May lead to intranasal vaccines for Covid-19 and other respiratory diseases
Massachusetts Institute of Technology
Adjuvants are
molecules commonly used to increase the immune response to vaccines, but they
haven't yet been used in RNA vaccines. In this study, the MIT researchers
engineered both the nanoparticles used to deliver the Covid-19 antigen, and the
antigen itself, to boost the immune response, without the need for a separate
adjuvant.
If further
developed for use in humans, this type of RNA vaccine could help to reduce
costs, reduce the dosage needed, and potentially lead to longer-lasting
immunity. The researchers' tests also showed that when delivered intranasally,
the vaccine induced a strong immune response when compared to the response
elicited by traditional, intramuscular vaccination.
"With intranasal vaccination, you might be able to kill Covid at the mucus membrane, before it gets into your body," says Daniel Anderson, a professor in MIT's Department of Chemical Engineering, a member of MIT's Koch Institute for Integrative Cancer Research and Institute for Medical Engineering and Science (IMES), and the senior author of the study.
"Intranasal vaccines may also
be easier to administer to many people, since they don't require an
injection."
The researchers believe that the effectiveness of other types of RNA vaccines that are now in development, including vaccines for cancer, could be improved by incorporating similar immune-stimulating properties.
Former MIT postdoc Bowen Li, who is now an assistant professor at the University of Toronto; graduate student Allen Jiang; and former MIT postdoc Idris Raji, who was a research fellow at Boston Children's Hospital, are the lead authors of the new study, which appears today in Nature Biomedical Engineering.
The research
team also includes Robert Langer, the David H. Koch Institute Professor at MIT
and a member of the Koch Institute, and several other MIT researchers.
Boosting immunity
RNA vaccines
consist of a strand of RNA that encodes a viral or bacterial protein, also
called an antigen. In the case of Covid-19 vaccines, this RNA codes for a
segment of the virus's spike protein. That RNA strand is packaged in a lipid
nanoparticle carrier, which protects the RNA from being broken down in the body
and helps it get into cells.
Once delivered
into cells, the RNA is translated into proteins that the immune system can
detect, generating antibodies and T cells that will recognize the protein if
the person later becomes infected with the SARS-CoV-2 virus.
The original
Covid-19 RNA vaccines developed by Moderna and Pfizer/BioNTech provoked strong
immune responses, but the MIT team wanted to see if they could make them more
effective by engineering them to have immune stimulatory properties.
In this study, the researchers employed two different strategies to boost the immune response. For the first, they focused on a protein called C3d, which is part of an arm of the immune response known as the complement system.
This set of proteins helps the
body fight off infection, and C3d's role is to bind to antigens and amplify the
antibody response to those antigens. For many years, scientists have been
evaluating the use of C3d as a molecular adjuvant for vaccines made from
proteins, such as the DPT vaccine.
"With the
promise of mRNA technologies being realized with the Covid vaccines, we thought
that this would be a fantastic opportunity to see if C3d might also be able to
play a role as an adjuvant in mRNA vaccine systems," Jiang says.
To that end, the
researchers engineered the mRNA to encode the C3d protein fused to the antigen,
so that both components are produced as one protein by cells that receive the
vaccine.
In the second
phase of their strategy, the researchers modified the lipid nanoparticles used
to deliver the RNA vaccine, so that in addition to helping with RNA delivery,
the lipids also intrinsically stimulate a stronger immune response.
To identify lipids that would work best, the researchers created a library of 480 lipid nanoparticles with different types of chemistries. All of these are "ionizable" lipids, which become positively charged when they enter acidic environments.
The original Covid RNA vaccines also included some
ionizable lipids because they help the nanoparticles to self-assemble with RNA
and they help target cells to take up the vaccine.
"We
understood that nanoparticles themselves could be immunostimulatory, but we
weren't quite sure what the chemistry was that was needed to optimize that
response. So instead of trying to make the perfect one, we made a library and
evaluated them, and through that we identified some chemistries that seemed to
improve their response," Anderson says.
Toward intranasal vaccines
The researchers
tested their new vaccine, which included both RNA-encoded C3d and a
top-performing ionizable lipid identified from their library screen, in mice.
They found that mice injected with this vaccine produced 10 times more
antibodies than mice given unadjuvanted Covid RNA vaccines. The new vaccine
also provoked a stronger response among T cells, which play important roles in
combating the SARS-CoV-2 virus.
"For the
first time, we've demonstrated a synergistic boost in immune responses by
engineering both the RNA and its delivery vehicles," Li says. "This
prompted us to investigate the feasibility of administering this new RNA
vaccine platform intranasally, considering the challenges presented by the
mucociliary blanket barrier in the upper airways."
When the
researchers delivered the vaccine intranasally, they observed a similarly
strong immune response in the mice. If developed for use in people, an
intranasal vaccine could potentially offer enhanced protection against
infection because it would generate an immune response within the mucosal
tissues that line the nasal passages and lungs.
Because
self-adjuvanting vaccines elicit a stronger response at a lower dose, this
approach could also help to reduce the cost of vaccine doses, which might allow
them to reach more people, especially in developing nations, the researchers
say.
Anderson's lab is now exploring whether this self-adjuvanting platform might also help boost the immune response of other types of RNA vaccines, including cancer vaccines.
Working with health care companies, the researchers also plan to test the
effectiveness and safety of these new vaccine formulations in larger animal
models, in hopes of eventually testing them in patients.
The research was funded by the National Institutes of Health and Translate Bio.
