The key to a better malaria vaccine | Faith Osier

41,441 views ・ 2018-11-06

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There are 200 million clinical cases
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of falciparum malaria in Africa every year,
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resulting in half a million deaths.
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I would like to talk to you about malaria vaccines.
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The ones that we have made to date are simply not good enough.
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Why?
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We've been working at it for 100 plus years.
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When we started, technology was limited.
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We could see just a tiny fraction of what the parasite really looked like.
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Today, we are awash with technology,
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advanced imaging and omics platforms --
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genomics, transcriptomics, proteomics.
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These tools have given us a clearer view
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of just how complex the parasite really is.
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However, in spite of this,
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our approach to vaccine design has remained pretty rudimentary.
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To make a good vaccine, we must go back to basics
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to understand how our bodies handle this complexity.
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People who are frequently infected with malaria
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learn to deal with it.
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They get the infection, but they don't get ill.
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The recipe is encoded in antibodies.
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My team went back to our complex parasite,
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probed it with samples from Africans who had overcome malaria
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to answer the question:
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"What does a successful antibody response look like?"
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We found over 200 proteins,
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many of which are not on the radar for malaria vaccines.
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My research community may be missing out important parts of the parasite.
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Until recently, when one had identified a protein of interest,
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they tested whether it might be important for a vaccine
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by conducting a cohort study.
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This typically involved about 300 participants in a village in Africa,
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whose samples were analyzed to see
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whether antibodies to the protein would predict who got malaria
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and who did not.
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In the past 30 years,
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these studies have tested a small number of proteins
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in relatively few samples
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and usually in single locations.
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The results have not been consistent.
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My team essentially collapsed 30 years of this type of research
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into one exciting experiment, conducted over just three months.
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Innovatively, we assembled 10,000 samples
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from 15 locations in seven African countries,
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spanning time, age and the variable intensity
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of malaria experienced in Africa.
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We used omics intelligence to prioritize our parasite proteins,
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synthesize them in the lab
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and in short, recreated the malaria parasite on a chip.
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We did this in Africa, and we're very proud of that.
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(Applause)
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The chip is a small glass slide,
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but it gives us incredible power.
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We simultaneously gathered data on over 100 antibody responses.
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What are we looking for?
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The recipe behind a successful antibody response,
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so that we can predict what might make a good malaria vaccine.
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We're also trying to figure out
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exactly what antibodies do to the parasite.
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How do they kill it?
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Do they attack from multiple angles? Is there synergy?
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How much antibody do you need?
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Our studies suggest that having a bit of one antibody won't be enough.
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It might take high concentrations of antibodies
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against multiple parasite proteins.
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We're also learning that antibodies kill the parasite in multiple ways,
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and studying any one of these in isolation may not adequately reflect reality.
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Just like we can now see the parasite in greater definition,
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my team and I are focused
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on understanding how our bodies overcome this complexity.
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We believe that this could provide the breakthroughs that we need
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to make malaria history through vaccination.
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Thank you.
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(Applause)
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(Cheers)
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(Applause)
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Shoham Arad: OK, how close are we actually to a malaria vaccine?
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Faith Osier: We're just at the beginning of a process
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to try and understand what we need to put in the vaccine
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before we actually start making it.
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So, we're not really close to the vaccine, but we're getting there.
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SA: And we're hopeful.
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FO: And we're very hopeful.
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SA: Tell me about SMART, tell me what does it stand for
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and why is it important to you?
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FO: So SMART stands for South-South Malaria Antigen Research Partnership.
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The South-South is referring to us in Africa,
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looking sideways to each other in collaboration,
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in contrast to always looking to America and looking to Europe,
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when there is quite some strength within Africa.
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So in SMART,
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apart from the goal that we have, to develop a malaria vaccine,
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we are also training African scientists,
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because the burden of disease in Africa is high,
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and you need people who will continue to push the boundaries
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in science, in Africa.
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SA: Yes, yes, correct.
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(Applause)
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OK, one last question.
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Tell me, I know you mentioned this a little bit,
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but how would things actually change if there were a malaria vaccine?
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FO: We would save half a million lives every year.
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Two hundred million cases.
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It's estimated that malaria costs Africa 12 billion US dollars a year.
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So this is economics.
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Africa would simply thrive.
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SA: OK. Thank you, Faith.
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Thank you so much.
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(Applause)
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