Your search keyword '"Aaron J. Stonestrom"' showing total 20 results

1. Interrogating Histone Acetylation and BRD4 as Mitotic Bookmarks of Transcription

Author

Simone Sidoli, Gerd A. Blobel, Chris C.-S. Hsiung, Aaron J. Stonestrom, Belinda Giardine, Cheryl A. Keller, Vivek Behera, Nicole Hamagami, Natarajan V. Bhanu, Hongxin Wang, Michael T. Werner, Benjamin A. Garcia, Zuo-Fei Yuan, and Ross C. Hardison

Subjects

0301 basic medicine, BRD4, Transcription, Genetic, Mitosis, Biology, General Biochemistry, Genetics and Molecular Biology, Article, Histones, 03 medical and health sciences, Mice, 0302 clinical medicine, Transcription (biology), Animals, lcsh:QH301-705.5, Gene, Binding protein, Nuclear Proteins, Acetylation, Chromatin, Cell biology, 030104 developmental biology, Histone, lcsh:Biology (General), biology.protein, 030217 neurology & neurosurgery, Transcription Factors

Abstract

In Brief Chromatin reader protein BRD4 is thought to bookmark mitotic chromatin to propagate transcriptional states across mitosis. Behera et al. profiled and perturbed mitotic BRD4 chromatin occupancy to show that BRD4 is dispensable for this process. Instead, BRD4 mitotic chromatin association is likely a mere reflection of mitotically stable histone marks., SUMMARY Global changes in chromatin organization and the cessation of transcription during mitosis are thought to challenge the resumption of appropriate transcription patterns after mitosis. The acetyl-lysine binding protein BRD4 has been previously suggested to function as a transcriptional “bookmark” on mitotic chromatin. Here, genome-wide location analysis of BRD4 in erythroid cells, combined with data normalization and peak characterization approaches, reveals that BRD4 widely occupies mitotic chromatin. However, removal of BRD4 from mitotic chromatin does not impair post-mitotic activation of transcription. Additionally, histone mass spectrometry reveals global preservation of most posttranslational modifications (PTMs) during mitosis. In particular, H3K14ac, H3K27ac, H3K122ac, and H4K16ac widely mark mitotic chromatin, especially at lineagespecific genes, and predict BRD4 mitotic binding genome wide. Therefore, BRD4 is likely not a mitotic bookmark but only a “passenger.” Instead, mitotic histone acetylation patterns may constitute the actual bookmarks that restore lineage-specific transcription patterns after mitosis., Graphical Abstract

Published

2018

2. The BET protein BRD2 cooperates with CTCF to enforce transcriptional and architectural boundaries

Author

Caroline Bartman, Jennifer E. Phillips-Cremins, Michael T. Werner, Sarah C. Hsu, Belinda Giardine, Aaron J. Stonestrom, Peng Huang, Daniel J. Emerson, Cheryl A. Keller, Perry Evans, Christopher R. Edwards, Gerd A. Blobel, Ross C. Hardison, Thomas G. Gilgenast, and Arjun Raj

Subjects

0301 basic medicine, BRD4, CCCTC-Binding Factor, Transcription, Genetic, Chromosomal Proteins, Non-Histone, Recombinant Fusion Proteins, Insulator (genetics), Biology, Transfection, Article, Cell Line, 03 medical and health sciences, Mice, Transcription (biology), Gene expression, Animals, GATA1 Transcription Factor, RNA, Messenger, Molecular Biology, Gene, Embryonic Stem Cells, In Situ Hybridization, Fluorescence, Genetics, Gene Editing, Messenger RNA, Binding Sites, Membrane Transport Proteins, Nuclear Proteins, Cell Biology, Chromatin Assembly and Disassembly, Chromatin, Single Molecule Imaging, Bromodomain, Repressor Proteins, 030104 developmental biology, Enhancer Elements, Genetic, Receptors, Estrogen, CTCF, CRISPR-Cas Systems, Protein Binding, Transcription Factors

Abstract

Bromodomain and extraterminal motif (BET) proteins are pharmacologic targets for the treatment of diverse diseases, yet the roles of individual BET family members remain unclear. We find that BRD2, but not BRD4, co-localizes with the architectural/insulator protein CCCTC-binding factor (CTCF) genome-wide. CTCF recruits BRD2 to co-bound sites whereas BRD2 is dispensable for CTCF occupancy. Disruption of a CTCF/BRD2-occupied element positioned between two unrelated genes enables regulatory influence to spread from one gene to another, suggesting that CTCF and BRD2 form a transcriptional boundary. Accordingly, single-molecule mRNA fluorescence in situ hybridization (FISH) reveals that, upon site-specific CTCF disruption or BRD2 depletion, expression of the two genes becomes increasingly correlated. HiC shows that BRD2 depletion weakens boundaries co-occupied by CTCF and BRD2, but not those that lack BRD2. These findings indicate that BRD2 supports boundary activity, and they raise the possibility that pharmacologic BET inhibitors can influence gene expression in part by perturbing domain boundary function.

Published

2017

3. TAp73 enhances the pentose phosphate pathway and supports cell proliferation

Author

Anthony A. Mancuso, Wenjing Du, Michael D. Brewer, Aaron J. Stonestrom, Mian Wu, Andy J. Minn, Tak W. Mak, Peng Jiang, and Xiaolu Yang

Subjects

Blotting, Western, Breast Neoplasms, Glucosephosphate Dehydrogenase, Biology, Pentose phosphate pathway, Antioxidants, Article, Pentose Phosphate Pathway, Mice, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Ribose, Animals, Humans, Cells, Cultured, Cell Proliferation, 030304 developmental biology, Regulation of gene expression, chemistry.chemical_classification, 0303 health sciences, Reactive oxygen species, Cell growth, Nuclear Proteins, DNA, Cell Biology, Metabolism, Cell biology, Gene Expression Regulation, Neoplastic, Disease Models, Animal, Enzyme, chemistry, Biochemistry, Gene Knockdown Techniques, 030220 oncology & carcinogenesis, Female, Reactive Oxygen Species, Flux (metabolism), NADP

Abstract

TAp73 is a structural homologue of the pre-eminent tumor suppressor p53. However, unlike p53, TAp73 is rarely mutated, and instead is frequently over-expressed in human tumors. It remains unclear whether TAp73 affords an advantage to tumor cells and if so, what is the underlying mechanism. Here we show that TAp73 supports the proliferation of human and mouse tumor cells. TAp73 activates the expression of the glucose-6-phosphate dehydrogenase (G6PD), the rate-limiting enzyme of the pentose phosphate pathway (PPP). By stimulating G6PD, TAp73 increases PPP flux and directs glucose to the production of NADPH and ribose, for the synthesis of macromolecules and detoxification of reactive oxygen species (ROS). The growth defect of TAp73-deficient cells can be rescued by either enforced G6PD expression or the presence of nucleosides plus an ROS scavenger. These findings establish a critical role for TAp73 in regulating metabolism, and connect TAp73 and the PPP to oncogenic cell growth.

Published

2013

4. A hyperactive transcriptional state marks genome reactivation at the mitosis–G1 transition

Author

Laavanya Sankaranarayanan, Peng Huang, Paul Ginart, Aaron J. Stonestrom, Ross C. Hardison, Carolyne J. Face, Caroline Bartman, Cheryl A. Keller, Kristen S. Jahn, Chris C.-S. Hsiung, Belinda Giardine, Arjun Raj, Perry Evans, and Gerd A. Blobel

Subjects

0301 basic medicine, Transcriptional Activation, Erythroblasts, Mitosis, RNA polymerase II, Enhancer RNAs, Cell Line, 03 medical and health sciences, Mice, Transcription (biology), Genetics, Animals, Enhancer, Promoter Regions, Genetic, Transcription factor, Cells, Cultured, Genome, biology, Cell Cycle, G1 Phase, Molecular biology, Chromatin, Up-Regulation, 030104 developmental biology, Terminator (genetics), Enhancer Elements, Genetic, biology.protein, DNA, Intergenic, Developmental Biology, Research Paper

Abstract

During mitosis, RNA polymerase II (Pol II) and many transcription factors dissociate from chromatin, and transcription ceases globally. Transcription is known to restart in bulk by telophase, but whether de novo transcription at the mitosis–G1 transition is in any way distinct from later in interphase remains unknown. We tracked Pol II occupancy genome-wide in mammalian cells progressing from mitosis through late G1. Unexpectedly, during the earliest rounds of transcription at the mitosis–G1 transition, ∼50% of active genes and distal enhancers exhibit a spike in transcription, exceeding levels observed later in G1 phase. Enhancer–promoter chromatin contacts are depleted during mitosis and restored rapidly upon G1 entry but do not spike. Of the chromatin-associated features examined, histone H3 Lys27 acetylation levels at individual loci in mitosis best predict the mitosis–G1 transcriptional spike. Single-molecule RNA imaging supports that the mitosis–G1 transcriptional spike can constitute the maximum transcriptional activity per DNA copy throughout the cell division cycle. The transcriptional spike occurs heterogeneously and propagates to cell-to-cell differences in mature mRNA expression. Our results raise the possibility that passage through the mitosis–G1 transition might predispose cells to diverge in gene expression states.

Published

2016

5. Molecular Basis and Consequences of the Cytochrome c-tRNA Interaction*

Author

Jeongsik Yong, Xiaolu Yang, Cuiping Liu, Thomas Christian, Ya-Ming Hou, Ryuichi Takase, and Aaron J. Stonestrom

Subjects

0301 basic medicine, Saccharomyces cerevisiae Proteins, Cytochrome, Apoptosis, Saccharomyces cerevisiae, Biochemistry, 03 medical and health sciences, Cytochrome C1, RNA, Transfer, Cytochrome c oxidase, Animals, Humans, Protein Structure, Quaternary, Molecular Biology, biology, Cytochrome c, Cytochrome P450 reductase, Cytochromes c, Cell Biology, TRNA binding, Cell biology, 030104 developmental biology, Coenzyme Q – cytochrome c reductase, biology.protein, Cattle, Apoptosome, Protein Binding

Abstract

The intrinsic apoptosis pathway occurs through the release of mitochondrial cytochrome c to the cytosol, where it promotes activation of the caspase family of proteases. The observation that tRNA binds to cytochrome c revealed a previously unexpected mode of apoptotic regulation. However, the molecular characteristics of this interaction, and its impact on each interaction partner, are not well understood. Using a novel fluorescence assay, we show here that cytochrome c binds to tRNA with an affinity comparable with other tRNA-protein binding interactions and with a molecular ratio of ∼3:1. Cytochrome c recognizes the tertiary structural features of tRNA, particularly in the core region. This binding is independent of the charging state of tRNA but is regulated by the redox state of cytochrome c. Compared with reduced cytochrome c, oxidized cytochrome c binds to tRNA with a weaker affinity, which correlates with its stronger pro-apoptotic activity. tRNA binding both facilitates cytochrome c reduction and inhibits the peroxidase activity of cytochrome c, which is involved in its release from mitochondria. Together, these findings provide new insights into the cytochrome c-tRNA interaction and apoptotic regulation.

Published

2016

6. Targeting recombinant thrombomodulin fusion protein to red blood cells provides multifaceted thromboprophylaxis

Author

John P. Atkinson, Samira Tliba, Aaron J. Stonestrom, Sergei Zaitsev, Bi-Sen Ding, Michael Neyman, Charles T. Esmon, M. Anna Kowalska, Ronald Carnemolla, Vladimir R. Muzykantov, Douglas B. Cines, Dirk Spitzer, and Mortimer Poncz

Subjects

Erythrocytes, Recombinant Fusion Proteins, Thrombomodulin, Immunology, Inflammation, Chemoprevention, Models, Biological, Biochemistry, Fibrin, Thrombosis and Hemostasis, Mice, Drug Delivery Systems, Thrombin, medicine, Animals, Humans, Platelet, Molecular Targeted Therapy, Platelet activation, Cells, Cultured, biology, business.industry, Thrombosis, Cell Biology, Hematology, Molecular biology, Blood proteins, biology.protein, Drosophila, medicine.symptom, business, Protein C, Protein Binding, Single-Chain Antibodies, medicine.drug

Abstract

Thrombin generates fibrin and activates platelets and endothelium, causing thrombosis and inflammation. Endothelial thrombomodulin (TM) changes thrombin's substrate specificity toward cleavage of plasma protein C into activated protein C (APC), which opposes its thrombotic and inflammatory activities. Endogenous TM activity is suppressed in pathologic conditions, and antithrombotic interventions involving soluble TM are limited by rapid blood clearance. To overcome this problem, we fused TM with a single chain fragment (scFv) of an antibody targeted to red blood cells. scFv/TM catalyzes thrombin-mediated generation of activated protein C and binds to circulating RBCs without apparent damage, thereby prolonging its circulation time and bioavailability orders of magnitude compared with soluble TM. In animal models, a single dose of scFv/TM, but not soluble TM, prevents platelet activation and vascular occlusion by clots. Thus, scFv/TM serves as a prodrug and provides thromboprophylaxis at low doses (0.15 mg/kg) via multifaceted mechanisms inhibiting platelets and coagulation.

Published

2012

7. DOT1L/KMT4 Recruitment and H3K79 Methylation Are Ubiquitously Coupled with Gene Transcription in Mammalian Cells

Author

Aaron J. Stonestrom, Adam L. Vakoc, Mitchell A. Lazar, Gerd A. Blobel, Martina I. Lefterova, Lei Ying, Junjie Chen, Michael Schupp, Christopher R. Vakoc, Ja Eun Kim, David J. Steger, and David Zhuo

Subjects

CD36 Antigens, Chromatin Immunoprecipitation, Transcription, Genetic, Methylation, Histones, Mice, Transcription (biology), Adipocytes, Animals, GATA1 Transcription Factor, Molecular Biology, Transcription factor, Cells, Cultured, Regulation of gene expression, biology, Lysine, Sodium Dodecyl Sulfate, Cell Differentiation, Articles, Histone-Lysine N-Methyltransferase, Methyltransferases, Cell Biology, DOT1L, Molecular biology, Chromatin, Globins, Mice, Inbred C57BL, PPAR gamma, Histone, biology.protein, Chromatin immunoprecipitation

Abstract

The histone H3 lysine 79 methyltransferase DOT1L/KMT4 can promote an oncogenic pattern of gene expression through binding with several MLL fusion partners found in acute leukemia. However, the normal function of DOT1L in mammalian gene regulation is poorly understood. Here we report that DOT1L recruitment is ubiquitously coupled with active transcription in diverse mammalian cell types. DOT1L preferentially occupies the proximal transcribed region of active genes, correlating with enrichment of H3K79 di- and trimethylation. Furthermore, Dot1l mutant fibroblasts lacked H3K79 di- and trimethylation at all sites examined, indicating that DOT1L is the sole enzyme responsible for these marks. Importantly, we identified chromatin immunoprecipitation (ChIP) assay conditions necessary for reliable H3K79 methylation detection. ChIP-chip tiling arrays revealed that levels of all degrees of genic H3K79 methylation correlate with mRNA abundance and dynamically respond to changes in gene activity. Conversion of H3K79 monomethylation into di- and trimethylation correlated with the transition from low- to high-level gene transcription. We also observed enrichment of H3K79 monomethylation at intergenic regions occupied by DNA-binding transcriptional activators. Our findings highlight several similarities between the patterning of H3K4 methylation and that of H3K79 methylation in mammalian chromatin, suggesting a widespread mechanism for parallel or sequential recruitment of DOT1L and MLL to genes in their normal "on" state.

Published

2008

8. Transport capabilities of eleven gram-positive bacteria: Comparative genomic analyses

Author

Ravi D. Barabote, Li-Wen Huang, Can Tran, Rikki N. Hvorup, Aaron J. Stonestrom, Graciela L. Lorca, David S. H. Kim, Milton H. Saier, Brit Winnen, Elizabeth Nguyen, and Vladimir Zlotopolski

Subjects

Gram-positive bacteria, Biophysics, Biology, Gram-Positive Bacteria, Biochemistry, Article, Microbiology, Bacterial genetics, 03 medical and health sciences, Species Specificity, Energetics, Lactic acid bacteria, Phylogeny, 030304 developmental biology, 2. Zero hunger, 0303 health sciences, 030306 microbiology, Transport proteins, Biological Transport, Brevibacterium, Genomics, Cell Biology, PEP group translocation, Genomic analyses, biology.organism_classification, Transmembrane protein, Major facilitator superfamily, Metabolism, Efflux, Carrier Proteins, Genome, Bacterial, Bacteria, Signal Transduction

Abstract

The genomes of eleven Gram-positive bacteria that are important for human health and the food industry, nine low G+C lactic acid bacteria and two high G+C Gram-positive organisms, were analyzed for their complement of genes encoding transport proteins. Thirteen to eighteen percent of their genes encode transport proteins, larger percentages than observed for most other bacteria. All of these bacteria possess channel proteins, some of which probably function to relieve osmotic stress. Amino acid uptake systems predominate over sugar and peptide cation symporters, and of the sugar uptake porters, those specific for oligosaccharides and glycosides often outnumber those for free sugars. About 10% of the total transport proteins are constituents of putative multidrug efflux pumps with Major Facilitator Superfamily (MFS)-type pumps (55%) being more prevalent than ATP-binding cassette (ABC)-type pumps (33%), which, however, usually greatly outnumber all other types. An exception to this generalization is Streptococcus thermophilus with 54% of its drug efflux pumps belonging to the ABC superfamily and 23% belonging each to the Multidrug/Oligosaccharide/Polysaccharide (MOP) superfamily and the MFS. These bacteria also display peptide efflux pumps that may function in intercellular signalling, and macromolecular efflux pumps, many of predictable specificities. Most of the bacteria analyzed have no pmf-coupled or transmembrane flow electron carriers. The one exception is Brevibacterium linens, which in addition to these carriers, also has transporters of several families not represented in the other ten bacteria examined. Comparisons with the genomes of organisms from other bacterial kingdoms revealed that lactic acid bacteria possess distinctive proportions of recognized transporter types (e.g., more porters specific for glycosides than reducing sugars). Some homologues of transporters identified had previously been identified only in Gram-negative bacteria or in eukaryotes. Our studies reveal unique characteristics of the lactic acid bacteria such as the universal presence of genes encoding mechanosensitive channels, competence systems and large numbers of sugar transporters of the phosphotransferase system. The analyses lead to important physiological predictions regarding the preferred signalling and metabolic activities of these industrially important bacteria.

Published

2007

9. Erythropoiesis provides a BRD's eye view of BET protein function

Author

Gerd A. Blobel, Michael T. Werner, Aaron J. Stonestrom, and Sarah C. Hsu

Subjects

0301 basic medicine, Protein function, BRD4, Protein family, Nuclear Proteins, chemical and pharmacologic phenomena, hemic and immune systems, Biology, Bioinformatics, Chromatin, Article, Bromodomain, 03 medical and health sciences, 030104 developmental biology, Protein Domains, Drug Discovery, Molecular Medicine, Erythropoiesis, Animals, Humans, Transcription Factors

Abstract

Pharmacologic inhibitors of the bromodomain and extra-terminal motif (BET) protein family are in clinical trials for the treatment of hematologic malignancies, yet the functions of individual BET proteins remain largely uncharacterized. We review the molecular roles of BETs in the context of erythropoiesis. Studies in this lineage have provided valuable insights into their mechanisms of action, and helped define the individual and overlapping functions of BET protein family members BRD2, BRD3, and BRD4. These studies have important ramifications for our understanding of the molecular and physiologic roles of BET proteins, and provide a framework for elucidating some of the beneficial and adverse effects of pharmacologic inhibitors.

Published

2015

10. Occupancy by key transcription factors is a more accurate predictor of enhancer activity than histone modifications or chromatin accessibility

Author

Ross C. Hardison, Yong Cheng, Cheryl A. Keller, Maria Long, Len A. Pennacchio, Aaron J. Stonestrom, Axel Visel, Weisheng Wu, Christapher S. Morrissey, Deepti Jain, Nergiz Dogan, Gerd A. Blobel, Mitchell J. Weiss, and Kuan Bei Chen

Subjects

Regulation of gene expression, Genetics, TAL1, Research, Histone modifications, Enhancer assay, Functional genomics, Biology, Chromatin, Cell biology, Gene regulation, Histone, Transcription (biology), GATA1, biology.protein, Epigenetics, Enhancer, Molecular Biology, Transcription factor

Abstract

Background Regulated gene expression controls organismal development, and variation in regulatory patterns has been implicated in complex traits. Thus accurate prediction of enhancers is important for further understanding of these processes. Genome-wide measurement of epigenetic features, such as histone modifications and occupancy by transcription factors, is improving enhancer predictions, but the contribution of these features to prediction accuracy is not known. Given the importance of the hematopoietic transcription factor TAL1 for erythroid gene activation, we predicted candidate enhancers based on genomic occupancy by TAL1 and measured their activity. Contributions of multiple features to enhancer prediction were evaluated based on the results of these and other studies. Results TAL1-bound DNA segments were active enhancers at a high rate both in transient transfections of cultured cells (39 of 79, or 56%) and transgenic mice (43 of 66, or 65%). The level of binding signal for TAL1 or GATA1 did not help distinguish TAL1-bound DNA segments as active versus inactive enhancers, nor did the density of regulation-related histone modifications. A meta-analysis of results from this and other studies (273 tested predicted enhancers) showed that the presence of TAL1, GATA1, EP300, SMAD1, H3K4 methylation, H3K27ac, and CAGE tags at DNase hypersensitive sites gave the most accurate predictors of enhancer activity, with a success rate over 80% and a median threefold increase in activity. Chromatin accessibility assays and the histone modifications H3K4me1 and H3K27ac were sensitive for finding enhancers, but they have high false positive rates unless transcription factor occupancy is also included. Conclusions Occupancy by key transcription factors such as TAL1, GATA1, SMAD1, and EP300, along with evidence of transcription, improves the accuracy of enhancer predictions based on epigenetic features. Electronic supplementary material The online version of this article (doi:10.1186/s13072-015-0009-5) contains supplementary material, which is available to authorized users.

Published

2015

11. Bioinformatic analyses of bacterial HPr kinase/phosphorylase homologues

Author

Aaron J. Stonestrom, Milton H. Saier, Ravi D. Barabote, and Claudio F. Gonzalez

Subjects

Phosphorylases, Molecular Sequence Data, Catabolite repression, macromolecular substances, Protein Serine-Threonine Kinases, Gram-Positive Bacteria, Microbiology, Homology (biology), Bacterial Proteins, Phylogenetics, Gram-Negative Bacteria, Cluster Analysis, Amino Acid Sequence, Molecular Biology, Phylogeny, Genetics, biology, Permease, Walker motifs, Computational Biology, General Medicine, PEP group translocation, biology.organism_classification, Databases as Topic, Biochemistry, Cyclic nucleotide-binding domain, bacteria, Sequence Alignment, Bacteria

Abstract

HPr kinase/phosphorylases (HprKs) regulate catabolite repression and sugar transport in Gram-positive bacteria by phosphorylating the small phosphotransferase system (PTS) protein HPr on a serine residue. We identified homologues of HprK in currently sequenced genomes and multiply aligned their sequences in order to perform phylogenetic and motif analyses. Seventy-eight homologues from bacteria and one from an archaeon comprise nine phylogenetic clusters. Some homologues come from bacteria whose genomes contain multiple highly divergent paralogues that cluster loosely together. Many of these proteins are truncated or show little or no identifiable similarity outside of the Walker A nucleotide binding domain. HprK homologues were identified in Gram-negative bacteria that appear to lack PTS permeases, suggesting modes of action and substrates that differ from those characterized in Gram-positive bacteria.

Published

2005

12. Biochemical Characterization of Phosphoryl Transfer Involving HPr of the Phosphoenolpyruvate-Dependent Phosphotransferase System in Treponema denticola, an Organism that Lacks PTS Permeases

Author

Milton H. Saier, Claudio F. Gonzalez, Aaron J. Stonestrom, and Graciela L. Lorca

Subjects

Molecular Sequence Data, macromolecular substances, Bacillus subtilis, Protein Serine-Threonine Kinases, Biochemistry, Glycogen phosphorylase, Adenosine Triphosphate, Bacterial Proteins, Phosphate Transport Proteins, Amino Acid Sequence, Treponema pallidum, Phosphorylation, Kinase activity, Phosphoenolpyruvate Sugar Phosphotransferase System, Treponema, biology, Permease, Escherichia coli Proteins, Genetic Complementation Test, Phosphotransferases (Nitrogenous Group Acceptor), Treponema denticola, PEP group translocation, biology.organism_classification, Molecular biology, carbohydrates (lipids), stomatognathic diseases, bacteria, Phosphoenolpyruvate carboxykinase, Phosphorus Radioisotopes, Sequence Alignment

Abstract

Treponema pallidum and Treponema denticola encode within their genomes homologues of energy coupling and regulatory proteins of the phosphoenolpyruvate:sugar phosphotransferase system (PTS) but no recognizable homologues of PTS permeases. These homologues include (1) Enzyme I, (2) HPr, (3) two IIA(Ntr)-like proteins, and (4) HPr(Ser) kinase/phosphorylase (HprK). Because the Enzyme I-encoding gene in T. pallidum is an inactive pseudogene and because all other pts genes in both T. pallidum and T. denticola are actively expressed, the primary sensory transduction mechanism for signal detection and transmission appears to involve HprK rather than EI. We have overexpressed and purified to near homogeneity four of the five PTS proteins from T. denticola. Purified HprK phosphorylates HPr with ATP, probably on serine, while Enzyme I phosphorylates HPr with PEP, probably on histidine. Furthermore, HPr(His)-P can transfer its phosphoryl group to IIA(Ntr)-1. Factors and conditions regulating phosphoryl transfer prove to differ from those described previously for Bacillus subtilis, but cross-enzymatic activities between the Treponema, Salmonella, and Bacillus phosphoryl-transfer systems could be demonstrated. Kinetic analyses revealed that the allosterically regulated HPr kinase/phosphorylase differs from its homologues in Bacillus subtilis and other low G+C Gram-positive bacteria in being primed for kinase activity rather than phosphorylase activity in the absence of allosteric effectors. The characteristics of this enzyme and the Treponema phosphoryl-transfer chain imply unique modes of signal detection and sensory transmission. This paper provides the first biochemical description of PTS phosphoryl-transfer chains in an organism that lacks PTS permeases.

Published

2004

13. Functions of BET proteins in erythroid gene expression

Author

Sarah C. Hsu, Aaron J. Stonestrom, Amy E. Campbell, Peng Huang, Belinda Giardine, Kristen S. Jahn, Cheryl A. Keller, Ross C. Hardison, Stephan Kadauke, Perry Evans, and Gerd A. Blobel

Subjects

BRD4, Immunology, chemical and pharmacologic phenomena, Biology, Protein Serine-Threonine Kinases, Biochemistry, Mice, Erythroid Cells, Transcription (biology), Gene expression, Animals, Humans, GATA1 Transcription Factor, Transcription factor, Cells, Cultured, Regulation of gene expression, RNA-Binding Proteins, hemic and immune systems, GATA1, Cell Biology, Hematology, Molecular biology, Bromodomain, Chromatin, Hematopoiesis, Protein Structure, Tertiary, Gene Expression Regulation, Gene Knockdown Techniques

Abstract

Inhibitors of bromodomain and extraterminal motif proteins (BETs) are being evaluated for the treatment of cancer and other diseases, yet much remains to be learned about how BET proteins function during normal physiology. We used genomic and genetic approaches to examine BET function in a hematopoietic maturation system driven by GATA1, an acetylated transcription factor previously shown to interact with BETs. We found that BRD2, BRD3, and BRD4 were variably recruited to GATA1-regulated genes, with BRD3 binding the greatest number of GATA1-occupied sites. Pharmacologic BET inhibition impaired GATA1-mediated transcriptional activation, but not repression, genome-wide. Mechanistically, BETs promoted chromatin occupancy of GATA1 and subsequently supported transcriptional activation. Using a combination of CRISPR-Cas9-mediated genomic engineering and shRNA approaches, we observed that depletion of either BRD2 or BRD4 alone blunted erythroid gene activation. Surprisingly, depletion of BRD3 only affected erythroid transcription in the context of BRD2 deficiency. Consistent with functional overlap among BET proteins, forced BRD3 expression substantially rescued defects caused by BRD2 deficiency. These results suggest that pharmacologic BET inhibition should be interpreted in the context of distinct steps in transcriptional activation and overlapping functions among BET family members.

Published

2014

14. The BET Protein BRD2 Cooperates with CTCF to Enforce a Transcriptional Boundary in Erythroid Cells

Author

Jennifer E. Phillips-Cremins, Sarah C. Hsu, Kristen S. Jahn, Caroline Bartman, Ross C. Hardison, Arjun Raj, Belinda Giardine, Michael T. Werner, Cheryl A. Keller, Thomas G. Gilgenast, Gerd A. Blobel, Daniel J. Emerson, Peng Huang, Aaron J. Stonestrom, and Christopher R. Edwards

Subjects

BRD4, Immunology, GATA1, Cell Biology, Hematology, Biology, Insulator (genetics), Biochemistry, Chromatin, Cell biology, Bromodomain, CTCF, Transcriptional regulation, Enhancer

Abstract

Pharmacologic inhibitors of the bromodomain and extraterminal motif (BET) family of proteins have shown promise in the treatment of hematologic and other malignancies and are being developed for clinical use. However, BET inhibitors do not discriminate between the family members BRD2, BRD3, and BRD4, and thus the mechanistic basis for their therapeutic efficacy is not well understood. In addition, BRD2 and BRD4 are individually required for the activation of genes driven by the erythroid transcription factor GATA1 (Stonestrom et al., Blood 2015), yet how BRD2 in particular contributes to this process has not been studied. We examined BRD2 occupancy genome-wide in erythroid cells and find that BRD2 colocalizes extensively with the architectural/insulator protein CCCTC-binding factor (CTCF). We define a functional hierarchy whereby CTCF is required for BRD2 to occupy co-bound sites, while CTCF binding is BRD2-independent. Using CRISPR/Cas9-based genome editing we identify a boundary element occupied by CTCF and BRD2 that is adjacent to a GATA1-driven enhancer and ensures appropriate transcriptional regulation at the locus. Employing single-molecule RNA FISH we show that either site-specific CTCF disruption or BRD2 depletion leads to increased correlation in mature mRNA levels between the genes flanking this boundary, suggesting that they become inappropriately coregulated. Taken together these findings indicate that BRD2 collaborates with CTCF to constrain the activity of an erythroid enhancer and reveal a potential new role for BET proteins in chromatin domain boundary function. Disclosures No relevant conflicts of interest to declare.

Published

2016

15. A Hyperactive Transcriptional State Marks Genome Reactivation during Mitotic Exit

Author

Cheryl A. Keller, Gerd A. Blobel, Ross C. Hardison, Caroline Bartman, Aaron J. Stonestrom, Belinda Giardine, Peng Huang, Chris C.-S. Hsiung, Paul Ginart, Perry Evans, Kristen S. Jahn, and Arjun Raj

Subjects

Genetics, Regulation of gene expression, Immunology, RNA polymerase II, Cell Biology, Hematology, Biology, Biochemistry, Transcription (biology), Mitotic exit, Transcriptional regulation, biology.protein, Enhancer, Mitosis, Gene

Abstract

The tremendous proliferative capacity of erythroid precursor cells underlies the production of over a million red blood cells per second in adult humans. During every mitosis the mammalian nucleus is disassembled and transcriptionally silent. Genome reactivation after mitosis is a key step in the propagation of transcriptional programs through cell generations, yet how this occurs remains largely unexplored. We carried out the first genome wide survey of transcription in cells emerging from mitosis using RNA polymerase II ChIP seq in purified populations at various post-mitotic time points. Using unsupervised approaches, we discover and classify genome reactivation patterns among genes. A surprisingly large fraction of genes (~25%) displays a post-mitotic spike in transcription. This spike represents the first complete round of transcription and accounts for the greatest gene-to-gene variance in temporal patterns of transcription in G1 phase. Another notable and contrasting pattern is gene activation late in the G1 phase. Single-molecule RNA FISH imaging demonstrates that the post-mitotic transcriptional spike represents the highest activity throughout the cell cycle and results in an increase in mature mRNAs, indicating that the phenomenon has the capacity to alter gene expression. Surprisingly, the post-mitotic transcriptional spike occurs independent of enhancer action and can be recapitulated with promoter sequences ectopically integrated into the genome. In contrast, late-G1 gene reactivation is distinct and requires enhancer function. Our findings uncover novel modes of transcriptional control during exit from mitosis with implications for our understanding of transitions in gene expression states in dividing cells. Disclosures No relevant conflicts of interest to declare.

Published

2015

16. Apoptotic regulation and tRNA

Author

Yide Mei, Xiaolu Yang, Ya-Ming Hou, and Aaron J. Stonestrom

Subjects

Caspase-9, Cell signaling, Programmed cell death, Cytochrome, biology, Cytochrome c, RNA, Cytochromes c, Apoptosis, Cell Biology, Mini-Review, Biochemistry, Models, Biological, Caspase 9, Cell biology, RNA, Transfer, Drug Discovery, Transfer RNA, biology.protein, Animals, Humans, Nucleic Acid Conformation, Biotechnology

Abstract

Apoptotic regulation is critical to organismal homeostasis and protection against many human disease processes such as cancer. Significant research efforts over the past several decades have illuminated many signaling molecules and effecter proteins responsible for this form of programmed cell death. Recent evidence suggests that transfer RNA (tRNA) regulates apoptotic sensitivity at the level of cytochrome c-mediated apoptosome formation. This finding unexpectedly places tRNA at the nexus of cellular biosynthesis and survival. Here we review the current understanding of both the apoptotic machinery and tRNA biology. We describe the evidence linking tRNA and cytochrome c in depth, and speculate on the implications of this link in cell biology.

Published

2010

17. tRNA and cytochrome c in cell death and beyond

Author

Jeongsik Yong, Xiaolu Yang, Aaron J. Stonestrom, and Yide Mei

Subjects

biology, Cytochrome, Cell Death, Cytochrome b, Cytochrome c, Extra View, RNA, Cytochromes c, Cell Biology, Mitochondrion, Cell biology, Biochemistry, RNA, Transfer, Coenzyme Q – cytochrome c reductase, biology.protein, Cytochrome c oxidase, Animals, Humans, Disease, Apoptosome, Molecular Biology, Developmental Biology, Protein Binding

Abstract

Both transfer RNA (tRNA) and cytochrome c are essential to cellular function: tRNA mediates protein synthesis while cytochrome c is required for oxidative phosphorylation and apoptosis induction. tRNA has recently been implicated as a direct regulator of the well-conserved apoptotic role of cytochrome c. Interaction between these molecules could potentially coordinate biosynthesis, energy production and apoptosis. Here we review the diversity and dynamics of tRNA and how this class of non-coding RNAs may regulate the role of cytochrome c in apoptosis. We comment on unanswered questions in the cell biology of this interaction and how answers may influence our understanding of disease.

Published

2010

18. Abstract 486: BET protein inhibition by JQ1 blocks EWS-FLI1 activity in Ewing sarcoma

Author

Gerd A. Blobel, Robert A. Young, Margaret M. Chou, Krista L. Bledsoe, Laura Quick, Stephan Kadauke, and Aaron J. Stonestrom

Subjects

Cancer Research, Oncogene, Microarray analysis techniques, Bone cancer, Cancer, Biology, medicine.disease, medicine.disease_cause, Virology, Bromodomain, Oncology, medicine, Cancer research, Sarcoma, Carcinogenesis, Transcription factor

Abstract

Ewing sarcoma is the second most common bone cancer in children, with an estimated 5-year survival rate of 20% for metastatic cases. These tumors harbor the characteristic chromosomal translocation t(11;22)(q24;q12), which leads to expression of the oncogenic chimeric transcription factor, EWS-FLI1. EWS-FLI1 drives Ewing sarcoma tumorigenesis, and is an attractive therapeutic target because it is expressed exclusively in tumor cells. However, directly targeting EWS-FLI1 has proved difficult. Thus, despite advances in our understanding of EWS-FLI1 function, treatment options remain limited, and to date, no targeted therapeutics have been developed. In this study, we investigated the effects of the epigenetic modifier drug, JQ1, on Ewing sarcoma pathogenesis. JQ1 is a small molecule inhibitor of the BET family of bromodomain proteins, which bind to acetylated histones and transcription factors to regulate gene expression. JQ1 selectively inhibits these acetylation-dependent BET protein interactions. Recent studies reveal that JQ1 has potent anti-neoplastic activity against multiple cancers, with c-MYC downregulation being a key mechanism by which it induces cell death in several tumor types. Because Ewing sarcoma cells express high levels of c-MYC, we predicted that they would be sensitive to the cytotoxic effects of JQ1. Our results demonstrate that JQ1 indeed inhibits growth of Ewing sarcoma cells, but unexpectedly, it does not function through inhibition of c-MYC. Using multiple patient-derived Ewing sarcoma cell lines, we find that JQ1 induces apoptosis as measured by PARP cleavage. Preliminary data further indicate that JQ1 suppresses growth of Ewing sarcoma xenografts in vivo. Mechanistic studies and microarray analysis reveal that JQ1 inhibits EWS-FLI1 activity, with multiple targets of the oncogene being rapidly downregulated upon JQ1 treatment. Studies are currently underway to identify the specific BET family members required for EWS-FLI1 function, and to determine the mechanism by which they regulate EWS-FLI1 activity. Given the emergence of numerous JQ1-derivative compounds targeting specific BET proteins, it is hopeful that this class of compounds may ultimately be used as targeted therapies for the treatment of Ewing sarcoma. Citation Format: Krista L. Bledsoe, Aaron Stonestrom, Stephan Kadauke, Laura Quick, Robert Young, Gerd A. Blobel, Margaret M. Chou. BET protein inhibition by JQ1 blocks EWS-FLI1 activity in Ewing sarcoma. [abstract]. In: Proceedings of the 106th Annual Meeting of the American Association for Cancer Research; 2015 Apr 18-22; Philadelphia, PA. Philadelphia (PA): AACR; Cancer Res 2015;75(15 Suppl):Abstract nr 486. doi:10.1158/1538-7445.AM2015-486

Published

2015

19. Dissection of BET Protein Function in a Hematopoietic Differentiation Model

Author

Peng Huang, Kristen S. Jahn, Chris Cs Hsuing, Sarah C. Hsu, Aaron J. Stonestrom, Ross C. Hardison, and Gerd A. Blobel

Subjects

Regulation of gene expression, Genetics, BRD4, biology, Cellular differentiation, Immunology, chemical and pharmacologic phenomena, hemic and immune systems, GATA1, Cell Biology, Hematology, Biochemistry, Bromodomain, Chromatin, Histone, biology.protein, Transcription factor

Abstract

The mammalian Bromodomain and Extra-Terminal motif (BET) proteins associate with acetylated histones and transcription factors including the master erythroid regulator GATA1. Pharmacologic inhibitors that broadly target BET family proteins are being evaluated in clinical trials for hematologic malignancies. Additionally, a rapidly growing number of studies in model organisms and in vitro systems suggests BET modulation is a therapeutic avenue in diverse disorders. However the mechanisms through which BET proteins act as well as the contributions of individual BET family members to biological processes remain mostly uncharacterized. Previously we showed that BET family members Brd3 and Brd4 can bind to GATA1 in an acetylation-dependent manner and that pharmacologic BET inhibition impairs erythroid maturation (Lamonica et al PNAS 2011). Using a combination of genome-wide occupancy analysis, pharmacologic inhibition, genome editing and knockdown we characterized the mechanism and function of BET proteins in the context of GATA1-driven erythroid differentiation. BET inhibitors prevented GATA1-mediated transcriptional activation, but not repression, genome-wide. Mechanistically, GATA1 required BETs both for initial chromatin association and for transcriptional activation following the establishment of GATA1 occupancy. As BET proteins associate with chromatin during mitosis when transcription is globally disrupted, they have been implicated as mitotic “bookmarks”. BET inhibition specifically during mitosis failed to elicit a measurable impact on post-mitotic gene activation, calling into question a role of BET proteins as mitotic bookmarks in this system. To determine the BET protein(s) most relevant to GATA1-activated transcription, we genomically disrupted BET family members Brd2, Brd3 and Brd4 using the CRISPR/Cas9 tool. Despite being present at nearly all GATA1-occupied sites genome-wide, Brd3 disruption had little impact on GATA1-dependent transcription. In contrast, both Brd2 and Brd4 were individually required for efficient gene activation by GATA1. A Brd3 requirement was only revealed in the setting of Brd2 deficiency, indicating functional compensation among select BET proteins. These results provide a comprehensive definition of the functions of BET proteins in a model of cellular differentiation. They further suggest that pharmacologic BET inhibition should be viewed in the context of distinct steps in transcriptional activation and overlapping functions among BET family members. Disclosures No relevant conflicts of interest to declare.

Published

2014

20. GATA1 and the BET Family Protein Brd3 Form a Mitotic Bookmarking Complex

Author

Stephan Kadauke, Gerd A. Blobel, Ross C. Hardison, Aaron J. Stonestrom, Amy E. Campbell, and Deepti Jain

Subjects

Zinc finger, Genetics, BRD4, Cell division, Bookmarking, Immunology, GATA1, Cell Biology, Hematology, Biology, Biochemistry, Bromodomain, Transcription (biology), Mitosis

Abstract

Abstract 282 Erythroid-specific transcription patterns are maintained throughout cell division. During mitosis, transcription is silenced globally. This raises the question whether mechanisms are in place that ensure the spatially and temporally correct reassembly of transcriptional regulators and thus maintain lineage fidelity. We recently found that, in contrast to most nuclear regulators, the master hematopoietic regulator GATA1 remains associated at a subset of its targets within mitotic chromosomes in erythroid cells (Kadauke et al., Cell 2012). GATA1 appears to function by creating an epigenetic “bookmark” to facilitate timely post-mitotic transcription reactivation of its mitotic target genes. GATA1 is acetylated at two lysine-rich domains near its zinc finger domains. We recently discovered that acetylated GATA1 recruits the double bromodomain protein Brd3 to erythroid target genes (Lamonica et al., PNAS 2011). Brd3 interacts with acetylated GATA1 via its first bromodomain, and Brd3 recruitment to GATA1 target sites is critically required for induction of terminal erythroid target genes such as α- and β-globin. Notably, Brd3 belongs to a family of proteins (called the BET family) of which two members (Brd2 and Brd4) are known to be retained on mitotic chromosomes. We now find by immunofluorescence and live cell confocal imaging that Brd3 globally binds to mitotic chromosomes. ChIP-seq experiments demonstrate a high degree of co-localization of Brd3 and GATA1 genome-wide both in interphase and in mitosis. We further demonstrate that GATA1 directly recruits Brd3 to mitotic GATA1 target sites. Transient mitosis-specific disruption of the Brd3-GATA1 interaction using the small molecule BET bromodomain inhibitor JQ1 removed Brd3, but not GATA1, from mitotic binding sites and led to a profound delay in the reactivation of GATA1-bookmarked genes. This suggests that Brd3 is an integral component of GATA1's bookmarking function. In concert, these studies support a requirement of mitotic bookmarking by a GATA1/Brd3 complex for the propagation of lineage-specific transcription programs in dividing erythroid cells. Disclosures: No relevant conflicts of interest to declare.

Published

2012