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Cleavage targets and the D-arginine-based inhibitors of the West Nile virus NS3 processing proteinase

  • Sergey A. Shiryaev
  • , Boris I. Ratnikov
  • , Alexei V. Chekanov
  • , Sergey Sikora
  • , Dmitri V. Rozanov
  • , Adam Godzik
  • , Jun Wang
  • , Jeffrey W. Smith
  • , Ziwei Huang
  • , Iris Lindberg
  • , Melanie A. Samuel
  • , Michael S. Diamond
  • , Alex Y. Strongin

Research output: Contribution to journalArticlepeer-review

Abstract

Mosquito-borne WNV (West Nile virus) is an emerging global threat. The NS3 proteinase, which is essential for the proteolytic processing of the viral polyprotein precursor, is a promising drug target. We have isolated and biochemically characterized the recombinant, highly active NS3 proteinase. We have determined that the NS3 proteinase functions in a manner that is distantly similar to furin in cleaving the peptide and protein substrates. We determined that aprotinin and D-arginine-based 9-12-mer peptides are potent inhibitors of WNV NS3 with Ki values of 26 nM and 1 nM respectively. Consistent with the essential role of NS3 activity in the life cycle of WNV and with the sensitivity of NS3 activity to the D-arginine-based peptides, we showed that nona-D-Arg-NH2 reduced WNV infection in primary neurons. We have also shown that myelin basic protein, a deficiency of which is linked to neurological abnormalities of the brain, is sensitive to NS3 proteolysis in vitro and therefore this protein represents a convenient test substrate for the studies of NS3. A three-dimensional model of WNV NS3 that we created may provide a structural guidance and a rationale for the subsequent design of fine-tuned inhibitors. Overall, our findings represent a foundation for in-depth mechanistic and structural studies as well as for the design of novel and efficient inhibitors of WNV NS3.

Original languageEnglish
Pages (from-to)503-511
Number of pages9
JournalBiochemical Journal
Volume393
Issue number2
DOIs
StatePublished - Jan 15 2006

Keywords

  • Dengue virus
  • Flavivirus
  • Furin
  • Peptide inhibitor
  • Proteinase
  • West Nile virus

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