Your search keyword '"Jacqueline A. Sloane-Stanley"' showing total 28 results

1. On-microscope staging of live cells reveals changes in the dynamics of transcriptional bursting during differentiation

Author

Jacqueline A. Sharpe, D.M. Jeziorska, B. Christoffer Lagerholm, Doug Higgs, Andrew J.H. Smith, Veronica J. Buckle, Jill M. Brown, Jacqueline A. Sloane-Stanley, Edward Tunnacliffe, Helena Ayyub, and Christian Babbs

Subjects

Transcriptional bursting, Transcriptional activity, Transcription (biology), Dynamics (mechanics), Gene expression, Erythropoiesis, Biology, Gene, Cell biology

Abstract

Determining the mechanisms by which genes are switched on and off during development and differentiation is a key aim of current biomedical research. Gene transcription has been widely observed to occur in a discontinuous fashion, with short bursts of activity interspersed with longer periods of inactivity. It is currently not known if or how this dynamic behaviour changes as mammalian cells differentiate. To investigate this, using a newly developed on-microscope analysis, we monitored mouse α-globin transcription in live cells throughout sequential stages of erythropoiesis. We find that changes in the overall levels of α-globin transcription are most closely associated with changes in the fraction of time a gene spends in the active transcriptional state. We identify differences in the patterns of transcriptional bursting throughout differentiation, with maximal transcriptional activity occurring in the mid-phase of differentiation. Early in differentiation, we observe increased fluctuation in the patterns of transcriptional activity whereas at the peak of gene expression, in early and intermediate erythroblasts, transcription appears to be relatively stable and efficient. Later during differentiation as α-globin expression declines, we again observed more variability in transcription within individual cells. We propose that the observed changes in transcriptional behaviour may reflect changes in the stability of enhancer-promoter interactions and the formation of active transcriptional compartments as gene expression is turned on and subsequently declines at sequential stages of differentiation.

Published

2021

2. Identification of the transcription factor MAZ as a regulator of erythropoiesis

Author

Darya Deen, Jan Frayne, Matthias Mann, Daniel C. J. Ferguson, Helena Ayyub, Vasiliki Samara, Michelle L. Holland, Falk Butter, Jacqueline A. Sloane-Stanley, Douglas Vernimmen, Ivan Ferrer-Vicens, David Garrick, and Deborah E. Daniels

Subjects

erythroid cells, globins, oncogenes, Regulator, dna, Biology, Erythroid Cells, hemic and lymphatic diseases, Humans, Erythropoiesis, genes, Enhancer, Promoter Regions, Genetic, Gene, Transcription factor, transcription factor, mass spectrometry, Zinc finger, Regulation of gene expression, Promoter, Hematology, binding (molecular function), Cell biology, DNA-Binding Proteins, Gene Expression Regulation, chromatography, affinity, K562 Cells, erythropoiesis, Transcription Factors

Abstract

Erythropoiesis requires a combination of ubiquitous and tissue-specific transcription factors (TFs). Here, through DNA affinity purification followed by mass spectrometry, we have identified the widely expressed protein MAZ (Myc-associated zinc finger) as a TF that binds to the promoter of the erythroid-specific human α-globin gene. Genome-wide mapping in primary human erythroid cells revealed that MAZ also occupies active promoters as well as GATA1-bound enhancer elements of key erythroid genes. Consistent with an important role during erythropoiesis, knockdown of MAZ reduces α-globin expression in K562 cells and impairs differentiation in primary human erythroid cells. Genetic variants in the MAZ locus are associated with changes in clinically important human erythroid traits. Taken together, these findings reveal the zinc-finger TF MAZ to be a previously unrecognized regulator of the erythroid differentiation program.

Published

2021

3. Reactivation of a developmentally silenced embryonic globin gene

Author

Jacqueline A. Sharpe, Megan Buckley, Helena Francis, Jacqueline A. Sloane-Stanley, Siyu Liu, Mira T. Kassouf, Maria C. Suciu, Christian Babbs, Jennifer Eglinton, Stephanie J Carpenter, Stuart H. Orkin, Andrew J. King, Aude-Anais Olijnik, Lars L. P. Hanssen, Danuta M. Jeziorska, Damien J. Downes, Nigel A. Roberts, Jelena Telenius, Robert A. Beagrie, A. Marieke Oudelaar, Peng Hua, Len A. Pennacchio, James O.J. Davies, Duantida Songdej, Douglas R. Higgs, and Jim R. Hughes

Subjects

0301 basic medicine, General Physics and Astronomy, Stem Cell Research - Embryonic - Non-Human, Mice, 0302 clinical medicine, hemic and lymphatic diseases, Developmental, Regulation of gene expression, Multidisciplinary, biology, Molecular medicine, Cooley's Anemia, Haematopoietic stem cells, Gene Expression Regulation, Developmental, Gene silencing, Acetylation, Hematology, Chromatin, Cell biology, DNA-Binding Proteins, Histone, Enhancer Elements, Genetic, 030220 oncology & carcinogenesis, Transcriptional Activation, Enhancer Elements, Heterochromatin, Science, Chromatin remodelling, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Rare Diseases, Genetic, Erythroid Cells, alpha-Globins, Genetics, Animals, Humans, Globin, Gene Silencing, zeta-Globins, Enhancer, Gene, General Chemistry, Stem Cell Research, Embryonic stem cell, Gene regulation, Histone Deacetylase Inhibitors, Repressor Proteins, 030104 developmental biology, Gene Expression Regulation, biology.protein, Transcription Factors

Abstract

The α- and β-globin loci harbor developmentally expressed genes, which are silenced throughout post-natal life. Reactivation of these genes may offer therapeutic approaches for the hemoglobinopathies, the most common single gene disorders. Here, we address mechanisms regulating the embryonically expressed α-like globin, termed ζ-globin. We show that in embryonic erythroid cells, the ζ-gene lies within a ~65 kb sub-TAD (topologically associating domain) of open, acetylated chromatin and interacts with the α-globin super-enhancer. By contrast, in adult erythroid cells, the ζ-gene is packaged within a small (~10 kb) sub-domain of hypoacetylated, facultative heterochromatin within the acetylated sub-TAD and that it no longer interacts with its enhancers. The ζ-gene can be partially re-activated by acetylation and inhibition of histone de-acetylases. In addition to suggesting therapies for severe α-thalassemia, these findings illustrate the general principles by which reactivation of developmental genes may rescue abnormalities arising from mutations in their adult paralogues., Globin loci harbor genes that are expressed embryonically and silenced postnatally. Here the authors show that zeta-globin silencing depends upon selective hypoacetylation of its TAD subdomain, which blocks its interaction with the alpha-globin super-enhancer, and zeta-globin can be reactivated by acetylation.

Published

2020

4. A functional overlap between actively transcribed genes and chromatin boundary elements

Author

R Stolper, Jim R. Hughes, Chris Preece, Lars L. P. Hanssen, C L Harrold, Daniel Biggs, Jacqueline A. Sharpe, Doug Higgs, Damien J. Downes, Jelena Telenius, Samy Alghadban, Jacqueline A. Sloane-Stanley, Mira T. Kassouf, Benjamin Davies, and M Gosden

Subjects

Cohesin complex, CTCF, Chromatin Loop, Locus (genetics), Promoter, Biology, Enhancer, Gene, Chromatin, Cell biology

Abstract

Mammalian genomes are subdivided into large (50-2000 kb) regions of chromatin referred to as Topologically Associating Domains (TADs or sub-TADs). Chromatin within an individual TAD contacts itself more frequently than with regions in surrounding TADs thereby directing enhancer-promoter interactions. In many cases, the borders of TADs are defined by convergently orientated boundary elements associated with CCCTC-binding factor (CTCF), which stabilises the cohesin complex on chromatin and prevents its translocation. This delimits chromatin loop extrusion which is thought to underlie the formation of TADs. However, not all CTCF-bound sites act as boundaries and, importantly, not all TADs are flanked by convergent CTCF sites. Here, we examined the CTCF binding sites within a ∼70 kb sub-TAD containing the duplicated mouse α-like globin genes and their five enhancers (5’-R1-R2-R3-Rm-R4-α1-α2-3’). The 5’ border of this sub-TAD is defined by a pair of CTCF sites. Surprisingly, we show that deletion of the CTCF binding sites within and downstream of the α-globin locus leaves the sub-TAD largely intact. The predominant 3’ border of the sub-TAD is defined by a steep reduction in contacts: this corresponds to the transcribed α2-globin gene rather than the CTCF sites at the 3’-end of the sub-TAD. Of interest, the almost identical α1- and α2-globin genes interact differently with the enhancers, resulting in preferential expression of the proximal α1-globin gene which behaves as a partial boundary between the enhancers and the distal α2-globin gene. Together, these observations provide direct evidence that actively transcribed genes can behave as boundary elements.Significance StatementMammalian genomes are complex, organised 3D structures, partitioned into Topologically Associating Domains (TADs): chromatin regions that preferentially self-interact. These chromatin interactions are thought to be driven by a mechanism that continuously extrudes chromatin loops, forming structures delimited by chromatin boundary elements and reflecting the activity of enhancers and promoters. Boundary elements bind architectural proteins such as CCCTC-binding factor (CTCF). Previously, an overlap between the functional roles of enhancers and promoters has been shown. However, whether there is overlap between enhancers/promoters and boundary elements is not known. Here, we show that actively transcribed genes can also behave as boundary elements, similar to CTCF boundaries. In both cases, multi-protein complexes bound to these regions may stall the process of chromatin loop extrusion.

Published

2020

5. Identification of MAZ as a novel transcription factor regulating erythropoiesis

Author

David Garrick, Falk Butter, Matthias Mann, Michelle L. Holland, Jacqueline A. Sloane-Stanley, Douglas Vernimmen, Helena Ayyub, Vasiliki Samara, and Darya Deen

Subjects

Zinc finger, Gene knockdown, chemistry.chemical_compound, chemistry, hemic and lymphatic diseases, Regulator, Erythropoiesis, Promoter, Biology, Gene, Transcription factor, DNA, Cell biology

Abstract

Erythropoiesis requires a combination of ubiquitous and tissue-specific transcription factors. Here, through DNA affinity purification followed by mass spectrometry, we have identified the widely expressed protein MAZ (Myc-associated zinc finger) as a transcription factor that binds to the promoter of the erythroid-specific human α-globin gene. Genome-wide mapping in primary human erythroid cells revealed that MAZ also occupies active promoters as well as GATA1-bound enhancer elements of key erythroid genes. Consistent with an important role during erythropoiesis, knockdown of MAZ in primary human erythroid cells impairs erythroid differentiation, and genetic variants in the MAZ locus are associated with clinically important human erythroid traits. Taken together, these findings reveal the Zinc-finger transcription factor MAZ to be a previously unrecognised regulator of the erythroid differentiation program.

Published

2020

6. Tissue-specific CTCF/Cohesin-mediated chromatin architecture delimits enhancer interactions and function in vivo

Author

A. Marieke Oudelaar, Jacqueline A. Sharpe, Mira T. Kassouf, Douglas R. Higgs, Lars L. P. Hanssen, Chris Preece, Benjamin Davies, Jacqueline A. Sloane-Stanley, Damien J. Downes, M Gosden, Daniel Biggs, and Jim R. Hughes

Subjects

0301 basic medicine, Male, CCCTC-Binding Factor, Genotype, Chromosomal Proteins, Non-Histone, Cell Cycle Proteins, Transfection, Chromatin remodeling, Article, Cell Line, 03 medical and health sciences, Histone H1, Erythroid Cells, alpha-Globins, Gene cluster, Histone code, Animals, Enhancer, Promoter Regions, Genetic, ChIA-PET, Embryonic Stem Cells, Binding Sites, Chemistry, Gene Expression Regulation, Developmental, Cell Biology, Chromatin Assembly and Disassembly, Hematopoietic Stem Cells, Chromatin, Cell biology, Mice, Inbred C57BL, Repressor Proteins, 030104 developmental biology, Enhancer Elements, Genetic, Phenotype, CTCF, Multigene Family, Mutation, Blood Group Antigens, Female, biological phenomena, cell phenomena, and immunity, Protein Binding

Abstract

The genome is organized via CTCF–cohesin-binding sites, which partition chromosomes into 1–5 megabase (Mb) topologically associated domains (TADs), and further into smaller sub-domains (sub-TADs). Here we examined in vivo an ∼80 kb sub-TAD, containing the mouse α-globin gene cluster, lying within a ∼1 Mb TAD. We find that the sub-TAD is flanked by predominantly convergent CTCF–cohesin sites that are ubiquitously bound by CTCF but only interact during erythropoiesis, defining a self-interacting erythroid compartment. Whereas the α-globin regulatory elements normally act solely on promoters downstream of the enhancers, removal of a conserved upstream CTCF–cohesin boundary extends the sub-TAD to adjacent upstream CTCF–cohesin-binding sites. The α-globin enhancers now interact with the flanking chromatin, upregulating expression of genes within this extended sub-TAD. Rather than acting solely as a barrier to chromatin modification, CTCF–cohesin boundaries in this sub-TAD delimit the region of chromatin to which enhancers have access and within which they interact with receptive promoters. Hanssen et al. show that CTCF–cohesin binding sites at the α-globin gene cluster function as boundaries to restrict the interaction of enhancers with the flanking chromatin, thus preventing abnormal gene expression.

Published

2017

7. Enhancers Predominantly Regulate Gene Expression in vivo Via Transcription Initiation

Author

Bryony Crompton, Robert A. Beagrie, Jelena Telenius, Sue Butler, Julia Truch, Jacqueline A. Sloane-Stanley, Douglas R. Higgs, Takayuki Nojima, Martin S.C. Larke, Damien J. Downes, M. A. Bender, Jacqueline A. Sharpe, Nick J. Proudfoot, A. Marieke Oudelaar, Jim R. Hughes, and Ron Schwessinger

Subjects

0303 health sciences, biology, RNA, RNA polymerase II, Cell biology, Transcription initiation, 03 medical and health sciences, 0302 clinical medicine, In vivo, Transcription (biology), Genetically Engineered Mouse, Gene expression, biology.protein, Enhancer, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

Gene transcription occurs via a cycle of linked events including initiation, promoter proximal pausing and elongation of RNA polymerase II (Pol II). A key question is how do transcriptional enhancers influence these events to control gene expression? Here we have used a new approach to quantify transcriptional initiation and pausing in vivo, while simultaneously identifying transcription start sites (TSSs) and pause-sites (TPSs) from single RNA molecules. When analyzed in parallel with nascent RNA-seq, these data show that differential gene expression is achieved predominantly via changes in transcription initiation rather than Pol II pausing. Using genetically engineered mouse models deleted for specific enhancers we show that these elements control gene expression via Pol II recruitment and/or initiation rather than via promoter proximal pause release. Together, our data show that enhancers, in general, control gene expression predominantly by Pol II recruitment and initiation rather than via pausing.

Published

2019

8. Enhancer deletion generates cellular phenotypic diversity due to bimodal gene expression

Author

Jacqueline A. Sharpe, William G. Wood, Douglas Vernimmen, Ailbhe Jane Brazel, Jacqueline A. Sloane-Stanley, Marco De Gobbi, and Andrew J.H. Smith

Subjects

0301 basic medicine, medicine.medical_specialty, Mice, Transgenic, Biology, 03 medical and health sciences, Mice, alpha-Globins, Internal medicine, Gene expression, medicine, Animals, Base sequence, Alpha globulin, Enhancer, Molecular Biology, Sequence Deletion, Genetics, Regulation of gene expression, Hematology, Base Sequence, Molecular Medicine, Cell Biology, Phenotype, Molecular medicine, 030104 developmental biology, Enhancer Elements, Genetic, Gene Expression Regulation

Published

2017

9. Intragenic Enhancers Act as Alternative Promoters

Author

Monika S. Kowalczyk, Douglas Vernimmen, Richard J. Gibbons, Mona Hosseini, David Garrick, Jim R. Hughes, Jacqueline A. Sloane-Stanley, Douglas R. Higgs, Marco De Gobbi, Jacqueline A. Sharpe, William G. Wood, Nicola Gray, Jill M. Brown, Magnus D. Lynch, Licio Collavin, Simon J. McGowan, Thomas A. Milne, Veronica J. Buckle, Stephen S. Taylor, Jonathan Flint, Kowalczyk, M, Hughes, Jr, Garrick, D, Lynch, Md, Sharpe, Ja, Sloane Stanley, Ja, Mcgowan, Sj, De Gobbi, M, Hosseini, M, Vernimmen, D, Brown, Jm, Gray, Ne, Collavin, Licio, Gibbons, Rj, Flint, J, Taylor, S, Buckle, Vj, Milne, Ta, Wood, Wg, and Higgs, Dr

Subjects

Gene isoform, Enhancer RNAs, Biology, Genome, alpha globins, C16orf35, NPRL3, Mice, Erythroid Cells, Transcription (biology), Gene expression, RNA Isoforms, Animals, RNA, Messenger, Promoter Regions, Genetic, Enhancer, Molecular Biology, Gene, Cells, Cultured, Genetics, alpha globin, Promoter, Cell Biology, Enhancer Elements, Genetic, Gene Expression Regulation, RNA, Poly A, Transcriptome

Abstract

A substantial amount of organismal complexity is thought to be encoded by enhancers which specify the location, timing, and levels of gene expression. In mammals there are more enhancers than promoters which are distributed both between and within genes. Here we show that activated, intragenic enhancers frequently act as alternative tissue-specific promoters producing a class of abundant, spliced, multiexonic poly(A) + RNAs (meRNAs) which reflect the host gene's structure. meRNAs make a substantial and unanticipated contribution to the complexity of the transcriptome, appearing as alternative isoforms of the host gene. The low protein-coding potential of meRNAs suggests that many meRNAs may be byproducts of enhancer activation or underlie as-yet-unidentified RNA-encoded functions. Distinguishing between meRNAs and mRNAs will transform our interpretation of dynamic changes in transcription both at the level of individual genes and of the genome as a whole. © 2012 Elsevier Inc..

Published

2016

10. Long-range chromosomal interactions regulate the timing of the transition between poised and active gene expression

Author

Douglas R. Higgs, William G. Wood, M De Gobbi, Jacqueline A. Sloane-Stanley, and Douglas Vernimmen

Subjects

Models, Molecular, Chromatin Immunoprecipitation, Range (biology), genetics/metabolism, Animals, Cell Line, Tumor, Chromatin Immunoprecipitation, Chromosomes, genetics/metabolism, Erythroid Cells, metabolism, Gene Expression Regulation, physiology, Globins, genetics/metabolism, Mice, Models, Biological, Models, Molecular, Nucleic Acid Conformation, Regulatory Elements, Transcriptional, genetics/physiology, RNA polymerase II, Biology, Models, Biological, Article, General Biochemistry, Genetics and Molecular Biology, Chromosomes, Cell Line, Chromosome conformation capture, Mice, Erythroid Cells, Transcription (biology), Models, Cell Line, Tumor, Gene expression, Transcriptional regulation, Animals, Regulatory Elements, Transcriptional, Molecular Biology, Gene, Genetics, Regulation of gene expression, Tumor, Transition (genetics), General Immunology and Microbiology, General transcription factor, General Neuroscience, Molecular, Cell Biology, Hematology, Biological, Regulatory Elements, Chromatin, Globins, Gene Expression Regulation, Evolutionary biology, physiology, biology.protein, Molecular Medicine, Nucleic Acid Conformation, metabolism

Abstract

To understand how mammalian genes are regulated from their natural chromosomal environment, we have analysed the molecular events occurring throughout a 150 kb chromatin segment containing the alpha globin gene locus as it changes from a poised, silent state in erythroid progenitors, to the fully activated state in late, erythroid cells. Active transcription requires the late recruitment of general transcription factors, mediator and Pol II not only to the promoter but also to its remote regulatory elements. Natural mutants of the alpha cluster show that whereas recruitment of the pre-initiation complex to the upstream elements occurs independently, recruitment to the promoter is largely dependent on the regulatory elements. An improved, quantitative chromosome conformation capture analysis demonstrates that this recruitment is associated with a conformational change, in vivo, apposing the promoter with its remote regulators, consistent with a chromosome looping mechanism. These findings point to a general mechanism by which a gene can be held in a poised state until the appropriate stage for expression, coordinating the level and timing of gene expression during terminal differentiation.

Published

2016

11. Genetic dissection of the α-globin super-enhancer in vivo

Author

Ruth M. Williams, Tatjana Sauka-Spengler, Jim R. Hughes, Lars L. P. Hanssen, Douglas R. Higgs, Mira T. Kassouf, Bryony Graham, Christian Babbs, Jacqueline A. Sloane-Stanley, James O.J. Davies, Sue Butler, William G. Wood, Len A. Pennacchio, Andrew J.H. Smith, Pik-Shan Li, Helena Ayyub, Maria C. Suciu, Richard J. Gibbons, Christina Rode, Jacqueline A. Sharpe, Deborah Hay, A. Marieke Oudelaar, and Jelena Telenius

Subjects

0301 basic medicine, Enhancer Elements, Knockout, Biology, Medical and Health Sciences, Article, Mice, 03 medical and health sciences, Super-enhancer, Erythroid Cells, Genetic, alpha-Globins, Genetics, Transcriptional regulation, Animals, Epigenetics, Enhancer, Gene, Regulation of gene expression, epigenetics, Mammalian, Hematology, Biological Sciences, Phenotype, Chromatin, 030104 developmental biology, Gene Expression Regulation, Embryo, gene regulation, Transcription, Transcription Factors, Developmental Biology

Abstract

© 2016 Nature America, Inc. All rights reserved. Many genes determining cell identity are regulated by clusters of Mediator-bound enhancer elements collectively referred to as super-enhancers. These super-enhancers have been proposed to manifest higher-order properties important in development and disease. Here we report a comprehensive functional dissection of one of the strongest putative super-enhancers in erythroid cells. By generating a series of mouse models, deleting each of the five regulatory elements of the α-globin super-enhancer individually and in informative combinations, we demonstrate that each constituent enhancer seems to act independently and in an additive fashion with respect to hematological phenotype, gene expression, chromatin structure and chromosome conformation, without clear evidence of synergistic or higher-order effects. Our study highlights the importance of functional genetic analyses for the identification of new concepts in transcriptional regulation.

Published

2016

12. An interspecies analysis reveals a key role for unmethylated CpG dinucleotides in vertebrate Polycomb complex recruitment

Author

Jacqueline A. Sloane-Stanley, Richard J. Gibbons, Marco De Gobbi, Tom Burdon, Magnus D. Lynch, Maria Flenley, Jacqueline A. Sharpe, Douglas R. Higgs, Stephen Meek, Douglas Vernimmen, Helena Ayyub, Andrew J.H. Smith, Linda Sutherland, Jim R. Hughes, and David Garrick

Subjects

Genetics, 0303 health sciences, General Immunology and Microbiology, General Neuroscience, Locus (genetics), Biology, Embryonic stem cell, General Biochemistry, Genetics and Molecular Biology, Chromatin, 03 medical and health sciences, 0302 clinical medicine, CpG site, DNA methylation, Transcriptional regulation, Polycomb-group proteins, 10. No inequality, Induced pluripotent stem cell, Molecular Biology, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

The role of DNA sequence in determining chromatin state is incompletely understood. We have previously demonstrated that large chromosomal segments from human cells recapitulate their native chromatin state in mouse cells, but the relative contribution of local sequences versus their genomic context remains unknown. In this study, we compare orthologous chromosomal regions for which the human locus establishes prominent sites of Polycomb complex recruitment in pluripotent stem cells, whereas the corresponding mouse locus does not. Using recombination-mediated cassette exchange at the mouse locus, we establish the primacy of local sequences in the encoding of chromatin state. We show that the signal for chromatin bivalency is redundantly encoded across a bivalent domain and that this reflects competition between Polycomb complex recruitment and transcriptional activation. Furthermore, our results suggest that a high density of unmethylated CpG dinucleotides is sufficient for vertebrate Polycomb recruitment. This model is supported by analysis of DNA methyltransferase-deficient embryonic stem cells.

Published

2011

13. A large deletion in the human -globin cluster caused by a replication error is associated with an unexpectedly mild phenotype

Author

Chris Fisher, Douglas R. Higgs, Jacqueline A. Sloane-Stanley, John Old, Michelle Rugless, David Garrick, and Helena Ayyub

Subjects

Adult, DNA Replication, Male, Gene Expression, Alpha (ethology), Biology, chemistry.chemical_compound, Gene expression, Genetics, Humans, Globin, Child, Molecular Biology, Gene, Cells, Cultured, Genetics (clinical), Functional analysis, DNA replication, General Medicine, Phenotype, Chromatin, Globins, chemistry, Multigene Family, Female, RNA Polymerase II, Chromosomes, Human, Pair 16, Gene Deletion, DNA

Abstract

We have characterized a newly identified 16.6 kb deletion which removes a significant proportion of the human alpha-globin cluster including the psizeta1, alpha(D), psialpha1 and alpha2-globin genes but leaves the duplicated alpha1 gene intact. This complicated rearrangement results from a combination of slippage and strand switching at sites of microhomology during replication. Functional analysis shows that expression of the remaining alpha1 gene is increased, rather than down-regulated by this deletion. This could be related to its proximity to the remote upstream alpha-globin regulatory elements or reduced competition for these elements in the absence of the dominant alpha2-globin gene. The finding of a very mild phenotype associated with such an extensive deletion in the alpha-globin cluster implies that much of the DNA removed by the deletion is likely to be functionally unimportant. These findings suggest that other than the upstream regulatory elements and promoter proximal elements there are unlikely to be additional positive cis-acting sequences in the alpha-globin cluster.

Published

2008

14. Tissue-specific histone modification and transcription factor binding in α globin gene expression

Author

William G. Wood, Douglas R. Higgs, Jacqueline A. Sloane-Stanley, Eduardo Anguita, Marco De Gobbi, Jacqueline A. Sharpe, Richard J. Gibbons, Ian Dunham, Christoph M. Koch, and Jim R. Hughes

Subjects

Transcription, Genetic, Enhancer Elements, Erythroblasts, Cells, T-Lymphocytes, Immunology, Biology, Methylation, Biochemistry, Chromosomes, Histones, Promoter Regions, Mice, Genetic, Gene expression, Animals, Humans, Histone code, genetics, Globin, Promoter Regions, Genetic, Gene, Transcription factor, Cells, Cultured, Acetylation, Animals, Cells, Cultured, Chromosomes, Human, Pair 16, Enhancer Elements, Genetic, Erythroblasts, immunology, Gene Expression Regulation, Globins, genetics, Histones, metabolism, Humans, K562 Cells, Methylation, Mice, Promoter Regions, Genetic, T-Lymphocytes, cytology, Telomere, Transcription Factors, metabolism, Transcription, Cultured, Pair 16, Acetylation, Cell Biology, Hematology, Telomere, Molecular biology, Globins, Enhancer Elements, Genetic, Histone, Gene Expression Regulation, cytology, biology.protein, K562 Cells, metabolism, Transcription, Chromosomes, Human, Pair 16, Transcription Factors

Abstract

To address the mechanism by which the human globin genes are activated during erythropoiesis, we have used a tiled microarray to analyze the pattern of transcription factor binding and associated histone modifications across the telomeric region of human chromosome 16 in primary erythroid and nonerythroid cells. This 220-kb region includes the α globin genes and 9 widely expressed genes flanking the α globin locus. This un-biased, comprehensive analysis of transcription factor binding and histone modifications (acetylation and methylation) described here not only identified all known cis-acting regulatory elements in the human α globin cluster but also demonstrated that there are no additional erythroid-specific regulatory elements in the 220-kb region tested. In addition, the pattern of histone modification distinguished promoter elements from potential enhancer elements across this region. Finally, comparison of the human and mouse orthologous regions in a unique mouse model, with both regions coexpressed in the same animal, showed significant differences that may explain how these 2 clusters are regulated differently in vivo.

Published

2007

15. Deletion of the mouse α-globin regulatory element (HS −26) has an unexpectedly mild phenotype

Author

Cristina Tufarelli, William G. Wood, E Anguita, Jacqueline A. Sharpe, Jacqueline A. Sloane-Stanley, and Douglas R. Higgs

Subjects

Genetically modified mouse, Immunology, Down-Regulation, Mean corpuscular hemoglobin, Alpha-thalassemia, Biology, Biochemistry, Cell Line, Mice, alpha-Thalassemia, hemic and lymphatic diseases, Genes, Regulator, Gene cluster, medicine, Animals, Humans, RNA, Messenger, Globin, Gene, Mice, Knockout, Genetics, medicine.diagnostic_test, Cell Biology, Hematology, medicine.disease, Phenotype, Molecular biology, Globins, Mutagenesis, Regulatory sequence, Multigene Family, Chromosome Deletion

Abstract

Natural deletions of the region upstream of the human alpha-globin gene cluster, together with expression studies in cell lines and transgenic mice, identified a single element (HS -40) as necessary and perhaps sufficient for high-level expression of the alpha-globin genes. A similar element occupies the corresponding position upstream of the mouse (m) alpha-globin genes (mHS -26) and was thought to have similar functional properties. We knocked out mHS -26 by homologous recombination and observed the surprising result that instead of the expected severe alpha-thalassemia phenotype, the mice had a mild disease. Transcription levels of the mouse genes were reduced by about 50%, but homozygotes were healthy, with normal hemoglobin levels and only mild decreases in mean corpuscular volume and mean corpuscular hemoglobin. These results may indicate differences in the regulation of the alpha-globin clusters in mice and humans or that additional cis-acting elements remain to be characterized in one or both clusters.

Published

2002

16. α-Thalassemia resulting from a negative chromosomal position effect

Author

Jacqueline A. Sharpe, Cynthia A. Heinlein, William G. Wood, Helena Ayyub, Douglas R. Higgs, Virginia Barbour, Jacqueline A. Sloane-Stanley, Cristina Tufarelli, Karel Indrak, and Zoe E. Smith

Subjects

Genetics, Chromosome engineering, Mutation, Immunology, Alpha-thalassemia, Cell Biology, Hematology, Biology, medicine.disease, medicine.disease_cause, Molecular biology, Biochemistry, Chromatin, Position effect, hemic and lymphatic diseases, DNA methylation, medicine, Globin, Gene

Abstract

To date, all of the chromosomal deletions that cause -thalassemia remove the structural  genes and/or their regulatory element (HS –40). A unique deletion occurs in a single family that juxtaposes a region that normally lies approximately 18-kilobase downstream of the human  cluster, next to a structurally normal -globin gene, and silences its expression. During development, the CpG island associated with the -globin promoter in the rearranged chromosome becomes densely methylated and insensitive to endonucleases, demonstrating that the normal chromatin structure around the -globin gene is perturbed by this mutation and that the gene is inactivated by a negative chromosomal position effect. These findings highlight the importance of the chromosomal environment in regulating globin gene expression.

Published

2000

17. Haemopoietic progenitor cell lines generated by the myeloproliferative leukaemia virus: a model system to analyse murine and human lineage-affiliated genes

Author

Andrew M. Thomson, Nigel A. Roberts, Jacqueline A. Sloane Stanley, William G. Wood, and Michèle Souyri

Subjects

Genetics, Genetically modified mouse, Hematology, Biology, Phenotype, Embryonic stem cell, Cell biology, Haematopoiesis, medicine.anatomical_structure, medicine, Bone marrow, Progenitor cell, Stem cell, Progenitor

Abstract

Multipotential progenitor and stem cells occur with a low frequency in haemopoietic tissue. As a result, it is often difficult to obtain sufficient numbers of cells to undertake many of the assays that would be informative about the molecular events involved in the regulation of lineage-affiliated genes within these multipotent cells. To circumvent this problem, we have used the myeloproliferative leukaemia virus (MPLV) to generate a phenotypically diverse array of haemopoietic progenitors from adult mouse bone marrow and embryonic blood. These cells could be expanded to perform a variety of analyses that would not previously have been possible using analogous primary cells. The validity of these assays was supported by the observation that the phenotype of several MPLV-infected lines was very similar to previously described primary haemopoietic progenitor cells. By using mice transgenic for the human alpha and beta globin gene clusters, we have shown that human genes may also be investigated. In addition, this strategy has a wide potential applicability including the rescue of haemopoietic progenitors from mouse embryos lacking genes critical for their survival as well as the study of any haemopoietic gene for which an appropriate transgenic mouse is available.

Published

1999

18. Globin Gene Switching in Transgenic Mice Carrying HS2-Globin Gene Constructs

Author

Jacqueline A. Sloane-Stanley, William G. Wood, Jacqueline A. Sharpe, Nigel A. Roberts, and Simon J. Stanworth

Subjects

Genetically modified mouse, Mutation, Hereditary persistence of fetal hemoglobin, Immunology, Reversion, Cell Biology, Hematology, Biology, medicine.disease_cause, medicine.disease, Biochemistry, Molecular biology, Gene expression, medicine, Globin, Enhancer, Gene

Abstract

We have examined the pattern of human globin gene switching in transgenic mice containing three different γ and β gene constructs (HS2GγAγδβ, HS2Aγβneo, and HS2Aγenβ) and compared the results with previously described transgenics (HS2Aγβ, HS2GγAγ-117δβ, and LCRεGγAγδβ). Developmental regulation was observed in all cases with identical patterns in lines bearing the same construct. Three different patterns of switching were observed: LCRεGγAγδβ and HS2Aγβneo mice switched rapidly, HS2GγAγδβ and HS2GγAγ-117δβ at an intermediate rate, and HS2Aγβ and HS2Aγenβ mice showed delayed switching, with a plateau in late fetal-early neonatal life and readily detectable levels of γ mRNA in adults. No difference was observed in the time of switching of the HS2GγAγδβ mice compared with those with the Aγ-117 hereditary persistence of fetal hemoglobin mutation, but adult levels of γ mRNA were significantly higher (≈5%) in lines carrying the mutation than in those without (≈1%). Reversion to the rapid switch of the LCRεGγAγδβ mice was observed in three lines with the HS2Aγβ neo construct in which expression of the tk-neo gene was approximately equal to that of the globin genes. The inclusion of the Aγ enhancer in HS2Aγβ mice did not alter the pattern of switching, or reduce the relatively high levels of γ mRNA in these lines. However, unlike other HS2 mice, the combination of HS2 and the Aγ enhancer resulted in copy number-dependent expression in HS2Aγenβ lines, with intrauterine death at ≈12.5 days gestation at high copy numbers. These results demonstrate that numerous elements throughout the β globin gene cluster interact to produce the correct pattern of developmental regulation of these genes. Furthermore, extinction of γ gene expression in adult life is not completely autonomous and is incomplete when HS2 is the only LCR element present.

Published

1997

19. Analysis of sequence variation underlying tissue-specific transcription factor binding and gene expression

Author

Christopher J Derry, Jacqueline A. Sloane-Stanley, Marco De Gobbi, Richard J. Gibbons, Jim R. Hughes, Karen M. Lower, Helena Ayyub, Douglas Vernimmen, Douglas R. Higgs, and David Garrick

Subjects

Molecular Sequence Data, Gene Expression, Genome-wide association study, Biology, Regulatory Sequences, Nucleic Acid, Genome, Polymorphism, Single Nucleotide, Erythroid Cells, Gene expression, Genetic variation, Genetics, Transcriptional regulation, Humans, Allele, Gene, Transcription factor, Genetics (clinical), Binding Sites, Base Sequence, Nucleoside Diphosphate Kinase D, Intracellular Signaling Peptides and Proteins, Genetic Variation, Genome-Wide Association Study, Protein Binding, Transcription Factors

Abstract

Although mutations causing monogenic disorders most frequently lie within the affected gene, sequence variation in complex disorders is more commonly found in noncoding regions. Furthermore, recent genome- wide studies have shown that common DNA sequence variants in noncoding regions are associated with "normal" variation in gene expression resulting in cell-specific and/or allele-specific differences. The mechanism by which such sequence variation causes changes in gene expression is largely unknown. We have addressed this by studying natural variation in the binding of key transcription factors (TFs) in the well-defined, purified cell system of erythropoiesis. We have shown that common polymorphisms frequently directly perturb the binding sites of key TFs, and detailed analysis shows how this causes considerable (~10-fold) changes in expression from a single allele in a tissue-specific manner. We also show how a SNP, located at some distance from the recognized TF binding site, may affect the recruitment of a large multiprotein complex and alter the associated chromatin modification of the variant regulatory element. This study illustrates the principles by which common sequence variation may cause changes in tissue-specific gene expression, and suggests that such variation may underlie an individual's propensity to develop complex human genetic diseases.

Published

2013

20. High-resolution analysis of cis-acting regulatory networks at the α-globin locus

Author

Karen M. Lower, Jiannis Ragoussis, Ian Dunham, Jim R. Hughes, Simon J. McGowan, Stephen S. Taylor, Jacqueline A. Sloane-Stanley, Marco De Gobbi, Douglas R. Higgs, Richard J. Gibbons, and Douglas Vernimmen

Subjects

CCCTC-Binding Factor, Sequence analysis, Gene regulatory network, Locus (genetics), beta-Globins, Biology, Regulatory Sequences, Nucleic Acid, General Biochemistry, Genetics and Molecular Biology, Chromosome conformation capture, Open Reading Frames, Gene mapping, alpha-Globins, Gene cluster, Protein Interaction Mapping, Humans, Gene Regulatory Networks, Promoter Regions, Genetic, Gene, Genetics, Genome, Human, Articles, Chromatin Assembly and Disassembly, Repressor Proteins, Genetic Loci, Human genome, General Agricultural and Biological Sciences, Chromosomes, Human, Pair 16

Abstract

We have combined the circular chromosome conformation capture protocol with high-throughput, genome-wide sequence analysis to characterize the cis -acting regulatory network at a single locus. In contrast to methods which identify large interacting regions (10–1000 kb), the 4C approach provides a comprehensive, high-resolution analysis of a specific locus with the aim of defining, in detail, the cis -regulatory elements controlling a single gene or gene cluster. Using the human α-globin locus as a model, we detected all known local and long-range interactions with this gene cluster. In addition, we identified two interactions with genes located 300 kb (NME4) and 625 kb (FAM173a) from the α-globin cluster.

Published

2013

21. Established Epigenetic Modifications Determine the Expression of Developmentally Regulated Globin Genes in Somatic Cell Hybrids

Author

S J Stanworth, Jacqueline A. Sharpe, Nigel A. Roberts, William G. Wood, and Jacqueline A. Sloane-Stanley

Subjects

Erythroblasts, Transgene, Mice, Transgenic, Hybrid Cells, Biology, Mice, hemic and lymphatic diseases, Gene cluster, Gene expression, Animals, Humans, RNA, Messenger, Epigenetics, Molecular Biology, Gene, Gene Expression Regulation, Developmental, Cell Biology, Transfection, Embryo, Mammalian, Fetal Blood, Embryonic stem cell, Molecular biology, Recombinant Proteins, Globins, Mice, Inbred C57BL, Blood, Liver, Gamma Rays, Naked DNA, Karyotyping, Multigene Family, Mice, Inbred CBA, Genes, Switch, Spleen, Research Article

Abstract

Somatic cell hybrids generated from transgenic mouse cells have been used to examine the developmental regulation of human gamma-to-beta-globin gene switching. In hybrids between mouse erythroleukemia (MEL) cells and transgenic erythroblasts taken at various stages of development, there was regulated expression of the human fetal gamma and adult beta genes, reproducing the in vivo pattern prior to fusion. Hybrids formed from embryonic blood cells produced predominantly gamma mRNA, whereas beta gene expression was observed in adult hybrids and a complete range of intermediate patterns was found in fetal liver hybrids. The adult environment of the MEL cells, therefore, did not appear to influence selective transcription from this gene complex. Irradiation of the embryonic erythroid cells prior to fusion resulted in hybrids containing only small fragments of donor chromosomes, but the pattern of gene expression did not differ from that of unirradiated hybrids. This finding suggests that continued expression of trans-acting factors from the donor erythroblasts is not necessary for continued expression of the human gamma gene in MEL cells. These results contrast with the lack of developmental regulation of the cluster after transfection of naked DNA into MEL cells and suggest that epigenetic processes established during normal development result in the gene cluster adopting a developmental stage-specific, stable conformation which is maintained through multiple rounds of replication and transcription in the MEL cell hybrids. On prolonged culture, hybrids that initially expressed only the gamma transgene switched to beta gene expression. The time period of switching, from approximately 10 to > 40 weeks, was similar to that seen previously in human fetal erythroblast x MEL cell hybrids but in this case bore no relationship to the time of in vivo switching. It seems unlikely, therefore, that switching in these hybrids is regulated by a developmental clock.

Published

1995

22. Nprl3 is required for normal development of the cardiovascular system

Author

Shoumo Bhattacharya, Monika S. Kowalczyk, William G. Wood, Richard J. Gibbons, Gillian M. Morriss-Kay, Luis Sanchez-Pulido, Jacqueline A. Sloane-Stanley, Christian Babbs, Jacqueline A. Sharpe, Dorota Szumska, Leslie B. Smoot, Jim R. Hughes, Chris P. Ponting, Douglas R. Higgs, Amy E. Roberts, and Hugh Watkins

Subjects

Heart Defects, Congenital, Male, DNA Mutational Analysis, Molecular Sequence Data, Biology, Cardiovascular System, Polymorphism, Single Nucleotide, Mice, Gene expression, Genetics, Animals, Humans, Abnormalities, Multiple, Amino Acid Sequence, Nuclear protein, Promoter Regions, Genetic, Gene, Peptide sequence, PI3K/AKT/mTOR pathway, Cells, Cultured, Genetic Association Studies, Mice, Knockout, Gene Expression Profiling, Myocardium, GTPase-Activating Proteins, Intracellular Signaling Peptides and Proteins, Nuclear Proteins, Molecular Sequence Annotation, NPRL3, Gene expression profiling, Phenotype, Female, Homologous recombination

Abstract

C16orf35 is a conserved and widely expressed gene lying adjacent to the human α-globin cluster in all vertebrate species. In-depth sequence analysis shows that C16orf35 (now called NPRL3) is an orthologue of the yeast gene Npr3 (nitrogen permease regulator 3) and, furthermore, is a paralogue of its protein partner Npr2. The yeast Npr2/3 dimeric protein complex senses amino acid starvation and appropriately adjusts cell metabolism via the TOR pathway. Here we have analysed a mouse model in which expression of Nprl3 has been abolished using homologous recombination. The predominant effect on RNA expression appears to involve genes that regulate protein synthesis and cell cycle, consistent with perturbation of the mTOR pathway. Embryos homozygous for this mutation die towards the end of gestation with a range of cardiovascular defects, including outflow tract abnormalities and ventriculoseptal defects consistent with previous observations, showing that perturbation of the mTOR pathway may affect development of the myocardium. NPRL3 is a candidate gene for harbouring mutations in individuals with developmental abnormalities of the cardiovascular system. © 2012 Springer Science+Business Media, LLC.

Published

2012

23. Polycomb eviction as a new distant enhancer function

Author

Magnus D. Lynch, Andrew J.H. Smith, David Garrick, Douglas Vernimmen, Jacqueline A. Sharpe, Jacqueline A. Sloane-Stanley, Douglas R. Higgs, and Marco De Gobbi

Subjects

Chromatin Immunoprecipitation, animal structures, Enhancer Elements, Cells, Polycomb-Group Proteins, macromolecular substances, Cell Line, CpG islands, Research Communication, Genetic, Genetics, Polycomb-group proteins, Animals, Humans, Erythropoiesis, Protein Methyltransferases, Enhancer, Psychological repression, Cells, Cultured, Medicine(all), Regulation of gene expression, Cultured, biology, fungi, Chromatin, Repressor Proteins, Enhancer Elements, Genetic, CpG site, Gene Expression Regulation, physiology, biology.protein, chromatin, Demethylase, CpG Islands, enhancer, Animals, Cell Line, Cells, Cultured, Chromatin Immunoprecipitation, Chromatin, metabolism, CpG Islands, Enhancer Elements, physiology, Erythropoiesis, physiology, Gene Expression Regulation, Humans, Protein Binding, Protein Methyltransferases, metabolism, Repressor Proteins, metabolism, polycomb, Chromatin immunoprecipitation, Developmental Biology, Protein Binding

Abstract

Remote distal enhancers may be located tens or thousands of kilobases away from their promoters. How they control gene expression is still poorly understood. Here, we analyze the influence of a remote enhancer on the balance between repression (Polycomb-PcG) and activation (Trithorax-TrxG) of a developmentally regulated gene associated with a CpG island. We reveal its essential, nonredundant role in clearing the PcG complex and H3K27me3 from the CpG island. In the absence of the enhancer, the H3K27me3 demethylase (JMJD3) is not recruited to the CpG island. We propose a new role of long-range regulatory elements in removing repressive PcG complexes. © 2011 by Cold Spring Harbor Laboratory Press.

Published

2011

24. Codanin-1 mutations in congenital dyserythropoietic anemia type 1 affect HP1{alpha} localization in erythroblasts

Author

Nigel A. Roberts, Jacqueline A. Sloane-Stanley, Douglas R. Higgs, Marco De Gobbi, Louise E. Bird, Tasneem Hassanali, Jacqueline A. Sharpe, Veronica J. Buckle, Raffaele Renella, Jill M. Brown, David J. P. Ferguson, William G. Wood, and Jacqueline Cordell

Subjects

Ineffective erythropoiesis, Male, Congenital dyserythropoietic anemia type II, Erythroblasts, Dyserythropoietic, analysis, Chromosomal Proteins, Non-Histone, Vesicular Transport Proteins, analysis/genetics, medicine.disease_cause, Inbred C57BL, Biochemistry, Congenital, Mice, genetics, Cells, Cultured, Anemia, Dyserythropoietic, Congenital, Genetics, Tumor, Cultured, medicine.diagnostic_test, biology, Nuclear Proteins, Anemia, Hematology, Chromatin, Cell biology, Chromosomal Proteins, Histone, Female, Dyserythropoietic anemia, metabolism/pathology, Cells, Immunology, Immunofluorescence, Cell Line, Congenital dyserythropoietic anemia type I, Cell Line, Tumor, medicine, Animals, Humans, Glycoproteins, genetics/pathology, Cell Biology, Non-Histone, medicine.disease, genetics/pathology, Animals, Carrier Proteins, genetics, Cell Line, Tumor, Cells, Cultured, Chromatin, pathology, Chromosomal Proteins, analysis, Erythroblasts, metabolism/pathology, Female, Glycoproteins, analysis/genetics, Humans, Male, Mice, Mice, Inbred C57BL, Mutation, Vesicular Transport Proteins, Mice, Inbred C57BL, Chromobox Protein Homolog 5, Mutation, biology.protein, pathology, Congenital dyserythropoietic anemia, Carrier Proteins

Abstract

Abstract 1003 Introduction: The Congenital dyserythropoietic anemias (CDAs) are a heterogeneous group of rare inborn disorders mainly affecting erythropoiesis. Distinct from other inherited bone marrow failure syndromes, they are marked by morphological abnormalities of the erythroblasts leading to ineffective erythropoiesis/dyserythropoiesis, while the other hematopoietic lineages appear to be unaffected. Based largely on the dysplastic changes observed in erythroblasts by light and electron microscopy, the CDAs have been divided into 3 major types (CDA-1, 2 and 3). Causative genes have been identified for CDA-1 (CDAN1/15q15) and CDA-2 (CDAN2/20p11), while the chromosomal locus is known for CDA-3 (15q22). The majority of CDA-1 cases are associated with CDAN1 missense mutations, leading to single amino-acid substitutions in the 134 kDa Codanin-1 protein. Electron microscopy of CDA-1 erythroblasts reveals a characteristic pattern of spongy (“Swiss cheese”) heterochromatin. We investigated the chromatin in CDA-1 patients, the localization, distribution and interactions of Codanin-1 and generated a murine knock-out model for CDAN1. Results: Given the grossly abnormal chromatin ultrastructure in CDA-1 erythroblasts, we examined its overall content. No gross differences between normal and patient samples were seen, both in the amounts of histone proteins or various epigenetic marks of histone tails, suggesting that histone signatures, involved in maintenance of chromatin structure and epigenetic regulation, are globally maintained CDA-1. We confirmed the latter by ChIP-on-chip analysis where immunoprecipitated H4 acetylated, H3K4 dimethylated, H3K9 trimethylated and H3K27 trimethylated chromatin from CDA-1 erythroblasts and normal controls was hybridized to ENCODE genome-wide microrrays. Using a hybridoma technique, we produced 3 novel monoclonal antibodies to Codanin-1. These consistently demonstrate its distribution in both nucleus and cytoplasm of cells by immunofluorescence and Western Blotting. While Codanin-1 is found in the nucleus, it is more abundant in the cytoplasm in primary human erythroblasts. This localization pattern was unchanged in CDA-1 erythroblasts. Within the nucleus, Codanin-1 is localized in foci, while in the cytoplasm it shows an aggregated distribution, with the endoplasmic reticulum and Golgi apparatus being the most likely locations. No differences were found in the distribution patterns of RNA-polymerase-II, PML, nucleophosmin, HP1β and HP1γ between patients' and control erythroblasts. However, the localization of HP1α, a key component of heterochromatin, was found to be markedly perturbed. HP1α accumulates in the Golgi apparatus of CDA-1 but not normal erythroblasts. This was not seen in lymphoblasts derived from CDA-1 patients, nor in erythroblasts from a patient with CDA-2. We confirmed that the abnormal localization of HP1α in CDA-1 patients is confined to the intermediate erythroblast maturation stage, where the characteristic ultrastructural chromatin pattern of CDA-1 is observed. Immunoprecipitation of erythroblast protein extracts with anti- HP1α antibodies co-precipitated Codanin-1, suggesting that an abnormality in Codanin-1 could be responsible for the aberrant localization of HP1α. By confocal immunofluorescence, we also found Codanin-1 to co-localize partially with SEC23B, the protein mutated in CDA-2, suggesting a molecular link between the two major types of CDA. We generated the first murine Cdan1 gene-trap model demonstrating its widespread expression during embryonic development. Cdan1gt/gt homozygotes die in-utero before the onset of primitive erythropoiesis, suggesting that Cdan1 has other critical roles during embryogenesis. Adult heterozygous Cdan1wt/gt mice had normal hematopoietic function and morphology, normal life expectancy and fertility. No extra-hematopoietic macroscopic phenotype could be identified. Conclusions: Our results show that the absence of the highly conserved and ubiquitously expressed Codanin-1 is embryonic lethal, and suggest that missense CDAN1 mutations are responsible for the erythroid specific phenotype of CDA-1 via the abnormal cellular trafficking of the heterochromatin protein HP1α. Moreover, our findings suggest that common molecular pathways underlie the CDAs. Disclosures: No relevant conflicts of interest to declare.

Published

2011

25. Chromosome looping at the human alpha-globin locus is mediated via the major upstream regulatory element (HS-40)

Author

Douglas R. Higgs, Fatima Marques-Kranc, Jacqueline A. Sloane-Stanley, Helen Wallace, Jacqueline A. Sharpe, Andrew J.H. Smith, William G. Wood, and Douglas Vernimmen

Subjects

Male, Immunology, Gene regulatory network, Mice, Transgenic, Biology, Biochemistry, Cell Line, Chromosome conformation capture, Mice, alpha-Globins, Animals, Chromosomes, Human, Humans, Erythropoiesis, Gene Regulatory Networks, Regulatory Elements, Transcriptional, Globin, Promoter Regions, Genetic, Gene, Cells, Cultured, Genetics, Regulation of gene expression, Base Sequence, Promoter, Cell Biology, Hematology, Cell biology, Mice, Inbred C57BL, Regulatory sequence, Multigene Family, Humanized mouse, Female, DNA Probes

Abstract

Previous studies in the mouse have shown that high levels of α-globin gene expression in late erythropoiesis depend on long-range, physical interactions between remote upstream regulatory elements and the globin promoters. Using quantitative chromosome conformation capture (q3C), we have now analyzed all interactions between 4 such elements lying 10 to 50 kb upstream of the human α cluster and their interactions with the α-globin promoter. All of these elements interact with the α-globin gene in an erythroid-specific manner. These results were confirmed in a mouse model of human α globin expression in which the human cluster replaces the mouse cluster in situ (humanized mouse). We have also shown that expression and all of the long-range interactions depend largely on just one of these elements; removal of the previously characterized major regulatory element (called HS −40) results in loss of all the interactions and α-globin expression. Reinsertion of this element at an ectopic location restores both expression and the intralocus interactions. In contrast to other more complex systems involving multiple upstream elements and promoters, analysis of the human α-globin cluster during erythropoiesis provides a simple and tractable model to understand the mechanisms underlying long-range gene regulation.

Published

2009

26. Defining the cause of skewed X-chromosome inactivation in X-linked mental retardation by use of a mouse model

Author

Patrick M. Nolan, Richard J. Gibbons, Mary R. Muers, Terry Hacker, David Garrick, Douglas R. Higgs, Jacqueline A. Sloane-Stanley, Jacqueline A. Sharpe, and William G. Wood

Subjects

Male, Heterozygote, X-linked Nuclear Protein, X Chromosome, Population, Mice, Transgenic, Biology, Cell fate determination, medicine.disease_cause, X-inactivation, Article, Mice, X Chromosome Inactivation, medicine, Genetics, Animals, Humans, Genetics(clinical), Allele, Selection, Genetic, education, Fluorescent Antibody Technique, Indirect, Skewed X-inactivation, Genetics (clinical), X chromosome, ATRX, Alleles, Crosses, Genetic, Mutation, education.field_of_study, DNA Helicases, Nuclear Proteins, Flow Cytometry, Immunohistochemistry, Mice, Inbred C57BL, Disease Models, Animal, Mental Retardation, X-Linked, Mice, Inbred CBA, Female

Abstract

Extreme skewing of X-chromosome inactivation (XCI) is rare in the normal female population but is observed frequently in carriers of some X-linked mutations. Recently, it has been shown that various forms of X-linked mental retardation (XLMR) have a strong association with skewed XCI in female carriers, but the mechanisms underlying this skewing are unknown. ATR-X syndrome, caused by mutations in a ubiquitously expressed, chromatin-associated protein, provides a clear example of XLMR in which phenotypically normal female carriers virtually all have highly skewed XCI biased against the X chromosome that harbors the mutant allele. Here, we have used a mouse model to understand the processes causing skewed XCI. In female mice heterozygous for a null Atrx allele, we found that XCI is balanced early in embryogenesis but becomes skewed over the course of development, because of selection favoring cells expressing the wild-type Atrx allele. Unexpectedly, selection does not appear to be the result of general cellular-viability defects in Atrx-deficient cells, since it is restricted to specific stages of development and is not ongoing throughout the life of the animal. Instead, there is evidence that selection results from independent tissue-specific effects. This illustrates an important mechanism by which skewed XCI may occur in carriers of XLMR and provides insight into the normal role of ATRX in regulating cell fate.

Published

2007

27. Discovering Regulatory SNPs by Genome-Wide Analysis of Differential Scl/TAL-1 Occupancy in Human Primary Erythroid Cells

Author

Douglas R. Higgs, Nigel A. Roberts, C J Derry, Stephen S. Taylor, Karen M. Lower, Emanuele Marchi, Catherine Porcher, M De Gobbi, Jacqueline A. Sloane-Stanley, Jim R. Hughes, and Richard J. Gibbons

Subjects

Genetics, Immunology, Single-nucleotide polymorphism, Promoter, Genome-wide association study, Cell Biology, Hematology, Biology, Biochemistry, Chromatin, SNP, Enhancer, Gene, Transcription factor

Abstract

Abstract 3381 It is well established that the level of gene expression can vary significantly between normal individuals, and that the majority of this variation is due to naturally occurring genomic variability caused by single nucleotide polymorphisms (SNPs). Therefore, identifying functional cis-regulatory polymorphisms and understanding how they influence gene expression is an important new task in many areas of medical research, including molecular hematology. We have previously shown that an entirely new form of alpha-thalassemia is caused by a gain of function regulatory SNP in an unremarkable non-coding region in the alpha-globin cluster. This SNP creates a novel, functional GATA site, which recruits a tissue-specific transcription factor (TF) complex. This creates a new promoter-like element, which interferes with activation of the globin genes (De Gobbi et al. Science 2006,312:1215–1257). Here, to investigate the extent and the impact of this class of regulatory SNP, using ChIP-Seq we characterized differences in the occupancy of Scl/TAL-1 (a tissue-specific TF critical for erythroid maturation) in the erythroblasts of two individuals from the same ethnic background (Caucasian 1, C1, and Caucasian 2, C2). Sequence reads from two biological replicates of each individual were merged and aligned to the human reference genome (NCBI36/hg18) and a total of 2936 Scl/TAL-1 bound regions were identified. Using two de novo motif finding algorithms (MEME and DREME), we identified GATA (WGATAR) and E-box (CAGMTG) sites as the preferred sequences associated with in vivo binding of Scl/TAL-1. In addition, other motifs were enriched at the Scl/TAL-1 targets; among these were binding sites for known TFs (Sp1/Klf, RUNX1 and NFE2). To identify differentially bound regions between C1 and C2, a two-class paired-test, Rank Product analysis (500 permutations, FDR Since it has been previously shown that the function of active transcriptional elements can be predicted on the basis of chromatin signatures (e.g. enhancers marked by H3K4me1 and promoters marked by H3K4me3), to further characterize the Scl/TAL-1 differentially occupied sites, we asked which chromatin signatures are associated with these regions. H3K4me1 and H3K4me3 ChIP-Seq experiments, together with analyses of publicly available data sets, showed that the most of the SNPs responsible for variation in the recruitment of Scl/TAL-1 (23/25) lie in DNA sequences that have chromatin signatures predictive of enhancer elements, suggesting a potential long-range function in modulating gene expression. Finally, Scl/TAL-1 ChIP-Seq analysis of erythroblasts of a third individual from a different ethnic background (African-Caribbean, A3) revealed more distinctive targets including a well known regulatory SNP at the promoter of the DARC gene (encoding the Duffy blood group), which alters a GATA binding motif in A3, conferring the malaria-resistant Duffy-null phenotype. Given the exponential growth in genome-wide association studies by which numerous SNPs are being either associated with hematological parameters, or implicated in the etiology of hematologic disorders, this study elucidates molecular mechanisms which might account for phenotypic diversity and highlights the importance of carrying out functional characterization of non-coding polymorphisms found to be associated with disease risk. Disclosures: No relevant conflicts of interest to declare.

Published

2011

28. Generation of bivalent chromatin domains during cell fate decisions

Author

Jim R. Hughes, Paresh Vyas, Stephen S. Taylor, Douglas Vernimmen, Douglas R. Higgs, Shamit Soneji, Jacqueline A. Sloane-Stanley, Sidinh Luc, Cristina Pina, David Garrick, Nicolas Goardon, Richard J. Gibbons, Karen M. Lower, Tariq Enver, Marco De Gobbi, Sten Eirik W. Jacobsen, Raffaele Renella, and Magnus D. Lynch

Subjects

Genetics, 0303 health sciences, lcsh:QH426-470, Research, Biology, Cell fate determination, Chromatin remodeling, Chromatin, Cell biology, 03 medical and health sciences, lcsh:Genetics, 0302 clinical medicine, Histone, 030220 oncology & carcinogenesis, biology.protein, H3K4me3, Epigenetics, Induced pluripotent stem cell, Molecular Biology, 030304 developmental biology, Bivalent chromatin

Abstract

Background In self-renewing, pluripotent cells, bivalent chromatin modification is thought to silence (H3K27me3) lineage control genes while 'poising' (H3K4me3) them for subsequent activation during differentiation, implying an important role for epigenetic modification in directing cell fate decisions. However, rather than representing an equivalently balanced epigenetic mark, the patterns and levels of histone modifications at bivalent genes can vary widely and the criteria for identifying this chromatin signature are poorly defined. Results Here, we initially show how chromatin status alters during lineage commitment and differentiation at a single well characterised bivalent locus. In addition we have determined how chromatin modifications at this locus change with gene expression in both ensemble and single cell analyses. We also show, on a global scale, how mRNA expression may be reflected in the ratio of H3K4me3/H3K27me3. Conclusions While truly 'poised' bivalently modified genes may exist, the original hypothesis that all bivalent genes are epigenetically premarked for subsequent expression might be oversimplistic. In fact, from the data presented in the present work, it is equally possible that many genes that appear to be bivalent in pluripotent and multipotent cells may simply be stochastically expressed at low levels in the process of multilineage priming. Although both situations could be considered to be forms of 'poising', the underlying mechanisms and the associated implications are clearly different.