Read Online Crystal structure of bovine coronavirus spike protein lectin domain. - G Peng Affiliation: Department of Pharmacology, University of Minnesota Medical School, Minneapolis, Minnesota 55455, USA.; L Xu; YL Lin; L Chen; JR Pasquarella; All authors file in PDF
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Crystal structure of bovine coronavirus spike protein lectin
Crystal structure of bovine coronavirus spike protein lectin domain.
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Author summary a novel coronavirus emerged in 2003 and was identified as the etiological agent of the deadly disease called severe acute respiratory syndrome. This coronavirus replicates and transcribes its giant genome using sixteen non-structural proteins (nsp1-16). Viral rnas are capped to ensure stability, efficient translation, and evading the innate immunity system of the host cell.
Crystal structure of bovine coronavirus spike protein lectin domain. Mechanisms of host receptor adaptation by severe acute respiratory syndrome coronavirus.
Here we report the discovery of a highly conserved region based on four crystal structures and one homology model of m pro representing all three genetic clusters of the genus coronavirus, and a uniform inhibition mechanism revealed from the structures of m pro-inhibitor complexes from sars-cov and tgev.
Sugars serve as receptors or coreceptors for tgev from group 1, bovine coronavirus (bcov) and human coronavirus oc43 (hcov-oc43) from group 2a, and avian infectious bronchitis virus (ibv) from group 3 (8 –14). Receptor is unknown for some coronaviruses such as group 2a human coronavirus hku1 (hcov-hku1).
Jan 7, 2013 three bovine nasal samples infected with bovine coronavirus were used to ( 2011) crystal structure of mouse coronavirus receptor-binding.
Infectious bronchitis virus: crystal structure of its in structural terms, coronavirus virions are roughly and bovine coronavirus (bcv) (cologna and hogue.
Sugar-binding assays reveal that galectin-like ntds of some coronaviruses such as human coronavirus oc43 and bovine coronavirus bind sugars.
Although bovine coronavirus (bcov) strains are frequently circulating in cattle farms worldwide structural similarity to the crystal structure of murine hepatitis.
Yaoqing chen,a crystal structure of bovine coronavirus spike protein lectin domain.
Fingerprint dive into the research topics of 'crystal structure of bovine coronavirus spike protein lectin domain'.
Background bovine coronavirus (bcov) is a widely distributed pathogen, causing disease and economic losses in the cattle industry worldwide. Prevention of virus spread is impeded by a lack of basic knowledge concerning viral shedding and transmission potential in individual animals. The aims of the study were to investigate the duration and quantity of bcov shedding in feces and nasal.
Dec 28, 2020 coronaviruses (covs) comprise a large group of positive stranded rna crystal structure of bovine coronavirus spike protein lectin domain.
Mar 23, 2021 thus, the antigenic recognition of some highly conserved structures of crystal structure of bovine coronavirus spike protein lectin domain.
Jan 12, 2021 these images – produced as x-ray beams bounce off atoms in the crystals and pass through gaps in the lattice, generating a pattern of spots.
Crystal structure of bovine coronavirus spike protein lectin domain the spike protein n-terminal domains (ntds) of bovine coronavirus (bcov) and mouse hepatitis coronavirus (mhv) recognize sugar and protein receptors, respectively, despite their significant sequence homology.
The entry of the sars coronavirus (scv) into cells is initiated by binding of its spike envelope glycoprotein (s) to a receptor, ace2. We and others identified the receptor-binding domain (rbd) by using s fragments of various lengths but all including the amino acid residue 318 and two other potential glycosylation sites. To further characterize the role of glycosylation and identify residues.
Aug 25, 2016 the available crystal structures of s1 domains and s2 hrs are (b) structure of bovine coronavirus (bcov) s1-ntd (pdb id: 4h14) (43).
Substance record sid 104038406 for 3,5,7,3',4'-pentahydroxyflavone submitted by ncbi structure.
1 kda transmissible gastroenteritis (corona)virus m pro is reported. 96 å resolution and revealed three dimers in the asymmetric unit. The mutual arrangement of the protomers in each of the dimers suggests that m pro self‐processing occurs in trans.
Background: coronavirus spike protein n-terminal domains (ntds) bind sugar or protein receptors. Results: we determined crystal structure of bovine coronavirus ntd and located its sugar-binding site using mutagenesis. Conclusion: bovine coronavirus ntd shares structural folds and sugar-binding sites with human galectins and has subtle yet functionally important differences from protein-binding.
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