Global aspects of viral glycosylation

Bagdonaite, Ieva; Wandall, Hans H.

doi:10.1093/glycob/cwy021

Cited by 219 publications

(227 citation statements)

References 340 publications

(432 reference statements)

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“…Since O-glycans are involved in proteinprotein interactions [19], we suggest that O-glycans at Thr323 may play a role on binding to ACE2 and O-glycans at Thr678, Thr686 may responsible for furin protease enzyme binding. It has been known that O-glycans are responsible for the protein stability and creating mucin like domain as glycan shields involved in immunoevasion [21]. Based on this, we suggest that the O-glycosylation positions found may be involved in the stability of the S1 protein and immunoevasion of virus to the host cell.…”

Section: Resultsmentioning

confidence: 58%

Glycoinformatics approach for identifying target positions to inhibit initial binding of SARS-CoV-2 S1 protein to the host cell

Uslupehlivan

Şener

2020

Preprint

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COVID-19 outbreak is still threatening the public health. Therefore, in the middle of the pandemic, all kind of knowledge on SARS-CoV-2 may help us to find the solution.Determining the 3D structures of the proteins involved in host-pathogen interactions are of great importance in the fight against infection. Besides, post-translational modifications of the protein on 3D structure should be revealed in order to understand the protein function since these modifications are responsible for the host-pathogen interaction. Based on these, we predicted O-glycosylation and phosphorylation positions using full amino acid sequence of S1 protein. Candidate positions were further analyzed with enzyme binding activity, solvent accessibility, surface area parameters and the positions determined with high accuracy rate were used to design full 3D glycoprotein structure of the S1 protein using carbohydrate force field. In addition, the interaction between the C-type lectin CD209L and α -mannose residues was examined and carbohydrate recognition positions were predicted. We suggest these positions as a potential target for the inhibition of the initial binding of SARS-CoV-2 S1 protein to the host cell.

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Section: Resultsmentioning

confidence: 58%

Glycoinformatics approach for identifying target positions to inhibit initial binding of SARS-CoV-2 S1 protein to the host cell

Uslupehlivan

Şener

2020

Preprint

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“…O-glycans, which are involved in protein stability and function, have been observed on some viral proteins and have been suggested to play roles in the biological activity of viral proteins (Andersen, K.G., Rambaut, A., et al 2020, Bagdonaite, I. andWandall, H.H. 2018).…”

Section: Discussionmentioning

confidence: 99%

“…it is unclear what function these predicted O-linked glycans perform, they have been suggested to create a 'mucin-like domain' which could shield SARS-CoV-2 spike protein epitopes or key residues(Bagdonaite, I. and Wandall, H.H. 2018).…”

mentioning

confidence: 99%

Deducing the N- and O- glycosylation profile of the spike protein of novel coronavirus SARS-CoV-2

Shajahan

Supekar

Gleinich

et al. 2020

Preprint

125

194

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AbstractThe current emergence of the novel coronavirus pandemic caused by SARS-CoV-2 demands the development of new therapeutic strategies to prevent rapid progress of mortalities. The coronavirus spike (S) protein, which facilitates viral attachment, entry and membrane fusion is heavily glycosylated and plays a critical role in the elicitation of the host immune response. The spike protein is comprised of two protein subunits (S1 and S2), which together possess 22 potential N-glycosylation sites. Herein, we report the glycosylation mapping on spike protein subunits S1 and S2 expressed on human cells through high resolution mass spectrometry. We have characterized the quantitative N-glycosylation profile on spike protein and interestingly, observed unexpected O-glycosylation modifications on the receptor binding domain (RBD) of spike protein subunit S1. Even though O-glycosylation has been predicted on the spike protein of SARS-CoV-2, this is the first report of experimental data for both the site of O-glycosylation and identity of the O-glycans attached on the subunit S1. Our data on the N- and O-glycosylation is strengthened by extensive manual interpretation of each glycopeptide spectra in addition to using bioinformatics tools to confirm the complexity of glycosylation in the spike protein. The elucidation of the glycan repertoire on the spike protein provides insights into the viral binding studies and more importantly, propels research towards the development of a suitable vaccine candidate.

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“…Mass spectrometry in the analysis of viral surface protein glycosylation MS, the production and detection of ions separated according to their mass-to-charge (m/z) ratios, can provide structural identification of glycans, site-specific glycan characterization and be utilized to track changes in glycan composition, pattern, and site-occupancy [34][35][36]37 ]. Analysis of protein glycosylation by MS is typically achieved using two main approaches: glycans are released from the peptide backbone either enzymatically or chemically, or the glycoprotein can be subjected to protease digestion, producing a mixture of peptides and glycopeptides.…”

Section: Introductionmentioning

confidence: 99%

Glycosylation of viral surface proteins probed by mass spectrometry

Hargett

Renfrow

2019

Current Opinion in Virology

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Viral Fusion Protein Structures and N-glycosylation Sites (NGS). Viral fusion proteins are typically trimers of heterodimers with a globular head domain and a stalk/transmembrane domain. A GlucNAc 1 or GlucNac 2 are modeled at each NGS (Blue). (a) Lassa virus (LASV) glycoprotein (GP) complex contains 11 (NGS) with 7 in GP1 and 4 in GP2 (PDB: 5VK2) [27]. (b) Human immunodeficiency virus (HIV-1) Envelope (Env) GP contains around 29 NGS with 25 in gp120 the outer Env domain and 4 in gp41 the transmembrane domain (PDB: 5FYK) [49 ]. (c) Ebola virus (EBOV) GP has 17 NGS with 15 on GP1 and 2 on GP2 (PDB: 6G9B) [101]. (d) Coronavirus (CoV) spike GP has 26 NGS with 15 in subunit 1 and 11 in subunit 2 (PDB: 6BFU) [89]. (e) Influenza virus hemagglutinin is a homotrimer with 11 NGS (PDB: 4FNK) [92].

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Global aspects of viral glycosylation

Cited by 219 publications

References 340 publications

Glycoinformatics approach for identifying target positions to inhibit initial binding of SARS-CoV-2 S1 protein to the host cell

Glycoinformatics approach for identifying target positions to inhibit initial binding of SARS-CoV-2 S1 protein to the host cell

Deducing the N- and O- glycosylation profile of the spike protein of novel coronavirus SARS-CoV-2

Glycosylation of viral surface proteins probed by mass spectrometry

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