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@ARTICLE{Schwarten:139657,
author = {Schwarten, Melanie and Solyom, Z. and Feuerstein, S. and
Aladag, Amine and Hoffmann, Silke and Willbold, Dieter and
Brutscher, B.},
title = {{I}nteraction of {N}onstructural {P}rotein 5{A} of the
{H}epatitis {C} {V}irus with {S}rc {H}omology 3 {D}omains
{U}sing {N}oncanonical {B}inding {S}ites},
journal = {Biochemistry},
volume = {52},
issn = {1520-4995},
address = {Columbus, Ohio},
publisher = {American Chemical Society},
reportid = {FZJ-2013-05635},
pages = {6160-6168},
year = {2013},
abstract = {Src homology 3 (SH3) domains are widely known for their
ability to interact with other proteins using the canonical
PxxP binding motif. Besides those well-characterized
interaction modes, there is an increasing number of SH3
domain-containing complexes that lack this motif. Here we
characterize the interaction of SH3 domains, in particular
the Bin1-SH3 domain, with the intrinsically disordered part
of nonstructural protein 5A of the hepatitis C virus using
noncanonical binding sites in addition to its PxxP motif.
These binding regions partially overlap with regions that
have previously been identified as having an increased
propensity to form α-helices. Remarkably, upon interaction
with the Bin1-SH3 domain, the α-helical propensity
decreases and a fuzzy complex is formed.},
cin = {ICS-6},
ddc = {570},
cid = {I:(DE-Juel1)ICS-6-20110106},
pnm = {452 - Structural Biology (POF2-452)},
pid = {G:(DE-HGF)POF2-452},
typ = {PUB:(DE-HGF)16},
UT = {WOS:000330099900004},
doi = {10.1021/bi400363v},
url = {https://juser.fz-juelich.de/record/139657},
}
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