Can we eat to starve cancer? | William Li

1,304,347 views ・ 2010-05-17

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00:17
Good afternoon.
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There's a medical revolution happening all around us,
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and it's one that's going to help us conquer
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some of society's most dreaded conditions,
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including cancer.
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The revolution is called angiogenesis,
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and it's based on the process that our bodies use to grow blood vessels.
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So why should we care about blood vessels?
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Well, the human body is literally packed with them --
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60,000 miles worth in a typical adult.
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End to end, that would form a line that would circle the earth twice.
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The smallest blood vessels are called capillaries.
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We've got 19 billion of them in our bodies.
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And these are the vessels of life,
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and as I'll show you, they can also be the vessels of death.
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Now, the remarkable thing about blood vessels
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is that they have this ability
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to adapt to whatever environment they're growing in.
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For example, in the liver, they form channels to detoxify the blood;
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in the lungs, they line air sacs for gas exchange.
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In muscle, they corkscrew,
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so that muscles can contract without cutting off circulation.
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And in nerves, they course along like power lines,
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keeping those nerves alive.
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We get most of these blood vessels
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when we're actually still in the womb.
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And what that means is that as adults,
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blood vessels don't normally grow.
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Except in a few special circumstances.
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In women, blood vessels grow every month,
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to build the lining of the uterus.
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During pregnancy, they form the placenta,
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which connects mom and baby.
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And after injury, blood vessels actually have to grow under the scab
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in order to heal a wound.
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And this is actually what it looks like,
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hundreds of blood vessels, all growing toward the center of the wound.
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So the body has the ability to regulate
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the amount of blood vessels that are present at any given time.
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It does this through an elaborate and elegant system of checks and balances,
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stimulators and inhibitors of angiogenesis,
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such that, when we need a brief burst of blood vessels,
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the body can do this by releasing stimulators,
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proteins called angiogenic factors,
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that act as natural fertilizer, and stimulate new blood vessels to sprout.
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When those excess vessels are no longer needed,
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the body prunes them back to baseline,
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using naturally-occurring inhibitors of angiogenesis.
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There are other situations where we start beneath the baseline,
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and we need to grow more blood vessels, just to get back to normal levels --
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for example, after an injury --
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and the body can do that too, but only to that normal level,
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that set point.
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But what we now know, is that for a number of diseases,
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there are defects in the system,
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where the body can't prune back extra blood vessels,
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or can't grow enough new ones in the right place at the right time.
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And in these situations, angiogenesis is out of balance.
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And when angiogenesis is out of balance,
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a myriad of diseases result.
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For example, insufficient angiogenesis -- not enough blood vessels --
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leads to wounds that don't heal, heart attacks,
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legs without circulation, death from stroke,
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nerve damage.
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And on the other end, excessive angiogenesis --
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too many blood vessels -- drives disease,
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and we see this in cancer, blindness,
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arthritis, obesity, Alzheimer's disease.
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In total, there are more than 70 major diseases
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affecting more than a billion people worldwide,
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that all look on the surface to be different from one another,
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but all actually share abnormal angiogenesis
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as their common denominator.
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And this realization is allowing us to re-conceptualize
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the way that we actually approach these diseases,
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by controlling angiogenesis.
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Now, I'm going to focus on cancer,
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because angiogenesis is a hallmark of cancer --
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every type of cancer.
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So here we go.
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This is a tumor: dark, gray, ominous mass growing inside a brain.
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And under the microscope,
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you can see hundreds of these brown-stained blood vessels,
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capillaries that are feeding cancer cells,
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bringing oxygen and nutrients.
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But cancers don't start out like this,
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and in fact, cancers don't start out with a blood supply.
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They start out as small, microscopic nests of cells,
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that can only grow to one half a cubic millimeter in size.
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That's the tip of a ballpoint pen.
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Then they can't get any larger because they don't have a blood supply,
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so they don't have enough oxygen or nutrients.
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In fact, we're probably forming these microscopic cancers
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all the time in our body.
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Autopsy studies from people who died in car accidents
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have shown that about 40 percent of women between the ages of 40 and 50
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actually have microscopic cancers in their breasts.
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About 50 percent of men in their 50s and 60s
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have microscopic prostate cancers,
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and virtually 100 percent of us, by the time we reach our 70s,
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will have microscopic cancers growing in our thyroid.
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Yet, without a blood supply,
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most of these cancers will never become dangerous.
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Dr. Judah Folkman, who was my mentor
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and who was the pioneer of the angiogenesis field,
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once called this "cancer without disease."
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So the body's ability to balance angiogenesis,
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when it's working properly,
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prevents blood vessels from feeding cancers.
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And this turns out to be
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one of our most important defense mechanisms
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against cancer.
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In fact, if you actually block angiogenesis
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and prevent blood vessels from ever reaching cancer cells,
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tumors simply can't grow up.
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But once angiogenesis occurs,
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cancers can grow exponentially.
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And this is actually how a cancer goes from being harmless,
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to being deadly.
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Cancer cells mutate,
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and they gain the ability to release lots of those angiogenic factors,
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natural fertilizer,
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that tip the balance in favor of blood vessels invading the cancer.
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And once those vessels invade the cancer,
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it can expand, it can invade local tissues,
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and the same vessels that are feeding tumors
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allow cancer cells to exit into the circulation as metastases.
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And unfortunately, this late stage of cancer
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is the one at which it's most likely to be diagnosed,
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when angiogenesis is already turned on,
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and cancer cells are growing like wild.
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So, if angiogenesis is a tipping point
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between a harmless cancer and a harmful one,
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then one major part of the angiogenesis revolution
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is a new approach to treating cancer
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by cutting off the blood supply.
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We call this antiangiogenic therapy,
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and it's completely different from chemotherapy,
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because it selectively aims
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at the blood vessels that are feeding the cancers.
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We can do this because tumor blood vessels are unlike normal, healthy vessels
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we see in other places of the body --
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they're abnormal, they're very poorly constructed,
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and because of that, they're highly vulnerable
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to treatments that target them.
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In effect, when we give cancer patients antiangiogenic therapy --
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here, an experimental drug for a glioma,
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which is a type of brain tumor --
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you can see that there are dramatic changes that occur
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when the tumor is being starved.
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Here's a woman with a breast cancer,
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being treated with the antiangiogenic drug called Avastin,
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which is FDA approved.
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And you can see that the halo of blood flow
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disappears after treatment.
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Well, I've just shown you two very different types of cancer
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that both responded to antiangiogenic therapy.
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So a few years ago, I asked myself,
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"Can we take this one step further and treat other cancers,
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even in other species?"
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So here is a nine year-old boxer named Milo,
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who had a very aggressive tumor
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called a malignant neurofibroma growing on his shoulder.
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It invaded into his lungs.
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His veterinarian only gave him three months to live.
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So we created a cocktail of antiangiogenic drugs
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that could be mixed into his dog food,
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as well as an antiangiogenic cream,
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that could be applied on the surface of the tumor.
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And within a few weeks of treatment,
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we were able to slow down that cancer's growth,
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such that we were ultimately able to extend Milo’s survival
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to six times what the veterinarian had initially predicted,
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all with a very good quality of life.
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And we've subsequently treated more than 600 dogs.
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We have about a 60 percent response rate,
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and improved survival for these pets
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that were about to be euthanized.
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So let me show you a couple of even more interesting examples.
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This is 20-year-old dolphin living in Florida,
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and she had these lesions in her mouth
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that, over the course of three years,
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developed into invasive squamous cell cancers.
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So we created an antiangiogenic paste.
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We had it painted on top of the cancer three times a week.
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And over the course of seven months,
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the cancers completely disappeared,
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and the biopsies came back as normal.
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Here's a cancer growing on the lip
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of a Quarter Horse named Guinness.
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It's a very, very deadly type of cancer called an angiosarcoma.
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It had already spread to his lymph nodes,
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so we used an antiangiogenic skin cream for the lip,
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and the oral cocktail, so we could treat from the inside as well as the outside.
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And over the course of six months,
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he experienced a complete remission.
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And here he is six years later,
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Guinness, with his very happy owner.
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(Applause)
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Now obviously, antiangiogenic therapy could be used for a wide range of cancers.
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And in fact, the first pioneering treatments
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for people as well as dogs,
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are already becoming available.
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There are 12 different drugs, 11 different cancer types.
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But the real question is:
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How well do these work in practice?
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So here's actually the patient survival data
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from eight different types of cancer.
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The bars represent survival time
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taken from the era in which there was only chemotherapy,
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or surgery, or radiation available.
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But starting in 2004,
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when antiangiogenic therapies first became available,
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you can see that there has been a 70 to 100 percent improvement in survival
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for people with kidney cancer, multiple myeloma,
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colorectal cancer, and gastrointestinal stromal tumors.
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That's impressive.
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But for other tumors and cancer types,
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the improvements have only been modest.
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So I started asking myself,
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"Why haven't we been able to do better?"
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And the answer, to me, is obvious:
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we're treating cancer too late in the game,
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when it's already established,
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and oftentimes, it's already spread or metastasized.
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And as a doctor,
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I know that once a disease progresses to an advanced stage,
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achieving a cure can be difficult, if not impossible.
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So I went back to the biology of angiogenesis, and started thinking:
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Could the answer to cancer be preventing angiogenesis,
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beating cancer at its own game,
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so the cancers could never become dangerous?
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This could help healthy people,
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as well as people who've already beaten cancer once or twice,
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and want to find a way to keep it from coming back.
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So to look for a way to prevent angiogenesis in cancer,
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I went back to look at cancer's causes.
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And what really intrigued me,
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was when I saw that diet accounts for 30 to 35 percent
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of environmentally-caused cancers.
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Now the obvious thing is to think about what we could remove from our diet,
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what to strip out, take away.
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But I actually took a completely opposite approach,
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and began asking: What could we be adding to our diet
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that's naturally antiangiogenic,
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and that could boost the body's defense system,
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and beat back those blood vessels that are feeding cancers?
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In other words, can we eat to starve cancer?
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(Laughter)
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Well, the answer is yes, and I'm going to show you how.
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And our search for this has taken us to the market,
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the farm and to the spice cabinet,
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because what we've discovered
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is that Mother Nature has laced a large number
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of foods and beverages and herbs
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with naturally-occurring inhibitors of angiogenesis.
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Here's a test system we developed.
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At the center is a ring
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from which hundreds of blood vessels are growing out in a starburst fashion.
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And we can use this system to test dietary factors
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at concentrations that are obtainable by eating.
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Let me show you what happens
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when we put in an extract from red grapes.
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The active ingredient is resveratrol,
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it's also found in red wine.
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This inhibits abnormal angiogenesis,
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by 60 percent.
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Here's what happens when we added an extract from strawberries.
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It potently inhibits angiogenesis.
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And extract from soybeans.
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And here is a growing list
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of antiangiogenic foods and beverages that we're interested in studying.
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For each food type,
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we believe that there are different potencies
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within different strains and varietals.
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And we want to measure this because,
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well, while you're eating a strawberry
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or drinking tea,
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why not select the one that's most potent
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for preventing cancer?
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So here are four different teas that we've tested.
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They're all common ones: Chinese jasmine, Japanese sencha,
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Earl Grey and a special blend that we prepared,
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and you can see clearly that the teas vary in their potency,
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from less potent to more potent.
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But what's very cool
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is when we combine the two less potent teas together,
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the combination, the blend, is more potent than either one alone.
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This means there's food synergy.
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Here's some more data from our testing.
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Now in the lab, we can simulate tumor angiogenesis,
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represented here in a black bar.
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And using this system, we can test the potency of cancer drugs.
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So the shorter the bar,
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the less angiogenesis -- that's good.
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And here are some common drugs
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that have been associated with reducing the risk of cancer in people.
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Statins, nonsteroidal anti-inflammatory drugs,
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and a few others -- they inhibit angiogenesis, too.
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And here are the dietary factors
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going head-to-head against these drugs.
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You can see they clearly hold their own,
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and in some cases, they're more potent than the actual drugs.
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Soy, parsley, garlic, grapes, berries.
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I could go home and cook a tasty meal using these ingredients.
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Imagine if we could create the world's first rating system,
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in which we could score foods
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according to their antiangiogenic, cancer-preventative properties.
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And that's what we're doing right now.
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Now, I've shown you a bunch of lab data,
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and so the real question is:
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What is the evidence in people
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that eating certain foods can reduce angiogenesis in cancer?
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Well, the best example I know
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is a study of 79,000 men followed over 20 years,
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in which it was found that men who consumed cooked tomatoes
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two to three times a week,
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had up to a 50 percent reduction
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in their risk of developing prostate cancer.
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Now, we know that tomatoes are a good source of lycopene,
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and lycopene is antiangiogenic.
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But what's even more interesting from this study,
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is that in those men who did develop prostate cancer,
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those who ate more servings of tomato sauce,
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actually had fewer blood vessels feeding their cancer.
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So this human study is a prime example
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of how antiangiogenic substances present in food and consumed at practical levels,
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can have an impact on cancer.
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And we're now studying the role of a healthy diet --
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with Dean Ornish at UCSF and Tufts University --
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the role of this healthy diet on markers of angiogenesis
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that we can find in the bloodstream.
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Obviously, what I've shared with you has some far-ranging implications,
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even beyond cancer research.
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Because if we're right, it could impact consumer education,
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food services, public health
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and even the insurance industry.
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And in fact, some insurance companies
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are already beginning to think along these lines.
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Check out this ad from BlueCross BlueShield of Minnesota.
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For many people around the world,
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dietary cancer prevention may be the only practical solution,
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because not everybody can afford expensive end-stage cancer treatments,
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but everybody could benefit from a healthy diet
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based on local, sustainable, antiangiogenic crops.
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Now, finally,
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I've talked to you about food,
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and I've talked to you about cancer,
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so there's just one more disease that I have to tell you about,
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and that's obesity.
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Because it turns out that adipose tissue -- fat --
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is highly angiogenesis-dependent.
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And like a tumor, fat grows when blood vessels grow.
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So the question is:
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Can we shrink fat by cutting off its blood supply?
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The top curve shows the body weight of a genetically obese mouse
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that eats nonstop until it turns fat,
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like this furry tennis ball.
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(Laughter)
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And the bottom curve is the weight of a normal mouse.
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If you take the obese mouse
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and give it an angiogenesis inhibitor, it loses weight.
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Stop the treatment, gains the weight back. Restart the treatment, loses the weight.
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Stop the treatment, it gains the weight back.
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And, in fact, you can cycle the weight up and down
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simply by inhibiting angiogenesis.
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17:27
So this approach that we're taking for cancer prevention
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may also have an application for obesity.
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The truly interesting thing about this
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is that we can't take these obese mice
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and make them lose more weight
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than what the normal mouse's weight is supposed to be.
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In other words, we can't create supermodel mice.
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(Laughter)
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And this speaks to the role of angiogenesis
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in regulating healthy set points.
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Albert Szent-Györgi once said,
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"Discovery consists of seeing what everyone has seen,
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and thinking what no one has thought."
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I hope I've convinced you
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that for diseases like cancer, obesity and other conditions,
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there may be a great power
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in attacking their common denominator: angiogenesis.
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And that's what I think the world needs now.
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Thank you.
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(Applause)
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June Cohen: I have a quick question for you.
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JC: So these drugs aren't exactly in mainstream cancer treatments right now.
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For anyone out here who has cancer, what would you recommend?
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Do you recommend pursuing these treatments now, for most cancer patients?
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William Li: There are antiangiogenic treatments
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that are FDA approved,
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and if you're a cancer patient,
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or working for one or advocating for one, you should ask about them.
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And there are many clinical trials.
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The Angiogenesis Foundation is following almost 300 companies,
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and there are about 100 more drugs in that pipeline.
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So, consider the approved ones,
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look for clinical trials,
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but then between what the doctor can do for you,
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we need to start asking what can we do for ourselves.
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This is one of the themes I'm talking about:
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We can empower ourselves
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to do the things that doctors can't do for us,
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which is to use knowledge and take action.
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And if Mother Nature has given us some clues,
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we think there might be a new future in the value of how we eat,
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and what we eat is really our chemotherapy three times a day.
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JC: Right. And along those lines,
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19:23
for people who might have risk factors for cancer,
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would you recommend pursuing any treatments prophylactically,
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19:29
or simply pursuing the right diet,
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19:31
with lots of tomato sauce?
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19:33
WL: Well, you know, there's abundant epidemiological evidence,
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and I think in the information age,
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it doesn't take long to go to a credible source like PubMed,
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the National Library of Medicine,
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to look for epidemiological studies for cancer risk reduction
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based on diet and based on common medications.
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And that's certainly something that anybody can look into.
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JC: Okay. Well, thank you so much.
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19:53
(Applause)
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