Modeling G4s in chromatin context confirms partial nucleosome exclusion and reveals nucleosome-disrupting effects of the least selective G4 ligands
Iuliia Pavlova
1, 2
,
Roman G. Novikov
3, 4
,
Mikhail Iudin
1, 2
,
Andrey Larin
1, 5
,
Vladislav Babenko
1, 5
,
Andrey V Aralov
6
,
Evgeny Gnuchikh
7
,
Makar Sardushkin
8
,
Dmitry Klinov
1, 9
,
Vladimir B. Tsvetkov
1, 10, 11
,
Anna Varizhuk
1, 2, 5
Publication type: Journal Article
Publication date: 2023-01-01
scimago Q2
wos Q3
SJR: 0.884
CiteScore: 6.0
Impact factor: 3.0
ISSN: 03009084, 61831638, 16386183
PubMed ID:
36063975
Biochemistry
General Medicine
Abstract
G-quadruplexes (G4s) are gaining increasing attention as possible regulators of chromatin packaging, and robust approaches to their studies in pseudo-native context are much needed. Here, we designed a simple in vitro model of G4-prone genomic DNA and employed it to elucidate the impact of G4s and G4-stabilizing ligands on nucleosome occupancy. We obtained two 226-bp dsDNA constructs composed of the strong nucleosome positioning sequence and an internucleosomal DNA-imitating tail. The tail was G4-free in the control construct and harbored a "strong" (stable) G4 motif in the construct of interest. An additional "weak" (semi-stable) G4 motif was found within the canonical nucleosome positioning sequence. Both G4s were confirmed by optical methods and 1H NMR spectroscopy. Electrophoretic mobility assays showed that the weak G4 motif did not obstruct nucleosome assembly, while the strong G4 motif in the tail sequence diminished nucleosome yield. Atomic force microscopy data and molecular modeling confirmed that the strong G4 was maintained in the tail of the correctly assembled nucleosome structure. Using both in vitro and in silico models, we probed three known G4 ligands and detected nucleosome-disrupting effects of the least selective ligand. Our results are in line with the negative correlation between stable G4s and nucleosome density, support G4 tolerance between regularly positioned nucleosomes, and highlight the importance of considering chromatin context when targeting genomic G4s.
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Pavlova I. et al. Modeling G4s in chromatin context confirms partial nucleosome exclusion and reveals nucleosome-disrupting effects of the least selective G4 ligands // Biochimie. 2023. Vol. 204. pp. 8-21.
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Pavlova I., Barinov N. A., Novikov R. G., Severov V., Iudin M., Vedekhina T., Larin A., Babenko V., Aralov A., Gnuchikh E., Sardushkin M., Klinov D., Tsvetkov V. B., Varizhuk A. Modeling G4s in chromatin context confirms partial nucleosome exclusion and reveals nucleosome-disrupting effects of the least selective G4 ligands // Biochimie. 2023. Vol. 204. pp. 8-21.
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TY - JOUR
DO - 10.1016/j.biochi.2022.08.016
UR - https://doi.org/10.1016/j.biochi.2022.08.016
TI - Modeling G4s in chromatin context confirms partial nucleosome exclusion and reveals nucleosome-disrupting effects of the least selective G4 ligands
T2 - Biochimie
AU - Pavlova, Iuliia
AU - Barinov, Nikolay A
AU - Novikov, Roman G.
AU - Severov, Viacheslav
AU - Iudin, Mikhail
AU - Vedekhina, Tatiana
AU - Larin, Andrey
AU - Babenko, Vladislav
AU - Aralov, Andrey V
AU - Gnuchikh, Evgeny
AU - Sardushkin, Makar
AU - Klinov, Dmitry
AU - Tsvetkov, Vladimir B.
AU - Varizhuk, Anna
PY - 2023
DA - 2023/01/01
PB - Elsevier
SP - 8-21
VL - 204
PMID - 36063975
SN - 0300-9084
SN - 6183-1638
SN - 1638-6183
ER -
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@article{2023_Pavlova,
author = {Iuliia Pavlova and Nikolay A Barinov and Roman G. Novikov and Viacheslav Severov and Mikhail Iudin and Tatiana Vedekhina and Andrey Larin and Vladislav Babenko and Andrey V Aralov and Evgeny Gnuchikh and Makar Sardushkin and Dmitry Klinov and Vladimir B. Tsvetkov and Anna Varizhuk},
title = {Modeling G4s in chromatin context confirms partial nucleosome exclusion and reveals nucleosome-disrupting effects of the least selective G4 ligands},
journal = {Biochimie},
year = {2023},
volume = {204},
publisher = {Elsevier},
month = {jan},
url = {https://doi.org/10.1016/j.biochi.2022.08.016},
pages = {8--21},
doi = {10.1016/j.biochi.2022.08.016}
}