Your search keyword '"Alex J. Kuo"' showing total 15 results

1. New-Onset IgG Autoantibodies in Hospitalized Patients with COVID-19

Author

Rong Mao, William H. Robinson, Sarah Greib, Kari C. Nadeau, Judith A. James, Iris Chang, Peggie Cheung, Andrew Gaano, Richard Wittman, Prasanna Jagannathan, Maja Artandi, Andreas Neubauer, Peter S. Kim, Monali Manohar, Payton A. Weidenbacher, Paul J. Utz, Chrysanthi Skevaki, Joyce Gonzalez, Kate Bennett, Shaurya Dhingra, Harald Renz, Wenzhao Meng, Taia T. Wang, Indira Neeli, Nuala J. Meyer, Alex J. Kuo, Sharon Chinthrajah, Neera Ahuja, Upinder Singh, Margrit Gündisch, Elisabeth Mack, Rajan Puri, Linda Barman, Allan Feng, Saborni Chakraborty, Marko Z. Radic, Abigail E. Powell, Ho-Ryun Chung, Sarah Esther Chang, Alex Ren Hsu, Sokratis A. Apostolidis, E. John Wherry, Heather M. Giannini, Jeffrey M. Schapiro, Reinhard Geßner, Amanda Finck, Evan Do, Eline T. Luning Prak, and Oluwatosin Oniyide

Subjects

Male, Methyltransferase, Coronavirus disease 2019 (COVID-19), Science, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), viruses, General Physics and Astronomy, Connective tissue, Autoimmunity, Antibodies, Viral, Autoantigens, General Biochemistry, Genetics and Molecular Biology, Immunoglobulin G, Article, Antibodies, Viral Proteins, Immune system, Humans, Medicine, Respiratory system, Connective Tissue Diseases, skin and connective tissue diseases, Myositis, Aged, Autoantibodies, NSP1, Multidisciplinary, biology, business.industry, SARS-CoV-2, fungi, Autoantibody, COVID-19, General Chemistry, Middle Aged, medicine.disease, Hospitalization, body regions, medicine.anatomical_structure, Viral infection, Antibodies, Antinuclear, Immunology, biology.protein, Cytokines, Female, Antibody, business

Abstract

COVID-19 is associated with a wide range of clinical manifestations, including autoimmune features and autoantibody production. Here we develop three protein arrays to measure IgG autoantibodies associated with connective tissue diseases, anti-cytokine antibodies, and anti-viral antibody responses in serum from 147 hospitalized COVID-19 patients. Autoantibodies are identified in approximately 50% of patients but in less than 15% of healthy controls. When present, autoantibodies largely target autoantigens associated with rare disorders such as myositis, systemic sclerosis and overlap syndromes. A subset of autoantibodies targeting traditional autoantigens or cytokines develop de novo following SARS-CoV-2 infection. Autoantibodies track with longitudinal development of IgG antibodies recognizing SARS-CoV-2 structural proteins and a subset of non-structural proteins, but not proteins from influenza, seasonal coronaviruses or other pathogenic viruses. We conclude that SARS-CoV-2 causes development of new-onset IgG autoantibodies in a significant proportion of hospitalized COVID-19 patients and are positively correlated with immune responses to SARS-CoV-2 proteins., Infection with SARS-CoV2 and the development of Coronavirus disease 2019 (COVID-19) has been linked to induction of autoimmunity and autoantibody production. Here the authors characterise the new-onset IgG autoantibody response in hospitalised patients with COVID-19 which they correlate to the magnitude of the SARS-CoV2 response.

Published

2021

2. The single-cell epigenomic and transcriptional landscape of immunity to influenza vaccination

Author

Peggie Cheung, Steven E. Bosinger, Robbert van der Most, Florian Wimmers, Mariko Hinton Foecke, Michele Donato, Chunfeng Li, Sarah E. Chang, Purvesh Khatri, Nadine Rouphael, Mark M. Davis, Mai Dvorak, Shankar Subramaniam, Mario Cortese, Nir Yosef, Alex J. Kuo, Sanne E. de Jong, Tal Ashuach, Paul J. Utz, Holden T. Maecker, Shakti Gupta, Bali Pulendran, and Thomas Hagan

Subjects

Epigenomics, Male, History, Transcription, Genetic, alpha-Tocopherol, Polysorbates, Antigens, CD34, medicine.disease_cause, Histones, Epigenome, 0302 clinical medicine, Interferon, Myeloid Cells, Vaccines, 0303 health sciences, Toll-Like Receptors, Vaccination, Cellular Reprogramming, Research Highlight, Chromatin, Computer Science Applications, Anti-Bacterial Agents, Causality, Drug Combinations, medicine.anatomical_structure, Influenza Vaccines, Interferon Type I, Cytokines, Female, Single-Cell Analysis, medicine.drug, Adult, Squalene, Adolescent, Biology, Antiviral Agents, General Biochemistry, Genetics and Molecular Biology, Article, Education, 03 medical and health sciences, Young Adult, Immunity, medicine, Humans, Monocytes and macrophages, 030304 developmental biology, Innate immune system, Influenza A Virus, H5N1 Subtype, Monocyte, Influenza A virus subtype H5N1, Immunity, Innate, Transcription Factor AP-1, Gene Expression Regulation, Immunology, Transcriptome, 030217 neurology & neurosurgery

Abstract

Emerging evidence indicates a fundamental role for the epigenome in immunity. Here, we mapped the epigenomic and transcriptional landscape of immunity to influenza vaccination in humans at the single-cell level. Vaccination against seasonal influenza induced persistently diminished H3K27ac in monocytes and myeloid dendritic cells (mDCs), which was associated with impaired cytokine responses to Toll-like receptor stimulation. Single-cell ATAC-seq analysis revealed an epigenomically distinct subcluster of monocytes with reduced chromatin accessibility at AP-1-targeted loci after vaccination. Similar effects were observed in response to vaccination with the AS03-adjuvanted H5N1 pandemic influenza vaccine. However, this vaccine also stimulated persistently increased chromatin accessibility at interferon response factor (IRF) loci in monocytes and mDCs. This was associated with elevated expression of antiviral genes and heightened resistance to the unrelated Zika and Dengue viruses. These results demonstrate that vaccination stimulates persistent epigenomic remodeling of the innate immune system and reveal AS03's potential as an epigenetic adjuvant.

Published

2021

3. Single-cell epigenetics – Chromatin modification atlas unveiled by mass cytometry

Author

Sarah E. Chang, Steven Schaffert, Mai Dvorak, Aditya M Rao, Peggie Cheung, Michele Donato, Alex J. Kuo, Francesco Vallania, Paul J. Utz, Purvesh Khatri, and Rong Mao

Subjects

0301 basic medicine, Immunology, Cell, Computational biology, Mass Spectrometry, Article, Epigenesis, Genetic, Histones, 03 medical and health sciences, Immune system, medicine, Humans, Immunology and Allergy, Mass cytometry, Epigenetics, biology, Flow Cytometry, Phenotype, Chromatin, Histone Code, 030104 developmental biology, Histone, medicine.anatomical_structure, biology.protein, Single-Cell Analysis, Protein Processing, Post-Translational, Cytometry

Abstract

Modifications of histone proteins are fundamental to the regulation of epigenetic phenotypes. Dysregulations of histone modifications have been linked to the pathogenesis of diverse human diseases. However, identifying differential histone modifications in patients with immune-mediated diseases has been challenging, in part due to the lack of a powerful analytic platform to study histone modifications in the complex human immune system. We recently developed a highly multiplexed platform, Epigenetic landscape profiling using cytometry by Time-Of-Flight (EpiTOF), to analyze the global levels of a broad array of histone modifications in single cells using mass cytometry. In this review, we summarize the development of EpiTOF and discuss its potential applications in biomedical research. We anticipate that this platform will provide new insights into the roles of epigenetic regulation in hematopoiesis, immune cell functions, and immune system aging, and reveal aberrant epigenetic patterns associated with immune-mediated diseases.

Published

2018

4. Repression of CTSG, ELANE and PRTN3-mediated histone H3 proteolytic cleavage promotes monocyte-to-macrophage differentiation

Author

Joshua E. Elias, Claudia Macaubas, Peggie Cheung, Peter A. Nigrovic, Alexei A. Grom, Paul J. Utz, Or Gozani, Tie-Mei Li, Purvesh Khatri, Lauren A. Henderson, Michele Donato, Elizabeth D. Mellins, John P. Coan, Grant S. Schulert, Lichao Zhang, Sarah E. Chang, Steven Schaffert, Mai Dvorak, Mariko Hinton Foecke, and Alex J. Kuo

Subjects

0301 basic medicine, Epigenomics, Male, Cathepsin G, THP-1 Cells, Epigenesis, Genetic, Histones, chemistry.chemical_compound, Gene Knockout Techniques, Jurkat Cells, 0302 clinical medicine, Immunology and Allergy, Macrophage, RNA-Seq, Child, Cell Differentiation, Chromatin, Recombinant Proteins, Cell biology, medicine.anatomical_structure, Histone, Neutrophil elastase, Child, Preschool, Female, Adolescent, Myeloblastin, Immunology, Primary Cell Culture, Biology, 03 medical and health sciences, Histone H3, Young Adult, medicine, Humans, Enzyme Assays, Cell Nucleus, Monocyte, Macrophages, Arthritis, Juvenile, 030104 developmental biology, chemistry, Proteolysis, biology.protein, Leukocytes, Mononuclear, CRISPR-Cas Systems, Leukocyte Elastase, 030215 immunology

Abstract

Chromatin undergoes extensive reprogramming during immune cell differentiation. Here we report the repression of controlled histone H3 amino terminus proteolytic cleavage (H3ΔN) during monocyte-to-macrophage development. This abundant histone mark in human peripheral blood monocytes is catalyzed by neutrophil serine proteases (NSPs) cathepsin G, neutrophil elastase and proteinase 3. NSPs are repressed as monocytes mature into macrophages. Integrative epigenomic analysis reveals widespread H3ΔN distribution across the genome in a monocytic cell line and primary monocytes, which becomes largely undetectable in fully differentiated macrophages. H3ΔN is enriched at permissive chromatin and actively transcribed genes. Simultaneous NSP depletion in monocytic cells results in H3ΔN loss and further increase in chromatin accessibility, which likely primes the chromatin for gene expression reprogramming. Importantly, H3ΔN is reduced in monocytes from patients with systemic juvenile idiopathic arthritis, an autoinflammatory disease with prominent macrophage involvement. Overall, we uncover an epigenetic mechanism that primes the chromatin to facilitate macrophage development. Chromatin undergoes extensive reprogramming during immune cell differentiation. Here Kuo and colleagues uncover an epigenetic mechanism that primes the chromatin to facilitate macrophage development.

Published

2019

5. Single-cell technologies — studying rheumatic diseases one cell at a time

Author

Peggie Cheung, Paul J. Utz, Alex J. Kuo, and Purvesh Khatri

Subjects

0301 basic medicine, Epigenomics, Proteomics, medicine.medical_specialty, Cell, Computational biology, Article, Immune tolerance, Transcriptome, 03 medical and health sciences, 0302 clinical medicine, Immune system, Rheumatology, Internal medicine, Rheumatic Diseases, Medicine, Humans, 030203 arthritis & rheumatology, business.industry, Gene Expression Profiling, Gene expression profiling, 030104 developmental biology, medicine.anatomical_structure, Single-Cell Analysis, business

Abstract

Cells, the basic units of life, have striking differences at transcriptomic, proteomic and epigenomic levels across tissues, organs, organ systems and organisms. The coordination of individual immune cells is essential for the generation of effective immune responses to pathogens while immune tolerance is maintained to protect the host. In rheumatic diseases, when immune responses are dysregulated, pathologically important cells might represent only a small fraction of the immune system. Interrogation of the contributions of individual immune cells to pathogenesis and disease progression should therefore reveal important insights into the complicated aetiology of rheumatic diseases. Technological advances are enabling the high-dimensional dissection of single cells at multiple omics levels, which could facilitate the identification of dysregulated molecular mechanisms in patients with rheumatic diseases and the discovery of new therapeutic targets and biomarkers. The single-cell technologies that have been developed over the past decade and the experimental platforms that enable multi-omics integrative analyses have already made inroads into immunology-related fields of study and have potential for use in rheumatology. Layers of omics data derived from single cells are likely to fundamentally change our understanding of the molecular pathways that underpin the pathogenesis of rheumatic diseases. Single-cell sequencing technologies enable transcriptomic, epigenomic and proteomic analysis of rare or heterogeneous populations of cells. In this Review, Kuo and colleagues discuss current and future uses of single-cell sequencing technologies for rheumatology research.

Published

2019

6. Single-Cell Chromatin Modification Profiling Reveals Increased Epigenetic Variations with Aging

Author

Mark M. Davis, Michele Donato, Francesco Vallania, Sarah E. Chang, Cornelia L. Dekker, Peggie Cheung, Steven Schaffert, Hayley Warsinske, Alex J. Kuo, Mai Dvorak, Paul J. Utz, and Purvesh Khatri

Subjects

Epigenomics, 0301 basic medicine, Adult, Male, Aging, Adolescent, Cell, Cell Separation, Article, General Biochemistry, Genetics and Molecular Biology, Monocytes, Flow cytometry, Epigenesis, Genetic, Immunophenotyping, Histones, 03 medical and health sciences, Young Adult, Immune system, medicine, Diseases in Twins, Humans, Mass cytometry, Cell Lineage, Epigenetics, Registries, Cellular Senescence, Aged, Principal Component Analysis, biology, medicine.diagnostic_test, Middle Aged, medicine.disease, Flow Cytometry, Chromatin, Cell biology, 030104 developmental biology, Histone, medicine.anatomical_structure, Immune System, biology.protein, Leukocytes, Mononuclear, Female, Protein Processing, Post-Translational, Transcriptional noise

Abstract

Post-translational modifications of histone proteins and exchanges of histone variants of chromatin are central to the regulation of nearly all DNA-templated biological processes. However, the degree and variability of chromatin modifications in specific human immune cells remain largely unknown. Here, we employ a highly multiplexed mass cytometry analysis to profile the global levels of a broad array of chromatin modifications in primary human immune cells at the single-cell level. Our data reveal markedly different cell-type- and hematopoietic-lineage-specific chromatin modification patterns. Differential analysis between younger and older adults shows that aging is associated with increased heterogeneity between individuals and elevated cell-to-cell variability in chromatin modifications. Analysis of a twin cohort unveils heritability of chromatin modifications and demonstrates that aging-related chromatin alterations are predominantly driven by non-heritable influences. Together, we present a powerful platform for chromatin and immunology research. Our discoveries highlight the profound impacts of aging on chromatin modifications.

Published

2018

7. Chd5 Requires PHD-Mediated Histone 3 Binding for Tumor Suppression

Author

Thomas Schalch, Alea A. Mills, Hannes Vogel, Molly Hammell, Shilpi Paul, Leemor Joshua-Tor, Alex J. Kuo, Or Gozani, and W. Richard McCombie

Subjects

Models, Molecular, Molecular Sequence Data, Plasma protein binding, medicine.disease_cause, Methylation, Article, General Biochemistry, Genetics and Molecular Biology, Chromodomain, Histones, Mice, Neuroblastoma, Structure-Activity Relationship, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, medicine, Animals, Humans, Amino Acid Sequence, lcsh:QH301-705.5, Cell Proliferation, 030304 developmental biology, Homeodomain Proteins, 0303 health sciences, Mutation, Genome, biology, Lysine, Binding protein, DNA Helicases, Cell Differentiation, Molecular biology, 3. Good health, Cell biology, Chromatin, Cell Transformation, Neoplastic, Histone, lcsh:Biology (General), Genetic Loci, 030220 oncology & carcinogenesis, biology.protein, Peptides, Carcinogenesis, Chromatin immunoprecipitation, Protein Binding

Abstract

SummaryChromodomain Helicase DNA binding protein 5 (CHD5) is a tumor suppressor mapping to 1p36, a genomic region that is frequently deleted in human cancer. Although CHD5 belongs to the CHD family of chromatin-remodeling proteins, whether its tumor-suppressive role involves an interaction with chromatin is unknown. Here we report that Chd5 binds the unmodified N terminus of H3 through its tandem plant homeodomains (PHDs). Genome-wide chromatin immunoprecipitation studies reveal preferential binding of Chd5 to loci lacking the active mark H3K4me3 and also identify Chd5 targets implicated in cancer. Chd5 mutations that abrogate H3 binding are unable to inhibit proliferation or transcriptionally modulate target genes, which leads to tumorigenesis in vivo. Unlike wild-type Chd5, Chd5-PHD mutants are unable to induce differentiation or efficiently suppress the growth of human neuroblastoma in vivo. Our work defines Chd5 as an N-terminally unmodified H3-binding protein and provides functional evidence that this interaction orchestrates chromatin-mediated transcriptional programs critical for tumor suppression.

Published

2013

8. NSD2 Links Dimethylation of Histone H3 at Lysine 36 to Oncogenic Programming

Author

Peggie Cheung, Yuanxin Xi, Alex J. Kuo, Ben Ho Park, Mitomu Kioi, Xiaobing Shi, Wei Li, Barry M. Zee, Or Gozani, Josh Lauring, Benjamin A. Garcia, and Kaifu Chen

Subjects

Transcription, Genetic, Mice, SCID, Methylation, Article, Translocation, Genetic, Histones, Mice, Histone H3, Transcription (biology), Animals, Humans, Histone code, Molecular Biology, Regulation of gene expression, biology, Gene Expression Profiling, Lysine, Histone-Lysine N-Methyltransferase, Cell Biology, Xenograft Model Antitumor Assays, Chromatin, Recombinant Proteins, Repressor Proteins, Cell Transformation, Neoplastic, Histone, Gene Expression Regulation, Histone methyltransferase, biology.protein, Cancer research, Multiple Myeloma, Genome-Wide Association Study, Signal Transduction

Abstract

The histone lysine methyltransferase NSD2 (MMSET/WHSC1) is implicated in diverse diseases and commonly overexpressed in multiple myeloma due to a recurrent t(4;14) chromosomal translocation. However, the precise catalytic activity of NSD2 is obscure, preventing progress in understanding how this enzyme influences chromatin biology and myeloma pathogenesis. Here, we show that dimethylation of histone H3 at lysine 36 (H3K36me2) is the principal chromatin-regulatory activity of NSD2. Catalysis of H3K36me2 by NSD2 is sufficient for gene activation. In t(4;14)-positive myeloma cells, the normal genome-wide and gene-specific distribution of H3K36me2 is obliterated, creating a chromatin landscape that selects for a transcription profile favorable for myelomagenesis. Catalytically active NSD2 confers xenograft tumor formation upon t(4;14)-negative cells and promotes oncogenic transformation of primary cells in an H3K36me2-dependent manner. Together, our findings establish H3K36me2 as the primary product generated by NSD2 and demonstrate that genomic disorganization of this canonical chromatin mark by NSD2 initiates oncogenic programming.

Published

2011

9. Binding of the MLL PHD3 Finger to Histone H3K4me3 Is Required for MLL-Dependent Gene Transcription

Author

Tatiana G. Kutateladze, Li Zhu, Robert A. Hom, Pei-Yun Chang, Alex J. Kuo, Or Gozani, Catherine A. Musselman, and Michael L. Cleary

Subjects

Models, Molecular, Transcription, Genetic, Recombinant Fusion Proteins, Molecular Sequence Data, Methylation, Proto-Oncogene Mas, Protein Structure, Secondary, Article, Cell Line, Histones, Histone H3, Structural Biology, hemic and lymphatic diseases, Animals, Humans, Amino Acid Sequence, Epigenetics, Nuclear Magnetic Resonance, Biomolecular, neoplasms, Molecular Biology, Regulation of gene expression, biology, Lysine, Molecular biology, Protein Structure, Tertiary, Chromatin, Histone, Gene Expression Regulation, PHD finger, Histone methyltransferase, Mutagenesis, Site-Directed, biology.protein, H3K4me3, Cattle, Sequence Alignment, Myeloid-Lymphoid Leukemia Protein, Protein Binding

Abstract

The MLL (Mixed Lineage Leukemia) proto-oncogene encodes a histone methyltransferase that creates the methylated histone H3K4 epigenetic marks, commonly associated with actively transcribed genes. In addition to its canonical histone methyltransferase SET domain, the MLL protein contains three plant homeodomain (PHD) fingers that are well conserved between species but whose potential roles and requirements for MLL function are unknown. Here we demonstrate that the third PHD domain of MLL (PHD3) binds histone H3 trimethylated at lysine 4 (H3K4me3) with high affinity and specificity, and H3K4me2 with eight-fold lower affinity. Biochemical and structural analysis using NMR and fluorescence spectroscopy identified key amino acids essential for the interaction with H3K4me3. Site-directed mutations of the residues involved in recognition of H3K4me3 compromised in vitro H3K4me3 binding but not in vivo localization of full-length MLL to chromatin sites in target promoters of MEIS1 and HOXA genes. Whereas intact PHD3 finger was necessary for MLL occupancy at these promoters, H3K4me3 binding was critical for MLL transcriptional activity. These results demonstrate that MLL occupancy and target gene activation can be functionally separated. Furthermore, these findings reveal that MLL not only “writes” the H3K4me3 mark, but also binds the mark as well, and this binding is required for the transcriptional maintenance functions of MLL.

Published

2010

10. ING4 Mediates Crosstalk between Histone H3 K4 Trimethylation and H3 Acetylation to Attenuate Cellular Transformation

Author

Matthew D. Simon, Kyle Johnson, Tatiana G. Kutateladze, Alex J. Kuo, Olivier Binda, Or Gozani, Tiffany Hung, Howard Y. Chang, and Karen S. Champagne

Subjects

Models, Molecular, Histone lysine methylation, Protein Conformation, SAP30, Biology, Crystallography, X-Ray, Methylation, Article, Substrate Specificity, Histones, Histone H3, Histone H1, Cell Line, Tumor, Histone methylation, Histone code, Humans, Molecular Biology, Cells, Cultured, Cell Nucleus, Binding Sites, Tumor Suppressor Proteins, Acetylation, Histone acetyltransferase, Cell Biology, Chromatin, Cell biology, Cell Transformation, Neoplastic, Biochemistry, Histone methyltransferase, biology.protein, Peptides

Abstract

Aberrations in chromatin dynamics play a fundamental role in tumorigenesis, yet relatively little is known of the molecular mechanisms linking histone lysine methylation to neoplastic disease. ING4 (Inhibitor of Growth 4) is a native subunit of an HBO1 histone acetyltransferase (HAT) complex and a tumor suppressor protein. Here we show a critical role for the specific read-out of histone H3 trimethylated at lysine 4 (H3K4me3) by the ING4 PHD finger in mediating ING4 gene expression and tumor suppressor functions. The interaction between ING4 and H3K4me3 augments the acetylation activity of HBO1 on H3 tails, and drives H3 acetylation at ING4 target promoters to effect a DNA damage-dependent gene expression program. Further, ING4 facilitates apoptosis in response to genotoxic stress and inhibits anchorage-independent cell growth, and these functions are dependent on ING4 interactions with H3K4me3. Together, our results demonstrate a mechanism for brokering crosstalk between H3K4 methylation and histone H3 acetylation, and reveal a new molecular link between chromatin modulation and tumor suppressor mechanisms.

Published

2009

11. Histone H3K4me3 Binding Is Required for the DNA Repair and Apoptotic Activities of ING1 Tumor Suppressor

Author

H. Lin, Pedro V. Peña, Rui Zhao, G. Li, Robert A. Hom, Alex J. Kuo, Oksana M. Subach, Or Gozani, K.S. Champagne, Vladislav V. Verkhusha, Tatiana G. Kutateladze, R.P.C. Wong, and Tiffany Hung

Subjects

Models, Molecular, DNA Repair, DNA repair, Molecular Sequence Data, Protein Array Analysis, Apoptosis, SAP30, Crystallography, X-Ray, medicine.disease_cause, Methylation, Article, Histones, Histone H3, Structural Biology, Neoplasms, Histone H2A, medicine, Humans, Histone code, Cancer epigenetics, Molecular Biology, biology, Lysine, Tumor Suppressor Proteins, Intracellular Signaling Peptides and Proteins, Nuclear Proteins, Protein Structure, Tertiary, Histone, Biochemistry, Mutation, biology.protein, Peptides, Carcinogenesis, Inhibitor of Growth Protein 1, Protein Binding

Abstract

Inhibitor of growth 1 (ING1) is implicated in oncogenesis, DNA damage repair, and apoptosis. Mutations within the ING1 gene and altered expression levels of ING1 are found in multiple human cancers. Here, we show that both DNA repair and apoptotic activities of ING1 require the interaction of the C-terminal plant homeodomain (PHD) finger with histone H3 trimethylated at Lys4 (H3K4me3). The ING1 PHD finger recognizes methylated H3K4 but not other histone modifications as revealed by the peptide microarrays. The molecular mechanism of the histone recognition is elucidated based on a 2.1 A-resolution crystal structure of the PHD-H3K4me3 complex. The K4me3 occupies a deep hydrophobic pocket formed by the conserved Y212 and W235 residues that make cation-pi contacts with the trimethylammonium group. Both aromatic residues are essential in the H3K4me3 recognition, as substitution of these residues with Ala disrupts the interaction. Unlike the wild-type ING1, the W235A mutant, overexpressed in the stable clones of melanoma cells or in HT1080 cells, was unable to stimulate DNA repair after UV irradiation or promote DNA-damage-induced apoptosis, indicating that H3K4me3 binding is necessary for these biological functions of ING1. Furthermore, N216S, V218I, and G221V mutations, found in human malignancies, impair the ability of ING1 to associate with H3K4me3 or to induce nucleotide repair and cell death, linking the tumorigenic activity of ING1 with epigenetic regulation. Together, our findings reveal the critical role of the H3K4me3 interaction in mediating cellular responses to genotoxic stresses and offer new insight into the molecular mechanism underlying the tumor suppressive activity of ING1.

Published

2008

12. RAG2 PHD finger couples histone H3 lysine 4 trimethylation with V(D)J recombination

Author

Tatiana G. Kutateladze, Dylan Carney, Kay L. Walter, Paul J. Utz, Wei Yang, Marjorie A. Oettinger, David N. Ciccone, Santiago Ramón-Maiques, Yang Shi, Sunmi Han, Mercedes Gallardo, Adam G. W. Matthews, Alex J. Kuo, Karen S. Champagne, Dmitri N. Ivanov, Peggie Cheung, and Or Gozani

Subjects

Models, Molecular, Histone H3 Lysine 4, Amino Acid Motifs, Biology, Methylation, Article, Substrate Specificity, Histones, Mice, Structure-Activity Relationship, Histone H3, Histone H1, Histone methylation, Histone H2A, Animals, Humans, Histone code, Gene Rearrangement, B-Lymphocyte, VDJ Recombinases, Homeodomain Proteins, Recombination, Genetic, Genetics, Binding Sites, Multidisciplinary, Lysine, V(D)J recombination, Immunologic Deficiency Syndromes, Tryptophan, DNA-Binding Proteins, Histone methyltransferase, Protein Binding

Abstract

Nuclear processes such as transcription, DNA replication and recombination are dynamically regulated by chromatin structure. Eukaryotic transcription is known to be regulated by chromatin-associated proteins containing conserved protein domains that specifically recognize distinct covalent post-translational modifications on histones. However, it has been unclear whether similar mechanisms are involved in mammalian DNA recombination. Here we show that RAG2--an essential component of the RAG1/2 V(D)J recombinase, which mediates antigen-receptor gene assembly--contains a plant homeodomain (PHD) finger that specifically recognizes histone H3 trimethylated at lysine 4 (H3K4me3). The high-resolution crystal structure of the mouse RAG2 PHD finger bound to H3K4me3 reveals the molecular basis of H3K4me3-recognition by RAG2. Mutations that abrogate RAG2's recognition of H3K4me3 severely impair V(D)J recombination in vivo. Reducing the level of H3K4me3 similarly leads to a decrease in V(D)J recombination in vivo. Notably, a conserved tryptophan residue (W453) that constitutes a key structural component of the K4me3-binding surface and is essential for RAG2's recognition of H3K4me3 is mutated in patients with immunodeficiency syndromes. Together, our results identify a new function for histone methylation in mammalian DNA recombination. Furthermore, our results provide the first evidence indicating that disrupting the read-out of histone modifications can cause an inherited human disease.

Published

2007

13. The BAH domain of ORC1 links H4K20me2 to DNA replication licensing and Meier-Gorlin syndrome

Author

Dinshaw J. Patel, Peggie Cheung, Jikui Song, Or Gozani, James K. Chen, Alex J. Kuo, Satoko Ishibe-Murakami, and Sayumi Yamazoe

Subjects

DNA Replication, Models, Molecular, Micrognathism, Origin Recognition Complex, Dwarfism, Replication Origin, Biology, Origin of replication, Crystallography, X-Ray, Methylation, Article, Cell Line, Histones, 03 medical and health sciences, 0302 clinical medicine, Control of chromosome duplication, Histone methylation, Animals, Humans, BAH domain, Growth Disorders, Zebrafish, 030304 developmental biology, Congenital Microtia, Genetics, 0303 health sciences, Multidisciplinary, Lysine, Cell Cycle, DNA replication, Ear, Patella, Zebrafish Proteins, Chromatin, Protein Structure, Tertiary, Disease Models, Animal, Licensing factor, Origin recognition complex, Carrier Proteins, 030217 neurology & neurosurgery

Abstract

The recognition of distinctly modified histones by specialized 'effector' proteins constitutes a key mechanism for transducing molecular events at chromatin to biological outcomes. Effector proteins influence DNA-templated processes, including transcription, DNA recombination and DNA repair; however, no effector functions have yet been identified within the mammalian machinery that regulate DNA replication. Here we show that ORC1--a component of ORC (origin of replication complex), which mediates pre-DNA replication licensing--contains a bromo adjacent homology (BAH) domain that specifically recognizes histone H4 dimethylated at lysine 20 (H4K20me2). Recognition of H4K20me2 is a property common to BAH domains present within diverse metazoan ORC1 proteins. Structural studies reveal that the specificity of the BAH domain for H4K20me2 is mediated by a dynamic aromatic dimethyl-lysine-binding cage and multiple intermolecular contacts involving the bound peptide. H4K20me2 is enriched at replication origins, and abrogating ORC1 recognition of H4K20me2 in cells impairs ORC1 occupancy at replication origins, ORC chromatin loading and cell-cycle progression. Mutation of the ORC1 BAH domain has been implicated in the aetiology of Meier-Gorlin syndrome (MGS), a form of primordial dwarfism, and ORC1 depletion in zebrafish results in an MGS-like phenotype. We find that wild-type human ORC1, but not ORC1-H4K20me2-binding mutants, rescues the growth retardation of orc1 morphants. Moreover, zebrafish depleted of H4K20me2 have diminished body size, mirroring the phenotype of orc1 morphants. Together, our results identify the BAH domain as a novel methyl-lysine-binding module, thereby establishing the first direct link between histone methylation and the metazoan DNA replication machinery, and defining a pivotal aetiological role for the canonical H4K20me2 mark, via ORC1, in primordial dwarfism.

Published

2011

14. The target of the NSD family of histone lysine methyltransferases depends on the nature of the substrate

Author

Or Gozani, Peggie Cheung, Qi Qiao, William J. Drury, Yan Li, Thomas A. Neubert, Alex J. Kuo, Rui-Ming Xu, Patrick Trojer, Danny Reinberg, and Chong-Feng Xu

Subjects

Genetic Vectors, Biology, Biochemistry, Mass Spectrometry, Histone H4, Histones, 03 medical and health sciences, Histone H3, Xenopus laevis, 0302 clinical medicine, Cell Line, Tumor, Histone methylation, Histone H2A, Histone code, Nucleosome, Animals, Humans, Transcription, Chromatin, and Epigenetics, Histone octamer, Molecular Biology, 030304 developmental biology, 0303 health sciences, Lysine, Cell Biology, DNA, Histone-Lysine N-Methyltransferase, Chromatin, Recombinant Proteins, Nucleosomes, Protein Structure, Tertiary, 030220 oncology & carcinogenesis, Histone methyltransferase, Protein Processing, Post-Translational

Abstract

The NSD (nuclear receptor SET domain-containing) family of histone lysine methyltransferases is a critical participant in chromatin integrity as evidenced by the number of human diseases associated with the aberrant expression of its family members. Yet, the specific targets of these enzymes are not clear, with marked discrepancies being reported in the literature. We demonstrate that NSD2 can exhibit disparate target preferences based on the nature of the substrate provided. The NSD2 complex purified from human cells and recombinant NSD2 both exhibit specific targeting of histone H3 lysine 36 (H3K36) when provided with nucleosome substrates, but histone H4 lysine 44 is the primary target in the case of octamer substrates, irrespective of the histones being native or recombinant. This disparity is negated when NSD2 is presented with octamer targets in conjunction with short single- or double-stranded DNA. Although the octamers cannot form nucleosomes, the target is nonetheless nucleosome-specific as is the product, dimethylated H3K36. This study clarifies in part the previous discrepancies reported with respect to NSD targets. We propose that DNA acts as an allosteric effector of NSD2 such that H3K36 becomes the preferred target.

Published

2009

15. Epigenome Microarray Platform for Proteome-Wide Dissection of Chromatin-Signaling Networks

Author

Alexsandra Espejo, Peggie Cheung, Chih Long Liu, Christian Bassi, Alex J. Kuo, Valentina Migliori, Dennis J. Bua, Ernesto Guccione, Bruno Amati, Mark T. Bedford, Fabio Casadio, and Or Gozani

Subjects

Proteome, Protein Array Analysis, lcsh:Medicine, Computational biology, Biology, Molecular Biology/Histone Modification, Chromatin remodeling, Cell Biology/Cell Signaling, Antibodies, Epigenesis, Genetic, Histones, 03 medical and health sciences, Genetics and Genomics/Epigenetics, Human proteome project, Nucleosome, Humans, Molecular Biology/Chromatin Structure, lcsh:Science, 030304 developmental biology, Epigenomics, Genetics, 0303 health sciences, Multidisciplinary, Genome, Human, lcsh:R, 030302 biochemistry & molecular biology, Epigenome, Chromatin, 3. Good health, lcsh:Q, Peptide microarray, Research Article, Protein Binding, Signal Transduction

Abstract

Knowledge of protein domains that function as the biological effectors for diverse post-translational modifications of histones is critical for understanding how nuclear and epigenetic programs are established. Indeed, mutations of chromatin effector domains found within several proteins are associated with multiple human pathologies, including cancer and immunodeficiency syndromes. To date, relatively few effector domains have been identified in comparison to the number of modifications present on histone and non-histone proteins. Here we describe the generation and application of human modified peptide microarrays as a platform for high-throughput discovery of chromatin effectors and for epitope-specificity analysis of antibodies commonly utilized in chromatin research. Screening with a library containing a majority of the Royal Family domains present in the human proteome led to the discovery of TDRD7, JMJ2C, and MPP8 as three new modified histone-binding proteins. Thus, we propose that peptide microarray methodologies are a powerful new tool for elucidating molecular interactions at chromatin.

Published

2009