New research led by scientists at The Scripps Research Institute (TSRI),
International AIDS Vaccine Initiative (IAVI) and The Rockefeller University
shows in mice that an experimental vaccine candidate designed at TSRI can
stimulate the immune system activity necessary to stop HIV infection. The
findings could provide key information for the development of an effective AIDS
vaccine.
The research, published June 18, 2015 in concurrent studies in the
journalsCell and Science, represents a leap forward in the effort to develop
avaccine against HIV, which has so far struggled to elicit antibodies (immune
system molecules) that can effectively fight off different strains of the
virus.
"The results are pretty spectacular," said Dennis Burton, chair of the TSRI
Department of Immunology and Microbial Science and scientific director of two
centers at TSRI, the IAVI Neutralizing Antibody Consortium (NAC) and the
National Institutes of Health (NIH) Center for HIV/AIDS Vaccine Immunology and
Immunogen Discovery (CHAVI-ID).
The Science study was co-led by Burton, TSRI Professor and IAVI NAC
Associate Director of Vaccine Design William Schief, and TSRI Professor David
Nemazee. The Cell study was co-led by Schief and Michel Nussenzweig, who is
Zanvil A. Cohn and Ralph M. Steinman Professor at The Rockefeller University and
a Howard Hughes Medical Institute (HHMI) investigator.
A Huge Challenge
The researchers' long-term goal is to design a vaccine that prompts the
body to produce antibodies that bind to HIV and prevent infection.
While many vaccines for other diseases use a dead or inactive version of
the disease-causing microbe itself to trigger antibody production, immunizations
with "native" HIV proteins are ineffective in triggering an effective immune
response, due to HIV's ability to evade detection from the immune system and
mutate rapidly into new strains.
This challenge has led many researchers to believe that a successful AIDS
vaccine will need to consist of a series of related, but slightly different
proteins (immunogens) to train the body to produce broadly neutralizing
antibodies against HIV—a twist on the traditional "booster" shot, where a person
is exposed to the same immunogen multiple times.
In the new studies, the scientists tested one of these potential proteins,
an immunogen called eOD-GT8 60mer, a protein nanoparticle designed to bind and
activate B cells needed to fight HIV. The eOD-GT8 60mer was developed in the
Schief lab and tested in mouse models engineered by the Nemazee lab to produce
antibodies that resemble human antibodies.
Using a technique called B cell sorting, the researchers showed that
immunization with eOD-GT8 60mer produced antibody "precursors"—with some of the
traits necessary to recognize and block HIV infection. This suggested that
eOD-GT8 60mer could be a good candidate to serve as the first in a series of
immunizations against HIV.
"The vaccine appears to work well in our mouse model to 'prime' the
antibody response," added Nemazee.
In the Cell paper, researchers used the same eOD-GT8 60mer immunogen but
used a slightly different mouse model. "The immunogen again launched the immune
system in the right direction," said Schief.
A concurrent study also in Science (led by Professor John Moore of Weill
Cornell Medical College and including contributions from Schief, Burton, TSRI
Associate Professor Andrew Ward, Ian Wilson, who is Hansen Professor of
Structural Biology and chair of the Department of Integrative Structural and
Computational Biology at TSRI, and other researchers) showed engineered
immunogens also triggered immune responses in rabbit models and non-human
primate models.
Next Steps
With eOD-GT8 60mer in the running as a potential contributor to an HIV
vaccine, the researchers are now investigating other immunogens that could work
in conjunction with it.
Schief said the Nemazee lab's mouse models will be crucial resources for
testing other engineered immunogens. He emphasized the importance of bringing
different disciplines together to engineer mouse models, design antibodies and
analyze results. "This was a beautiful collaboration of three labs at TSRI,"
said Schief.
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