Autoimmune-disease drugs may reduce vaccine response; antibody
treatments ineffective vs Brazil variant
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 [April 13, 2021]
By Nancy Lapid
(Reuters) -The following is a roundup of
some of the latest scientific studies on the novel coronavirus and
efforts to find treatments and vaccines for COVID-19, the illness caused
by the virus.
Autoimmune disease treatments may reduce vaccine responses
Immunosuppressive drugs for inflammatory diseases like rheumatoid
arthritis, multiple sclerosis, and ulcerative colitis can impair the
body's response to the COVID-19 vaccines from Pfizer/BioNTech and
Moderna, according to new data. In 133 fully vaccinated people with such
conditions, antibody levels and virus neutralization were about
three-fold lower than in a comparison group of vaccinated individuals
not taking those medicine, researchers reported on Friday on medRxiv
ahead of peer review. Most patients in the study "were able to mount
antibody responses in response to SARS-CoV-2 vaccination, which is
reassuring," said coauthor Alfred Kim from Washington University School
of Medicine in St. Louis. It is not clear yet whether reduced antibody
levels will result in decreased protection from infection or
hospitalization, Kim said. Particularly concerning, he said, is the
10-fold reduction in vaccine-induced antibody levels seen in patients
who routinely use steroids such as prednisone and methylprednisolone and
a 36-fold reduction seen with drugs that deplete B cells, including
Roche's Rituxan (rituximab) and Ocrevus (ocrelizumab). Reductions in
antibody levels were more modest with widely used rheumatoid arthritis
drugs in the class known as TNF inhibitors such as Abbvie's Humira (adalimumab)
and Amgen's Enbrel (etanercept); antimetabolites like methotrexate and
sulfasalazine; JAK inhibitors like Pfizer's Xeljanz (tofacitinib),
gut-specific agents such as Takeda Pharmaceutical Co's Entyvio (vedolizumab),
and IL-12/23 inhibitors including Johnson & Johnson's Stelara (ustekinumab).
Most antibody drugs ineffective against Brazil variant
The coronavirus variant first identified in Brazil, known as P.1, is
resistant to three of the four antibody therapies with emergency use
authorization in the United States, according to a laboratory study. In
test-tube experiments, researchers exposed the P.1 variant to various
monoclonal antibodies, including the four currently being used to treat
U.S. COVID-19 patients - imdevimab and casirivimab from Regneron
Pharmaceuticals, and bamlanivimab and etesevimab from Eli Lilly and Co.
Only imdevimab retained any potency, researchers found. The neutralizing
ability of the other three were "markedly or completely abolished,"
according to a peer reviewed report available on bioRxiv and
provisionally accepted by the journal Cell Host & Microbe. The
researchers also exposed P.1 to plasma from COVID-19 survivors and blood
from recipients of vaccines from Pfizer/BioNTech or Moderna. Compared to
their effects against the original version of the coronavirus, the
plasma and the vaccine-induced antibodies were less effective at
neutralizing P.1. In earlier studies, however, they were even less
effective against the B.1.351 variant first identified in South Africa.
This suggests that the Brazil variant might not pose as great a threat
of reinfection or decreased vaccine protection as the South Africa
variant, said coauthor David Ho from Columbia University. Real-world
evidence is needed to confirm the lab results, he said.
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The word "COVID-19" is reflected in a drop on a syringe needle in
this illustration taken November 9, 2020. REUTERS/Dado Ruvic/Illustration
South Africa variant can 'break through' Pfizer vaccine
The B.1.351 coronavirus variant discovered in South Africa can
"break through" Pfizer/BioNTech's COVID-19 vaccine protection to
some extent, Israeli researchers have found. They compared almost
400 people who had tested positive for COVID-19 after one or two
doses of the vaccine, against the same number of similar people with
COVID-19 who were unvaccinated. The prevalence of the variant in
Israel is low, and overall, it accounted for about 1% of all the
COVID-19 cases in the study. But among those who received both doses
of the vaccine, a larger proportion of COVID-19 infections were
caused by B.1.351. The "disproportionately higher rate" of the South
African variant in the fully vaccinated group (5.4%) compared to the
rate in the unvaccinated group (0.7%) "means that the South African
variant is able, to some extent, to break through the vaccine's
protection," said Tel Aviv University's Adi Stern. In a report
posted on Friday on medRxiv ahead of peer review, Stern's team said
the research was not intended to deduce overall vaccine
effectiveness against any variant, since it only looked at people
who had already tested positive for COVID-19, not at overall
infection rates in the community.
(Reporting by Nancy Lapid and Maayan Lubell; Editing by Bill
Berkrot)
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