RNASEK Is a V-ATPase-Associated Factor Required for Endocytosis and the Replication of Rhinovirus, Influenza A Virus, and Dengue Virus

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. [Display omitted] •Host proteins that modulate HRV replication were found by using MORR screens•RNASEK is needed for the replication of HRV, influenza A virus, and dengue virus•RNASEK localizes to the cell surface and endosomal pathway along with the V-ATPase•RNASEK is needed for endocytosis, and its loss produces enlarged clathrin-coated pits Perreira et al. screened multiple orthologous RNAi reagents and identified host proteins that modulate human rhinovirus (HRV) replication. They found that RNASEK is needed for the replication of HRV, influenza A virus, and dengue virus, associates with the vacuolar ATPase (V-ATPase), and is required for endocytosis.