Mechanism of curaxin-dependent nucleosome unfolding by FACT

Olesya I. Volokh; Anastasia L. Sivkina; Andrey V. Moiseenko; Anna V. Popinako; Maria G. Karlova; Maria E. Valieva; Elena Y. Kotova; Mikhail P. Kirpichnikov; Timothy Formosa; Vasily M. Studitsky; Olga S. Sokolova

doi:10.3389/fmolb.2022.1048117

Mechanism of curaxin-dependent nucleosome unfolding by FACT

Olesya I. Volokh
, Anastasia L. Sivkina
, Andrey V. Moiseenko
, Anna V. Popinako
, Maria G. Karlova
, Maria E. Valieva
, Elena Y. Kotova
, Mikhail P. Kirpichnikov
, Timothy Formosa
, Vasily M. Studitsky
, Olga S. Sokolova

Research output: Contribution to journal › Article › peer-review

8 Scopus citations

Abstract

Human FACT (FACT) is a multifunctional histone chaperone involved in transcription, replication and DNA repair. Curaxins are anticancer compounds that induce FACT-dependent nucleosome unfolding and trapping of FACT in the chromatin of cancer cells (c-trapping) through an unknown molecular mechanism. Here, we analyzed the effects of curaxin CBL0137 on nucleosome unfolding by FACT using spFRET and electron microscopy. By itself, FACT adopted multiple conformations, including a novel, compact, four-domain state in which the previously unresolved NTD of the SPT16 subunit of FACT was localized, apparently stabilizing a compact configuration. Multiple, primarily open conformations of FACT-nucleosome complexes were observed during curaxin-supported nucleosome unfolding. The obtained models of intermediates suggest “decision points” in the unfolding/folding pathway where FACT can either promote disassembly or assembly of nucleosomes, with the outcome possibly being influenced by additional factors. The data suggest novel mechanisms of nucleosome unfolding by FACT and c-trapping by curaxins.

Original language	English
Article number	1048117
Pages (from-to)	1048117
Journal	Frontiers in Molecular Biosciences
Volume	9
DOIs	https://doi.org/10.3389/fmolb.2022.1048117
State	Published - Nov 22 2022

Keywords

FACT
SPT16
SSRP1
SpFRET microscopy
nucleosome
transmission electron microscopy

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.3389/fmolb.2022.1048117

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title = "Mechanism of curaxin-dependent nucleosome unfolding by FACT",

abstract = "Human FACT (FACT) is a multifunctional histone chaperone involved in transcription, replication and DNA repair. Curaxins are anticancer compounds that induce FACT-dependent nucleosome unfolding and trapping of FACT in the chromatin of cancer cells (c-trapping) through an unknown molecular mechanism. Here, we analyzed the effects of curaxin CBL0137 on nucleosome unfolding by FACT using spFRET and electron microscopy. By itself, FACT adopted multiple conformations, including a novel, compact, four-domain state in which the previously unresolved NTD of the SPT16 subunit of FACT was localized, apparently stabilizing a compact configuration. Multiple, primarily open conformations of FACT-nucleosome complexes were observed during curaxin-supported nucleosome unfolding. The obtained models of intermediates suggest “decision points” in the unfolding/folding pathway where FACT can either promote disassembly or assembly of nucleosomes, with the outcome possibly being influenced by additional factors. The data suggest novel mechanisms of nucleosome unfolding by FACT and c-trapping by curaxins.",

keywords = "FACT, SPT16, SSRP1, SpFRET microscopy, nucleosome, transmission electron microscopy",

author = "Volokh, \{Olesya I.\} and Sivkina, \{Anastasia L.\} and Moiseenko, \{Andrey V.\} and Popinako, \{Anna V.\} and Karlova, \{Maria G.\} and Valieva, \{Maria E.\} and Kotova, \{Elena Y.\} and Kirpichnikov, \{Mikhail P.\} and Timothy Formosa and Studitsky, \{Vasily M.\} and Sokolova, \{Olga S.\}",

note = "Publisher Copyright: Copyright {\textcopyright} 2022 Volokh, Sivkina, Moiseenko, Popinako, Karlova, Valieva, Kotova, Kirpichnikov, Formosa, Studitsky and Sokolova.",

year = "2022",

month = nov,

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doi = "10.3389/fmolb.2022.1048117",

language = "English",

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AU - Volokh, Olesya I.

AU - Sivkina, Anastasia L.

AU - Moiseenko, Andrey V.

AU - Popinako, Anna V.

AU - Karlova, Maria G.

AU - Valieva, Maria E.

AU - Kotova, Elena Y.

AU - Kirpichnikov, Mikhail P.

AU - Formosa, Timothy

AU - Studitsky, Vasily M.

AU - Sokolova, Olga S.

PY - 2022/11/22

Y1 - 2022/11/22

N2 - Human FACT (FACT) is a multifunctional histone chaperone involved in transcription, replication and DNA repair. Curaxins are anticancer compounds that induce FACT-dependent nucleosome unfolding and trapping of FACT in the chromatin of cancer cells (c-trapping) through an unknown molecular mechanism. Here, we analyzed the effects of curaxin CBL0137 on nucleosome unfolding by FACT using spFRET and electron microscopy. By itself, FACT adopted multiple conformations, including a novel, compact, four-domain state in which the previously unresolved NTD of the SPT16 subunit of FACT was localized, apparently stabilizing a compact configuration. Multiple, primarily open conformations of FACT-nucleosome complexes were observed during curaxin-supported nucleosome unfolding. The obtained models of intermediates suggest “decision points” in the unfolding/folding pathway where FACT can either promote disassembly or assembly of nucleosomes, with the outcome possibly being influenced by additional factors. The data suggest novel mechanisms of nucleosome unfolding by FACT and c-trapping by curaxins.

AB - Human FACT (FACT) is a multifunctional histone chaperone involved in transcription, replication and DNA repair. Curaxins are anticancer compounds that induce FACT-dependent nucleosome unfolding and trapping of FACT in the chromatin of cancer cells (c-trapping) through an unknown molecular mechanism. Here, we analyzed the effects of curaxin CBL0137 on nucleosome unfolding by FACT using spFRET and electron microscopy. By itself, FACT adopted multiple conformations, including a novel, compact, four-domain state in which the previously unresolved NTD of the SPT16 subunit of FACT was localized, apparently stabilizing a compact configuration. Multiple, primarily open conformations of FACT-nucleosome complexes were observed during curaxin-supported nucleosome unfolding. The obtained models of intermediates suggest “decision points” in the unfolding/folding pathway where FACT can either promote disassembly or assembly of nucleosomes, with the outcome possibly being influenced by additional factors. The data suggest novel mechanisms of nucleosome unfolding by FACT and c-trapping by curaxins.

KW - FACT

KW - SPT16

KW - SSRP1

KW - SpFRET microscopy

KW - nucleosome

KW - transmission electron microscopy

UR - https://www.scopus.com/pages/publications/85143329193

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DO - 10.3389/fmolb.2022.1048117

M3 - Article

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AN - SCOPUS:85143329193

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JO - Frontiers in Molecular Biosciences

JF - Frontiers in Molecular Biosciences

M1 - 1048117

ER -

Mechanism of curaxin-dependent nucleosome unfolding by FACT

Abstract

Keywords

UN SDGs

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