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| Hauptseite > Publikationsdatenbank > 1H, 13C, and 15Nresonance assignment of a 179 residue fragment of hepatitis C virus non-structural protein 5A |
| Hauptseite > Publikationsdatenbank > 1H, 13C, and 15Nresonance assignment of a 179 residue fragment of hepatitis C virus non-structural protein 5A |
| Journal Article | PreJuSER-16572 |
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2011
Springer Netherlands
Dordrecht [u.a.]
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Please use a persistent id in citations: doi:10.1007/s12104-011-9309-2
Abstract: Non-structural protein 5A (NS5A) plays an important role in the life cycle of hepatitis C virus. This proline-rich phosphoprotein is organized into three domains. Besides its role in virus replication and virus assembly, NS5A is involved in a variety of cellular regulation processes. Recent studies on domain 2 and 3 revealed that both belong to the class of intrinsically disordered proteins as they adopt a natively unfolded state. In particular, domain 2 together with its vicinal regions is responsible for NS5A's multiple interactions with other proteins necessary for virus persistence. The low chemical shift dispersion observed for instrinsically disordered proteins presents a challenge for NMR spectroscopy. Here we report sequential resonance assignment of a 179-residue fragment of NS5A, comprising the entire domain 2, using a set of sensitivity and resolution optimized 3D correlation experiments, as well as amino-acid-type editing in (1)H-(15)N correlation spectra. Our assignment reveals the presence of several segments with high propensity to form α-helical structure that may be of importance to the function of this protein fragment as a versatile interaction platform.
Keyword(s): Binding Sites (MeSH) ; Hepacivirus: chemistry (MeSH) ; Isotopes: chemistry (MeSH) ; Nuclear Magnetic Resonance, Biomolecular (MeSH) ; Protein Conformation (MeSH) ; Protein Structure, Tertiary (MeSH) ; Recombinant Proteins: chemistry (MeSH) ; Viral Nonstructural Proteins: chemistry (MeSH) ; Isotopes ; NS-5 protein, hepatitis C virus ; Recombinant Proteins ; Viral Nonstructural Proteins ; J ; HCV (auto) ; NS5A (auto) ; Domain 2 (auto) ; Heteronuclear NMR (auto) ; Resonance assignment (auto) ; Intrinsically disordered proteins (auto)
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