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 The proposals have generated fierce debate among scientists. Here is
the rationale behind, and criticism of, these alternative
strategies:
WHY DELAY THE SECOND DOSE?
In clinical trials, companies tested specific doses of their
vaccines at precise time intervals to generate evidence showing how
well they work. All COVID-19 vaccines approved, so far, are designed
to teach the immune system to recognise and defend against the virus
with a first dose, and then provide a second booster dose to
reinforce that lesson.
Faced with a fast-spreading pandemic and new, more transmissible
coronavirus variants, some countries are hoping to widen
immunisation by giving some protection to as many people as possible
with a first dose, and delaying second doses.
Maximising the number of people who have partial immunity "should
reduce the number of severe COVID-19 cases and thus alleviate the
burden on hospitals", said Michael Head, a global health expert at
Britain's University of Southampton.
WHAT ABOUT SWITCHING BETWEEN COVID VACCINES?
Mixing or switching between COVID-19 vaccines is largely driven by
the same aim - vaccinating as many people as possible as the
pandemic still rages.
Giving a priming dose of one vaccine and a booster dose of another
offers flexibility to offer whichever shots are available, rather
than holding shots back so individuals always get both doses of the
same vaccine.
HAVE THESE STRATEGIES BEEN TESTED IN RIGOROUS TRIALS?
No.
None of the late-stage COVID-19 vaccine trials compared these
dose-sparing strategies or the effects of mixing vaccine types, said
Stephen Evans, a professor of pharmacoepidemiology at the London
School of Hygiene & Tropical Medicine (LSHTM).
Officials have cited limited evidence from trials that the Pfizer/BioNTech,
the Oxford University/AstraZeneca and the Moderna vaccines all
confer some protection against COVID-19 after the first dose.
Britain's MHRA health regulator said on Dec. 30 it had found an 80%
success rate for the Oxford/AstraZeneca vaccine when two full doses
are administered, three months apart, higher than the average that
the developers themselves had found.
The UK government's vaccine advisory committee said on Dec. 31 that
the Pfizer/BioNTech vaccine conferred 89% protection from two weeks
after the first dose, and that for the Oxford/AstraZeneca vaccine
"the evidence shows that the initial dose ... offers as much as 70%
protection against the effects of the virus". It did not give
detailed data.
Moderna reported its vaccine was 80% protective after one dose, with
efficacy peaking two weeks after the first shot.
But there is no long-term evidence that any of these vaccines will
offer lasting immunity based on just one dose, or how effective they
will be if the second dose is delayed.
BioNTech and Pfizer warned on Monday they had no evidence their
vaccine would continue to be protective if the second dose was given
more than 21 days after the first.
Evans said that ideally "it is safest and most cautious" to use
vaccines in conditions exactly matching those of their trials, but
added: "In the real world, this is never so."
Anthony Fauci, director of the U.S. National Institute of Allergy
and Infectious Diseases, told CNN on Friday the United States was
unlikely to delay giving second doses.
"We're going to keep doing what we're doing," he said.
Likewise, scientists have raised concerns over the idea of mixing
two different types of vaccines. Some experts speculate that,
because all of the vaccines target the same outer "spike" protein of
the virus, they could work together to train the body to fight off
the virus.
But there is no evidence this approach will work.
"There is literally zero data. It has not been tested, or if it has
been tested, the data have not been made available," said John
Moore, a professor of microbiology and immunology at Weill Cornell
Medical College in New York.
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 WHAT ABOUT REDUCING THE AMOUNT
OF VACCINE IN EACH DOSE?
In the United States, some health officials are
considering offering half doses of Moderna's
vaccine to individuals aged 18 to 55. There is
some clinical trial data backing this strategy.
Moncef Slaoui, chief adviser to the U.S. vaccine
programme Operation Warp Speed, told CBS on
Sunday that evidence from a Moderna trial showed
the half dose induced an "identical immune
response" to the higher 100 microgram dose in
adults aged 55 and under. He said the U.S.
government was discussing the issue with Moderna
and regulators. Slaoui said he
believed injecting half of the volume of vaccine was "a more
responsible approach that would be based on facts and data".
Several U.S. scientists agreed, but noted the data was not publicly
available. "It's very fuzzy. I want to see that data," said Eric
Topol, a genomics expert and director of the Scripps Research
Translational Institute in La Jolla, California.
SO ARE THESE STRATEGIES SAFE? AND WILL THEY WORK?
It's not clear.
While there is no scientific evidence on the impact of delaying
COVID-19 vaccine doses, some experts believe it could be safe to
wait and the potential payoff in protecting a larger swath of the
population may be worth it. Others aren't so sure.
"There's just no data," said Ian Jones, a professor of virology at
Britain's Reading University.
The British Society of Immunology said in a statement on Monday that
delaying a second dose by eight weeks "would be unlikely to have a
negative effect on the overall immune response". It added that it
would not expect any extra safety risks from the delay beyond the
potential increased risk of disease during the interim between
doses.
Some scientists also said that while there was no evidence to
support the strategy of mixing vaccine doses from different
manufacturers - a method known as heterologous prime-boost -
evidence from other vaccines provided some reassurance.
"Based on previous studies which combine different vaccine types, a
combination of the AstraZeneca and Pfizer vaccines is likely to be
safe," said Helen Fletcher, a professor of immunology at LSHTM.
Topol called the mix-and-match strategy "a big mistake" with
"unpredictable" results - including the potential for adverse
reactions or a significant drop-off in efficacy. "It makes no sense
whatsoever," he said.
Some worry about safety issues, particularly with delaying the
second dose for several weeks. The gap could allow time for the
virus to evolve and develop resistance to the vaccine.
Weak antibody protection could also increase the risk of having an
abnormal immune response - such as antibody-dependent enhancement -
when people encounter the real virus, Topol said.
HOW PRACTICAL IS IT TO PROLONG DOSING TIME SCHEDULES?
Extending the interval poses adherence risks, raising the chance
people may forget or fail to return for a second dose.
It also increases the length of time during which they are less than
optimally protected, and it could make it harder for health
authorities to keep track of who has had which vaccine, when, and
how often.
Given these risks, immunology and public health experts say clear
communication is imperative to ensure people understand that
although dosing schedules may be subject to change, two COVID-19
vaccine doses are needed to give the best protection.
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