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The Ebola Virus Matrix Protein Penetrates into the Plasma Membrane: A KEY STEP IN VIRAL PROTEIN 40 (VP40) OLIGOMERIZATION AND VIRAL EGRESS*
Authors:Emmanuel Adu-Gyamfi  Smita P. Soni  Yi Xue  Michelle A. Digman  Enrico Gratton  Robert V. Stahelin
Affiliation:From the §Department of Biochemistry and Molecular Biology, Indiana University School of Medicine, South Bend, Indiana 46617.;the Department of Chemistry and Biochemistry, the Eck Institute for Global Health, and the Center for Rare and Neglected Diseases, University of Notre Dame, South Bend, Indiana 46556, and ;the Department of Biomedical Engineering, University of California, Irvine, California 92697
Abstract:Ebola, a fatal virus in humans and non-human primates, has no Food and Drug Administration-approved vaccines or therapeutics. The virus from the Filoviridae family causes hemorrhagic fever, which rapidly progresses and in some cases has a fatality rate near 90%. The Ebola genome encodes seven genes, the most abundantly expressed of which is viral protein 40 (VP40), the major Ebola matrix protein that regulates assembly and egress of the virus. It is well established that VP40 assembles on the inner leaflet of the plasma membrane; however, the mechanistic details of plasma membrane association by VP40 are not well understood. In this study, we used an array of biophysical experiments and cellular assays along with mutagenesis of VP40 to investigate the role of membrane penetration in VP40 assembly and egress. Here we demonstrate that VP40 is able to penetrate specifically into the plasma membrane through an interface enriched in hydrophobic residues in its C-terminal domain. Mutagenesis of this hydrophobic region consisting of Leu213, Ile293, Leu295, and Val298 demonstrated that membrane penetration is critical to plasma membrane localization, VP40 oligomerization, and viral particle egress. Taken together, VP40 membrane penetration is an important step in the plasma membrane localization of the matrix protein where oligomerization and budding are defective in the absence of key hydrophobic interactions with the membrane.
Keywords:Lipid-binding Protein   Membrane Bilayer   Membrane Biophysics   Virus   Virus Assembly   Ebola   Lipid Binding   Membrane Penetration   Oligomerization   Plasma Membrane
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