A Fusion-Inhibiting Peptide against Rift Valley Fever Virus Inhibits Multiple, Diverse Viruses

A Fusion-Inhibiting Peptide against Rift Valley Fever Virus Inhibits Multiple, Diverse Viruses

For enveloped viruses, fusion of the viral envelope with a cellular membrane is critical for a productive infection to occur. This fusion process is mediated by at least three classes of fusion proteins (Class I, II, and III) based on the protein sequence and structure. For Rift Valley fever virus (...

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Bibliographische Detailangaben
Hauptverfasser: Koehler, Jeffrey W, Smith, Jeffrey M, Ripoll, Daniel R, Spik, Kristin W, Taylor, Shannon L, Badger, Catherine V, Grant, Rebecca J, Ogg, Monica M, Wallqvist, Anders, Guttieri, Mary C
Format: Report
Sprache:eng
Schlagworte:
ASSAYING
Biochemistry
Biology
CELLS(BIOLOGY)
CELLULAR MEMBRANES
CULTURES(BIOLOGY)
DENGUE VIRUS
FUSION-INHIBITING PEPTIDES
GLYCOPROTEINS
INHIBITION
MEMBRANES(BIOLOGY)
Microbiology
PEPTIDES
RIBONUCLEIC ACIDS
RIFT VALLEY FEVER VIRUS
RNA VIRUSES
RNA(RIBONUCLEIC ACIDS)
RVFV(RIFT VALLEY FEVER VIRUS)
VIRAL ENVELOPES
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Zusammenfassung:For enveloped viruses, fusion of the viral envelope with a cellular membrane is critical for a productive infection to occur. This fusion process is mediated by at least three classes of fusion proteins (Class I, II, and III) based on the protein sequence and structure. For Rift Valley fever virus (RVFV), the glycoprotein Gc (Class II fusion protein) mediates this fusion event following entry into the endocytic pathway, allowing the viral genome access to the cell cytoplasm. Here, we show that peptides analogous to the RVFV Gc stem region inhibited RVFV infectivity in cell culture by inhibiting the fusion process. Further, we show that infectivity can be inhibited for diverse, unrelated RNA viruses that have Class I (Ebola virus), Class II (Andes virus), or Class III (vesicular stomatitis virus) fusion proteins using this single peptide. Our findings are consistent with an inhibition mechanism similar to that proposed for stem peptide fusion inhibitors of dengue virus in which the RVFV inhibitory peptide first binds to both the virion and cell membranes, allowing it to traffic with the virus into the endocytic pathway. Upon acidification and rearrangement of Gc, the peptide is then able to specifically bind to Gc and prevent fusion of the viral and endocytic membranes, thus inhibiting viral infection. These results could provide novel insights into conserved features among the three classes of viral fusion proteins and offer direction for the future development of broadly active fusion inhibitors. Prepared in collaboration with the DoD Biotechnology High Performance Computing Software Applications Institute, Telemedicine and Advanced Technology Research Center, United States Army Medical Research and Materiel Command, Fort Detrick, MD. Prepared in cooperation with the Department ofMicrobiology and Immunology, Tulane University, New Orleans, LA. Published in PLOS Neglected Tropical Diseases, v7 n9 article ID e2430, 12 Sep 2013. Sponsored in part by the Defense High-Performance Computing Modernization Program, Lorton, VA.