Abstract
Hepatitis C virus (HCV) is an important cause of chronic liver disease, but the molecular mechanisms of viral pathogenesis remain to be established. The HCV non-structural protein NS3 complexes with NS4A and has three enzymatic activities: a proteinase and a helicase/NTPase. Recently, catalytically inactive NS3 fragments containing an arginine-rich motif have been reported to interact with, and inhibit, the catalytic subunit of cAMP-dependent protein kinase (PKA C-subunit). Here we demonstrate that full-length, catalytically active NS3/4A, purified from recombinant baculovirus-infected insect cells, is also able to inhibit PKA C-subunitin vitro. This inhibition was abrogated by mutation of either the arginine-rich motif or the conserved helicase motif II, both of which also abolished NTPase activity. As PKA C-subunit inhibition was also enhanced by poly(U) (an activator of NS3 NTPase activity), we hypothesized that PKA C-subunit inhibition could be due to NS3/4A-mediated ATP hydrolysis. This was confirmed by experiments in which a constant ATP concentration was maintained by addition of an ATP regeneration system – under these conditions PKA C-subunit inhibition was not observed. Interestingly, the mutations also abrogated the ability of wild-type NS3/4A to inhibit the PKA-regulated transcription factor CREB in transiently transfected hepatoma cells. Our data are thus not consistent with the previously proposed model in which the arginine-rich motif of NS3 was suggested to act as a pseudosubstrate inhibitor of PKA C-subunit. However,in vivoeffects of NS3/4A suggest that ATPase activity may play a role in viral pathology in the infected liver.
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Dates
Type | When |
---|---|
Created | 10 years ago (Aug. 26, 2015, 11:45 a.m.) |
Deposited | 3 years, 3 months ago (May 20, 2022, 7:30 p.m.) |
Indexed | 2 months ago (July 2, 2025, 2:15 p.m.) |
Issued | 24 years, 2 months ago (July 1, 2001) |
Published | 24 years, 2 months ago (July 1, 2001) |
Published Print | 24 years, 2 months ago (July 1, 2001) |
@article{Aoubala_2001, title={The inhibition of cAMP-dependent protein kinase by full-length hepatitis C virus NS3/4A complex is due to ATP hydrolysis}, volume={82}, ISSN={1465-2099}, url={http://dx.doi.org/10.1099/0022-1317-82-7-1637}, DOI={10.1099/0022-1317-82-7-1637}, number={7}, journal={Journal of General Virology}, publisher={Microbiology Society}, author={Aoubala, Mustapha and Holt, John and Clegg, Roger A. and Rowlands, David J. and Harris, Mark}, year={2001}, month=jul, pages={1637–1646} }