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How early life experience is written into DNA

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    So it all came to life
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    in a dark bar in Madrid.
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    I encountered my colleague
    from McGill, Michael Meaney.
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    And we were drinking a few beers,
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    and like scientists do,
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    he told me about his work.
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    And he told me that he is interested
    in how mother rats lick their pups
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    after they were born.
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    And I was sitting there and saying,
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    "This is where my tax
    dollars are wasted --
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    (Laughter)
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    on this kind of soft science."
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    And he started telling me
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    that the rats, like humans,
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    lick their pups in very different ways.
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    Some mothers do a lot of that,
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    some mothers do very little,
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    and most are in between.
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    But what's interesting about it
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    is when he follows these pups
    when they become adults --
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    like, years in human life,
    long after their mother died.
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    They are completely different animals.
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    The animals that were licked
    and groomed heavily,
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    the high-licking and grooming,
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    are not stressed.
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    They have different sexual behavior.
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    They have a different way of living
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    than those that were not treated
    as intensively by their mothers.
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    So then I was thinking to myself:
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    Is this magic?
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    How does this work?
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    As geneticists would like you to think,
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    perhaps the mother had
    the "bad mother" gene
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    that caused her pups to be stressful,
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    and then it was passed
    from generation to generation;
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    it's all determined by genetics.
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    Or is it possible that something
    else is going on here?
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    In rats, we can ask
    this question and answer it.
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    So what we did is
    a cross-fostering experiment.
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    You essentially separate the litter,
    the babies of this rat, at birth,
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    to two kinds of fostering mothers --
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    not the real mothers,
    but mothers that will take care of them:
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    high-licking mothers
    and low-licking mothers.
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    And you can do the opposite
    with the low-licking pups.
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    And the remarkable answer was,
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    it wasn't important
    what gene you got from your mother.
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    It was not the biological mother
    that defined this property of these rats.
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    It is the mother that
    took care of the pups.
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    So how can this work?
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    I am an a epigeneticist.
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    I am interested in how genes are marked
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    by a chemical mark
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    during embryogenesis, during the time
    we're in the womb of our mothers,
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    and decide which gene will be expressed
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    in what tissue.
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    Different genes are expressed in the brain
    than in the liver and the eye.
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    And we thought: Is it possible
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    that the mother is somehow
    reprogramming the gene of her offspring
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    through her behavior?
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    And we spent 10 years,
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    and we found that there is a cascade
    of biochemical events
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    by which the licking and grooming
    of the mother, the care of the mother,
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    is translated to biochemical signals
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    that go into the nucleus and into the DNA
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    and program it differently.
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    So now the animal can prepare
    itself for life:
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    Is life going to be harsh?
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    Is there going to be a lot of food?
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    Are there going to be a lot of cats
    and snakes around,
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    or will I live
    in an upper-class neighborhood
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    where all I have to do
    is behave well and proper,
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    and that will gain me social acceptance?
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    And now one can think about
    how important that process can be
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    for our lives.
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    We inherit our DNA from our ancestors.
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    The DNA is old.
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    It evolved during evolution.
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    But it doesn't tell us
    if you are going to be born in Stockholm,
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    where the days are long in the summer
    and short in the winter,
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    or in Ecuador,
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    where there's an equal number of hours
    for day and night all year round.
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    And that has such an enormous [effect]
    on our physiology.
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    So what we suggest is,
    perhaps what happens early in life,
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    those signals that come
    through the mother,
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    tell the child what kind of social world
    you're going to be living in.
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    It will be harsh, and you'd better
    be anxious and be stressful,
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    or it's going to be an easy world,
    and you have to be different.
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    Is it going to be a world
    with a lot of light or little light?
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    Is it going to be a world
    with a lot of food or little food?
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    If there's no food around,
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    you'd better develop your brain to binge
    whenever you see a meal,
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    or store every piece of food
    that you have as fat.
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    So this is good.
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    Evolution has selected this
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    to allow our fixed, old DNA
    to function in a dynamic way
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    in new environments.
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    But sometimes things can go wrong;
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    for example, if you're born
    to a poor family
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    and the signals are, "You better binge,
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    you better eat every piece of food
    you're going to encounter."
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    But now we humans
    and our brain have evolved,
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    have changed evolution even faster.
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    Now you can buy McDonald's for one dollar.
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    And therefore, the preparation
    that we had by our mothers
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    is turning out to be maladaptive.
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    The same preparation that was supposed
    to protect us from hunger and famine
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    is going to cause obesity,
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    cardiovascular problems
    and metabolic disease.
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    So this concept that genes
    could be marked by our experience,
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    and especially the early life experience,
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    can provide us a unifying explanation
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    of both health and disease.
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    But is true only for rats?
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    The problem is, we cannot
    test this in humans,
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    because ethically, we cannot administer
    child adversity in a random way.
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    So if a poor child develops
    a certain property,
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    we don't know whether
    this is caused by poverty
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    or whether poor people have bad genes.
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    So geneticists will try to tell you
    that poor people are poor
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    because their genes make them poor.
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    Epigeneticists will tell you
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    poor people are in a bad environment
    or an impoverished environment
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    that creates that phenotype,
    that property.
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    So we moved to look
    into our cousins, the monkeys.
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    My colleague, Stephen Suomi,
    has been rearing monkeys
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    in two different ways:
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    randomly separated the monkey
    from the mother
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    and reared her with a nurse
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    and surrogate motherhood conditions.
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    So these monkeys didn't have
    a mother; they had a nurse.
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    And other monkeys were reared
    with their normal, natural mothers.
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    And when they were old,
    they were completely different animals.
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    The monkeys that had a mother
    did not care about alcohol,
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    they were not sexually aggressive.
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    The monkeys that didn't have a mother
    were aggressive, were stressed
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    and were alcoholics.
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    So we looked at their DNA
    early after birth, to see:
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    Is it possible that the mother is marking?
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    Is there a signature of the mother
    in the DNA of the offspring?
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    These are Day-14 monkeys,
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    and what you see here is the modern way
    by which we study epigenetics.
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    We can now map those chemical marks,
    which we call methylation marks,
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    on DNA at a single nucleotide resolution.
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    We can map the entire genome.
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    We can now compare the monkey
    that had a mother or not.
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    And here's a visual presentation of this.
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    What you see is the genes
    that got more methylated are red.
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    The genes that got
    less methylated are green.
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    You can see many genes are changing,
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    because not having a mother
    is not just one thing --
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    it affects the whole way;
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    it sends signals about the whole way
    your world is going to look
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    when you become an adult.
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    And you can see the two groups of monkeys
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    extremely well-separated from each other.
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    How early does this develop?
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    These monkeys already
    didn't see their mothers,
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    so they had a social experience.
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    Do we sense our social status,
    even at the moment of birth?
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    So in this experiment,
    we took placentas of monkeys
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    that had different social status.
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    What's interesting about social rank
    is that across all living beings,
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    they will structure
    themselves by hierarchy.
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    Monkey number one is the boss;
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    monkey number four is the peon.
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    You put four monkeys in a cage,
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    there will always be a boss
    and always be a peon.
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    And what's interesting
    is that the monkey number one
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    is much healthier than monkey number four.
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    And if you put them in a cage,
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    monkey number one will not eat as much.
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    Monkey number four will eat [a lot].
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    And what you see here
    in this methylation mapping,
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    a dramatic separation at birth
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    of the animals that had
    a high social status
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    versus the animals
    that did not have a high status.
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    So we are born already knowing
    the social information,
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    and that social information
    is not bad or good,
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    it just prepares us for life,
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    because we have to program
    our biology differently
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    if we are in the high
    or the low social status.
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    But how can you study this in humans?
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    We can't do experiments,
    we can't administer adversity to humans.
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    But God does experiments with humans,
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    and it's called natural disasters.
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    One of the hardest natural disasters
    in Canadian history
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    happened in my province of Quebec.
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    It's the ice storm of 1998.
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    We lost our entire electrical grid
    because of an ice storm
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    when the temperatures
    were, in the dead of winter in Quebec,
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    minus 20 to minus 30.
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    And there were pregnant
    mothers during that time.
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    And my colleague Suzanne King
    followed the children of these mothers
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    for 15 years.
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    And what happened was,
    that as the stress increased --
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    and here we had objective
    measures of stress:
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    How long were you without power?
    Where did you spend your time?
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    Was it in your mother-in-law's apartment
    or in some posh country home?
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    So all of these added up
    to a social stress scale,
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    and you can ask the question:
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    How did the children look?
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    And it appears that as stress increases,
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    the children develop more autism,
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    they develop more metabolic diseases
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    and they develop more autoimmune diseases.
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    We would map the methylation state,
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    and again, you see the green genes
    becoming red as stress increases,
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    the red genes becoming green
    as stress increases,
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    an entire rearrangement
    of the genome in response to stress.
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    So if we can program genes,
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    if we are not just the slaves
    of the history of our genes,
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    that they could be programmed,
    can we deprogram them?
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    Because epigenetic causes
    can cause diseases like cancer,
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    metabolic disease
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    and mental health diseases.
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    Let's talk about cocaine addiction.
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    Cocaine addiction is a terrible situation
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    that can lead to death
    and to loss of human life.
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    We asked the question:
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    Can we reprogram the addicted brain
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    to make that animal not addicted anymore?
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    We used a cocaine addiction model
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    that recapitulates what happens in humans.
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    In humans, you're in high school,
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    some friends suggest you use some cocaine,
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    you take cocaine, nothing happens.
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    Months pass by, something reminds you
    of what happened the first time,
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    a pusher pushes cocaine,
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    and you become addicted
    and your life has changed.
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    In rats, we do the same thing.
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    My colleague, Gal Yadid,
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    he trains the animals
    to get used to cocaine,
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    then for one month, no cocaine.
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    Then he reminds them of the party
    when they saw the cocaine the first time
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    by cue, the colors of the cage
    when they saw cocaine.
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    And they go crazy.
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    They will press the lever to get cocaine
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    until they die.
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    We first determined that the difference
    between these animals
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    is that during that time
    when nothing happens,
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    there's no cocaine around,
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    their epigenome is rearranged.
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    Their genes are re-marked
    in a different way,
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    and when the cue comes,
    their genome is ready
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    to develop this addictive phenotype.
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    So we treated these animals with drugs
    that either increase DNA methylation,
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    which was the epigenetic
    marker to look at,
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    or decrease epigenetic markings.
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    And we found that
    if we increased methylation,
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    these animals go even crazier.
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    They become more craving for cocaine.
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    But if we reduce the DNA methylation,
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    the animals are not addicted anymore.
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    We have reprogrammed them.
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    And a fundamental difference
    between an epigenetic drug
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    and any other drug
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    is that with epigenetic drugs,
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    we essentially remove
    the signs of experience,
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    and once they're gone,
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    they will not come back
    unless you have the same experience.
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    The animal now is reprogrammed.
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    So when we visited the animals
    30 days, 60 days later,
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    which is in human terms
    many years of life,
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    they were still not addicted --
    by a single epigenetic treatment.
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    So what did we learn about DNA?
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    DNA is not just a sequence of letters;
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    it's not just a script.
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    DNA is a dynamic movie.
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    Our experiences are being written
    into this movie, which is interactive.
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    You're, like, watching a movie
    of your life, with the DNA,
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    with your remote control.
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    You can remove an actor and add an actor.
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    And so you have, in spite
    of the deterministic nature of genetics,
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    you have control of the way
    your genes look,
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    and this has a tremendous
    optimistic message
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    for the ability to now encounter
    some of the deadly diseases
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    like cancer, mental health,
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    with a new approach,
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    looking at them as maladaptation.
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    And if we can epigenetically intervene,
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    [we can] reverse the movie
    by removing an actor
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    and setting up a new narrative.
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    So what I told you today is,
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    our DNA is really combined
    of two components,
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    two layers of information.
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    One layer of information is old,
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    evolved from millions
    of years of evolution.
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    It is fixed and very hard to change.
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    The other layer of information
    is the epigenetic layer,
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    which is open and dynamic
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    and sets up a narrative
    that is interactive,
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    that allows us to control,
    to a large extent, our destiny,
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    to help the destiny of our children
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    and to hopefully conquer disease
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    and serious health challenges
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    that have plagued humankind
    for a long time.
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    So even though we are determined
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    by our genes,
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    we have a degree of freedom
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    that can set up our life
    to a life of responsibility.
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    Thank you.
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    (Applause)
Title:
How early life experience is written into DNA
Speaker:
Moshe Szyf
Description:

Moshe Szyf is a pioneer in the field of epigenetics, the study of how living things reprogram their genome in response to social factors like stress and lack of food. His research suggests that biochemical signals passed from mothers to offspring tell the child what kind of world they're going to live in, changing the expression of genes. "DNA isn't just a sequence of letters; it's not just a script." Szyf says. "DNA is a dynamic movie in which our experiences are being written."

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Video Language:
English
Team:
closed TED
Project:
TEDTalks
Duration:
16:35

English subtitles

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