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Malaria vaccine development: Recent progress, future challenges

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Established in 1999 as a program of PATH. Current donors: Bill & Melinda Gates Foundation, ... USAID, ExxonMobil Foundation, private individuals. PATH Malaria ... – PowerPoint PPT presentation

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Title: Malaria vaccine development: Recent progress, future challenges


1
Malaria vaccine developmentRecent progress,
future challenges
Christian Loucq, MDDirector, PATH Malaria
Vaccine Initiative All Party Parliamentary Group
on Malariaand Neglected Tropical
DiseasesOctober 26, 2009
2
PATH Malaria Vaccine InitiativeMission and vision
To accelerate the development of malaria vaccines
and ensuretheir availability and accessibility
in the developing world
A world free from malaria
Established in 1999 as a program of PATH.Current
donors Bill Melinda Gates Foundation,USAID,
ExxonMobil Foundation, private individuals
3
PATH a catalyst for global health
MVI a global programof PATH
4
Role of MACEPA
  • Many groups/organizations involved in the
    purchasing and distribution of bednets, few are
    measuring impact of the interventions
  • One of the important roles of MACEPA supported
    the coordination of malaria ME in Zambia
  • Partner in the development of the RBM MERG
    Malaria Indicator Survey (MIS)
  • Document and disseminate success stories


5
PATH background
  • International nonprofit to help provide
    appropriate health technologies and vital
    strategies to improve global health and
    well-being
  • Particular focus on
  • HIV, TB, and malaria (MACEPA and MVI)
  • Health technologies designed for low-resource
    settings
  • Safer childbirth and healthy children
  • Health equity for women
  • Basic protection of vaccines

6
Why a malaria vaccine?
  • Malaria
  • 900,000 deaths
  • US 12 billion
  • 40 percent of public health spending
  • Control
  • Elimination / Eradication

7
Why a malaria vaccine?
8
Malaria 101
  • A parasitic infection transmitted to humans
    through the bite of infected female Anopheles
    mosquitoes
  • Five Plasmodium sp. infect humans falciparum and
    vivax cause the vast majority of clinical cases
  • Almost all serious disease/deaths are caused by
    P. falciparum malaria in children under 5 years
    of age

9
Challenges to developing malaria vaccines
  • Scientific
  • No vaccine is in human use against a parasite
  • Malaria parasite has 6,000 genes, many more than
    a virus
  • How best to provoke immune response?
  • How to predict a vaccine candidates success?
  • Commercial
  • Limited market in developed countries
  • Endemic countries mostly poor
  • High-risk, high-level investment

10
Where are we today?
  • Worlds most clinically advanced vaccine
    candidate is RTS,S
  • Collaboration with GSK Bio (Belgium), 11 study
    centers (in seven African countries), and
    Northern institutions
  • Phase 3 trial now up and running in all seven
    countries, 10 of 11 sites

11
RTS,S project is MVIs largest collaboration
12
Where are we today?
  • A second vaccine approach approved for
    first-in-human trial in the United States
  • Sanaria Inc. seeks to replicate original
    experiment with irradiated mosquitoes

13
How MVI works
  • MVI partners to achieve its mission success
    depends on the strength of its collaborations
  • MVI is a non-profit vaccine investor. Partners
    include academia, government agencies, biotechs,
    pharmaceutical companies
  • MVI identifies potentially promising malaria
    vaccine candidates and approaches, then
  • MVI systematically move candidates and approaches
    through the development process.

14
MVI Portfolio
Selected projects
15
MVI collaborators include
16
Goals in sight?
  • Vaccine goal for 2015 in sight
  • 50 efficacy against severe disease
  • Lasts more than one year
  • Another tool to achieve malaria control
  • Next-generation vaccine could be in the pipeline
    now
  • Higher efficacy, lasts longer than 4 years
  • Transmission blocking?
  • Key to malaria elimination, eradication

17
Malaria vaccine community goal
  • By 2025, to develop and license a malaria vaccine
    that has a protective efficacy of more than 80
    against clinical disease and lasts longer than
    four years
  • BUT,
  • Could we do more?

18
Goal Malaria eradication
19
What comes next?
  • Focus on questions to be answered

20
Different types of vaccine target different
stages of the lifecycle
  • Pre-erythrocytic vaccines
  • Blood-stage vaccines
  • Transmission-blocking vaccines

21
Different types of vaccine target different
stages of the lifecycle
22
Transmission-blocking vaccines target the
parasite in the mosquitoand mosquito itself
23
Transmission-blocking vaccines
  • Goal Interrupt lifecycle to reduce transmission
  • Strategies
  • 1. Block production of gametocytes
  • (highly effective PE vaccine)
  • 2. Block oocyst formation in mosquito
    (prevent transmission of the disease)
  • TBVs target transmission
  • No direct, immediate benefit to vaccinee
  • Infections reduced due to reduced transmission
    (herd effect)

2
1
24
MFA with sera (12) from baboons immunized with
CH-rPfs48/45 in Montanide ISA-51
Doses Blocking (MFA) Primary 93 3
(8894) Boost 1 97 1 (9598) Boost 2
(15d) 97 1 (9599) Boost 2 (30 d) 97 1
(9698) Boost 2 (3 mo) 97 1 (9599)
Chowdhury, DR. et al. PLoS One July 2009.
4(7)110
25
MFA to evaluate transmission blocking antibodies
  • Cultured serum gametocytes fed to starved
    mosquitoes through membrane
  • Count oocysts in midgut 1 week later.
  • Result oocyst reduction

26
Vaccines Critical component of coordinated
eradication effort
  • Vector control
  • Insecticide treated bednets
  • Indoor residual spraying
  • Integrated vector management
  • Drug therapy
  • Vaccines

27
Final thoughts
  • Malaria eradication will not happen without
    vaccines
  • Funding for RD and introduction is needed
  • CollaborationCoordinationCommitment

28
Tomorrow
29
Thank You
  • www.path.org
  • www.malariavaccine.org
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