| Title | RNASEK Is a V-ATPase-Associated Factor Required for Endocytosis and the Replication of Rhinovirus, Influenza A Virus, and Dengue Virus. | ||
| Author | Perreira, Jill M; Aker, Aaron M; Savidis, George; Chin, Christopher R; McDougall, William M; Portmann, Jocelyn M; Meraner, Paul; Smith, Miles C; Rahman, Motiur; Baker, Richard E; Gauthier, Annick; Franti, Michael; Brass, Abraham L | ||
| Journal | Cell Rep | Publication Year/Month | 2015-Aug |
| PMID | 26212330 | PMCID | -N/A- |
| Affiliation + expend | 1.Microbiology and Physiological Systems Department, University of Massachusetts Medical School, University of Massachusetts, Worcester, MA 01655, USA. | ||
Human rhinovirus (HRV) causes upper respiratory infections and asthma exacerbations. We screened multiple orthologous RNAi reagents and identified host proteins that modulate HRV replication. Here, we show that RNASEK, a transmembrane protein, was needed for the replication of HRV, influenza A virus, and dengue virus. RNASEK localizes to the cell surface and endosomal pathway and closely associates with the vacuolar ATPase (V-ATPase) proton pump. RNASEK is required for endocytosis, and its depletion produces enlarged clathrin-coated pits (CCPs) at the cell surface. These enlarged CCPs contain endocytic cargo and are bound by the scissioning GTPase, DNM2. Loss of RNASEK alters the localization of multiple V-ATPase subunits and lowers the levels of the ATP6AP1 subunit. Together, our results show that RNASEK closely associates with the V-ATPase and is required for its function; its loss prevents the early events of endocytosis and the replication of multiple pathogenic viruses.