Mark Kendall: Demo: A needle-free vaccine patch that's safer and way cheaper

152,638 views ・ 2014-01-14

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00:12
It's a pleasure to be here
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in Edinburgh, Scotland,
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the birthplace of the needle and syringe.
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Less than a mile from here in this direction,
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in 1853 a Scotsman
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filed his very first patent on the needle and syringe.
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His name was Alexander Wood,
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and it was at the Royal College of Physicians.
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This is the patent.
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What blows my mind when I look at it even today
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is that it looks almost identical
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to the needle in use today.
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Yet, it's 160 years old.
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So we turn to the field of vaccines.
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Most vaccines are delivered with
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the needle and syringe, this 160-year-old technology.
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And credit where it's due -- on many levels,
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vaccines are a successful technology.
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After clean water and sanitation,
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vaccines are the one technology that has increased
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our life span the most.
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That's a pretty hard act to beat.
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01:12
But just like any other technology,
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vaccines have their shortcomings,
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and the needle and syringe
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is a key part within that narrative --
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this old technology.
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So let's start with the obvious:
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Many of us don't like the needle and syringe.
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I share that view.
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However, 20 percent of the population
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have a thing called needle phobia.
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That's more than disliking the needle;
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that is actively avoiding being vaccinated
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because of needle phobia.
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And that's problematic in terms of the rollout of vaccines.
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Now, related to this is another key issue,
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which is needlestick injuries.
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And the WHO has figures
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that suggest about 1.3 million deaths per year
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take place due to cross-contamination
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with needlestick injuries.
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These are early deaths that take place.
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Now, these are two things that you probably may have heard of,
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but there are two other shortcomings
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of the needle and syringe you may not have heard about.
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One is it could be holding back
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the next generation of vaccines
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in terms of their immune responses.
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And the second is that it could be responsible
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for the problem of the cold chain that I'll tell you about as well.
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I'm going to tell you about some work
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that my team and I are doing in Australia
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at the University of Queensland
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on a technology designed to tackle those four problems.
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And that technology is called the Nanopatch.
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Now, this is a specimen of the Nanopatch.
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To the naked eye
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it just looks like a square
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smaller than a postage stamp,
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but under a microscope
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what you see are thousands of tiny projections
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that are invisible to the human eye.
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And there's about 4,000 projections
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on this particular square compared to the needle.
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And I've designed those projections
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to serve a key role, which is to work with the skin's immune system.
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So that's a very important function
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tied in with the Nanopatch.
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Now we make the Nanopatch
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with a technique
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called deep reactive ion etching.
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And this particular technique is one that's been borrowed
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from the semiconductor industry,
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and therefore is low cost
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and can be rolled out in large numbers.
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Now we dry-coat vaccines to the projections of the Nanopatch
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and apply it to the skin.
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Now, the simplest form of application
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is using our finger,
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but our finger has some limitations,
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so we've devised an applicator.
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And it's a very simple device --
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you could call it a sophisticated finger.
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It's a spring-operated device.
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What we do is when we apply the Nanopatch to the skin as so --
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(Click) --
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immediately a few things happen.
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So firstly, the projections on the Nanopatch
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breach through the tough outer layer
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and the vaccine is very quickly released --
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within less than a minute, in fact.
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Then we can take the Nanopatch off
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and discard it.
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And indeed we can make a reuse of the applicator itself.
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So that gives you an idea of the Nanopatch,
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and immediately you can see some key advantages.
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We've talked about it being needle-free --
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these are projections that you can't even see --
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and, of course, we get around
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the needle phobia issue as well.
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Now, if we take a step back and think about
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these other two really important advantages:
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One is improved immune responses through delivery,
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and the second is getting rid of the cold chain.
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So let's start with the first one, this immunogenicity idea.
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It takes a little while to get our heads around,
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but I'll try to explain it in simple terms.
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So I'll take a step back and explain to you
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how vaccines work in a simple way.
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So vaccines work by introducing into our body
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a thing called an antigen
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which is a safe form of a germ.
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Now that safe germ, that antigen,
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tricks our body into mounting an immune response,
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learning and remembering how to deal with intruders.
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When the real intruder comes along
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the body quickly mounts an immune response
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to deal with that vaccine
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and neutralizes the infection.
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So it does that well.
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Now, the way it's done today with the needle and syringe,
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most vaccines are delivered that way --
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with this old technology and the needle.
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But it could be argued that the needle is holding back our immune responses;
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it's missing our immune sweet spot in the skin.
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To describe this idea,
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we need to take a journey through the skin,
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starting with one of those projections
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and applying the Nanopatch to the skin.
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And we see this kind of data.
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Now, this is real data --
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that thing that we can see there is one projection
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from the Nanopatch that's been applied to the skin
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and those colors are different layers.
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Now, to give you an idea of scale,
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if the needle was shown here, it would be too big.
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It would be 10 times bigger
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than the size of that screen, going 10 times deeper as well.
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It's off the grid entirely.
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You can see immediately that we have those projections in the skin.
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That red layer is a tough outer layer of dead skin,
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but the brown layer and the magenta layer
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are jammed full of immune cells.
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As one example, in the brown layer
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there's a certain type of cell called a Langerhans cell --
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every square millimeter of our body
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is jammed full of those Langerhans cells,
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those immune cells, and there's others shown as well
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that we haven't stained in this image.
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But you can immediately see that the Nanopatch
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achieves that penetration indeed.
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We target thousands upon thousands of these particular cells
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just residing within a hair's width
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of the surface of the skin.
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Now, as the guy that's invented this thing and designed it to do that,
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I found that exciting. But so what?
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So what if you've targeted cells?
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In the world of vaccines, what does that mean?
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The world of vaccines is getting better.
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It's getting more systematic.
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However, you still don't really know
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if a vaccine is going to work
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until you roll your sleeves up
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and vaccinate and wait.
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It's a gambler's game even today.
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So, we had to do that gamble.
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We obtained an influenza vaccine,
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we applied it to our Nanopatches
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and we applied the Nanopatches to the skin,
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and we waited --
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and this is in the live animal.
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We waited a month,
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and this is what we found out.
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This is a data slide showing the immune responses
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that we've generated with a Nanopatch
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compared to the needle and syringe into muscle.
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So on the horizontal axis we have the dose shown in nanograms.
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On the vertical axis we have the immune response generated,
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and that dashed line indicates the protection threshold.
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If we're above that line it's considered protective;
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if we're below that line it's not.
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So the red line is mostly below that curve
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and indeed there's only one point that is achieved with the needle that's protective,
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and that's with a high dose of 6,000 nanograms.
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But notice immediately the distinctly different curve
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that we achieve with the blue line.
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That's what's achieved with the Nanopatch;
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the delivered dose of the Nanopatch is
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a completely different immunogenicity curve.
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That's a real fresh opportunity.
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Suddenly we have a brand new lever
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in the world of vaccines.
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We can push it one way,
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where we can take a vaccine that works but is too expensive
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and can get protection
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with a hundredth of the dose compared to the needle.
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That can take a vaccine that's suddenly 10 dollars down to 10 cents,
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and that's particularly important within the developing world.
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But there's another angle to this as well --
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you can take vaccines that currently don't work
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and get them over that line
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and get them protective.
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And certainly in the world of vaccines
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that can be important.
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Let's consider the big three:
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HIV, malaria, tuberculosis.
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They're responsible for about 7 million deaths per year,
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and there is no adequate vaccination method for any of those.
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So potentially, with this new lever that we have with the Nanopatch,
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we can help make that happen.
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We can push that lever to help get those candidate vaccines over the line.
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Now, of course, we've worked within my lab
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with many other vaccines that have attained
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similar responses and similar curves to this,
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what we've achieved with influenza.
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I'd like to now switch to talk about
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another key shortcoming of today's vaccines,
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and that is the need to maintain the cold chain.
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As the name suggests -- the cold chain --
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it's the requirements of keeping a vaccine right from production
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all the way through to when the vaccine is applied,
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to keep it refrigerated.
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Now, that presents some logistical challenges
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but we have ways to do it.
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This is a slightly extreme case in point
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but it helps illustrate the logistical challenges,
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in particular in resource-poor settings,
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of what's required to get vaccines
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refrigerated and maintain the cold chain.
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If the vaccine is too warm the vaccine breaks down,
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but interestingly it can be too cold
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and the vaccine can break down as well.
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Now, the stakes are very high.
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The WHO estimates that within Africa,
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up to half the vaccines used there
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are considered to not be working properly
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because at some point the cold chain has fallen over.
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So it's a big problem, and it's tied in with the needle and syringe
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because it's a liquid form vaccine, and when it's liquid it needs the refrigeration.
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A key attribute of our Nanopatch
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is that the vaccine is dry,
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and when it's dry it doesn't need refrigeration.
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Within my lab we've shown that we can keep
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the vaccine stored at 23 degrees Celsius
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for more than a year without any loss in activity at all.
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That's an important improvement.
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(Applause)
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We're delighted about it as well.
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And the thing about it is that we have well and truly proven
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the Nanopatch within the laboratory setting.
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And as a scientist, I love that and I love science.
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However, as an engineer,
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as a biomedical engineer
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and also as a human being,
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I'm not going to be satisfied
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until we've rolled this thing out, taken it out of the lab
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and got it to people in large numbers
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and particularly the people that need it the most.
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So we've commenced this particular journey,
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and we've commenced this journey in an unusual way.
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We've started with Papua New Guinea.
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Now, Papua New Guinea is an example of a developing world country.
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It's about the same size as France,
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but it suffers from many of the key barriers
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existing within the world of today's vaccines.
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There's the logistics:
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Within this country there are only 800 refrigerators to keep vaccines chilled.
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Many of them are old, like this one in Port Moresby, many of them are breaking down
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and many are not in the Highlands where they are required.
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That's a challenge.
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But also, Papua New Guinea has the world's highest incidence of HPV,
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human papillomavirus, the cervical cancer [risk factor].
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Yet, that vaccine is not available in large numbers
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because it's too expensive.
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So for those two reasons, with the attributes of the Nanopatch,
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we've got into the field and worked with the Nanopatch,
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and taken it to Papua New Guinea
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and we'll be following that up shortly.
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Now, doing this kind of work is not easy.
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It's challenging,
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but there's nothing else in the world I'd rather be doing.
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And as we look ahead
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I'd like to share with you a thought:
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It's the thought of a future where
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the 17 million deaths per year
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that we currently have due to infectious disease
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is a historical footnote.
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And it's a historical footnote that has been achieved
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by improved, radically improved vaccines.
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Now standing here today in front of you
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at the birthplace of the needle and syringe,
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a device that's 160 years old,
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I'm presenting to you an alternative approach
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that could really help make that happen --
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and it's the Nanopatch with its attributes of being needle-free, pain-free,
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the ability for removing the cold chain and improving the immunogenicity.
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13:28
Thank you.
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13:30
(Applause)
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