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Literature DB >> 23663837

The Ebola virus matrix protein deeply penetrates the plasma membrane: an important step in viral egress.

Smita P Soni¹, Emmanuel Adu-Gyamfi, Sylvia S Yong, Clara S Jee, Robert V Stahelin.

Abstract

Ebola virus, from the Filoviridae family has a high fatality rate in humans and nonhuman primates and to date, to the best of our knowledge, has no FDA approved vaccines or therapeutics. Viral protein 40 (VP40) is the major Ebola virus matrix protein that regulates assembly and egress of infectious Ebola virus particles. It is well established that VP40 assembles on the inner leaflet of the plasma membrane; however, the mechanistic details of VP40 membrane binding that are important for viral release remain to be elucidated. In this study, we used fluorescence quenching of a tryptophan on the membrane-binding interface with brominated lipids along with mutagenesis of VP40 to understand the depth of membrane penetration into lipid bilayers. Experimental results indicate that VP40 penetrates 8.1 Å into the hydrocarbon core of the plasma membrane bilayer. VP40 also induces substantial changes to membrane curvature as it tubulates liposomes and induces vesiculation into giant unilamellar vesicles, effects that are abrogated by hydrophobic mutations. This is a critical step in viral egress as cellular assays demonstrate that hydrophobic residues that penetrate deeply into the plasma membrane are essential for plasma membrane localization and virus-like particle formation and release from cells.

Entities: Chemical Species

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Year: 2013 PMID： 23663837 PMCID： PMC3647161 DOI： 10.1016/j.bpj.2013.03.021

Source DB: PubMed Journal: Biophys J ISSN： 0006-3495 Impact factor: 4.033

52 in total

1. VP40 octamers are essential for Ebola virus replication.

Authors: Thomas Hoenen; Viktor Volchkov; Larissa Kolesnikova; Eva Mittler; Joanna Timmins; Michelle Ottmann; Olivier Reynard; Stephan Becker; Winfried Weissenhorn
Journal: J Virol Date: 2005-02 Impact factor: 5.103

2. A reconstituted replication and transcription system for Ebola virus Reston and comparison with Ebola virus Zaire.

Authors: Yannik Boehmann; Sven Enterlein; Anke Randolf; Elke Mühlberger
Journal: Virology Date: 2005-02-05 Impact factor: 3.616

3. Membrane insertion of the FYVE domain is modulated by pH.

Authors: Ju He; Mohsin Vora; Rachel M Haney; Grigory S Filonov; Catherine A Musselman; Christopher G Burd; Andrei G Kutateladze; Vladislav V Verkhusha; Robert V Stahelin; Tatiana G Kutateladze
Journal: Proteins Date: 2009-09

4. Opposing mechanisms involving RNA and lipids regulate HIV-1 Gag membrane binding through the highly basic region of the matrix domain.

Authors: Vineela Chukkapalli; Seung J Oh; Akira Ono
Journal: Proc Natl Acad Sci U S A Date: 2010-01-04 Impact factor: 11.205

5. Bactericidal and membrane disruption activities of the eosinophil cationic protein are largely retained in an N-terminal fragment.

Authors: Marc Torrent; Beatriz G de la Torre; Victòria M Nogués; David Andreu; Ester Boix
Journal: Biochem J Date: 2009-07-15 Impact factor: 3.857

6. Interaction between the human immunodeficiency virus type 1 Gag matrix domain and phosphatidylinositol-(4,5)-bisphosphate is essential for efficient gag membrane binding.

Authors: Vineela Chukkapalli; Ian B Hogue; Vitaly Boyko; Wei-Shau Hu; Akira Ono
Journal: J Virol Date: 2007-12-19 Impact factor: 5.103

Review 7. No exit: targeting the budding process to inhibit filovirus replication.

Authors: Ronald N Harty
Journal: Antiviral Res Date: 2008-12-27 Impact factor: 5.970

8. Conserved motifs within Ebola and Marburg virus VP40 proteins are important for stability, localization, and subsequent budding of virus-like particles.

Authors: Yuliang Liu; Luis Cocka; Atsushi Okumura; Yong-An Zhang; J Oriol Sunyer; Ronald N Harty
Journal: J Virol Date: 2009-12-23 Impact factor: 5.103

9. Structural and membrane binding analysis of the Phox homology domain of Bem1p: basis of phosphatidylinositol 4-phosphate specificity.

Authors: Robert V Stahelin; Dimitrios Karathanassis; Diana Murray; Roger L Williams; Wonhwa Cho
Journal: J Biol Chem Date: 2007-06-20 Impact factor: 5.157

10. Vesicle formation by self-assembly of membrane-bound matrix proteins into a fluidlike budding domain.

Authors: Anna V Shnyrova; Juan Ayllon; Ilya I Mikhalyov; Enrique Villar; Joshua Zimmerberg; Vadim A Frolov
Journal: J Cell Biol Date: 2007-11-19 Impact factor: 10.539

28 in total

Review 1. Conformational plasticity of the Ebola virus matrix protein.

Authors: Jens Radzimanowski; Gregory Effantin; Winfried Weissenhorn
Journal: Protein Sci Date: 2014-09-04 Impact factor: 6.725

2. Solution Structure, Self-Assembly, and Membrane Interactions of the Matrix Protein from Newcastle Disease Virus at Neutral and Acidic pH.

Authors: E V Shtykova; M V Petoukhov; L A Dadinova; N V Fedorova; V Yu Tashkin; T A Timofeeva; A L Ksenofontov; N A Loshkarev; L A Baratova; C M Jeffries; D I Svergun; O V Batishchev
Journal: J Virol Date: 2019-03-05 Impact factor: 5.103

3. pH-Dependent Formation and Disintegration of the Influenza A Virus Protein Scaffold To Provide Tension for Membrane Fusion.

Authors: O V Batishchev; L A Shilova; M V Kachala; V Y Tashkin; V S Sokolov; N V Fedorova; L A Baratova; D G Knyazev; J Zimmerberg; Y A Chizmadzhev
Journal: J Virol Date: 2015-10-14 Impact factor: 5.103

The Ebola virus matrix protein deeply penetrates the plasma membrane: an important step in viral egress.

1. VP40 octamers are essential for Ebola virus replication.

2. A reconstituted replication and transcription system for Ebola virus Reston and comparison with Ebola virus Zaire.

3. Membrane insertion of the FYVE domain is modulated by pH.

4. Opposing mechanisms involving RNA and lipids regulate HIV-1 Gag membrane binding through the highly basic region of the matrix domain.

5. Bactericidal and membrane disruption activities of the eosinophil cationic protein are largely retained in an N-terminal fragment.

6. Interaction between the human immunodeficiency virus type 1 Gag matrix domain and phosphatidylinositol-(4,5)-bisphosphate is essential for efficient gag membrane binding.

Review 7. No exit: targeting the budding process to inhibit filovirus replication.

8. Conserved motifs within Ebola and Marburg virus VP40 proteins are important for stability, localization, and subsequent budding of virus-like particles.

9. Structural and membrane binding analysis of the Phox homology domain of Bem1p: basis of phosphatidylinositol 4-phosphate specificity.

10. Vesicle formation by self-assembly of membrane-bound matrix proteins into a fluidlike budding domain.

Review 1. Conformational plasticity of the Ebola virus matrix protein.

2. Solution Structure, Self-Assembly, and Membrane Interactions of the Matrix Protein from Newcastle Disease Virus at Neutral and Acidic pH.

3. pH-Dependent Formation and Disintegration of the Influenza A Virus Protein Scaffold To Provide Tension for Membrane Fusion.

4. Investigation of the Lipid Binding Properties of the Marburg Virus Matrix Protein VP40.

5. Host Cell Plasma Membrane Phosphatidylserine Regulates the Assembly and Budding of Ebola Virus.

6. The multifunctional Ebola virus VP40 matrix protein is a promising therapeutic target.

7. Could the Ebola virus matrix protein VP40 be a drug target?

8. The Ebola virus protein VP40 hexamer enhances the clustering of PI(4,5)P₂ lipids in the plasma membrane.

9. The Ebola virus matrix protein VP40 selectively induces vesiculation from phosphatidylserine-enriched membranes.

10. Monitoring peripheral protein oligomerization on biological membranes.