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Opensource drug discovery | Dr Jay Bradner | TEDxBoston

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    I moved to Boston
    10 years ago from Chicago,
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    with an interest in cancer
    and in chemistry.
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    You might know that chemistry
    is the science of making molecules
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    or, to my taste,
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    new drugs for cancer.
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    And you might also know that,
    for science and medicine,
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    Boston is a bit of a candy store.
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    You can't roll a stop sign in Cambridge
    without hitting a graduate student.
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    The bar is called the Miracle of Science.
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    The billboards say "Lab Space Available."
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    And it's fair to say
    that in these 10 years,
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    we've witnessed absolutely the start
    of a scientific revolution --
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    that of genome medicine.
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    We know more about the patients
    that enter our clinic now
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    than ever before.
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    And we're able, finally,
    to answer the question
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    that's been so pressing for so many years:
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    Why do I have cancer?
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    This information
    is also pretty staggering.
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    You might know that, so far,
    in just the dawn of this revolution,
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    we know that there are perhaps
    40,000 unique mutations
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    affecting more than 10,000 genes,
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    and that there are 500 of these genes
    that are bona-fide drivers,
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    causes of cancer.
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    Yet comparatively,
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    we have about a dozen
    targeted medications.
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    And this inadequacy of cancer medicine
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    really hit home when my father
    was diagnosed with pancreatic cancer.
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    We didn't fly him to Boston.
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    We didn't sequence his genome.
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    It's been known for decades
    what causes this malignancy.
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    It's three proteins: ras, myc, p53.
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    This is old information
    we've known since about the 80s,
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    yet there's no medicine I can prescribe
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    to a patient with this
    or any of the numerous solid tumors
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    caused by these three ...
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    Horsemen of the Apocalypse that is cancer.
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    There's no ras, no myc, no p53 drug.
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    And you might fairly ask: Why is that?
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    And the very unsatisfying
    yet scientific answer is:
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    it's too hard.
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    That for whatever reason,
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    these three proteins have entered
    a space, in the language of our field,
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    that's called the undruggable genome --
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    which is like calling
    a computer unsurfable
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    or the Moon unwalkable.
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    It's a horrible term of trade.
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    But what it means
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    is that we've failed to identify
    a greasy pocket in these proteins,
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    into which we, like molecular locksmiths,
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    can fashion an active, small,
    organic molecule or drug substance.
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    Now, as I was training
    in clinical medicine
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    and hematology and oncology
    and stem-cell transplantation,
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    what we had instead,
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    cascading through the regulatory
    network at the FDA,
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    were these substances:
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    arsenic,
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    thalidomide,
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    and this chemical derivative
    of nitrogen mustard gas.
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    And this is the 21st century.
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    And so, I guess you'd say,
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    dissatisfied with the performance
    and quality of these medicines,
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    I went back to school, in chemistry,
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    with the idea that perhaps by learning
    the trade of discovery chemistry
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    and approaching it in the context
    of this brave new world
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    of the open source,
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    the crowd source,
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    the collaborative network
    that we have access to within academia,
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    that we might more quickly bring
    powerful and targeted therapies
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    to our patients.
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    And so, please consider
    this a work in progress,
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    but I'd like to tell you today a story
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    about a very rare cancer
    called midline carcinoma,
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    about the undruggable protein target
    that causes this cancer,
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    called BRD4,
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    and about a molecule developed at my lab
    at Dana-Farber Cancer Institute,
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    called JQ1,
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    which we affectionately named for Jun Qi,
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    the chemist that made this molecule.
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    Now, BRD4 is an interesting protein.
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    You might ask: with all the things
    cancer's trying to do to kill our patient,
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    how does it remember it's cancer?
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    When it winds up its genome,
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    divides into two cells and unwinds again,
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    why does it not turn
    into an eye, into a liver,
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    as it has all the genes
    necessary to do this?
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    It remembers that it's cancer.
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    And the reason is that cancer,
    like every cell in the body,
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    places little molecular bookmarks,
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    little Post-it notes,
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    that remind the cell, "I'm cancer;
    I should keep growing."
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    And those Post-it notes involve this
    and other proteins of its class --
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    so-called bromodomains.
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    So we developed an idea, a rationale,
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    that perhaps if we made a molecule
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    that prevented
    the Post-it note from sticking
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    by entering into the little pocket
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    at the base of this spinning protein,
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    then maybe we could convince cancer cells,
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    certainly those addicted
    to this BRD4 protein,
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    that they're not cancer.
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    And so we started to work on this problem.
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    We developed libraries of compounds
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    and eventually arrived
    at this and similar substances
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    called JQ1.
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    Now, not being a drug company,
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    we could do certain things,
    we had certain flexibilities,
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    that I respect that a pharmaceutical
    industry doesn't have.
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    We just started mailing it to our friends.
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    I have a small lab.
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    We thought we'd just send it to people
    and see how the molecule behaves.
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    We sent it to Oxford, England,
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    where a group of talented
    crystallographers provided this picture,
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    which helped us understand exactly
    how this molecule is so potent
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    for this protein target.
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    It's what we call a perfect fit
    of shape complementarity,
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    or hand in glove.
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    Now, this is a very rare cancer,
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    this BRD4-addicted cancer.
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    And so we worked with samples of material
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    that were collected by young pathologists
    at Brigham and Women's Hospital.
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    And as we treated these cells
    with this molecule,
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    we observed something really striking.
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    The cancer cells --
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    small, round and rapidly dividing,
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    grew these arms and extensions.
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    They were changing shape.
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    In effect,
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    the cancer cell
    was forgetting it was cancer
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    and becoming a normal cell.
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    This got us very excited.
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    The next step would be to put
    this molecule into mice.
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    The only problem was there's no
    mouse model of this rare cancer.
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    And so at the time
    we were doing this research,
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    I was caring for a 29-year-old
    firefighter from Connecticut
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    who was very much at the end of life
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    with this incurable cancer.
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    This BRD4-addicted cancer
    was growing throughout his left lung.
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    And he had a chest tube in
    that was draining little bits of debris.
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    And every nursing shift,
    we would throw this material out.
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    And so we approached this patient
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    and asked if he would collaborate with us.
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    Could we take this precious
    and rare cancerous material
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    from this chest tube
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    and drive it across town
    and put it into mice
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    and try to do a clinical trial
    at a stage that with a prototype drug,
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    well, that would be, of course, impossible
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    and, rightly, illegal to do in humans.
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    And he obliged us.
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    At the Lurie Family Center
    for Animal Imaging,
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    our colleague, Andrew Kung,
    grew this cancer successfully in mice
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    without ever touching plastic.
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    And you can see this PET scan
    of a mouse -- what we call a pet PET.
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    The cancer is growing
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    as this red, huge mass
    in the hind limb of this animal.
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    And as we treat it with our compound,
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    this addiction to sugar,
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    this rapid growth, faded.
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    And on the animal on the right,
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    you see that the cancer was responding.
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    We've completed, now, clinical trials
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    in four mouse models of this disease.
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    And every time, we see the same thing.
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    The mice with this cancer
    that get the drug live,
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    and the ones that don't rapidly perish.
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    So we started to wonder,
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    what would a drug company
    do at this point?
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    Well, they probably
    would keep this a secret
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    until they turn the prototype drug
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    into an active pharmaceutical substance.
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    So we did just the opposite.
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    We published a paper
    that described this finding
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    at the earliest prototype stage.
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    We gave the world the chemical
    identity of this molecule,
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    typically a secret in our discipline.
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    We told people exactly how to make it.
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    We gave them our email address,
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    suggesting that if they write us,
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    we'll send them a free molecule.
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    (Laughter)
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    We basically tried to create
    the most competitive environment
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    for our lab as possible.
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    And this was, unfortunately, successful.
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    (Laughter)
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    Because now, we've shared this molecule,
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    just since December of last year,
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    with 40 laboratories in the United States
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    and 30 more in Europe --
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    many of them pharmaceutical companies,
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    seeking now to enter this space,
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    to target this rare cancer
    that, thankfully right now,
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    is quite desirable
    to study in that industry.
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    But the science that's coming back
    from all of these laboratories
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    about the use of this molecule
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    has provided us insights
    we might not have had on our own.
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    Leukemia cells treated with this compound
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    turn into normal white blood cells.
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    Mice with multiple myeloma,
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    an incurable malignancy
    of the bone marrow,
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    respond dramatically
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    to the treatment with this drug.
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    You might know that fat has memory.
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    I'll nicely demonstrate that for you.
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    (Laughter)
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    In fact, this molecule
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    prevents this adipocyte,
    this fat stem cell,
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    from remembering how to make fat,
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    such that mice on a high-fat diet,
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    like the folks
    in my hometown of Chicago --
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    (Laughter)
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    fail to develop fatty liver,
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    which is a major medical problem.
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    What this research taught us --
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    not just my lab, but our institute,
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    and Harvard Medical School
    more generally --
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    is that we have unique
    resources in academia
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    for drug discovery;
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    that our center, which has tested
    perhaps more cancer molecules
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    in a scientific way
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    than any other,
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    never made one of its own.
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    For all the reasons you see listed here,
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    we think there's a great
    opportunity for academic centers
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    to participate in this earliest,
    conceptually tricky
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    and creative discipline
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    of prototype drug discovery.
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    So what next?
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    We have this molecule,
    but it's not a pill yet.
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    It's not orally bioavailable.
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    We need to fix it so we can
    deliver it to our patients.
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    And everyone in the lab,
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    especially following the interaction
    with these patients,
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    feels quite compelled
    to deliver a drug substance
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    based on this molecule.
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    It's here where I'd say
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    that we could use your help
    and your insights,
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    your collaborative participation.
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    Unlike a drug company,
    we don't have a pipeline
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    that we can deposit these molecules into.
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    We don't have a team
    of salespeople and marketeers
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    to tell us how to position
    this drug against the other.
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    What we do have is the flexibility
    of an academic center
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    to work with competent, motivated,
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    enthusiastic, hopefully well-funded people
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    to carry these molecules
    forward into the clinic
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    while preserving our ability
    to share the prototype drug worldwide.
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    This molecule will soon leave our benches
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    and go into a small start-up company
    called Tensha Therapeutics.
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    And, really, this is the fourth
    of these molecules
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    to kind of "graduate"
    from our little pipeline
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    of drug discovery,
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    two of which -- a topical drug
    for lymphoma of the skin
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    and an oral substance for the treatment
    of multiple myeloma --
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    will actually come to the bedside
    for the first clinical trial
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    in July of this year -- for us,
    a major and exciting milestone.
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    I want to leave you with just two ideas.
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    The first is: if anything is unique
    about this research,
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    it's less the science than the strategy.
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    This, for us, was a social experiment --
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    an experiment in "What would happen
    if we were as open and honest
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    at the earliest phase
    of discovery chemistry research
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    as we could be?"
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    This string of letters and numbers
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    and symbols and parentheses
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    that can be texted, I suppose,
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    or Twittered worldwide,
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    is the chemical identity
    of our pro compound.
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    It's the information that we most need
    from pharmaceutical companies,
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    the information on how these early
    prototype drugs might work.
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    Yet this information is largely a secret.
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    And so we seek, really, to download
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    from the amazing successes
    of the computer-science industry,
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    two principles -- that of open source
    and that of crowdsourcing --
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    to quickly, responsibly accelerate
    the delivery of targeted therapeutics
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    to patients with cancer.
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    Now, the business model
    involves all of you.
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    This research is funded by the public.
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    It's funded by foundations.
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    And one thing I've learned in Boston
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    is that you people will do anything
    for cancer, and I love that.
  • 12:21 - 12:24
    You bike across the state,
    you walk up and down the river.
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    (Laughter)
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    I've never seen, really, anywhere,
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    this unique support for cancer research.
  • 12:32 - 12:34
    And so I want to thank you
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    for your participation, your collaboration
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    and most of all,
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    for your confidence in our ideas.
  • 12:40 - 12:46
    (Applause)
Title:
Opensource drug discovery | Dr Jay Bradner | TEDxBoston
Description:

How does cancer know it's cancer? At Jay Bradner's lab, they found a molecule that might hold the answer, JQ1 - and instead of patenting JQ1, they published their findings and mailed samples to 40 other labs to work on. An inspiring look at the open-source future of medical research.

This talk was given at a TEDx event using the TED conference format but independently organized by a local community. Learn more at http://ted.com/tedx
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Video Language:
English
Team:
closed TED
Project:
TEDxTalks
Duration:
12:49

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