The hepatitis C virus non-structural NS5A protein inhibits activating protein-1 function by perturbing ras-ERK pathway signaling
The hepatitis C virus non-structural NS5A protein inhibits activating protein-1 function by perturbing ras-ERK pathway signaling
The hepatitis C virus nonstructural 5A (NS5A) protein is a pleiotropic phosphoprotein that has been shown to associate with a wide variety of cellular signaling proteins. Of particular interest is the observation that a highly conserved C-terminal Class II polyproline motif within NS5A mediated association with the Src homology 3 domains of members of the Src family of tyrosine kinases and the mitogenic adaptor protein Grb2 (A. Macdonald, K. Crowder, A. Street, C. McCormick, and M. Harris, submitted for publication). In this study, we analyzed the consequences of NS5A expression on mitogenic signaling pathways within a variety of cell lines. Utilizing a transient luciferase reporter system, we observed that NS5A inhibited the activity of the mitogenic and stress-activated transcription factor activating protein-1 (AP1). This inhibition was dependent upon a Class II polyproline motif within NS5A. Using a combination of dominant active and negative mutants of components of the MAPK signaling pathways, selective inhibitors, together with immunoblotting with phospho-specific and phosphorylation-independent antibodies, we determined the signaling pathways targeted by NS5A to inhibit AP1. These studies demonstrated that in both stable NS5A-expressing cells and Huh-7-derived cells harboring subgenomic hepatitis C virus (HCV) replicons, this inhibition was mediated through the ERK signaling pathway. Importantly, a comparable inhibition of AP1 reporter activity was observed in hepatocyte-derived cell lines transduced with a baculovirus vector driving expression of full-length HCV polyprotein. In conclusion, these data strongly suggest a role for the NS5A protein in the perturbation of mitogenic signaling pathways in HCV-infected hepatocytes.
17775-17784
MacDonald, A.
bd82e461-4bdf-4b90-a773-4b512cd027ac
Crowder, K.
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Street, A.
006fad38-42eb-4176-807b-5eff687f0472
McCormick, C.
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Saksela, K.
26f5c76e-808e-48de-ab74-f6683c796981
Harris, M.
b0e2d8cb-44f8-47a5-8e1b-6ca9c04fe776
16 May 2003
MacDonald, A.
bd82e461-4bdf-4b90-a773-4b512cd027ac
Crowder, K.
d2ba0f96-8890-48cf-87a3-a9114eae9ced
Street, A.
006fad38-42eb-4176-807b-5eff687f0472
McCormick, C.
0fce14bf-2f67-4d08-991f-114dd1e7f0bd
Saksela, K.
26f5c76e-808e-48de-ab74-f6683c796981
Harris, M.
b0e2d8cb-44f8-47a5-8e1b-6ca9c04fe776
MacDonald, A., Crowder, K., Street, A., McCormick, C., Saksela, K. and Harris, M.
(2003)
The hepatitis C virus non-structural NS5A protein inhibits activating protein-1 function by perturbing ras-ERK pathway signaling.
The Journal of Biological Chemistry, 278 (20), .
(doi:10.1074/jbc.M210900200).
Abstract
The hepatitis C virus nonstructural 5A (NS5A) protein is a pleiotropic phosphoprotein that has been shown to associate with a wide variety of cellular signaling proteins. Of particular interest is the observation that a highly conserved C-terminal Class II polyproline motif within NS5A mediated association with the Src homology 3 domains of members of the Src family of tyrosine kinases and the mitogenic adaptor protein Grb2 (A. Macdonald, K. Crowder, A. Street, C. McCormick, and M. Harris, submitted for publication). In this study, we analyzed the consequences of NS5A expression on mitogenic signaling pathways within a variety of cell lines. Utilizing a transient luciferase reporter system, we observed that NS5A inhibited the activity of the mitogenic and stress-activated transcription factor activating protein-1 (AP1). This inhibition was dependent upon a Class II polyproline motif within NS5A. Using a combination of dominant active and negative mutants of components of the MAPK signaling pathways, selective inhibitors, together with immunoblotting with phospho-specific and phosphorylation-independent antibodies, we determined the signaling pathways targeted by NS5A to inhibit AP1. These studies demonstrated that in both stable NS5A-expressing cells and Huh-7-derived cells harboring subgenomic hepatitis C virus (HCV) replicons, this inhibition was mediated through the ERK signaling pathway. Importantly, a comparable inhibition of AP1 reporter activity was observed in hepatocyte-derived cell lines transduced with a baculovirus vector driving expression of full-length HCV polyprotein. In conclusion, these data strongly suggest a role for the NS5A protein in the perturbation of mitogenic signaling pathways in HCV-infected hepatocytes.
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Published date: 16 May 2003
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Local EPrints ID: 27243
URI: http://eprints.soton.ac.uk/id/eprint/27243
ISSN: 0021-9258
PURE UUID: 6d7952e1-9f6d-4cfe-b533-d1465211b44a
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Date deposited: 27 Apr 2006
Last modified: 16 Mar 2024 03:47
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Author:
A. MacDonald
Author:
K. Crowder
Author:
A. Street
Author:
K. Saksela
Author:
M. Harris
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