Role for Actin in the Polarized Release of Rotavirus

1 May 2007

journal article
research article
Published by American Society for Microbiology in Journal of Virology

Vol. 81 (9) , 4892-4894
https://doi.org/10.1128/jvi.02698-06

Abstract

Rotaviruses are characterized by polarized release from the apical side of infected enterocytes, and the rotavirus VP4 spike protein specifically binds to the actin network at the apical pole of differentiated enterocytic cells. To determine the functional consequences of this VP4-actin interaction, fluorescence recovery after photobleaching experiments were carried out to measure the diffusional mobility of VP4 associated with the microfilaments. Results show that VP4 binds to barbed ends of microfilaments by using actin treadmilling. Actin treadmilling inhibition results in the loss of rotavirus apical preferential release, suggesting a major role for actin in polarized rotavirus release.

Keywords

This publication has 9 references indexed in Scilit:

Rotavirus Spike Protein VP4 Binds to and Remodels Actin Bundles of the Epithelial Brush Border into Actin Bodies
Journal of Virology, 2006
Spike Protein VP4 Assembly with Maturing Rotavirus Requires a Postendoplasmic Reticulum Event in Polarized Caco-2 Cells
Journal of Virology, 2004
Introduction of C3 Exoenzyme into Cultured Endothelium by Lipofectamine
Analytical Biochemistry, 2000
The motor protein myosin-I produces its working stroke in two steps
Nature, 1999
Myosin II-independent F-actin flow contributes to cell locomotion in Dictyostelium
Journal of Cell Science, 1999
Rotavirus is released from the apical surface of cultured human intestinal cells through nonconventional vesicular transport that bypasses the Golgi apparatus
Journal of Virology, 1997
Jasplakinolide, a cytotoxic natural product, induces actin polymerization and competitively inhibits the binding of phalloidin to F-actin.
Journal of Biological Chemistry, 1994