Interaction between viral proteins is necessary for viral replication and viral particle assembly. We used the yeast two-hybrid assay to identify interactions among all the mature proteins of the hepatitis C virus. The interaction between NS3 and NS3 was one of the strongest viral protein-protein interactions detected. The minimal region required for this interaction was mapped to a specific subdomain of 174 amino acids in the N terminus of the helicase region. Random mutations in the minimal region were generated by PCR, and mutants that failed to interact with a wild-type minimal fragment were isolated using the yeast two-hybrid assay as a screen. Three of these mutations resulted in a reduction or a loss of interaction between helicases. Analytical gel filtration showed that in the presence of an oligonucleotide, wild-type helicases form dimers whereas the mutants remain mostly monomeric. All three mutants were partially or almost inactive when assayed for helicase activity in vitro. Mixing a mutant helicase (Y267S) with wild-type helicase did not dramatically affect helicase activity. These data indicate that dimerization of the helicase is important for helicase activity. The mutations that reduce self-association of the helicase may define the key residues involved in NS3-NS3 dimerization.
Mutations that affect dimer formation and helicase activity of the hepatitis C virus helicase.
影响丙型肝炎病毒解旋酶二聚体形成和解旋酶活性的突变
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作者:Khu Y L, Koh E, Lim S P, Tan Y H, Brenner S, Lim S G, Hong W J, Goh P Y
| 期刊: | Journal of Virology | 影响因子: | 3.800 |
| 时间: | 2001 | 起止号: | 2001 Jan;75(1):205-14 |
| doi: | 10.1128/JVI.75.1.205-214.2001 | 研究方向: | 免疫/内分泌 |
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