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Literature DB >> 25410852

Focal adhesion kinase is involved in rabies virus infection through its interaction with viral phosphoprotein P.

Baptiste Fouquet¹, Jovan Nikolic¹, Florence Larrous², Hervé Bourhy², Christoph Wirblich³, Cécile Lagaudrière-Gesbert⁴, Danielle Blondel⁴.

Abstract

UNLABELLED: The rabies virus (RABV) phosphoprotein P is a multifunctional protein: it plays an essential role in viral transcription and replication, and in addition, RABV P has been identified as an interferon antagonist. Here, a yeast two-hybrid screen revealed that RABV P interacts with the focal adhesion kinase (FAK). The binding involved the 106-to-131 domain, corresponding to the dimerization domain of P and the C-terminal domain of FAK containing the proline-rich domains PRR2 and PRR3. The P-FAK interaction was confirmed in infected cells by coimmunoprecipitation and colocalization of FAK with P in Negri bodies. By alanine scanning, we identified a single mutation in the P protein that abolishes this interaction. The mutant virus containing a substitution of Ala for Arg in position 109 in P (P.R109A), which did not interact with FAK, is affected at a posttranscriptional step involving protein synthesis and viral RNA replication. Furthermore, FAK depletion inhibited viral protein expression in infected cells. This provides the first evidence of an interaction of RABV with FAK that positively regulates infection. IMPORTANCE: Rabies virus exhibits a small genome that encodes a limited number of viral proteins. To maintain efficient virus replication, some of them are multifunctional, such as the phosphoprotein P. We and others have shown that P establishes complex networks of interactions with host cell components. These interactions have revealed much about the role of P and about host-pathogen interactions in infected cells. Here, we identified another cellular partner of P, the focal adhesion kinase (FAK). Our data shed light on the implication of FAK in RABV infection and provide evidence that P-FAK interaction has a proviral function.

Entities: Chemical Disease Gene Mutation Species

Mesh：

Substances：

Year: 2014 PMID： 25410852 PMCID： PMC4300764 DOI： 10.1128/JVI.02602-14

Source DB: PubMed Journal: J Virol ISSN： 0022-538X Impact factor: 5.103

46 in total

1. Functional interaction map of lyssavirus phosphoprotein: identification of the minimal transcription domains.

Authors: Y Jacob; E Real; N Tordo
Journal: J Virol Date: 2001-10 Impact factor: 5.103

2. Analysis of relative gene expression data using real-time quantitative PCR and the 2(-Delta Delta C(T)) Method.

Authors: K J Livak; T D Schmittgen
Journal: Methods Date: 2001-12 Impact factor: 3.608

3. Molecular basis for the interaction between rabies virus phosphoprotein P and the dynein light chain LC8: dissociation of dynein-binding properties and transcriptional functionality of P.

Authors: Nicolas Poisson; Eleonore Real; Yves Gaudin; Marie-Christine Vaney; Stephen King; Yves Jacob; Noël Tordo; Danielle Blondel
Journal: J Gen Virol Date: 2001-11 Impact factor: 3.891

Review 4. Focal adhesion kinase: the first ten years.

Authors: J Thomas Parsons
Journal: J Cell Sci Date: 2003-04-15 Impact factor: 5.285

5. Focal adhesion kinase as a marker of malignant phenotype in breast and cervical carcinomas.

Authors: Maja H Oktay; Kutluk Oktay; Diane Hamele-Bena; Arzu Buyuk; Leopold G Koss
Journal: Hum Pathol Date: 2003-03 Impact factor: 3.466

6. A novel expression cassette of lyssavirus shows that the distantly related Mokola virus can rescue a defective rabies virus genome.

Authors: Philippe Le Mercier; Yves Jacob; Kyle Tanner; Noël Tordo
Journal: J Virol Date: 2002-02 Impact factor: 5.103

7. Rabies virus P and small P products interact directly with PML and reorganize PML nuclear bodies.

Authors: Danielle Blondel; Tarick Regad; Nicolas Poisson; Benjamen Pavie; Francis Harper; Pier Paolo Pandolfi; Hugues De Thé; Mounira K Chelbi-Alix
Journal: Oncogene Date: 2002-11-14 Impact factor: 9.867

8. Sendai virus C proteins must interact directly with cellular components to interfere with interferon action.

Authors: D Garcin; J Curran; D Kolakofsky
Journal: J Virol Date: 2000-10 Impact factor: 5.103

9. Localization of focal adhesion kinase isoforms in cells of the central nervous system.

Authors: Andrea Contestabile; Dario Bonanomi; Ferran Burgaya; Jean Antoine Girault; Flavia Valtorta
Journal: Int J Dev Neurosci Date: 2003-04 Impact factor: 2.457

10. Herpes simplex virus type 2 glycoprotein H interacts with integrin αvβ3 to facilitate viral entry and calcium signaling in human genital tract epithelial cells.

Authors: Natalia Cheshenko; Janie B Trepanier; Pablo A González; Eliseo A Eugenin; William R Jacobs; Betsy C Herold
Journal: J Virol Date: 2014-06-18 Impact factor: 5.103

22 in total

Focal adhesion kinase is involved in rabies virus infection through its interaction with viral phosphoprotein P.

1. Functional interaction map of lyssavirus phosphoprotein: identification of the minimal transcription domains.

2. Analysis of relative gene expression data using real-time quantitative PCR and the 2(-Delta Delta C(T)) Method.

3. Molecular basis for the interaction between rabies virus phosphoprotein P and the dynein light chain LC8: dissociation of dynein-binding properties and transcriptional functionality of P.

Review 4. Focal adhesion kinase: the first ten years.

5. Focal adhesion kinase as a marker of malignant phenotype in breast and cervical carcinomas.

6. A novel expression cassette of lyssavirus shows that the distantly related Mokola virus can rescue a defective rabies virus genome.

7. Rabies virus P and small P products interact directly with PML and reorganize PML nuclear bodies.

8. Sendai virus C proteins must interact directly with cellular components to interfere with interferon action.

9. Localization of focal adhesion kinase isoforms in cells of the central nervous system.

10. Herpes simplex virus type 2 glycoprotein H interacts with integrin αvβ3 to facilitate viral entry and calcium signaling in human genital tract epithelial cells.

1. Vesicular Stomatitis Virus Phosphoprotein Dimerization Domain Is Dispensable for Virus Growth.

2. The LC8-RavP ensemble Structure Evinces A Role for LC8 in Regulating Lyssavirus Polymerase Functionality.

Review 3. Phase-Separated Subcellular Compartmentation and Related Human Diseases.

4. Rabies Virus Infection Induces the Formation of Stress Granules Closely Connected to the Viral Factories.

5. Negri bodies are viral factories with properties of liquid organelles.

6. Phenotypic Consequences In vivo and In vitro of Rearranging the P Gene of RABV HEP-Flury.

Review 7. The importance of immune evasion in the pathogenesis of rabies virus.

8. Identification and characterization of the role of c-terminal Src kinase in dengue virus replication.

9. Transcriptomics Sequencing Provides Insights into Understanding the Mechanism of Grass Carp Reovirus Infection.

Review 10. Rabies Infection: An Overview of Lyssavirus-Host Protein Interactions.