Decoy particles trick coronavirus as it evolves
Emerging therapeutics could overcome drug-resistant variants
Date:
April 11, 2022
Source:
Northwestern University
Summary:
Decoy nanoparticles mimic cells, attracting viruses to bind to
them rather than infecting healthy cells. Researchers tested the
strategy against the novel coronavirus and five of its variants,
finding it was consistently effective.
FULL STORY ==========================================================================
They might look like cells and act like cells. But a new potential
COVID-19 treatment is actually a cleverly disguised trickster, which
attracts viruses and binds them, rendering them inactive.
==========================================================================
As the ever-evolving SARS-CoV-2 virus begins to evade once promising treatments, such as monoclonal antibody therapies, researchers have become
more interested in these "decoy" nanoparticles. Mimicking regular cells,
decoy nanoparticles soak up viruses like a sponge, inhibiting them from infecting the rest of the body.
In a new study, Northwestern University synthetic biologists set out to elucidate the design rules needed make decoy nanoparticles effective and resistant to viral escape. After designing and testing various iterations,
the researchers identified a broad set of decoys -- all manufacturable
using different methods -- that were incredibly effective against the
original virus as well as mutant variants.
In fact, decoy nanoparticles were up to 50 times more effective at
inhibiting naturally occurring viral mutants, compared to traditional, protein-based inhibitor drugs. When tested against a viral mutant designed
to resist such treatments, decoy nanoparticles were up to 1,500 times
more effective at inhibiting infection.
Although much more research and clinical evaluations are needed, the researchers believe decoy nanoparticle infusions someday could potentially
be used to treat patients with severe or prolonged viral infections.
The study was published late last week (April 7) in the journal Small. In
the paper, the team tested decoy nanoparticles against the parent
SARS-CoV-2 virus and five variants (including beta, delta, delta-plus
and lambda) in a cellular culture.
==========================================================================
"We showed that decoy nanoparticles are effective inhibitors of all
these different viral variants," said Northwestern's Joshua Leonard,
co-senior author of the study. "Even variants that escape other drugs did
not escape our decoy nanoparticles." "As we were conducting the study, different variants kept popping up around the world," added Northwestern's
Neha Kamat, co-senior author of the study. "We kept testing our decoys
against the new variants, and they just kept working.
It's very effective." Leonard is an associate professor of chemical
and biological engineering in Northwestern's McCormick School of
Engineering. Kamat is an assistant professor of biomedical engineering
in McCormick. Both are key members of Northwestern's Center for Synthetic Biology.
'Evolutionary rock and a hard place' As the SARS-CoV-2 virus has mutated
to create new variants, some treatments have become less effective in
fighting the ever-evolving virus. Just last month, the U.S. Food and
Drug Administration (FDA) paused several monoclonal antibody treatments,
for example, due to their failure against the BA.2 omicron subvariant.
==========================================================================
But even where treatments fail, the decoy nanoparticles in the new
study never lost effectiveness. Leonard said this is because the
decoys put SARS-CoV- 2 "between an evolutionary rock and a hard place." SARS-CoV-2 infects human cells by binding its infamous spike protein to
the human angiotensin-converting enzyme 2 (ACE2) receptor. A protein on
the surface of cells, ACE2 provides an entry point for the virus.
To design decoy nanoparticles, the Northwestern team used nanosized
particles (extracellular vesicles) naturally released from all cell
types. They engineered cells producing these particles to overexpress
the gene for ACE2, leading to many ACE2 receptors on the particles'
surfaces. When the virus came into contact with the decoy, it bonded
tightly to these receptors rather than to real cells, rendering the
virus unable to infect cells.
"For the virus to get into a cell, it has to bind to the ACE2 receptor," Leonard said. "Decoy nanoparticles present an evolutionary challenge for
SARS- CoV-2. The virus would have to come up with an entirely different
way to enter cells in order to avoid the need to use ACE2 receptors. There
is no obvious evolutionary escape route." Future benefits In addition
to being effective against drug-resistant viruses, decoy nanoparticles
come with several other benefits. Because they are biological (rather
than synthetic) materials, the nanoparticles are less likely to elicit
an immune response, which causes inflammation and can interfere with the
drug's efficacy. They also exhibit low toxicity, making them particularly well-suited for use in sustained or repeated administration for treating severely ill patients.
When the COVID-19 pandemic began, researchers and clinicians experienced
an unnerving gap between discovering the virus and developing new drugs
to treat it. For the next pandemic, decoy nanoparticles could provide
a quick, effective treatment before vaccines are developed.
"The decoy strategy is one of the most immediate things you can try,"
Leonard said. "As soon as you know the receptor that the virus uses,
you can start building decoy particles with those receptors. We could potentially fast-track an approach like this to reduce severe illness and
death in the crucial early stages of future viral pandemics." The study, "Elucidating design principles for engineering cell-derived vesicles to
inhibit SARS-CoV-2 infection," was supported by the National Science
Foundation (grant numbers 1844219 and 1844336) and a gift from Kairos
Ventures.
========================================================================== Story Source: Materials provided by Northwestern_University. Original
written by Amanda Morris. Note: Content may be edited for style and
length.
========================================================================== Journal Reference:
1. Taylor F. Gunnels, Devin M. Stranford, Roxana E. Mitrut, Neha
P. Kamat,
Joshua N. Leonard. Elucidating Design Principles for Engineering
Cell‐Derived Vesicles to Inhibit SARS‐CoV‐2
Infection.
Small, 2022; 2200125 DOI: 10.1002/smll.202200125 ==========================================================================
Link to news story:
https://www.sciencedaily.com/releases/2022/04/220411184330.htm
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