Next big COVID-19 treatment may be manufactured antibodies
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[August 03, 2020]
By Deena Beasley
(Reuters) - As the world awaits a COVID-19
vaccine, the next big advance in battling the pandemic could come from a
class of biotech therapies widely used against cancer and other
disorders - antibodies designed specifically to attack this new virus.
Development of monoclonal antibodies to target the virus has been
endorsed by leading scientists. Anthony Fauci, the top U.S. infectious
diseases expert, called them "almost a sure bet" against COVID-19.
When a virus gets past the body's initial defenses, a more specific
response kicks in, triggering production of cells that target the
invader. These include antibodies that recognize and lock onto a virus,
preventing the infection from spreading.
Monoclonal antibodies - grown in bioreactor vats - are copies of these
naturally-occurring proteins.
Scientists are still working out the exact role of neutralizing
antibodies in recovery from COVID-19, but drugmakers are confident that
the right antibodies or a combination can alter the course of the
disease that has claimed more than 675,000 lives globally.
"Antibodies can block infectivity. That is a fact," Regeneron
Pharmaceuticals executive Christos Kyratsous told Reuters.
Regeneron is testing a two-antibody cocktail, which it believes limits
the ability of the virus' to escape better than one, with data on its
efficacy expected by late summer or early fall. "Protection will wane
over time. Dosing is something we don't know yet," said Kyratsous.
The U.S. government in June awarded Regeneron a $450 million supply
contract. The company said it can immediately begin production at its
U.S. plant if regulators approve the treatment.
Eli Lilly and Co <LLY.N, AstraZeneca, Amgen, and GlaxoSmithKline were
cleared by the U.S. government to pool manufacturing resources in order
to scale up supplies if any of these drugs prove successful.
Even with that unusual cooperation among rivals, manufacturing these
medicines is complex and capacity is limited. There is also a debate
over whether a single antibody will be powerful enough to stop COVID-19.
AstraZeneca said it plans to start human trials of its dual-antibody
combination within weeks.
Lilly, which began human testing in June of two antibody candidates in
separate trials, is focusing on a one-drug approach.
"If you need a higher dosage or more antibodies, fewer people can be
treated," Lilly Chief Scientific Officer Dan Skovronsky said.
'INSTANT IMMUNITY'
Unlike vaccines, which activate the body's own immune system, the impact
of infused antibodies eventually dissipates.
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A man walks past a sign at an AstraZeneca site in Macclesfield,
central England May 19, 2014. REUTERS/Phil Noble/File Photo
Still, drugmakers say monoclonal antibodies could temporarily
prevent infection in at-risk people such as medical workers and the
elderly. They could also be used as a therapeutic bridge until
vaccines become widely available.
"In a prophylactic setting we think we may achieve coverage for up
to six months," said Phil Pang, chief medical officer of Vir
Biotechnology, which aims to start testing an antibody in
non-hospitalized patients next month with partner GSK.
"The advantage of an antibody is that it is basically instant
immunity," said Mark Brunswick, senior vice president at Sorrento
Therapeutics, which aims to begin human trials next month of a
single antibody candidate.
Safety risks for monoclonal antibodies are considered low, but their
cost can be quite high. These type of drugs for cancer can cost over
$100,000 a year.
There is also concern that the coronavirus could become resistant to
specific antibodies. Researchers are already at work on
second-generation compounds with targets other than the crown-like
spikes the virus uses to invade cells.
"We are trying to develop something that is complementary," Amgen
research chief David Reese said. Amgen is working with Adaptive
Biotechnologies Corp.
Researchers in a recent paper published in the journal Nature said
they had discovered several new, very potent, antibodies directed to
an area where the virus attaches to human cells and to a region of
the spike that has not attracted attention.
"To avoid development of resistance you want to target different
sites," study author and Columbia University professor David Ho told
Reuters.
There are also questions about when in the course of the illness it
might be best to employ these new weapons.
"Giving an antibody later on after infection might not be that
helpful, said Florian Krammer, microbiology professor at New York's
Icahn School of Medicine. "Given early, they probably work well."
(Reporting By Deena Beasley, editing by Peter Henderson and Bill
Berkrot)
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