Phosphorylation at serine 235 of the hepatitis C virus (HCV) non-structural protein 5A (NS5A) is a critical post-translational modification required for viral replication. Because of virological and medical interests, it is necessary to identify the kinases responsible for NS5A S235 phosphorylation. Using HEK293T cells as a platform, we found both calmodulin-dependent kinase II (CaMKII) and casein kinase I α (CKIα) inhibitor reduced NS5A S235 phosphorylation without cytotoxicity. However, only shRNA-mediated CKIα knockdown reduced S235 phosphorylation and HCV RNA levels in the HCV-infected Huh7.5.1 cells, indicating a critical role CKIα-mediated NS5A S235 phosphorylation in HCV replication. HCV replication often requires host factors such as the vesicle-associated membrane protein-associated protein A (hVAP-A) that forms clusters in the HCV-infected cells. Upon CKIα knockdown, the hVAP-A clusters dispersed throughout the cytosol. The above data suggest that CKIα-mediated NS5A S235 phosphorylation facilitates HCV replication complex formation in the infected cells. We are currently using LC-MS/MS based protein mass spectrometry to profile the host protein factors that interact with S235D vs. S235A NS5A. Our findings will potentially provide a complete protein repertoire that participates in NS5A S235 phosphorylation-mediated HCV replication.