Phosphorylation of the hepatitis C virus (HCV) non-structure protein 5A (NS5A) plays critical roles in the viral life cycle. Based on genetic mutations followed by functional assays, numerous studies have pinpointed several serine residues that are critical for NS5A hyper-phosphorylation and for the viral life cycle. However, the hyper-phosphorylated NS5A species were not directly measured and whether phosphorylation among these sites is interdependent was unknown. Using three phosphorylation-specific antibodies, we profiled the NS5A species with single, double or triple phosphorylation at S232, S235 and/or S238. S232, S235 and S238 constitute respectively about 6, 92 and 46% of the hyper-phosphorylated NS5A. S232 phosphorylation occurs independently of S235 and S238 phosphorylation whereas S238 phosphorylation occurs only when S235 is phosphorylated. Our data suggest that S232 phosphorylation primes S235 by casein kinase 1  that requires priming phosphorylation at the -3 amino acid. S238 phosphorylation is perhaps a by-stander event dispensable for viral activity. S235 phosphorylation is the major and functional phosphorylation event that occurs at the time and intracellular location corresponding to viral replication. Mechanistically, S235-phosphoryalted NS5A probably facilitates clustering of the replication protein complexes in the ER lipid raft membranes for HCV replication.