The Effects of Histone H2B Ubiquitylations on the Nucleosome Structure and Internucleosomal Interactions

Sengupta, Bhaswati; Huynh, Mai; Smith, Charlotte B.; McGinty, Robert K.; Lee, Tae-Hee

doi:10.1021/acs.biochem.2c00422

Cited by 7 publications

(4 citation statements)

References 52 publications

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“…These results suggest that the effects of H2BK34ub on transcription kinetics can be the major mechanisms of facilitated transcription by H2B ubiquitylations. The effects are likely due to localized perturbations of the nucleosome structure near the DNA-(H2B-H2B) contact region, which has been validated by our recent structural study based on smFRET 56 . We suspect that the weaker effects of H2BK120ub is due to its non-ideal location to affect DNA-histone interactions.…”

Section: Discussionsupporting

confidence: 61%

The Effects of Histone H2B ubiquitylations and H3K79me₃on Transcription Elongation

Huynh

Sengupta

Lee

2023

Preprint

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Post-translational modifications of histone proteins often mediate gene regulation by altering the global and local stability of the nucleosome, the basic gene-packing unit of eukaryotes. We employed semi-synthetic approaches to introduce histone H2B ubiquitylations at K34 (H2BK34ub) and K120 (H2BK120ub) and H3 K79 trimethylation (H3K79me3). With these modified histones, we investigated their effects on the kinetics of transcription elongation by RNA Polymerase II (Pol II) using single-molecule FRET. Pol II pauses at several locations within the nucleosome for a few seconds to minutes, which governs the overall transcription efficiency. We found that H2B ubiquitylations suppress pauses and shorten the pause durations near the nucleosome entry while H3K79me3 shortens the pause durations and increases the rate of RNA elongation near the center of the nucleosome. We also found that H2BK34ub facilitates partial rewrapping of the nucleosome upon Pol II passage. These observations suggest that H2B ubiquitylations promote transcription elongation and help maintain the chromatin structure by inducing and stabilizing nucleosome intermediates and that H3K79me3 facilitates Pol II progression possibly by destabilizing the local structure of the nucleosome. Our results provide the mechanisms of how these modifications coupled by a network of regulatory proteins facilitate transcription in two different regions of the nucleosome and help maintain the chromatin structure during active transcription.

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Section: Discussionsupporting

confidence: 61%

The Effects of Histone H2B ubiquitylations and H3K79me₃on Transcription Elongation

Huynh

Sengupta

Lee

2023

Preprint

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“… Since then, it has been shown that H2BK34ub nucleosomes have the ubiquitin moieties protrude between the two gyres of the nucleosomal DNA, weakening the structural integrity of the nucleosome and distorting DNA toward the entry region of the nucleosome. , These results suggest that the effects of H2BK34ub on transcription kinetics can be the major mechanisms of facilitated transcription by H2B ubiquitylations. The effects are likely due to localized perturbations of the nucleosome structure near the DNA–(H2B-H2B) contact region, which has been validated by our recent structural study based on smFRET . We suspect that the weaker effects of H2BK120ub are due to its nonideal location to affect DNA–histone interactions.…”

Section: Discussionmentioning

confidence: 99%

Effects of Histone H2B Ubiquitylations and H3K79me₃ on Transcription Elongation

2023

Self Cite

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Post-translational modifications of histone proteins often mediate gene regulation by altering the global and local stability of the nucleosome, the basic gene-packing unit of eukaryotes. We employed semisynthetic approaches to introduce histone H2B ubiquitylations at K34 (H2BK34ub) and K120 (H2BK120ub) and H3K79 trimethylation (H3K79me3). With these modified histones, we investigated their effects on the kinetics of transcription elongation by RNA polymerase II (Pol II) using single-molecule FRET. Pol II pauses at several locations within the nucleosome for a few seconds to minutes, which governs the overall transcription efficiency. We found that H2B ubiquitylations suppress pauses and shorten the pause durations near the nucleosome entry while H3K79me3 shortens the pause durations and increases the rate of RNA elongation near the center of the nucleosome. We also found that H2BK34ub facilitates partial rewrapping of the nucleosome upon Pol II passage. These observations suggest that H2B ubiquitylations promote transcription elongation and help maintain the chromatin structure by inducing and stabilizing nucleosome intermediates and that H3K79me3 facilitates Pol II progression possibly by destabilizing the local structure of the nucleosome. Our results provide the mechanisms of how these modifications coupled by a network of regulatory proteins facilitate transcription in two different regions of the nucleosome and help maintain the chromatin structure during active transcription.

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“…However, affinity of nucleosomes to positioning sequences can prevent the assembly of nucleosome clusters. It has also been discussed 47 that the relaxed DNA− (H2A−H2B) region may contribute to long-range internucleosomal interactions between DNA and histone tails. Therefore, the decrease in the binding between DNA and histone octamers on the nonspecific substrate compared to that on the 601 sequence benefits the long-range internucleosomal interactions and, ultimately, the compaction of the oligonucleosomes.…”

Section: ■ Discussionmentioning

confidence: 99%

Beyond Sequence: Internucleosomal Interactions Dominate Array Assembly

et al. 2022

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The organization of the nucleosome array is a critical component of the chromatin assembly into higher order structure as well as its function. Here, we investigated the contributions of the DNA sequence and internucleosomal interactions on the organization of the nucleosomal arrays in compact structures using atomic force microscopy. We assembled nucleosomes on DNA substrates allowing for the formation of tetranucleosomes. We found that nucleosomes are capable of close positioning with no discernible space between them, even in the case of assembled dinucleosomes. This morphology of the array is in contrast with that observed for arrays assembled with repeats of the nucleosome positioning motifs separated by uniform spacers. Simulated assembly of tetranucleosomes by random placement along the substrates revealed that nucleosome array compaction is promoted by the interaction of the nucleosomes. We developed a theoretical model to account for the role of DNA sequence and internucleosomal interactions in the formation of the nucleosome structures. These findings suggest that, in the chromatin assembly, the affinity of the nucleosomes to the DNA sequence and the strengths of the internucleosomal interactions are the two major factors defining the compactness of the chromatin.

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The Effects of Histone H2B Ubiquitylations on the Nucleosome Structure and Internucleosomal Interactions

Cited by 7 publications

References 52 publications

The Effects of Histone H2B ubiquitylations and H3K79me₃on Transcription Elongation

The Effects of Histone H2B ubiquitylations and H3K79me₃on Transcription Elongation

Effects of Histone H2B Ubiquitylations and H3K79me₃ on Transcription Elongation

Beyond Sequence: Internucleosomal Interactions Dominate Array Assembly

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The Effects of Histone H2B Ubiquitylations on the Nucleosome Structure and Internucleosomal Interactions

Cited by 7 publications

References 52 publications

The Effects of Histone H2B ubiquitylations and H3K79me3on Transcription Elongation

The Effects of Histone H2B ubiquitylations and H3K79me3on Transcription Elongation

Effects of Histone H2B Ubiquitylations and H3K79me3 on Transcription Elongation

Beyond Sequence: Internucleosomal Interactions Dominate Array Assembly

Contact Info

Product

Resources

About

The Effects of Histone H2B ubiquitylations and H3K79me₃on Transcription Elongation

The Effects of Histone H2B ubiquitylations and H3K79me₃on Transcription Elongation

Effects of Histone H2B Ubiquitylations and H3K79me₃ on Transcription Elongation