The SARS-CoV-2 Omicron (B.1.1.529) variant possesses numerous spike (S) mutations particularly in the S receptor-binding domain (S-RBD) that significantly improve transmissibility and evasion of neutralizing antibodies. But exactly how the mutations in the Omicron variant enhance viral escape from immunological protection remains to be understood. The S-RBD remains the principal target for neutralizing antibodies and therapeutics, thus new structural insights into the Omicron S-RBD and characterization of the post-translational glycosylation changes can inform rational design of vaccines and therapeutics. Here we report the molecular variations and O-glycoform changes of the Omicron S-RBD variant as compared to wild-type (WA1/2020) and Delta (B.1.617.2) variants using high-resolution top-down mass spectrometry (MS). A novel O-glycosite (Thr376) unique to the Omicron variant is identified. Moreover, we have directly quantified the Core 1 and Core 2 O-glycan structures and characterized the O-glycoform structural heterogeneity of the three variants. Our findings reveal high resolution detail of Omicron O-glycoforms and their utilization to provide direct molecular evidence of proteoform alterations in the Omicron variant which could shed light on how this variant escapes immunological protection.
[doi:10.25345/C5SJ19V9T]
[dataset license: CC0 1.0 Universal (CC0 1.0)]
Keywords: O-Glycoform ; O-glycosylation ; Omicron ; COVID-19 ; Spike protein ; Regional-binding domain ; Top-down mass spectrometry
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Principal Investigators: (in alphabetical order) |
David S. Roberts, University of Wisconsin-Madison, USA Ying Ge, University of Wisconsin-Madison, United States of America |
| Submitting User: | dsroberts |
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