The chromatin remodeller ACF acts as a dimeric motor to space nucleosomes

Racki, Lisa R.; Yang, Ji-Young; Naber, Nariman; Partensky, Peretz D.; Acevedo, Ashley; Purcell, Thomas J.; Cooke, Roger; Cheng, Yifan; Narlikar, Geeta J.

doi:10.1038/nature08621

Cited by 163 publications

(209 citation statements)

References 48 publications

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“…In order to maintain a controlled distribution of distances, nucleosomes need to be repositioned, most likely by ATP-dependent chromatin-remodeling enzymes such as ACF and CHD1 (65)(66)(67)(68)(69). Catalyzed nucleosome repositioning has been the subject of numerous experimental and theoretical studies (5,(70)(71)(72)(73)(74) but the exact mechanism by which these proteins move the histones along the DNA sequence remains unclear, partially because the mechanisms of remodelers can be heavily convoluted with nucleosome positioning effects that are encoded in the DNA.…”

Section: Discussionmentioning

confidence: 99%

Sequence-based prediction of single nucleosome positioning and genome-wide nucleosome occupancy

Heijden

Vugt

Logie

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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Nucleosome positioning dictates eukaryotic DNA compaction and access. To predict nucleosome positions in a statistical mechanics model, we exploited the knowledge that nucleosomes favor DNA sequences with specific periodically occurring dinucleotides. Our model is the first to capture both dyad position within a few base pairs, and free binding energy within 2 kBT, for all the known nucleosome positioning sequences. By applying Percus’s equation to the derived energy landscape, we isolate sequence effects on genome-wide nucleosome occupancy from other factors that may influence nucleosome positioning. For both in vitro and in vivo systems, three parameters suffice to predict nucleosome occupancy with correlation coefficients of respectively 0.74 and 0.66. As predicted, we find the largest deviations in vivo around transcription start sites. This relatively simple algorithm can be used to guide future studies on the influence of DNA sequence on chromatin organization.

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Section: Discussionmentioning

confidence: 99%

Sequence-based prediction of single nucleosome positioning and genome-wide nucleosome occupancy

Heijden

Vugt

Logie

et al. 2012

Proc. Natl. Acad. Sci. U.S.A.

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“…Nucleosome adsorption is known to occur efficiently in vivo by ATP-independent histone chaperone-mediated pathways; here we consider only ATP-independent nucleosome adsorption. On the other hand, thermally excited desorption and sliding are very slow, and ATP-dependent enzymes are known to assist nucleosomes in these processes (11)(12)(13)(14)(15)(16)(17). We consider both ATP-dependent and ATP-independent desorption and sliding processes.…”

Section: Modelmentioning

confidence: 99%

“…However, disrupting nucleosomes requires passage of energy barriers of tens of k B T per nucleosome (7,8). In vivo this is facilitated by ATP-consuming "chromatin remodeling complexes" (9,10), which catalyze nucleosome repositioning and disassembly (11)(12)(13)(14)(15)(16)(17).…”

mentioning

confidence: 99%

“…In addition to thermal fluctuation dynamics (always present as a "background" to any active remodeling machinery) we consider two general types of remodeling machines that: (i) slide nucleosomes along the DNA to cause repositioning, and (ii) remove (eject) histone octamers from DNA. These two processes have been implicated to be catalyzed by remodelers in the ISWI [e.g., yeast ISWI (14), ACF (17)] and SNF2 [e.g., RSC (11), yeast SWI/SNF (12,15)] subfamilies, respectively. Using experimentally determined thermal and ATP-dependent enzyme rates we show that active sliding is necessary to achieve biological densities of nucleosomes within biologically relevant time scales, but that active nucleosome removal is also needed, to obtain nucleosome positioning at biological densities.…”

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confidence: 99%

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Nucleosome positioning in a model of active chromatin remodeling enzymes

Padinhateeri

Marko

2011

Proc. Natl. Acad. Sci. U.S.A.

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Accounting for enzyme-mediated active sliding, disassembly, and sequence-dependent positioning of nucleosomes, we simulate nucleosome occupancy over cell-cycle-scale times using a stochastic kinetic model. We show that ATP-dependent active nucleosome sliding and nucleosome removal processes are essential to obtain in vivo-like nucleosome positioning. While active sliding leads to dense nucleosome filling, sliding events alone cannot ensure sequence-dependent nucleosome positioning: Active nucleosome removal is the crucial remodeling event that drives positioning. We also show that remodeling activity changes nucleosome dynamics from glassy to liquid-like, and that remodeling dramatically influences exposure dynamics of promoter regions.ATP-dependent nucleosome removal | ATP-dependent nucleosome sliding | protein-DNA interactions | chromatin dynamics D NA in each eukaryotic cell is folded and packaged, with the help of many proteins, into chromatin. In the first level of packaging, 147-base-pair (≈50 nm) stretches of DNA are wrapped around histone protein octamers into nucleosomes (1). To a first approximation, chromatin can be considered as a linear array of nucleosomes, and a body of experimental evidence indicates that primary DNA sequence controls the position of at least a fraction of nucleosomes: Histone-DNA affinities vary with sequence over a roughly 8 k B T range (2). Nevertheless, the overall degree to which nucleosomes are positioned by DNA sequence is a subject of ongoing debate (3-5). Transcription, replication, recombination, and DNA repair all need access to bare DNA and hence the organization of nucleosomes must be accomplished in a way that allows rapid, localized access to DNA (6). However, disrupting nucleosomes requires passage of energy barriers of tens of k B T per nucleosome (7,8). In vivo this is facilitated by ATP-consuming "chromatin remodeling complexes" (9, 10), which catalyze nucleosome repositioning and disassembly (11-17).Previously, Teif and Rippe have studied models for the influence of remodeling enzymes on the equilibrium distribution of nucleosomes (18). Nucleosomes by themselves cannot reach thermal equilibrium on cell-cycle time scales, and no one has yet explored the kinetics of nucleosome filling in the presence of remodeling factors. Here we study the kinetics of nucleosomes in the presence of chromatin remodeling complexes in a stochastic model, focusing on assembly and positioning dynamics of nucleosomes. In addition to thermal fluctuation dynamics (always present as a "background" to any active remodeling machinery) we consider two general types of remodeling machines that: (i) slide nucleosomes along the DNA to cause repositioning, and (ii) remove (eject) histone octamers from DNA. These two processes have been implicated to be catalyzed by remodelers in the ISWI [e.g., yeast ISWI (14), ACF (17)] and SNF2 [e.g., RSC (11), yeast SWI/SNF (12, 15)] subfamilies, respectively. Using experimentally determined thermal and ATP-dependent enzyme rates we show that active sliding...

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“…This FRET response is highly sensitive over a window around the characteristic Förster radius of the dye pair, which is typically in the range 10-100 Å. spFRET can be performed in solution (Tóth et al 2001), or particles can be spread on an imaging surface and the relative signal of the FRET dyes observed for each single molecule spot simultaneously for thousands of spots with high time resolution (Koopmans et al 2007). spFRET revealed rates of site exposure of DNA from the edge of the nucleosome (Li et al 2005) and quantitation of nucleosome sliding (Racki et al 2009). …”

Section: Single Molecule Imagingmentioning

confidence: 99%

Principles and practice of nucleosome positioningin vitro

Flaus

2011

Frontiers in Life Science

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The chromatin remodeller ACF acts as a dimeric motor to space nucleosomes

Cited by 163 publications

References 48 publications

Sequence-based prediction of single nucleosome positioning and genome-wide nucleosome occupancy

Sequence-based prediction of single nucleosome positioning and genome-wide nucleosome occupancy

Nucleosome positioning in a model of active chromatin remodeling enzymes

Principles and practice of nucleosome positioningin vitro

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