% IMPORTANT: The following is UTF-8 encoded. This means that in the presence
% of non-ASCII characters, it will not work with BibTeX 0.99 or older.
% Instead, you should use an up-to-date BibTeX implementation like “bibtex8” or
% “biber”.
@ARTICLE{Slyom:276570,
author = {Sólyom, Zsófia and Ma, Peixiang and Schwarten, Melanie
and Bosco, Michaël and Polidori, Ange and Durand, Grégory
and Willbold, Dieter and Brutscher, Bernhard},
title = {{T}he {D}isordered {R}egion of the {HCV} {P}rotein
{NS}5{A}: {C}onformational {D}ynamics, {SH}3 {B}inding, and
{P}hosphorylation},
journal = {Biophysical journal},
volume = {109},
number = {7},
issn = {0006-3495},
address = {Cambridge, Mass.},
publisher = {Cell Press},
reportid = {FZJ-2015-06935},
pages = {1483 - 1496},
year = {2015},
abstract = {Intrinsically disordered proteins (IDPs) perform their
physiological role without possessing a well-defined
threedimensional structure. Still, residual structure and
conformational dynamics of IDPs are crucial for the
mechanisms underlying their functions. For example, regions
of transient secondary structure are often involved in
molecular recognition, with the structure being stabilized
(or not) upon binding. Long-range interactions, on the other
hand, determine the hydrodynamic radius of the IDP, and thus
the distance over which the protein can catch binding
partners via so-called fly-casting mechanisms. The
modulation of long-range interactions also presents a
convenient way of fine-tuning the protein’s interaction
network, by making binding sites more or less accessible.
Here we studied, mainly by nuclear magnetic resonance
spectroscopy, residual secondary structure and long-range
interactions in nonstructural protein 5A (NS5A) from
hepatitis C virus (HCV), a typical viral IDP with multiple
functions during the viral life cycle. NS5A comprises an
N-terminal folded domain, followed by a large (~250-residue)
disordered C-terminal part. Comparing nuclear magnetic
resonance spectra of full-length NS5A with those of a
protein construct composed of only the C-terminal residues
191–447 (NS5A-D2D3) allowed us to conclude that there is
no significant interaction between the globular and
disordered parts of NS5A. NS5A-D2D3, despite its overall
high flexibility, shows a large extent of local residual
(a-helical and b-turn) structure, as well as a network of
electrostatic long-range interactions. Furthermore, we could
demonstrate that these long-range interactions become
modulated upon binding to the host protein Bin1, as well as
after NS5A phosphorylation by CK2. As the charged peptide
regions involved in these interactions are well conserved
among the different HCV genotypes, these transient
long-range interactions may be important for some of the
functions of NS5A over the course of the HCV life cycle.},
cin = {ICS-6},
ddc = {570},
cid = {I:(DE-Juel1)ICS-6-20110106},
pnm = {553 - Physical Basis of Diseases (POF3-553)},
pid = {G:(DE-HGF)POF3-553},
typ = {PUB:(DE-HGF)16},
UT = {WOS:000362467100022},
pubmed = {pmid:26445449},
doi = {10.1016/j.bpj.2015.06.040},
url = {https://juser.fz-juelich.de/record/276570},
}
guest ::