Abstract OR-19: Integrative Approach on Nucleosome Complexes Modeling

Background: Nucleosomes are the key structural elements of chromatin in all higher organisms. While X-ray crystallography studies of nucleosomes have consistently yielded similar atomistic structures, many biophysical and biochemical techniques suggest that nucleosomes and nucleosome complexes exhib...

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Main Authors: Grigoriy A. Armeev, Anna Panchenko, Alexey K. Shaytan
Format: Article
Language:English
Published: International Medical Research and Development Corporation 2019-06-01
Series:International Journal of Biomedicine
Subjects:
Online Access:http://ijbm.org/articles/IJBM_2019_9_S1_OR19.pdf
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spelling doaj-578420bf670c40d6b9c32b2f38bbbc5b2020-11-25T01:30:15ZengInternational Medical Research and Development CorporationInternational Journal of Biomedicine2158-05102158-05292019-06-019Suppl_1S13S1410.21103/IJBM.9.Suppl_1.OR19Abstract OR-19: Integrative Approach on Nucleosome Complexes ModelingGrigoriy A. Armeev0Anna Panchenko1Alexey K. Shaytan2Faculty of Biology, Lomonosov Moscow State University, Moscow, RussiaNational Institutes of Health, National Center for Biotechnology Information, Moscow, RussiaFaculty of Biology, Lomonosov Moscow State University, Moscow, RussiaBackground: Nucleosomes are the key structural elements of chromatin in all higher organisms. While X-ray crystallography studies of nucleosomes have consistently yielded similar atomistic structures, many biophysical and biochemical techniques suggest that nucleosomes and nucleosome complexes exhibit substantial conformational polymorphism, which is functionally important. The interpretation of such experimental data with such sufficient details is often a tedious task, thus a set of molecular modeling tools is required. Methods: We performed full-atom molecular dynamics of nucleosomes and DNA fluorescent labels to sample the conformations used for single particle Förster Resonance Energy Transfer (spFRET) measurements. We developed an approach for donor and acceptor quantum yield estimation, during spFRET measurements in a single laser excitation setup. We also implemented a set of methods for the integrative modeling of nucleosome structures based on spFRET constraints. Results: Using these approaches, we have constructed atomistic models of nucleosomes structural reorganization induced by histone chaperones or histone H1. Besides the distances derived from corrected spFRET efficiencies, histone - DNA contacts are crucial for nucleosome formation and function. We used hydroxyl DNA footprinting data, in conjunction with atomistic structures of nucleosomes enhanced by molecular dynamics simulations, to develop a computational method for the precise determination of DNA positioning in nucleosomes with single base pair resolution. Conclusion: We have developed a set of techniques for chromatin modeling on the nucleosomal level. Such approaches tightly integrate various experimental data (mainly corrected spFRET efficiencies and hydroxyl DNA footprints) into molecular modeling pipelines.http://ijbm.org/articles/IJBM_2019_9_S1_OR19.pdfnucleosomechromatin
collection DOAJ
language English
format Article
sources DOAJ
author Grigoriy A. Armeev
Anna Panchenko
Alexey K. Shaytan
spellingShingle Grigoriy A. Armeev
Anna Panchenko
Alexey K. Shaytan
Abstract OR-19: Integrative Approach on Nucleosome Complexes Modeling
International Journal of Biomedicine
nucleosome
chromatin
author_facet Grigoriy A. Armeev
Anna Panchenko
Alexey K. Shaytan
author_sort Grigoriy A. Armeev
title Abstract OR-19: Integrative Approach on Nucleosome Complexes Modeling
title_short Abstract OR-19: Integrative Approach on Nucleosome Complexes Modeling
title_full Abstract OR-19: Integrative Approach on Nucleosome Complexes Modeling
title_fullStr Abstract OR-19: Integrative Approach on Nucleosome Complexes Modeling
title_full_unstemmed Abstract OR-19: Integrative Approach on Nucleosome Complexes Modeling
title_sort abstract or-19: integrative approach on nucleosome complexes modeling
publisher International Medical Research and Development Corporation
series International Journal of Biomedicine
issn 2158-0510
2158-0529
publishDate 2019-06-01
description Background: Nucleosomes are the key structural elements of chromatin in all higher organisms. While X-ray crystallography studies of nucleosomes have consistently yielded similar atomistic structures, many biophysical and biochemical techniques suggest that nucleosomes and nucleosome complexes exhibit substantial conformational polymorphism, which is functionally important. The interpretation of such experimental data with such sufficient details is often a tedious task, thus a set of molecular modeling tools is required. Methods: We performed full-atom molecular dynamics of nucleosomes and DNA fluorescent labels to sample the conformations used for single particle Förster Resonance Energy Transfer (spFRET) measurements. We developed an approach for donor and acceptor quantum yield estimation, during spFRET measurements in a single laser excitation setup. We also implemented a set of methods for the integrative modeling of nucleosome structures based on spFRET constraints. Results: Using these approaches, we have constructed atomistic models of nucleosomes structural reorganization induced by histone chaperones or histone H1. Besides the distances derived from corrected spFRET efficiencies, histone - DNA contacts are crucial for nucleosome formation and function. We used hydroxyl DNA footprinting data, in conjunction with atomistic structures of nucleosomes enhanced by molecular dynamics simulations, to develop a computational method for the precise determination of DNA positioning in nucleosomes with single base pair resolution. Conclusion: We have developed a set of techniques for chromatin modeling on the nucleosomal level. Such approaches tightly integrate various experimental data (mainly corrected spFRET efficiencies and hydroxyl DNA footprints) into molecular modeling pipelines.
topic nucleosome
chromatin
url http://ijbm.org/articles/IJBM_2019_9_S1_OR19.pdf
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