Search

Your search keyword '"Vlaming, Hanneke"' showing total 33 results
Start Over Author "Vlaming, Hanneke"
33 results on '"Vlaming, Hanneke"'

5. Conserved crosstalk between histone deacetylation and H3K79 methylation generates DOT1L‐dose dependency in HDAC1‐deficient thymic lymphoma

Author

Vlaming, Hanneke, McLean, Chelsea M, Korthout, Tessy, Alemdehy, Mir Farshid, Hendriks, Sjoerd, Lancini, Cesare, Palit, Sander, Klarenbeek, Sjoerd, Kwesi‐Maliepaard, Eliza Mari, Molenaar, Thom M, Hoekman, Liesbeth, Schmidlin, Thierry T, Altelaar, AF Maarten, van Welsem, Tibor, Dannenberg, Jan‐Hermen, Jacobs, Heinz, and van Leeuwen, Fred

Published
2019
Full Text
View/download PDF

7. List of Contributors

Author

Antoniou-Kourounioti, Rea, primary, Bakker, Barbara M., additional, Bancaud, Aurélien, additional, Bystricky, Kerstin, additional, Chung, Ho-Ryun, additional, Corrales, Marc, additional, De Vos, Dirk, additional, Dodd, Ian B., additional, Filion, Guillaume J., additional, Gadal, Olivier, additional, Giorgetti, Luca, additional, Heard, Edith, additional, Hibino, Kayo, additional, Howard, Martin, additional, Kaizu, Kazunari, additional, Maeshima, Kazuhiro, additional, Moore, Benjamin L., additional, Nicodemi, Mario, additional, Perner, Juliane, additional, Pombo, Ana, additional, Rehmsmeier, Marc, additional, Ringrose, Leonie, additional, Semple, Colin A., additional, Sneppen, Kim, additional, Takahashi, Koichi, additional, Tiana, Guido, additional, van Leeuwen, Fred, additional, and Vlaming, Hanneke, additional

Published
2017
Full Text
View/download PDF

12. Strength is in engagement:The rise of an online scientific community during the COVID-19 pandemic

Author

Cucinotta, Christine E, Martin, Benjamin J E, Noé González, Melvin, Raman, Pravrutha, Teif, Vladimir B, Vlaming, Hanneke, Cucinotta, Christine E, Martin, Benjamin J E, Noé González, Melvin, Raman, Pravrutha, Teif, Vladimir B, and Vlaming, Hanneke

Abstract

Many scientists, confined to home office by COVID-19, have been gathering in online communities, which could become viable alternatives to physical meetings and conferences.

Published
2021

13. Epigenetics Identifier screens reveal regulators of chromatin acylation and limited specificity of acylation antibodies

Author

ZonMw, Dutch Research Council, European Research Council, Kollenstart, Leonie [0000-0003-3401-2512], Van der Horst, Sophie C. [0000-0002-9347-7240], George M. C., Janssen [0000-0001-9091-4030], Van Veelen, Peter A. [0000-0002-7898-9408], Van Leeuwen, Fred [0000-0002-7267-7251], Van Attikum, Haico [0000-0001-8590-0240], Kollenstart, Leonie, Van der Horst, Sophie C., Vreeken, Kees, George M. C., Janssen, Martino, Fabrizio, Vlaming, Hanneke, Van Veelen, Peter A., Van Leeuwen, Fred, Van Attikum, Haico, ZonMw, Dutch Research Council, European Research Council, Kollenstart, Leonie [0000-0003-3401-2512], Van der Horst, Sophie C. [0000-0002-9347-7240], George M. C., Janssen [0000-0001-9091-4030], Van Veelen, Peter A. [0000-0002-7898-9408], Van Leeuwen, Fred [0000-0002-7267-7251], Van Attikum, Haico [0000-0001-8590-0240], Kollenstart, Leonie, Van der Horst, Sophie C., Vreeken, Kees, George M. C., Janssen, Martino, Fabrizio, Vlaming, Hanneke, Van Veelen, Peter A., Van Leeuwen, Fred, and Van Attikum, Haico

Abstract

The collection of known posttranslational modifications (PTMs) has expanded rapidly with the identification of various non-acetyl histone lysine acylations, such as crotonylation, succinylation and butyrylation, yet their regulation is still not fully understood. Through an unbiased chromatin immunoprecipitation (ChIP)-based approach called Epigenetics-IDentifier (Epi-ID), we aimed to identify regulators of crotonylation, succinylation and butyrylation in thousands of yeast mutants simultaneously. However, highly correlative results led us to further investigate the specificity of the pan-K-acyl antibodies used in our Epi-ID studies. This revealed cross-reactivity and lack of specificity of pan-K-acyl antibodies in various assays. Our findings suggest that the antibodies might recognize histone acetylation in vivo, in addition to histone acylation, due to the vast overabundance of acetylation compared to other acylation modifications in cells. Consequently, our Epi-ID screen mostly identified factors affecting histone acetylation, including known (e.g. GCN5, HDA1, and HDA2) and unanticipated (MET7, MTF1, CLB3, and RAD26) factors, expanding the repertoire of acetylation regulators. Antibody-independent follow-up experiments on the Gcn5-Ada2-Ada3 (ADA) complex revealed that, in addition to acetylation and crotonylation, ADA has the ability to butyrylate histones. Thus, our Epi-ID screens revealed limits of using pan-K-acyl antibodies in epigenetics research, expanded the repertoire of regulators of histone acetylation, and attributed butyrylation activity to the ADA complex.

Published
2021

16. The histone methyltransferase DOT1L prevents antigen-independent differentiation and safeguards epigenetic identity of CD8 + T cells

Author

Kwesi-Maliepaard, Eliza Mari, primary, Aslam, Muhammad Assad, additional, Alemdehy, Mir Farshid, additional, van den Brand, Teun, additional, McLean, Chelsea, additional, Vlaming, Hanneke, additional, van Welsem, Tibor, additional, Korthout, Tessy, additional, Lancini, Cesare, additional, Hendriks, Sjoerd, additional, Ahrends, Tomasz, additional, van Dinther, Dieke, additional, den Haan, Joke M. M., additional, Borst, Jannie, additional, de Wit, Elzo, additional, van Leeuwen, Fred, additional, and Jacobs, Heinz, additional

Published
2020
Full Text
View/download PDF

18. The histone methyltransferase DOT1L prevents antigen-independent differentiation and safeguards epigenetic identity of CD8+ T cells

Author

Kwesi-Maliepaard, Eliza Mari, primary, Aslam, Muhammad Assad, additional, Alemdehy, Mir Farshid, additional, van den Brand, Teun, additional, McLean, Chelsea, additional, Vlaming, Hanneke, additional, van Welsem, Tibor, additional, Korthout, Tessy, additional, Lancini, Cesare, additional, Hendriks, Sjoerd, additional, Ahrends, Tomasz, additional, van Dinther, Dieke, additional, den Haan, Joke M.M., additional, Borst, Jannie, additional, de Wit, Elzo, additional, van Leeuwen, Fred, additional, and Jacobs, Heinz, additional

Published
2019
Full Text
View/download PDF

19. Evolutionarily-conserved chromatin crosstalk generates a DOT1L-dose dependency in thymic lymphoma caused by loss of HDAC1

Author

Vlaming, Hanneke, primary, McLean, Chelsea M., additional, Korthout, Tessy, additional, Alemdehy, Mir Farshid, additional, Hendriks, Sjoerd, additional, Lancini, Cesare, additional, Palit, Sander, additional, Klarenbeek, Sjoerd, additional, Kwesi-Maliepaard, Eliza Mari, additional, Molenaar, Thom M., additional, Hoekman, Liesbeth, additional, Schmidlin, Thierry T., additional, Altelaar, A.F. Maarten, additional, van Welsem, Tibor, additional, Dannenberg, Jan-Hermen, additional, Jacobs, Heinz, additional, and Leeuwen, Fred van, additional

Published
2019
Full Text
View/download PDF

20. Modeling Distributive Histone Modification by Dot1 Methyltransferases: From Mechanism to Biological Insights

Author

De Vos, Dirk, Vlaming, Hanneke, Bakker, Barbara M., van Leeuwen, Fred, Center for Liver, Digestive and Metabolic Diseases (CLDM), and Lifestyle Medicine (LM)

Subjects
Dot1, H3K79, Demethylase, Processive, Modeling, Distributive, H3K76, Methyltransferase, Histone methylation, Simulation
Abstract

Methylation of histone proteins plays a crucial role controlling genome activity. To understand how the responsible histone methyltransferases are regulated it is important to know their fundamental biochemical properties within the cell and relate these to cellular methylation dynamics. Repeated experiment-modeling cycles have led to insights into the in vivo dynamics of methylation of lysine 79 on histone H3 (H3K79) by the methyltransferase Disruptor of Telomeric Silencing 1 (Dot1). Genetic perturbation in yeast, quantitative measurements, and computational modeling were combined to show that Dot1 employs an uncommon, distributive methylation mechanism. A steady-state in vivo methylation model using this information has provided validated explanations for methylation defects in mutants. Subsequent single-cell models have provided insights into the dynamics of H3K79 methylation throughout the cell cycle and uncovered a role for histone protein aging. These integrated modeling approaches will aid in understanding how regulatory mechanisms influence Dot1's role in gene expression, cell cycle progression, and cancer and can be applied to other methylation systems.

Published
2017

21. The histone methyltransferase DOT1L prevents antigen-independent differentiation and safeguards epigenetic identity of CD8+ T cells.

Author

Kwesi-Maliepaard, Eliza Mari, Aslam, Muhammad Assad, Alemdehy, Mir Farshid, den Brand, Teun van, McLean, Chelsea, Vlaming, Hanneke, Welsem, Tibor van, Korthout, Tessy, Lancini, Cesare, Hendriks, Sjoerd, Ahrends, Tomasz, Dinther, Dieke van, den Haan, Joke M. M., Borst, Jannie, Wit, Elzo de, Leeuwen, Fred van, and Jacobs, Heinz

Subjects
T cells, CYTOTOXIC T cells, T cell differentiation, T cell receptors, PHYSIOLOGY
Abstract

Cytotoxic T cell differentiation is guided by epigenome adaptations, but how epigenetic mechanisms control lymphocyte development has not been well defined. Here we show that the histone methyltransferase DOT1L, which marks the nucleosome core on active genes, safeguards normal differentiation of CD8+ T cells. T cell-specific ablation of Dot1L resulted in loss of naïve CD8+ T cells and premature differentiation toward a memory-like state, independent of antigen exposure and in a cell-intrinsic manner. Mechanistically, DOT1L controlled CD8+ T cell differentiation by ensuring normal T cell receptor density and signaling. DOT1L also maintained epigenetic identity, in part by indirectly supporting the repression of developmentally regulated genes. Finally, deletion of Dot1L in T cells resulted in an impaired immune response. Through our study, DOT1L is emerging as a central player in physiology of CD8+ T cells, acting as a barrier to prevent premature differentiation and controlling epigenetic integrity. [ABSTRACT FROM AUTHOR]

Published
2020
Full Text
View/download PDF

22. Dot1 promotes H2B ubiquitination by a methyltransferase-independent mechanism

Author

van Welsem, Tibor, primary, Korthout, Tessy, additional, Ekkebus, Reggy, additional, Morais, Dominique, additional, Molenaar, Thom M, additional, van Harten, Kirsten, additional, Poramba-Liyanage, Deepani W, additional, Sun, Su Ming, additional, Lenstra, Tineke L, additional, Srivas, Rohith, additional, Ideker, Trey, additional, Holstege, Frank C P, additional, van Attikum, Haico, additional, El Oualid, Farid, additional, Ovaa, Huib, additional, Stulemeijer, Iris J E, additional, Vlaming, Hanneke, additional, and van Leeuwen, Fred, additional

Published
2018
Full Text
View/download PDF

23. Direct screening for chromatin status on DNA barcodes in yeast delineates the regulome of H3K79 methylation by Dot1

Author

Vlaming, Hanneke, Molenaar, Thom, van Welsem, Tibor, Poramba-Liyanage, Deepani, Smith, Desiree, Velds, Arno, Hoekman, Liesbeth, Korthout, Tessy, Hendriks, Sjoerd, Altelaar, A.F.M., van Leeuwen, Fred, Biomolecular Mass Spectrometry and Proteomics, Sub Biomol.Mass Spect. and Proteomics, Graduate School, Biomolecular Mass Spectrometry and Proteomics, and Sub Biomol.Mass Spect. and Proteomics

Subjects
Genetics, Microbial, 0301 basic medicine, Chromatin Immunoprecipitation, Histone-modifying enzymes, Saccharomyces cerevisiae Proteins, Dot1, QH301-705.5, Science, S. cerevisiae, DNA repair, SAGA, Saccharomyces cerevisiae, Computational biology, Biology, adenosine kinase, Methylation, General Biochemistry, Genetics and Molecular Biology, Chromatin remodeling, Histones, 03 medical and health sciences, Gene Expression Regulation, Fungal, Histone methylation, Histone code, Genetic Testing, H3K79 methylation, Biology (General), DNA, Fungal, Molecular Biology, Epigenomics, Genetics, General Immunology and Microbiology, histone modifications, General Neuroscience, Nuclear Proteins, Histone-Lysine N-Methyltransferase, Sequence Analysis, DNA, General Medicine, Chromatin, Tools and Resources, 3. Good health, 030104 developmental biology, Genes and Chromosomes, Histone methyltransferase, Medicine, Protein Processing, Post-Translational, Bivalent chromatin
Abstract

Given the frequent misregulation of chromatin in cancer, it is important to understand the cellular mechanisms that regulate chromatin structure. However, systematic screening for epigenetic regulators is challenging and often relies on laborious assays or indirect reporter read-outs. Here we describe a strategy, Epi-ID, to directly assess chromatin status in thousands of mutants. In Epi-ID, chromatin status on DNA barcodes is interrogated by chromatin immunoprecipitation followed by deep sequencing, allowing for quantitative comparison of many mutants in parallel. Screening of a barcoded yeast knock-out collection for regulators of histone H3K79 methylation by Dot1 identified all known regulators as well as novel players and processes. These include histone deposition, homologous recombination, and adenosine kinase, which influences the methionine cycle. Gcn5, the acetyltransferase within the SAGA complex, was found to regulate histone methylation and H2B ubiquitination. The concept of Epi-ID is widely applicable and can be readily applied to other chromatin features. DOI: http://dx.doi.org/10.7554/eLife.18919.001, eLife digest To fit into the nucleus of eukaryotic cells (which include plant, animal and yeast cells), DNA wraps around histone proteins to form a structure called chromatin. Histones can be modified by a variety of chemical tags, which affect how easily nearby DNA can be accessed by other molecules in the cell. These modifications therefore help to control the activity of the genes encoded in the DNA and other key processes such as DNA repair. If histone modifications are not regulated correctly, diseases such as cancer may result. Enzymes generally perform the actual modification, but there is another layer of regulation that controls the activity of these enzymes that not much is known about. The activity of an enzyme that performs a histone modification known as H3K79 methylation (which involves a methyl chemical group being added to a particular region of a particular histone protein) has been linked to some forms of leukemia. Collections of mutant yeast cells can be used to identify the factors that regulate histone modifications in both yeast and human cells. However, current methods that screen for these regulators are time consuming. To make the search for histone modification regulators more efficient, Vlaming et al. developed a new screening procedure called Epi-ID that can measure the amount of a specific histone modification in thousands of budding yeast mutants at the same time. In Epi-ID, each mutant yeast cell has a unique DNA sequence, or “barcode”. The mutant cells are mixed together and the barcodes that are modified by a particular histone modification – such as H3K79 methylation – are isolated and then counted using a DNA sequencing technique. A high barcode count of a certain mutant indicates that more of the histone modification occurs in that mutant. Using Epi-ID to survey H3K79 methylation enabled Vlaming et al. to successfully identify all previously known H3K79 methylation regulators, as well several new ones. These new regulators included enzymes that deposit histones on DNA, that carry out DNA repair, and that modify or de-modify histone proteins. To move forward with the newly identified regulators, it will be important to analyze how they control H3K79 methylation in yeast cells and to determine whether the regulators also control H3K79 methylation in human cells. Finally, Epi-ID can be used to identify regulators of other types of histone modifications. A better understanding of chromatin regulation – and H3K79 methylation regulation in particular – can increase our understanding of diseases in which chromatin is deregulated, and may yield new strategies for the treatment of such diseases. DOI: http://dx.doi.org/10.7554/eLife.18919.002

Published
2016

24. Flexibility in crosstalk between H2B ubiquitination and H3 methylation in vivo (Corrigendum)

Author

Vlaming, Hanneke, van Welsem, Tibor, de Graaf, Erik L, Ontoso, David, Altelaar, A F Maarten, San-Segundo, Pedro A, Heck, Albert J R, van Leeuwen, Fred, Sub Biomol.Mass Spectrometry & Proteom., Sub Biomol.Mass Spect. and Proteomics, and Biomolecular Mass Spectrometry and Proteomics

Abstract

Histone H2B ubiquitination is a dynamic modification that promotes methylation of histone H3K79 and H3K4. This crosstalk is important for the DNA damage response and has been implicated in cancer. Here, we show that in engineered yeast strains, ubiquitins tethered to every nucleosome promote H3K79 and H3K4 methylation from a proximal as well as a more distal site, but only if in a correct orientation. This plasticity indicates that the exact location of the attachment site, the native ubiquitin-lysine linkage and ubiquitination cycles are not critical for trans-histone crosstalk in vivo. The flexibility in crosstalk also indicates that other ubiquitination events may promote H3 methylation.

Published
2014

25. Author response: Direct screening for chromatin status on DNA barcodes in yeast delineates the regulome of H3K79 methylation by Dot1

Author

Vlaming, Hanneke, primary, Molenaar, Thom M, additional, van Welsem, Tibor, additional, Poramba-Liyanage, Deepani W, additional, Smith, Desiree E, additional, Velds, Arno, additional, Hoekman, Liesbeth, additional, Korthout, Tessy, additional, Hendriks, Sjoerd, additional, Altelaar, AF Maarten, additional, and van Leeuwen, Fred, additional

Published
2016
Full Text
View/download PDF

26. Dot1 histone methyltransferases share a distributive mechanism but have highly diverged catalytic properties

Author

Stulemeijer, Iris J E, De Vos, Dirk, Van Harten, Kirsten, Joshi, Onkar K., Blomberg, Olga, Van Welsem, Tibor, Terweij, Marit, Vlaming, Hanneke, De Graaf, Erik L., Altelaar, A. F Maarten, Bakker, Barbara M., Van Leeuwen, Fred, Stulemeijer, Iris J E, De Vos, Dirk, Van Harten, Kirsten, Joshi, Onkar K., Blomberg, Olga, Van Welsem, Tibor, Terweij, Marit, Vlaming, Hanneke, De Graaf, Erik L., Altelaar, A. F Maarten, Bakker, Barbara M., and Van Leeuwen, Fred

Abstract

The conserved histone methyltransferase Dot1 establishes an H3K79 methylation pattern consisting of mono-, di- and trimethylation states on histone H3 via a distributive mechanism. This mechanism has been shown to be important for the regulation of the different H3K79 methylation states in yeast. Dot1 enzymes in yeast, Trypanosoma brucei (TbDot1A and TbDot1B, which methylate H3K76) and human (hDot1L) generate very divergent methylation patterns. To understand how these species-specific methylation patterns are generated, the methylation output of the Dot1 enzymes was compared by expressing them in yeast at various expression levels. Computational simulations based on these data showed that the Dot1 enzymes have highly distinct catalytic properties, but share a distributive mechanism. The mechanism of methylation and the distinct rate constants have implications for the regulation of H3K79/K76 methylation. A mathematical model of H3K76 methylation during the trypanosome cell cycle suggests that temporally-regulated consecutive action of TbDot1A and TbDot1B is required for the observed regulation of H3K76 methylation states.

Published
2015

27. Dot1 histone methyltransferases share a distributive mechanism but have highly diverged catalytic properties

Author

Biomolecular Mass Spectrometry and Proteomics, Sub Biomol.Mass Spectrometry & Proteom., Sub Biomol.Mass Spect. and Proteomics, Stulemeijer, Iris J E, De Vos, Dirk, Van Harten, Kirsten, Joshi, Onkar K., Blomberg, Olga, Van Welsem, Tibor, Terweij, Marit, Vlaming, Hanneke, De Graaf, Erik L., Altelaar, A. F Maarten, Bakker, Barbara M., Van Leeuwen, Fred, Biomolecular Mass Spectrometry and Proteomics, Sub Biomol.Mass Spectrometry & Proteom., Sub Biomol.Mass Spect. and Proteomics, Stulemeijer, Iris J E, De Vos, Dirk, Van Harten, Kirsten, Joshi, Onkar K., Blomberg, Olga, Van Welsem, Tibor, Terweij, Marit, Vlaming, Hanneke, De Graaf, Erik L., Altelaar, A. F Maarten, Bakker, Barbara M., and Van Leeuwen, Fred

Published
2015

29. Yeast PP4 Interacts with ATR Homolog Ddc2-Mec1 and Regulates Checkpoint Signaling

Author

Hustedt, Nicole, primary, Seeber, Andrew, additional, Sack, Ragna, additional, Tsai-Pflugfelder, Monika, additional, Bhullar, Bhupinder, additional, Vlaming, Hanneke, additional, van Leeuwen, Fred, additional, Guénolé, Aude, additional, van Attikum, Haico, additional, Srivas, Rohith, additional, Ideker, Trey, additional, Shimada, Kenji, additional, and Gasser, Susan M., additional

Published
2015
Full Text
View/download PDF

30. Flexibility in crosstalk between H2B ubiquitination and H3 methylation in vivo

Author

Sub Biomol.Mass Spectrometry & Proteom., Sub Biomol.Mass Spect. and Proteomics, Biomolecular Mass Spectrometry and Proteomics, Vlaming, Hanneke, van Welsem, Tibor, de Graaf, Erik L, Ontoso, David, Altelaar, A F Maarten, San-Segundo, Pedro A, Heck, Albert J R, van Leeuwen, Fred, Sub Biomol.Mass Spectrometry & Proteom., Sub Biomol.Mass Spect. and Proteomics, Biomolecular Mass Spectrometry and Proteomics, Vlaming, Hanneke, van Welsem, Tibor, de Graaf, Erik L, Ontoso, David, Altelaar, A F Maarten, San-Segundo, Pedro A, Heck, Albert J R, and van Leeuwen, Fred

Published
2014

31. Flexibility in crosstalk between H2B ubiquitination and H3 methylation in vivo (Corrigendum)

Author

Sub Biomol.Mass Spectrometry & Proteom., Sub Biomol.Mass Spect. and Proteomics, Biomolecular Mass Spectrometry and Proteomics, Vlaming, Hanneke, van Welsem, Tibor, de Graaf, Erik L, Ontoso, David, Altelaar, A F Maarten, San-Segundo, Pedro A, Heck, Albert J R, van Leeuwen, Fred, Sub Biomol.Mass Spectrometry & Proteom., Sub Biomol.Mass Spect. and Proteomics, Biomolecular Mass Spectrometry and Proteomics, Vlaming, Hanneke, van Welsem, Tibor, de Graaf, Erik L, Ontoso, David, Altelaar, A F Maarten, San-Segundo, Pedro A, Heck, Albert J R, and van Leeuwen, Fred

Published
2014

32. Flexibility in crosstalk between H2B ubiquitination and H3 methylation in vivo

Author

Biomolecular Mass Spectrometry and Proteomics, Sub Biomol.Mass Spectrometry & Proteom., Sub Biomol.Mass Spect. and Proteomics, Vlaming, Hanneke, van Welsem, Tibor, de Graaf, Erik L, Ontoso, David, Altelaar, A F Maarten, San-Segundo, Pedro A, Heck, Albert J R, van Leeuwen, Fred, Biomolecular Mass Spectrometry and Proteomics, Sub Biomol.Mass Spectrometry & Proteom., Sub Biomol.Mass Spect. and Proteomics, Vlaming, Hanneke, van Welsem, Tibor, de Graaf, Erik L, Ontoso, David, Altelaar, A F Maarten, San-Segundo, Pedro A, Heck, Albert J R, and van Leeuwen, Fred

Published
2014

33. Flexibility in crosstalk between H2B ubiquitination and H3 methylation in vivo

Author

Dutch Cancer Society, Netherlands Genomics Initiative, Vlaming, Hanneke, Welsem, Tibor van, Graaf, Erik L. de, Ontoso, David, Maarten Altelaar, A. F., San-Segundo, Pedro A., Heck, Albert J. R., Leeuwen, Fred van, Dutch Cancer Society, Netherlands Genomics Initiative, Vlaming, Hanneke, Welsem, Tibor van, Graaf, Erik L. de, Ontoso, David, Maarten Altelaar, A. F., San-Segundo, Pedro A., Heck, Albert J. R., and Leeuwen, Fred van

Abstract

Histone H2B ubiquitination is a dynamic modification that promotes methylation of histone H3K79 and H3K4. This crosstalk is important for the DNA damage response and has been implicated in cancer. Here, we show that in engineered yeast strains, ubiquitins tethered to every nucleosome promote H3K79 and H3K4 methylation from a proximal as well as a more distal site, but only if in a correct orientation. This plasticity indicates that the exact location of the attachment site, the native ubiquitin-lysine linkage and ubiquitination cycles are not critical for trans-histone crosstalk in vivo. The flexibility in crosstalk also indicates that other ubiquitination events may promote H3 methylation.

Published
2014

Catalog

Books, media, physical & digital resources
See catalog results