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Oligomerization and cooperative RNA synthesis activity of hepatitis C virus RNA-dependent RNA polymerase
Authors:Wang Q May  Hockman Michelle A  Staschke Kirk  Johnson Robert B  Case Katharine A  Lu Jirong  Parsons Steve  Zhang Faming  Rathnachalam Radhakrishnan  Kirkegaard Karla  Colacino Joseph M
Affiliation:Lilly Research Laboratories, Eli Lilly and Company, Indianapolis, Indiana 46285. Department of Microbiology and Immunology, Stanford University School of Medicine, Stanford, California 94305.
Abstract:The NS5B RNA-dependent RNA polymerase encoded by hepatitis C virus (HCV) plays a key role in viral replication. Reported here is evidence that HCV NS5B polymerase acts as a functional oligomer. Oligomerization of HCV NS5B protein was demonstrated by gel filtration, chemical cross-linking, temperature sensitivity, and yeast cell two-hybrid analysis. Mutagenesis studies showed that the C-terminal hydrophobic region of the protein was not essential for its oligomerization. Importantly, HCV NS5B polymerase exhibited cooperative RNA synthesis activity with a dissociation constant, K(d), of approximately 22 nM, suggesting a role for the polymerase-polymerase interaction in the regulation of HCV replicase activity. Further functional evidence includes the inhibition of the wild-type NS5B polymerase activity by a catalytically inactive form of NS5B. Finally, the X-ray crystal structure of HCV NS5B polymerase was solved at 2.9 A. Two extensive interfaces have been identified from the packing of the NS5B molecules in the crystal lattice, suggesting a higher-order structure that is consistent with the biochemical data.
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