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@ARTICLE{Schwarten:9748,
author = {Schwarten, M. and Stoldt, M. and Mohrlüder, J. and
Willbold, D.},
title = {{S}olution structure of {A}tg8 reveals conformational
polymorphism of the {N}-terminal domain},
journal = {Biochemical and biophysical research communications},
volume = {395},
issn = {0006-291X},
address = {Orlando, Fla.},
publisher = {Academic Press},
reportid = {PreJuSER-9748},
pages = {426 - 431},
year = {2010},
note = {We thank Sameer Singh for carefully reading the manuscript
as well as Clara Gruning, Justin Lecher and Sven Schunke for
helpful discussions. This study was supported by a
fellowship of the International Helmholtz Research School of
Biophysics and Soft Matter (IHRS BioSoft) to M. Schwarten
and a research Grant from the Deutsche
Forschungsgemeinschaft (DFG) to D. Willbold (Wi1472/5).},
abstract = {During autophagy a crescent shaped like membrane is formed,
which engulfs the material that is to be degraded. This
membrane grows further until its edges fuse to form the
double membrane covered autophagosome. Atg8 is a protein,
which is required for this initial step of autophagy.
Therefore, a multistage conjugation process of newly
synthesized Atg8 to phosphatidylethanolamine is of critical
importance. Here we present the high resolution structure of
unprocessed Atg8 determined by nuclear magnetic resonance
spectroscopy. Its C-terminal subdomain shows a well-defined
ubiquitin-like fold with slightly elevated mobility in the
pico- to nanosecond timescale as determined by heteronuclear
NOE data. In comparison to unprocessed Atg8, cleaved
Atg8(G116) shows a decreased mobility behaviour. The
N-terminal domain adopts different conformations within the
micro- to millisecond timescale. The possible biological
relevance of the differences in dynamic behaviours between
both subdomains as well as between the cleaved and uncleaved
forms is discussed.},
keywords = {Autophagy / Microtubule-Associated Proteins: chemistry /
Nuclear Magnetic Resonance, Biomolecular / Protein Folding /
Protein Structure, Tertiary / Saccharomyces cerevisiae:
chemistry / Saccharomyces cerevisiae: physiology /
Saccharomyces cerevisiae Proteins: chemistry / Ubiquitin:
chemistry / ATG8 protein, S cerevisiae (NLM Chemicals) /
Microtubule-Associated Proteins (NLM Chemicals) /
Saccharomyces cerevisiae Proteins (NLM Chemicals) /
Ubiquitin (NLM Chemicals) / J (WoSType)},
cin = {ISB-3 / JARA-HPC},
ddc = {570},
cid = {I:(DE-Juel1)VDB942 / $I:(DE-82)080012_20140620$},
pnm = {Funktion und Dysfunktion des Nervensystems / BioSoft:
Makromolekulare Systeme und biologische
Informationsverarbeitung},
pid = {G:(DE-Juel1)FUEK409 / G:(DE-Juel1)FUEK505},
shelfmark = {Biochemistry $\&$ Molecular Biology / Biophysics},
typ = {PUB:(DE-HGF)16},
pubmed = {pmid:20382112},
UT = {WOS:000277801200026},
doi = {10.1016/j.bbrc.2010.04.043},
url = {https://juser.fz-juelich.de/record/9748},
}
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