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Previous COVID-19 may cut risk of reinfection 84%

Filed Under: 
COVID-19
Mary Van Beusekom | News Writer | CIDRAP News
 |
Apr 12, 2021
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micrograph_of_sars-cov-2-niaid.jpg

Magnified view of COVID-19 viruses
NIAID

micrograph_of_sars-cov-2-niaid.jpg

Magnified view of COVID-19 viruses
NIAID

People who had COVID-19 had an 84% lower risk of becoming reinfected
and a 93% lower risk of symptomatic infection during 7 months of
follow-up, according to findings from a large, multicenter study
published late last week in The Lancet.

The prospective cohort SARS-CoV-2 Immunity and Reinfection Evaluation
(SIREN) study, by Public Health England Colindale researchers,
involved 25,661 workers at public hospitals throughout England who
were tested for SARS-CoV-2 every 2 to 4 weeks and antibodies at
enrollment and every 4 weeks. Volunteers also completed
questionnaires on symptoms and exposures every 2 weeks.

Of the 25,661 participants, 32.3% were assigned to the baseline
positive (possibly or probably previously infected) group, and 67.7%
were assigned to the negative group. Of the 8,278 positive
participants, 91.2% had SARS-CoV-2 antibodies at study enrollment,
while 7.0% were negative for antibodies but had a previously positive
antibody and/or coronavirus test, and 1.8% had tested positive for
COVID-19 but didn't have linked antibody data.

Far fewer symptomatic infections

From June 2020 to January 2021, 1.4% of the 8,278 participants who
previously had COVID-19 were infected, compared with 9.8% of 17,383
initially coronavirus-naive participants. Infections in the
baseline-positive group peaked in the first week of April, while they
peaked in the negative group the last week of December.

Incidence density was 7.6 new infections per 100,000 person-days in
those previously infected, versus 57.3 per 100,000 person-days in
those without previous infection. Compared with primary infections,
the adjusted incidence rate ratio was 0.16 for reinfections. Median
time between primary infection and reinfection was more than 200
days.

Among the baseline-positive group, 50.3% of infections were
symptomatic, with 32.3% involving usual coronavirus symptoms. Among
the baseline-negative cohort, 80.3% of infections were symptomatic,
66.1% of them involving usual COVID-19 symptoms.

The authors noted that, late in the follow-up period, from Dec 8,
2020, to Jan 11, 2021, 52.2% of all participants were vaccinated
against SARS-CoV-2. Thus, 0.4% of the study's person-time follow-up
included participants 21 or more days after vaccination, which the
researchers said likely had only a modest effect on the results.

Median participant age in the baseline-positive cohort was 45.7
years, 84.2% were women, and 87.3% were White. Median follow-up was
275 days in the positive group and 195 days in the negative group.

"This study shows that previous infection with SARS-CoV-2 induces
effective immunity to future infections in most individuals," the
authors wrote. "The importance of understanding the nature and rate
of SARS-CoV-2 reinfection to guide non-pharmaceutical interventions
and public health control measures is essential in this evolving
pandemic."

Natural immunity vs vaccine protection

In a commentary in the same journal, Florian Krammer, PhD, of the
Icahn School of Medicine at Mount Sinai in New York City, said that
although natural infection tends to induce lower and more variable
antibody concentrations than COVID-19 vaccines, "the findings of the
authors suggest that infection and the development of an antibody
response provides protection similar to or even better than currently
used SARS-CoV-2 vaccines.

He added, "The SIREN study adds to a growing number of studies, which
demonstrate that infection does protect against reinfection, and
probably in an antibody-dependent manner."

Krammer pointed out that the researchers didn't link quantitative
antibody measurements to protection against infection afforded by
natural infection versus vaccines, a topic that should be a priority
for future studies.

"Establishment of antibody titres as a correlate of protection and
defining a protective titre would be extremely important for public
health considerations and for patient management," he wrote. "A
correlate of protection and a protective threshold would also allow
for the development of additional SARS-CoV-2 vaccines based on small
immunogenicity-based phase 3 trials rather than large and costly
field efficacy trials, which are becoming exceedingly difficult to
perform."

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