BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Hepatitis, Hypothalamus, DNA fingerprint, Fenofibrate, rs4950928, IGF1, Coagulation)
Bookmark Forward

Conserved arginine residues in the carboxyl terminus of the equine arteritis virus E protein may play a role in heparin binding but may not affect viral infectivity in equine endothelial cells.

Zhengchun Lu, Sanjay Sarkar, Jianqiang Zhang, Udeni B R Balasuriya

Archives of virology 2016 Apr


filter terms:
  • amino acid sequence (2)
  • antibodies (4)
  • basic amino acid (1)
  • bind (1)
  • blood vessels (1)
  • cell (2)
  • cellular (1)
  • clone (1)
  • E protein (5)
  • endothelial cells (4)
  • glycosaminoglycans (3)
  • heparin (13)
  • macrophages (1)
  • minor (1)
  • mutagenesis (2)
  • receptor (1)
  • sequence analysis (1)
  • tropism (1)
  • viral protein (1)
  • virus (12)
  • vitro (1)
    • Sizes of these terms reflect their relevance to your search.

    Equine arteritis virus (EAV), the causative agent of equine viral arteritis, has relatively broad cell tropism in vitro. In horses, EAV primarily replicates in macrophages and endothelial cells of small blood vessels. Until now, neither the cellular receptor(s) nor the mechanism(s) of virus attachment and entry have been determined for this virus. In this study, we investigated the effect of heparin on EAV infection in equine endothelial cells (EECs). Heparin, but not other glycosaminoglycans, could reduce EAV infection up to 93 %. Sequence analysis of the EAV E minor envelope protein revealed a conserved amino acid sequence (52 RSLVARCSRGARYR 65) at the carboxy terminus of the E protein, which was predicted to be the heparin-binding domain. The basic arginine (R) amino acid residues were subsequently mutated to glycine by site-directed mutagenesis of ORF2a in an E protein expression vector and an infectious cDNA clone of EAV. Two single mutations in E (R52G and R57G) did not affect the heparin-binding capability, whereas the E double mutation (R52,60G) completely eliminated the interaction between the E protein and heparin. Although the mutant R52,60G EAV did not bind heparin, the mutations did not completely abolish infectivity, indicating that heparin is not the only critical factor for EAV infection. This also suggested that other viral envelope protein(s) might be involved in attachment through heparin or other cell-surface molecules, and this warrants further investigation.

    Citation

    Zhengchun Lu, Sanjay Sarkar, Jianqiang Zhang, Udeni B R Balasuriya. Conserved arginine residues in the carboxyl terminus of the equine arteritis virus E protein may play a role in heparin binding but may not affect viral infectivity in equine endothelial cells. Archives of virology. 2016 Apr;161(4):873-86

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 26739582

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.