Nonstructural protein 5B (NS5B) is essential for Hepatitis C Virus (HCV) replication as it carries the viral RNA-dependent RNA polymerase (RdRp) enzymatic activity. HCV replication occurs in a membrane-associated multiprotein complex in which HCV NS5A and host Cyclophilin A (CypA) have been shown to be present together with the viral polymerase. We used NMR spectroscopy to perform a per residue level characterization of the molecular interactions between the unfolded domains 2 and 3 of NS5A (NS5A-D2 and NS5A-D3), CypA and NS5B(Δ21). We show that three regions of NS5A-D2 (residues 250-262 (region A), 274-287 (region B) and 306-333 (region C)) interact with NS5B(Δ21) whereas NS5A-D3 does not. We show that both NS5B(Δ21) and CypA share a common binding site on NS5A, which contains residues P306 to E323. No direct molecular interaction has been detected by NMR spectroscopy between HCV NS5B(Δ21) and host CypA. We show that Cyclosporine A (CsA) added to a sample containing NS5B(Δ21), NS5A-D2 and CypA specifically inhibits the interaction between CypA and NS5A-D2 without altering the one between NS5A-D2 and NS5B(Δ21). A high quality heteronuclear NMR spectrum of HCV NS5B(Δ21) has been obtained and was used to characterize the binding site into the polymerase of NS5A-D2. Moreover these data highlight the potential of using NMR of NS5B(Δ21) as a powerful tool to characterize, in solution, the interactions of the HCV polymerase with all kind of molecules (proteins, inhibitors, RNA). This work brings new insights into the comprehension of the molecular interplay between NS5B, NS5A and CypA, three essentials proteins for HCV replication.