Structure of the Dnmt1 Reader Module Complexed with a Unique Two-Mono-Ubiquitin Mark on Histone H3 Reveals the Basis for DNA Methylation Maintenance

Ishiyama, Satoshi; Nishiyama, Atsuya; Saeki, Yasushi; Moritsugu, Kei; Morimoto, Daichi; Yamaguchi, Luna; Arai, Naoko; Matsumura, Rumie; Kawakami, Toru; Mishima, Yuichiro; Hojo, Hironobu; Shimamura, Shintaro; Ishikawa, Fuyuki; Tsuji, Shoji; Tanaka, Keiji; Ariyoshi, Mariko; Shirakawa, Masahiro; Ikeguchi, Mitsunori; Kidera, Akinori; Suetake, Isao; Arita, Kyohei; Nakanishi, Makoto

doi:10.1016/j.molcel.2017.09.037

Cited by 139 publications

(215 citation statements)

References 75 publications

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“…We previously used ubiquitinated H3 peptide analogs with an unnatural isopeptide mimetic structure for investigating the effect of this molecule on Dnmt1 enzymatic activity . In this research, in order to confirm the reliability of the analogs, we synthesized ubiquitinated H3 peptides with a native isopeptide structure at Lys18 or/and 23 position(s), as shown in Scheme .…”

Section: Resultsmentioning

confidence: 99%

“…Analogs with the structures shown in Figure B showed a much enhanced Dnmt1 activity. The disulfide analogs, shown in Figure C, cannot be used in this measurement, because the experiment was performed under reduced conditions in the presence of DTT, but isothermal calorimetry and X‐ray crystal experiments showed a tight binding of the analogs to the domain of Dnmt1 with the similar order in enzymatic enhancement at the ubiquitinated positions under non‐reducing conditions . Compared with these structures, the native isopeptide structure might be more flexible than the analogs.…”

Section: Resultsmentioning

confidence: 99%

“…For Dnmt1, in which N‐terminal 290 amino acids are truncated, the expression plasmid using pFASTBAC system (Invitrogen) was prepared, and expressed in insect cells . Ubiqutinated histone H3 peptides and their analogs were renatured …”

Section: Methodsmentioning

confidence: 99%

“…Methylation activity measurements using radioisotopes were performed as described . Hemi‐methylated DNA, which is comprised of 42bp and 12 methylated CpG, were used as substrates .…”

Section: Methodsmentioning

confidence: 99%

“…In the cell division process, newly synthesized DNA is hemi‐methylated and is converted to its fully methylated form mainly by DNA methyltransferase 1 (Dnmt1) to maintain the methylation pattern . The ubiquitination of H3 at Lys18 or/and 23 was reported to regulate the maintenance DNA methylation by Dnmt1 …”

Section: Introductionmentioning

confidence: 99%

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Chemical synthesis of the ubiquitinated form of histone H3 and its effect on DNA methyltransferase 1

Kawakami

Mishima

Takazawa

et al. 2019

Journal of Peptide Science

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Posttranslational modifications of histone proteins, which form nucleosome cores, play an important role in gene regulation. Ubiquitination is one such modification. We previously reported on the synthesis of ubiquitinated histone H3 with an isopeptide mimetic structure. In this report, we describe the preparation of ubiquitinated histone H3 peptides with a native isopeptide structure, which showed a slightly weaker effect on the enzymatic activity of DNA methyltransferase 1 than the previous ubiquitinated H3 peptide analogs. These findings show that a native structure is important for determining the mechanism of the function, although ubiquitinated H3 peptide analogs can mimic the role of the original ubiquitinated H3. We also report on the successful preparation of the ubiquitinated full length histone H3.

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Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

Section: Methodsmentioning

confidence: 99%

“…Methylation activity measurements using radioisotopes were performed as described . Hemi‐methylated DNA, which is comprised of 42bp and 12 methylated CpG, were used as substrates .…”

Section: Methodsmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 3 more Smart Citations

Chemical synthesis of the ubiquitinated form of histone H3 and its effect on DNA methyltransferase 1

Kawakami

Mishima

Takazawa

et al. 2019

Journal of Peptide Science

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The Chromatin Interaction System

Kreuz

David

Medina

et al. 2022

Protein Interactions

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Molecular investigation of the tandem Tudor domain and plant homeodomain histone binding domains of the epigenetic regulator UHRF2

et al. 2021

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Ubiquitin‐like containing PHD and ring finger (UHRF)1 and UHRF2 are multidomain epigenetic proteins that play a critical role in bridging crosstalk between histone modifications and DNA methylation. Both proteins contain two histone reader domains, called tandem Tudor domain (TTD) and plant homeodomain (PHD), which read the modification status on histone H3 to regulate DNA methylation and gene expression. To shed light on the mechanism of histone binding by UHRF2, we have undergone a detailed molecular investigation with the TTD, PHD and TTD‐PHD domains and compared the binding activity to its UHRF1 counterpart. We found that unlike UHRF1 where the PHD is the primary binding contributor, the TTD of UHRF2 has modestly higher affinity toward the H3 tail, while the PHD has a weaker binding interaction. We also demonstrated that like UHRF1, the aromatic amino acids within the TTD are important for binding to H3K9me3 and a conserved aspartic acid within the PHD forms an ionic interaction with R2 of H3. However, while the aromatic amino acids in the TTD of UHRF1 contribute to selectivity, the analogous residues in UHRF2 contribute to both selectivity and affinity. We also discovered that the PHD of UHRF2 contains a distinct asparagine in the H3R2 binding pocket that lowers the binding affinity of the PHD by reducing a potential electrostatic interaction with the H3 tail. Furthermore, we demonstrate the PHD and TTD of UHRF2 cooperate to interact with the H3 tail and that dual domain engagement with the H3 tail relies on specific amino acids. Lastly, our data indicate that the unique stretch region in the TTD of UHRF2 can decrease the melting temperature of the TTD‐PHD and represents a disordered region. Thus, these subtle but important mechanistic differences are potential avenues for selectively targeting the histone binding interactions of UHRF1 and UHRF2 with small molecules.

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Structure of the Dnmt1 Reader Module Complexed with a Unique Two-Mono-Ubiquitin Mark on Histone H3 Reveals the Basis for DNA Methylation Maintenance

Cited by 139 publications

References 75 publications

Chemical synthesis of the ubiquitinated form of histone H3 and its effect on DNA methyltransferase 1

Chemical synthesis of the ubiquitinated form of histone H3 and its effect on DNA methyltransferase 1

The Chromatin Interaction System

Molecular investigation of the tandem Tudor domain and plant homeodomain histone binding domains of the epigenetic regulator UHRF2

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