 "Covid-19: How Omicron escapes from all four classes of antibodies")
The dozens of mutations found in the spike protein of the Omicron variant help it to evade all four of the classes of antibodies that can target the SARS-CoV-2 virus that causes Covid-19, suggests a study.
This includes antibodies generated by vaccinated or previously infected people, as well as most of the monoclonal antibody treatments that have been developed, said Ram Sasisekharan, Professor of Biological Engineering and Health Sciences and Technology (HST) at MIT.
According to Sasisekharan, the traditional approach of only examining changes in the virus' genetic sequence reduces the complexity of the spike protein's three-dimensional surface and doesn't describe the multidimensional complexity of the protein surfaces that antibodies are attempting to bind to.
"It is important to get a more comprehensive picture of the many mutations seen in Omicron, especially in the context of the spike protein, given that the spike protein is vital for the virus's function, and all the major vaccines are based on that protein, he said.
"There is a need for tools or approaches that can rapidly determine the impact of mutations in new virus variants of concern, especially for SARS-CoV-2," said Sasisekharan in the journal Cell Reports Medicine.
Even though Omicron is able to evade most antibodies to some degree, vaccines still offer protection, Sasisekharan said.
"What's good about vaccines is they don't just generate B cells, which produce the monoclonal [antibody] response, but also T cells, which provide additional forms of protection," he said.
The team focused their analysis on the receptor binding domain (RBD), which is the part of the spike protein targeted by antibodies.
Using their network modeling approach, the researchers studied how each of the mutations on the RBD changes the protein's shape and affects its interactions with four classes of human antibodies that target SARS-CoV-2. Class 1 and 2 antibodies target the RBD site that binds to the ACE2 receptor, while class 3 and 4 antibodies bind to other parts of the RBD.
The researchers compared the Omicron variant to the original SARS-CoV-2 virus, as well as the Beta and Delta variants. The Beta and Delta variants have mutations that help them evade class 1 and 2 antibodies, but not class 3 and 4. Omicron, on the other hand, has mutations that affect the binding of all four classes of antibodies.
The findings from the new study could help to identify regions of the RBD that could be targeted with future vaccines and therapeutic antibodies.
--IANS
rvt/shb/
(Only the headline and picture of this report may have been reworked by the Business Standard staff; the rest of the content is auto-generated from a syndicated feed.)
You’ve reached your limit of {{free_limit}} free articles this month.
Subscribe now for unlimited access.
Already subscribed? Log in
Subscribe to read the full story →
Smart Quarterly
₹900
3 Months
₹300/Month
Smart Essential
₹2,700
1 Year
₹225/Month
Super Saver
₹3,900
2 Years
₹162/Month
Renews automatically, cancel anytime
Here’s what’s included in our digital subscription plans
Exclusive premium stories online
Over 30 premium stories daily, handpicked by our editors
Complimentary Access to The New York Times
News, Games, Cooking, Audio, Wirecutter & The Athletic
Business Standard Epaper
Digital replica of our daily newspaper — with options to read, save, and share
Curated Newsletters
Insights on markets, finance, politics, tech, and more delivered to your inbox
Market Analysis & Investment Insights
In-depth market analysis & insights with access to The Smart Investor
Archives
Repository of articles and publications dating back to 1997
Ad-free Reading
Uninterrupted reading experience with no advertisements
Seamless Access Across All Devices
Access Business Standard across devices — mobile, tablet, or PC, via web or app