Unknown

Dataset Information

0

Antigenic modules in the N-terminal S1 region of the transmissible gastroenteritis virus spike protein.

ABSTRACT: The N-terminal S1 region of the transmissible gastroenteritis virus (TGEV) spike (S) glycoprotein contains four antigenic sites (C, B, D and A, from the N- to the C-terminal end) and is engaged in host-cell receptor recognition. The most N-terminal portion of the S1 region, which comprises antigenic sites C and B, is needed for the enteric tropism of TGEV, whereas the major antigenic site A at the C-terminal moiety is required for both respiratory and enteric cell tropism, and is engaged in recognition of the aminopeptidase N (APN) receptor. This study determined the kinetics for binding of a soluble S1 protein to the APN protein. Moreover, the S1 region of the TGEV S protein was dissected, with the aim of identifying discrete modules displaying unique antigenic sites and receptor-binding functions. Following protease treatments and mammalian cell expression methods, four modules or domains (D1-D4) were defined at the S1 region. Papain treatment identified an N-terminal domain (D1) resistant to proteolysis, whereas receptor binding defined a soluble and functional APN receptor-binding domain (D3). This domain was recognized by neutralizing antibodies belonging to the antigenic site A and therefore could be used as an immunogen for the prevention of viral infection. The organization of the four modules in the S1 region of the TGEV S glycoprotein is discussed.

SUBMITTER: Reguera J 

PROVIDER: S-EPMC3139418 | biostudies-literature | 2011 May

REPOSITORIES: biostudies-literature

Json Xml
altmetric image

Publications

Antigenic modules in the N-terminal S1 region of the transmissible gastroenteritis virus spike protein.

Reguera Juan J   Ordoño Desiderio D   Santiago César C   Enjuanes Luis L   Casasnovas José M JM  

The Journal of general virology 20110112 Pt 5

The N-terminal S1 region of the transmissible gastroenteritis virus (TGEV) spike (S) glycoprotein contains four antigenic sites (C, B, D and A, from the N- to the C-terminal end) and is engaged in host-cell receptor recognition. The most N-terminal portion of the S1 region, which comprises antigenic sites C and B, is needed for the enteric tropism of TGEV, whereas the major antigenic site A at the C-terminal moiety is required for both respiratory and enteric cell tropism, and is engaged in reco  ...[more]

Similar Datasets

Unknown Sialic acid binding properties of soluble coronavirus spike (S1) proteins: differences between infectious bronchitis virus and transmissible gastroenteritis virus.
| S-EPMC3761233 | biostudies-literature
Unknown The N-Terminal Domain of Spike Protein Is Not the Enteric Tropism Determinant for Transmissible Gastroenteritis Virus in Piglets.
| S-EPMC6520731 | biostudies-literature
Unknown Characterization and utility of monoclonal antibodies against spike protein of transmissible gastroenteritis virus.
| S-EPMC7197895 | biostudies-literature
Unknown Antigenic relationships among porcine epidemic diarrhea virus and transmissible gastroenteritis virus strains.
| S-EPMC4337547 | biostudies-literature
Genomics Transmissible gastroenteritis virus
| PRJNA852690 | ENA
Unknown Bacterial expression of antigenic sites A and D in the spike protein of transmissible gastroenteritis virus and evaluation of their inhibitory effects on viral infection.
| S-EPMC7089297 | biostudies-literature
Unknown Minimum Determinants of Transmissible Gastroenteritis Virus Enteric Tropism Are Located in the N-Terminus of Spike Protein.
| S-EPMC7168613 | biostudies-literature
Unknown Immune responses induced by recombinant Lactobacillus plantarum expressing the spike protein derived from transmissible gastroenteritis virus in piglets.
| S-EPMC7080080 | biostudies-literature
Genomics The porcine microRNA transcriptome response to transmissible gastroenteritis virus infection
2015-01-08 | GSE64737 | GEO
Unknown UBXN1 interacts with the S1 protein of transmissible gastroenteritis coronavirus and plays a role in viral replication.
| S-EPMC6487014 | biostudies-literature