
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that they actually just listed it
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as a side effect, an adverse side effect.
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As you can see here,
a lot of these patients in 1954
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are experiencing severe euphoria.
4:07 - 4:11

And they were worried that this
might somehow interfere
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with their recovering from tuberculosis.
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So they recommended that Iproniazid
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only be used in cases of extreme TB
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and in patients that were highly
emotionally stable,
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which is of course the exact opposite
of how we use it as an antidepressant.
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They were so used to looking at it
from the perspective of this one disease,
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they could not see the larger implications
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for another disease.
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And to be fair,
it's not entirely their fault.
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Functional fixedness is a bias
that affects all of us.
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It's a tendency to only be able to think
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of an object in terms
of its traditional use or function.
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And mental set is another thing. Right?
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That's sort of this
pre-conceived framework
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with which we approach problems.
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And that actually make repurposing
pretty hard for all of us,
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which is I guess why they gave
a TV show to the guy who was,
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like, really great at repurposing.
5:05 - 5:07

(Laughter)
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So the effects in both the case
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of Iproniazid and Imipramine,
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they were so strong, right,
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there was mania or people
dancing in the halls.
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It's actually not that surprising
they were caught.
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But it does make you wonder
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what else we've missed.
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So Iproniazid and Imipramine,
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they're more than just a case study
in repurposing.
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They have two other things in common
that are really important.
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One, they have terrible side effects
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that includes liver toxicity,
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weight gain of over 50 pounds,
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suicidality.
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And two, they both
increase levels of serotonin,
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which is a chemical signal in the brain,
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or a neurotransmitter.
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And those two things together,
right, one or the two
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may not have been that important,
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but the two together meant
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that we had to develop
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safer drugs,
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and that serotonin
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seemed like a pretty good place to start.
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So we developed drugs
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to more specifically focus on serotonin,
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the selective serotonin
reuptake inhibitors, so the SSRIs,
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the most famous of which is Prozac.
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And that was 30 years ago,
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and since then we have mostly
just worked on optimizing those drugs.
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And the SSRIs, they are better
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than the drugs that came before them,
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but they still have a lot side effects,
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including weight gain, insomnia,
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suicidality,
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and they take a really long time to work,
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something like four to six weeks
in a lot of patients.
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And that's in the patients
where they do work.
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There are a lot of patients
where these drugs don't work.
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And that means now, in 2016,
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we still have no cures
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for any mood disorders,
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just drugs that suppress symptoms,
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which is kind of the difference between
taking a painkiller for an infection
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versus an antibiotic.
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Painkiller will make you feel better,
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but is not going to do anything
to treat that underlying disease.
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And it was this flexibility, right,
in our thinking
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that let us recognize that
Iproniazid and Imipramine
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could be repurposed in this way,
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which led us to the serotonin hypothesis,
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which we then, ironically, fixated on.
7:12 - 7:14

This is brain signaling, serotonin
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from an SSRI commercial.
7:16 - 7:18

In case you're not clear,
this is a dramatization.
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And in science, we try
and remove our bias, right,
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by running double-blinded experiments
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or being statistically agnostic
as to what our results will be.
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But bias creeps in more insidiously
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in what we choose to study
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and how we choose to study it.
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So we've focused on serotonin now
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for the past 30 years,
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often to the exclusion of other things.
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We still have no cures,
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and what if serotonin
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isn't all there is to depression?
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What if it's not even the key part of it?
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That means no matter how much time
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or money or effort that we put into it,
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it will never lead to a cure.
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In the past few years,
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doctors have discovered
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probably what is the first truly new
antidepressant since the SSRIs,
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Calypsol,
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and this drug works very quickly,
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within a few hours or a day,
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and it doesn't work on serotonin.
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It works on glutamate,
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which is another neurotransmitter.
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And it's also repurposed.
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It was traditionally used
as anesthesia in surgery.
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But unlike those other drugs,
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which were recognized pretty quickly,
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it took us 20 years
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to realize that Calypsol
was an antidepressant,
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despite the fact that it's actually
a better antidepressant,
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probably, than those other drugs.
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It's actually probably because of
the fact that it's a better antidepressant
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that it was harder for us to recognize.
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There was no mania to signal its effects.
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So in 2013, up at Columbia University,
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I was working with my colleague,
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Dr. ???,
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and we were studying Calypsol
as an antidepressant in mice.
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And Calypsol has, like,
a really short half-life,
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which means it's out of your body
within a few hours.
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And we were just piloting.
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So we would give an injection to mice,
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and then we'd wait a week,
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and then we'd run
another experiment to save money.
9:08 - 9:10

And one of the experiments
I was running,
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we would stress the mice,
9:12 - 9:14

and we used that as a model
of depression.
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And at first it kind of just looked
like it didn't really work at all.
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So we could have stopped there.
9:20 - 9:23

But I have run this model
of depression for years,
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and the data just looked kind of weird.
9:25 - 9:26

It didn't really look right to me.
9:26 - 9:28

So I went back,
9:28 - 9:29

and we reanalyzed it
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based on whether or not they had gotten
9:31 - 9:33

that one injection of Calypsol
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a week beforehand.
9:35 - 9:37

And it looked kind of like this.
9:37 - 9:39

So if you look at the far left,
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if you put a mouse in a new space,
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this is the box, it's very exciting,
9:44 - 9:46

a mouse will walk around and explore,
9:46 - 9:50

and you can see that pink line
is actually the measure of them walking.
9:50 - 9:54

And we also give it another mouse
in a pencil cup
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that it can decide to interact with.
9:56 - 9:59

This is also a dramatization,
in case that's not clear.
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And a normal mouse will explore.
10:03 - 10:05

It will be social.
10:05 - 10:06

Check out what's going on.
10:06 - 10:08

If you stress a mouse
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in this depression model,
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which is the middle box,
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they aren't social, they don't explore.
10:13 - 10:17

They mostly just kind of hide
in that back corner behind a cup.
10:17 - 10:20

Yet the mice that had gotten
that one injection of Calpysol
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here on your right,
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they were exploring. They were social.
10:24 - 10:28

They looked like they had never
been stressed at all,
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which is impossible.
10:30 - 10:33

So we could have just stopped there,
10:33 - 10:37

but Christine had also used
Calypsol before as anesthesia,
10:37 - 10:39

and a few years ago she had seen
that it seemed to have
10:39 - 10:42

some weird effects on cells
and some other behavior
10:42 - 10:44

that also seemed to last
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long after the drug, maybe a few weeks.
10:48 - 10:48

So we were like, okay,
10:48 - 10:50

maybe this is not completely impossible,
10:50 - 10:52

but we were really skeptical.
10:52 - 10:54

So we did what you do in science
when you're not sure,
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and we ran it again.
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And I remember being in the animal room
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moving mice from box to box
11:02 - 11:03

to test them,
11:03 - 11:07

and Christine was actually sitting
on the floor with the computer in her lap
11:07 - 11:08

so the mice couldn't see her,
11:08 - 11:11

and she was analyzing
the data in real time.
11:11 - 11:12

And I remember us yelling,
11:12 - 11:15

which you're not supposed to do
in an animal room where you're testing
11:15 - 11:17

because it had worked.
11:17 - 11:21

It seemed like these mice
were protected against stress,
11:21 - 11:24

or they were inappropriately happy,
however you want to call it.
11:24 - 11:28

And we we really excited.
11:28 - 11:30

And then we were really skeptical,
11:30 - 11:32

because it was too good to be true.
11:32 - 11:34

So we ran it again.
11:34 - 11:37

And then we ran it again
in a PTSD model,
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and we ran it again
in a physiological model,
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where all we did was give stress hormones.
11:41 - 11:43

And we had our undergrads run it.
11:43 - 11:47

And then we had our collaborators
halfway across the world in France run it.
11:47 - 11:51

And every time someone ran it,
they confirmed the same thing.
11:51 - 11:54

It seemed like this
one injection of Calypsol
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was somehow protecting
against stress for weeks.
11:57 - 11:59

And we only published this a year ago,
11:59 - 12:04

but since then other labs
have independently confirmed this effect.
12:04 - 12:06

So we don't know what causes depression,
12:06 - 12:13

but we do know that stress is the
initial trigger in 80 percent of cases,
12:13 - 12:15

and depression and PTSD
are different diseases,
12:15 - 12:17

but this is something
they share in common.
12:17 - 12:19

Right? It is traumatic stress
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like active combat or natural disasters
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or community violence or sexual assault
12:24 - 12:27

that causes post-traumatic
stress disorder,
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and not everyone that is exposed to stress
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develops a mood disorder.
12:33 - 12:36

And this ability to experience stress
and be resilient
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and bounce back and not develop
depression or PTSD
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is known as stress resilience,
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and in varies between people.
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And we have always thought of it
as just sort of this passive property.
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Right? It's the absence
of susceptibility factors
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and risk factors for these disorders.
12:53 - 12:56

But what if it were active?
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Maybe we could enhance it,
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sort of akin to putting on armor.
13:01 - 13:04

We had accidentally discovered
13:04 - 13:07

the first resilience-enhancing drug.
13:07 - 13:10

And like I said, we only gave
a tiny amount of the drug,
13:10 - 13:11

and it lasted for weeks,
13:11 - 13:14

and that's not like anything you see
with antidepressants.
13:14 - 13:19

But it is actually kind of similar
to what you see in immune vaccines.
13:19 - 13:22

So in immune vaccines, right,
you'll get your shots,
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and then weeks, months, years later
13:26 - 13:28

when you're actually exposed to bacteria,
13:28 - 13:31

it's not the vaccine in your body
that protects you.
13:31 - 13:32

It's your own immune system
13:32 - 13:36

that's developed resistance and resilience
to this bacteria, that fights it off,
13:36 - 13:39

and you actually never get the infection,
13:39 - 13:41

which is very different from, say,
our treatments. Right?
13:41 - 13:45

In that case, you get the infection,
you're exposed to the bacteria,
13:45 - 13:49

you're sick, and then you take,
say, an antibiotic which cures it,
13:49 - 13:53

and those drugs are actually working
to kill the bacteria.
13:53 - 13:55

Or similar to as I said before, right,
with this palliatave,
13:55 - 13:58

you'll take something that will
suppress the symptoms,
13:58 - 14:01

but it won't treat
the underlying infection,
14:01 - 14:03

and you'll only feel better
14:03 - 14:04

during the time in which you're taking it,
14:04 - 14:06

which is why you have to keep taking it.
14:06 - 14:09

And in depression, right, and PTSD,
14:09 - 14:11

here we have your stress exposure,
14:11 - 14:14

we only have palliative care.
14:14 - 14:16

Antidepressants only suppress symptoms,
14:16 - 14:19

and that is why you basically
have to keep taking them
14:19 - 14:21

for the life of the disease,
14:21 - 14:24

which is often the length
of your own life.
14:24 - 14:28

So we're calling our resilience
enhancing drugs "paravaccines,"
14:28 - 14:30

which means vaccine-like,
14:30 - 14:32

because it seems like they might
have the potential
14:32 - 14:34

to protect against stress
14:34 - 14:37

and prevent mice from developing
14:37 - 14:41

depression and post-traumatic
stress disorder.
14:41 - 14:44

Also, not all antidepressants
are also paravaccines.
14:44 - 14:47

We tried Prozac as well,
14:47 - 14:49

and that had no effect.
14:49 - 14:52

So if this were to translate into humans,
14:52 - 14:55

we might be able to protect people
14:55 - 14:57

who are predictably at risk
14:57 - 15:01

against stress-induced disorders
like depression and PTSD.
15:01 - 15:04

So that's first responders
and firefighters,
15:04 - 15:08

refugees, prisoners and prison guards,
15:08 - 15:11

soldiers, you name it.
15:11 - 15:13

And to give you a sense
15:13 - 15:15

of the scale of these diseases,
15:15 - 15:19

in 2010, the global burden of disease
15:19 - 15:23

was estimated at 2.5 trillion dollars,
15:23 - 15:25

and since they are chronic,
15:25 - 15:28

that cost is compounding
and is therefore expected to rise
15:28 - 15:32

up to six trillion dollars
in just the next 15 years.
15:32 - 15:35

As I mentioned before,
repurposing can be challenging
15:35 - 15:39

because of our prior biases.
15:39 - 15:42

Calypsol has another name,
15:42 - 15:44

Ketamine,
15:44 - 15:46

which also goes by another name,
15:46 - 15:47

Special K,
15:47 - 15:50

which is a club drug and drug of abuse.
15:50 - 15:54

It's still used across the world
as an anesthetic.
15:54 - 15:57

It's used in children.
We use it on the battlefield.
15:57 - 15:59

It's actually the drug of choice
in a lot of developing nations
15:59 - 16:01

because it doesn't affect breathing.
16:01 - 16:07

It is on the World Health Organization
list of most essential medicines.
16:07 - 16:10

If we had discovered Ketamine
as a paravaccine first,
16:10 - 16:13

it'd be pretty easy for us to develop it,
16:13 - 16:17

but as is, we have to compete
with our functional fixedness
16:17 - 16:22

and mental set that kind of interfere.
16:22 - 16:25

Fortunately, it's not the only compound
we have discovered
16:25 - 16:29

that has these prophylactic,
paravaccine qualities,
16:29 - 16:32

but all of the other
drugs we've discovered,
16:32 - 16:35

or compounds if you will,
they're totally new,
16:35 - 16:38

they have to go through
the entire FDA approval process,
16:38 - 16:40

if they make it,
16:40 - 16:42

before they can ever be used in humans.
16:42 - 16:44

And that will be years.
16:44 - 16:46

So if we want something sooner,
16:46 - 16:49

Ketamine is already FDA-approved.
16:49 - 16:51

It's generic, it's available.
16:51 - 16:56

We could develop it for a fraction
of the price and a fraction of the time.
16:56 - 16:59

But actually, beyond functional fixedness
16:59 - 17:01

and mental set,
17:01 - 17:04

there's a real other challenge
to repurposing drugs,
17:04 - 17:06

which is policy.
17:06 - 17:08

There are no incentives in place
17:08 - 17:12

once a drug is generic and off patent
and no longer exclusive
17:12 - 17:15

to encourage pharma companies
to develop them,
17:15 - 17:16

because they don't make money.
17:16 - 17:18

And that's not true for just Ketamine.
17:18 - 17:21

That is true for all drugs.
17:21 - 17:26

Regardless, the idea itself
is completely novel in psychiatry,
17:26 - 17:30

to use drugs to prevent mental illness
17:30 - 17:32

as opposed to just treat it.
17:32 - 17:34

It is possible
17:34 - 17:38

that 20, 50, 100 years from now,
17:38 - 17:42

we will look back now
at depression and PTSD
17:42 - 17:45

the way we look back
at tuberculosis sanitariums
17:45 - 17:47

as a thing of the past.
17:47 - 17:53

This could be the beginning
of the end of mental health epidemic.
17:53 - 17:57

But as a great scientist once said,
17:57 - 18:00

only a fool is sure of anything.
18:00 - 18:04

A wise man keeps on guessing.
18:04 - 18:06

Thank you guys.
18:06 - 18:11

(Applause)

Title:: Could a drug prevent depression and PTSD?
Speaker:: Rebecca Brachman
Description:: more » « less
Video Language:: English
Team:: closed TED
Project:: TEDTalks
Duration:: 18:23

	Brian Greene edited English subtitles for Could a drug prevent depression and PTSD?
	Brian Greene approved English subtitles for Could a drug prevent depression and PTSD?
	Brian Greene edited English subtitles for Could a drug prevent depression and PTSD?
	Brian Greene edited English subtitles for Could a drug prevent depression and PTSD?
	Brian Greene edited English subtitles for Could a drug prevent depression and PTSD?
	Brian Greene edited English subtitles for Could a drug prevent depression and PTSD?
	Joanna Pietrulewicz accepted English subtitles for Could a drug prevent depression and PTSD?
	Joanna Pietrulewicz edited English subtitles for Could a drug prevent depression and PTSD?

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	Revision Number	Author	Created
	10	Brian Greene
	9	Brian Greene
	8	Brian Greene
	7	Brian Greene
	6	Brian Greene
	5	Joanna Pietrulewicz
	4	Joanna Pietrulewicz
	3	Joseph Geni
	2	Joseph Geni
	1	Amara Bot

Could a drug prevent depression and PTSD?

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