Your search keyword '"Higgs DR"' showing total 4,981 results

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

Author

Kowalczyk MS, Hughes JR, Babbs C, Sanchez-Pulido L, Szumska D, Sharpe JA, Sloane-Stanley JA, Morriss-Kay GM, Smoot LB, Roberts AE, Watkins H, Bhattacharya S, Gibbons RJ, Ponting CP, Wood WG, and Higgs DR

Subjects

Abnormalities, Multiple genetics, Amino Acid Sequence, Animals, Cells, Cultured, DNA Mutational Analysis, Female, GTPase-Activating Proteins, Gene Expression Profiling, Genetic Association Studies, Heart Defects, Congenital pathology, Humans, Intracellular Signaling Peptides and Proteins deficiency, Intracellular Signaling Peptides and Proteins physiology, Male, Mice, Mice, Knockout, Molecular Sequence Annotation, Molecular Sequence Data, Myocardium pathology, Phenotype, Polymorphism, Single Nucleotide, Promoter Regions, Genetic, Cardiovascular System embryology, Heart Defects, Congenital genetics, Intracellular Signaling Peptides and Proteins genetics, Nuclear Proteins genetics

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.

Published

2012

152. Intragenic enhancers act as alternative promoters.

Author

Kowalczyk MS, 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 L, Gibbons RJ, Flint J, Taylor S, Buckle VJ, Milne TA, Wood WG, and Higgs DR

Subjects

Animals, Cells, Cultured, Erythroid Cells, Mice, Poly A, RNA chemistry, RNA physiology, RNA Isoforms chemistry, RNA, Messenger chemistry, RNA, Messenger physiology, Transcriptome, Enhancer Elements, Genetic physiology, Gene Expression Regulation, Promoter Regions, Genetic physiology

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., (Copyright © 2012 Elsevier Inc. All rights reserved.)

Published

2012

153. Molecular biology: RNA discrimination.

Author

Kowalczyk MS, Higgs DR, and Gingeras TR

Subjects

Animals, Humans, MicroRNAs genetics, MicroRNAs metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, RNA, Untranslated classification, RNA, Untranslated genetics, Transcription, Genetic, RNA, Untranslated metabolism

Published

2012

154. Thalassaemia.

Author

Higgs DR, Engel JD, and Stamatoyannopoulos G

Subjects

Genetic Therapy, Humans, Stem Cell Transplantation, Thalassemia diagnosis, Thalassemia genetics, Thalassemia physiopathology, Thalassemia therapy

Abstract

Thalassaemia is one of the most common genetic diseases worldwide, with at least 60,000 severely affected individuals born every year. Individuals originating from tropical and subtropical regions are most at risk. Disorders of haemoglobin synthesis (thalassaemia) and structure (eg, sickle-cell disease) were among the first molecular diseases to be identified, and have been investigated and characterised in detail over the past 40 years. Nevertheless, treatment of thalassaemia is still largely dependent on supportive care with blood transfusion and iron chelation. Since 1978, scientists and clinicians in this specialty have met regularly in an international effort to improve the management of thalassaemia, with the aim of increasing the expression of unaffected fetal genes to improve the deficiency in adult β-globin synthesis. In this Seminar we discuss important advances in the understanding of the molecular and cellular basis of normal and abnormal expression of globin genes. We will summarise new approaches to the development of tailored pharmacological agents to alter regulation of globin genes, the first trial of gene therapy for thalassaemia, and future prospects of cell therapy., (Copyright © 2012 Elsevier Ltd. All rights reserved.)

Published

2012

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

Author

Lynch MD, Smith AJ, De Gobbi M, Flenley M, Hughes JR, Vernimmen D, Ayyub H, Sharpe JA, Sloane-Stanley JA, Sutherland L, Meek S, Burdon T, Gibbons RJ, Garrick D, and Higgs DR

Subjects

Animals, Cells, Cultured metabolism, Chromatin genetics, Chromosome Mapping, Chromosomes, Human, Pair 16, DNA Methylation, DNA, Recombinant genetics, Embryonic Stem Cells metabolism, Humans, Mice, Mice, Transgenic, Pluripotent Stem Cells metabolism, Polycomb-Group Proteins, Recombination, Genetic, Regulatory Sequences, Nucleic Acid, Species Specificity, Transcription, Genetic, CpG Islands physiology, Gene Expression Regulation genetics, Repressor Proteins metabolism, alpha-Globins genetics

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

2012

156. Polycomb eviction as a new distant enhancer function.

Author

Vernimmen D, Lynch MD, De Gobbi M, Garrick D, Sharpe JA, Sloane-Stanley JA, Smith AJ, and Higgs DR

Subjects

Animals, Cell Line, Cells, Cultured, Chromatin metabolism, Chromatin Immunoprecipitation, CpG Islands, Erythropoiesis physiology, Gene Expression Regulation, Humans, Polycomb-Group Proteins, Protein Binding, Protein Methyltransferases metabolism, Enhancer Elements, Genetic physiology, Repressor Proteins metabolism

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.

Published

2011

157. Functional significance of mutations in the Snf2 domain of ATRX.

Author

Mitson M, Kelley LA, Sternberg MJ, Higgs DR, and Gibbons RJ

Subjects

Amino Acid Sequence, Animals, Cell Line, DNA Helicases chemistry, Enzyme Activation physiology, Humans, Insecta, Mental Retardation, X-Linked enzymology, Mental Retardation, X-Linked genetics, Models, Molecular, Molecular Sequence Data, Nuclear Proteins chemistry, Protein Conformation, Protein Stability, Sequence Alignment, Translocation, Genetic genetics, Ubiquitin-Protein Ligases chemistry, X-linked Nuclear Protein, alpha-Thalassemia enzymology, alpha-Thalassemia genetics, DNA Helicases genetics, DNA Helicases metabolism, Mutation genetics, Nuclear Proteins genetics, Nuclear Proteins metabolism, Ubiquitin-Protein Ligases genetics

Abstract

ATRX is a member of the Snf2 family of chromatin-remodelling proteins and is mutated in an X-linked mental retardation syndrome associated with alpha-thalassaemia (ATR-X syndrome). We have carried out an analysis of 21 disease-causing mutations within the Snf2 domain of ATRX by quantifying the expression of the ATRX protein and placing all missense mutations in their structural context by homology modelling. While demonstrating the importance of protein dosage to the development of ATR-X syndrome, we also identified three mutations which primarily affect function rather than protein structure. We show that all three of these mutant proteins are defective in translocating along DNA while one mutant, uniquely for a human disease-causing mutation, partially uncouples adenosine triphosphate (ATP) hydrolysis from DNA binding. Our results highlight important mechanistic aspects in the development of ATR-X syndrome and identify crucial functional residues within the Snf2 domain of ATRX. These findings are important for furthering our understanding of how ATP hydrolysis is harnessed as useful work in chromatin remodelling proteins and the wider family of nucleic acid translocating motors.

Published

2011

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

Author

Renella R, Roberts NA, Brown JM, De Gobbi M, Bird LE, Hassanali T, Sharpe JA, Sloane-Stanley J, Ferguson DJ, Cordell J, Buckle VJ, Higgs DR, and Wood WG

Subjects

Animals, Carrier Proteins genetics, Cell Line, Tumor, Cells, Cultured, Chromatin pathology, Chromobox Protein Homolog 5, Erythroblasts metabolism, Female, Glycoproteins analysis, Humans, Male, Mice, Mice, Inbred C57BL, Nuclear Proteins, Vesicular Transport Proteins analysis, Anemia, Dyserythropoietic, Congenital genetics, Anemia, Dyserythropoietic, Congenital pathology, Chromosomal Proteins, Non-Histone analysis, Erythroblasts pathology, Glycoproteins genetics, Mutation

Abstract

Congenital dyserythropoietic anemia type 1 (CDA-1), a rare inborn anemia characterized by abnormal chromatin ultrastructure in erythroblasts, is caused by abnormalities in codanin-1, a highly conserved protein of unknown function. We have produced 3 monoclonal antibodies to codanin-1 that demonstrate its distribution in both nucleus and cytoplasm by immunofluorescence and allow quantitative measurements of patient and normal material by Western blot. A detailed analysis of chromatin structure in CDA-1 erythroblasts shows no abnormalities in overall histone composition, and the genome-wide epigenetic landscape of several histone modifications is maintained. However, immunofluorescence analysis of intermediate erythroblasts from patients with CDA-1 reveals abnormal accumulation of HP1α in the Golgi apparatus. A link between mutant codanin-1 and the aberrant localization of HP1α is supported by the finding that codanin-1 can be coimmunoprecipitated by anti-HP1α antibodies. Furthermore, we show colocalization of codanin-1 with Sec23B, the protein defective in CDA-2 suggesting that the CDAs might be linked at the molecular level. Mice containing a gene-trapped Cdan1 locus demonstrate its widespread expression during development. Cdan1(gt/gt) homozygotes die in utero before the onset of primitive erythropoiesis, suggesting that Cdan1 has other critical roles during embryogenesis.

Published

2011

159. Combinatorial readout of histone H3 modifications specifies localization of ATRX to heterochromatin.

Author

Eustermann S, Yang JC, Law MJ, Amos R, Chapman LM, Jelinska C, Garrick D, Clynes D, Gibbons RJ, Rhodes D, Higgs DR, and Neuhaus D

Subjects

Binding Sites, Chromatin Assembly and Disassembly, Chromobox Protein Homolog 5, Chromosomal Proteins, Non-Histone chemistry, Chromosomal Proteins, Non-Histone metabolism, DNA Helicases metabolism, DNA Helicases physiology, Heterochromatin chemistry, Histone Code, Histones chemistry, Methylation, Nuclear Magnetic Resonance, Biomolecular, Nuclear Proteins metabolism, Nuclear Proteins physiology, X-linked Nuclear Protein, DNA Helicases chemistry, Heterochromatin metabolism, Histones metabolism, Nuclear Proteins chemistry

Abstract

Accurate read-out of chromatin modifications is essential for eukaryotic life. Mutations in the gene encoding X-linked ATRX protein cause a mental-retardation syndrome, whereas wild-type ATRX protein targets pericentric and telomeric heterochromatin for deposition of the histone variant H3.3 by means of a largely unknown mechanism. Here we show that the ADD domain of ATRX, in which most syndrome-causing mutations occur, engages the N-terminal tail of histone H3 through two rigidly oriented binding pockets, one for unmodified Lys4 and the other for di- or trimethylated Lys9. In vivo experiments show this combinatorial readout is required for ATRX localization, with recruitment enhanced by a third interaction through heterochromatin protein-1 (HP1) that also recognizes trimethylated Lys9. The cooperation of ATRX ADD domain and HP1 in chromatin recruitment results in a tripartite interaction that may span neighboring nucleosomes and illustrates how the 'histone-code' is interpreted by a combination of multivalent effector-chromatin interactions.

Published

2011

160. Generation of bivalent chromatin domains during cell fate decisions.

Author

De Gobbi M, Garrick D, Lynch M, Vernimmen D, Hughes JR, Goardon N, Luc S, Lower KM, Sloane-Stanley JA, Pina C, Soneji S, Renella R, Enver T, Taylor S, Jacobsen SE, Vyas P, Gibbons RJ, and Higgs DR

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.

Published

2011

161. Global gene expression analysis of human erythroid progenitors.

Author

Merryweather-Clarke AT, Atzberger A, Soneji S, Gray N, Clark K, Waugh C, McGowan SJ, Taylor S, Nandi AK, Wood WG, Roberts DJ, Higgs DR, Buckle VJ, and Robson KJ

Subjects

Cell Differentiation genetics, Cells, Cultured, Cluster Analysis, Erythroblasts metabolism, Erythroblasts physiology, Erythroid Precursor Cells chemistry, Erythropoiesis physiology, Flow Cytometry, Gene Expression Regulation, Developmental, Humans, Polymerase Chain Reaction, Erythroid Precursor Cells metabolism, Erythroid Precursor Cells physiology, Erythropoiesis genetics, Gene Expression Profiling methods, Microarray Analysis methods

Abstract

Understanding the pattern of gene expression during erythropoiesis is crucial for a synthesis of erythroid developmental biology. Here, we isolated 4 distinct populations at successive erythropoietin-dependent stages of erythropoiesis, including the terminal, pyknotic stage. The transcriptome was determined using Affymetrix arrays. First, we demonstrated the importance of using defined cell populations to identify lineage and temporally specific patterns of gene expression. Cells sorted by surface expression profile not only express significantly fewer genes than unsorted cells but also demonstrate significantly greater differences in the expression levels of particular genes between stages than unsorted cells. Second, using standard software, we identified more than 1000 transcripts not previously observed to be differentially expressed during erythroid maturation, 13 of which are highly significantly terminally regulated, including RFXAP and SMARCA4. Third, using matched filtering, we identified 12 transcripts not previously reported to be continuously up-regulated in maturing human primary erythroblasts. Finally, using transcription factor binding site analysis, we identified potential transcription factors that may regulate gene expression during terminal erythropoiesis. Our stringent lists of differentially regulated and continuously expressed transcripts containing many genes with undiscovered functions in erythroblasts are a resource for future functional studies of erythropoiesis. Our Human Erythroid Maturation database is available at https://cellline.molbiol.ox.ac.uk/eryth/index.html. [corrected].

Published

2011

162. Systematic documentation and analysis of human genetic variation in hemoglobinopathies using the microattribution approach.

Author

Giardine B, Borg J, Higgs DR, Peterson KR, Philipsen S, Maglott D, Singleton BK, Anstee DJ, Basak AN, Clark B, Costa FC, Faustino P, Fedosyuk H, Felice AE, Francina A, Galanello R, Gallivan MV, Georgitsi M, Gibbons RJ, Giordano PC, Harteveld CL, Hoyer JD, Jarvis M, Joly P, Kanavakis E, Kollia P, Menzel S, Miller W, Moradkhani K, Old J, Papachatzopoulou A, Papadakis MN, Papadopoulos P, Pavlovic S, Perseu L, Radmilovic M, Riemer C, Satta S, Schrijver I, Stojiljkovic M, Thein SL, Traeger-Synodinos J, Tully R, Wada T, Waye JS, Wiemann C, Zukic B, Chui DH, Wajcman H, Hardison RC, and Patrinos GP

Subjects

Base Sequence, DNA genetics, Data Mining, Genome, Human, Hemoglobins genetics, Human Genome Project, Humans, Molecular Sequence Data, Mutation, Promoter Regions, Genetic, Publishing, Databases, Genetic, Genetic Variation, Hemoglobinopathies genetics

Abstract

We developed a series of interrelated locus-specific databases to store all published and unpublished genetic variation related to hemoglobinopathies and thalassemia and implemented microattribution to encourage submission of unpublished observations of genetic variation to these public repositories. A total of 1,941 unique genetic variants in 37 genes, encoding globins and other erythroid proteins, are currently documented in these databases, with reciprocal attribution of microcitations to data contributors. Our project provides the first example of implementing microattribution to incentivise submission of all known genetic variation in a defined system. It has demonstrably increased the reporting of human variants, leading to a comprehensive online resource for systematically describing human genetic variation in the globin genes and other genes contributing to hemoglobinopathies and thalassemias. The principles established here will serve as a model for other systems and for the analysis of other common and/or complex human genetic diseases.

Published

2011

163. Hb S-β-thalassemia: molecular, hematological and clinical comparisons.

Author

Serjeant GR, Serjeant BE, Fraser RA, Hambleton IR, Higgs DR, Kulozik AE, and Donaldson A

Subjects

Adult, Anemia, Sickle Cell genetics, Anemia, Sickle Cell mortality, Anemia, Sickle Cell physiopathology, Child, Codon, Fetal Hemoglobin genetics, Genetic Association Studies, Hematologic Tests, Hemoglobin A2 genetics, Hemoglobins, Abnormal genetics, Humans, Infant, Newborn, Mutation, Neonatal Screening, Sequence Analysis, DNA, Survival Rate, beta-Thalassemia mortality, beta-Thalassemia physiopathology, beta-Thalassemia genetics

Abstract

Clinical and hematological features are presented for 261 patients with identified β-thalassemia (β-thal) mutations. Mutations causing Hb S [β6(A3)Glu→Val]-β(0)-thal were IVS-II-849 (A>G) in 44%, frameshift codon (FSC) 6 (-A) in 14%, Hb Monroe [β30(B12)Arg→Thr] in 14%, and IVS-II-1 (G>A) in 10%. Mutations causing Hb S-β(+)-thal with 14-25% Hb A (type III) were -29 (A>G) mutation in 60%, -88 (C>T) in 22% and the polyadenylation signal site (polyA) (T>C) mutation in 14%, and in Hb S-β(+)-thal with 1-7% Hb A (type I), all had the IVS-I-5 (G>C) mutation. Hematologically, only minor differences occurred between the four Hb S-β(0)-thal mutations, but among the three mutations causing Hb S-β(+)-thal type III, levels of Hb A(2), Hb F, hemoglobin (Hb), MCV and MCH were highest in the -88 and lowest in the polyA mutations. Clinically, Hb S-β(0)-thal and Hb S-β(+)-thal type I were generally severe, and Hb S-β(+)-thal type III disease with the -88 mutation was milder than that caused by the polyA mutation.

Published

2011

164. ATRX: taming tandem repeats.

Author

Gibbons RJ and Higgs DR

Subjects

CpG Islands, DNA Helicases genetics, DNA Replication, G-Quadruplexes, Histones genetics, Histones metabolism, Humans, Mental Retardation, X-Linked genetics, Mitochondrial Proteins genetics, Mitochondrial Proteins metabolism, NM23 Nucleoside Diphosphate Kinases genetics, NM23 Nucleoside Diphosphate Kinases metabolism, Nuclear Proteins genetics, Nucleoside Diphosphate Kinase D, X-linked Nuclear Protein, alpha-Thalassemia genetics, DNA Helicases metabolism, Nuclear Proteins metabolism, Tandem Repeat Sequences

Published

2010

165. The molecular basis of α-thalassemia: a model for understanding human molecular genetics.

Author

Higgs DR and Gibbons RJ

Subjects

Erythropoiesis genetics, Humans, Models, Genetic, Multigene Family, Mutation, Fetal Hemoglobin genetics, Hemoglobin A genetics, alpha-Globins genetics, alpha-Thalassemia genetics

Abstract

Down-regulation of α-globin synthesis causes α-thalassemia with underproduction of fetal (HbF, α(2)γ(2)) and adult (HbA, α(2)β(2)) hemoglobin. This article focuses on the human α-globin cluster, which has been characterized in great depth over the past 30 years. In particular the authors describe how the α genes are normally switched on during erythropoiesis and switched off as hematopoietic stem cells commit to nonerythroid lineages. In addition, the principles by which α-globin expression may be perturbed by natural mutations that cause α-thalassemia are reviewed., (Copyright © 2010 Elsevier Inc. All rights reserved.)

Published

2010

166. ATR-X syndrome protein targets tandem repeats and influences allele-specific expression in a size-dependent manner.

Author

Law MJ, Lower KM, Voon HP, Hughes JR, Garrick D, Viprakasit V, Mitson M, De Gobbi M, Marra M, Morris A, Abbott A, Wilder SP, Taylor S, Santos GM, Cross J, Ayyub H, Jones S, Ragoussis J, Rhodes D, Dunham I, Higgs DR, and Gibbons RJ

Subjects

Animals, Cells, Cultured, Chromatin Immunoprecipitation, Chromosomes, Mammalian metabolism, CpG Islands, DNA Helicases genetics, DNA, Ribosomal metabolism, G-Quadruplexes, Gene Expression, Genome-Wide Association Study, Histones metabolism, Humans, Mice, Minisatellite Repeats, Mutation, Nuclear Proteins genetics, Telomere metabolism, X-linked Nuclear Protein, DNA Helicases metabolism, Nuclear Proteins metabolism

Abstract

ATRX is an X-linked gene of the SWI/SNF family, mutations in which cause syndromal mental retardation and downregulation of α-globin expression. Here we show that ATRX binds to tandem repeat (TR) sequences in both telomeres and euchromatin. Genes associated with these TRs can be dysregulated when ATRX is mutated, and the change in expression is determined by the size of the TR, producing skewed allelic expression. This reveals the characteristics of the affected genes, explains the variable phenotypes seen with identical ATRX mutations, and illustrates a new mechanism underlying variable penetrance. Many of the TRs are G rich and predicted to form non-B DNA structures (including G-quadruplex) in vivo. We show that ATRX binds G-quadruplex structures in vitro, suggesting a mechanism by which ATRX may play a role in various nuclear processes and how this is perturbed when ATRX is mutated., (Copyright © 2010 Elsevier Inc. All rights reserved.)

Published

2010

167. Medicine. Sickle cell disease at 100 years.

Author

Orkin SH and Higgs DR

Subjects

Carrier Proteins genetics, Fetal Hemoglobin analysis, Fetal Hemoglobin biosynthesis, GTP-Binding Proteins genetics, Gene Expression Regulation, Genes, myb, Hemoglobin, Sickle chemistry, Hemoglobin, Sickle genetics, Humans, Multigene Family, Mutation, Nuclear Proteins genetics, Repressor Proteins, beta-Globins genetics, gamma-Globins genetics, Anemia, Sickle Cell blood, Anemia, Sickle Cell genetics, Anemia, Sickle Cell therapy, Fetal Hemoglobin genetics

Published

2010

168. Alpha-thalassaemia.

Author

Harteveld CL and Higgs DR

Subjects

Gene Deletion, Hemoglobins, Abnormal genetics, Hemoglobins, Abnormal metabolism, Humans, Mutation, alpha-Globins genetics, alpha-Globins metabolism, alpha-Thalassemia epidemiology, alpha-Thalassemia metabolism, alpha-Thalassemia diagnosis, alpha-Thalassemia genetics

Abstract

Alpha-thalassaemia is inherited as an autosomal recessive disorder characterised by a microcytic hypochromic anaemia, and a clinical phenotype varying from almost asymptomatic to a lethal haemolytic anaemia.It is probably the most common monogenic gene disorder in the world and is especially frequent in Mediterranean countries, South-East Asia, Africa, the Middle East and in the Indian subcontinent. During the last few decades the incidence of alpha thalassaemia in North-European countries and Northern America has increased because of demographic changes. Compound heterozygotes and some homozygotes have a moderate to severe form of alpha thalassaemia called HbH disease. Hb Bart's hydrops foetalis is a lethal form in which no alpha-globin is synthesized. Alpha thalassaemia most frequently results from deletion of one or both alpha genes from the chromosome and can be classified according to its genotype/phenotype correlation. The normal complement of four functional alpha-globin genes may be decreased by 1, 2, 3 or all 4 copies of the genes, explaining the clinical variation and increasing severity of the disease. All affected individuals have a variable degree of anaemia (low Hb), reduced mean corpuscular haemoglobin (MCH/pg), reduced mean corpuscular volume (MCV/fl) and a normal/slightly reduced level of HbA2. Molecular analysis is usually required to confirm the haematological observations (especially in silent alpha-thalassaemia and alpha-thalassaemia trait). The predominant features in HbH disease are anaemia with variable amounts of HbH (0.8-40%). The type of mutation influences the clinical severity of HbH disease. The distinguishing features of the haemoglobin Bart's hydrops foetalis syndrome are the presence of Hb Bart's and the total absence of HbF. The mode of transmission of alpha thalassaemia is autosomal recessive. Genetic counselling is offered to couples at risk for HbH disease or haemoglobin Bart's Hydrops Foetalis Syndrome. Carriers of alpha+- or alpha0-thalassaemia alleles generally do not need treatment. HbH patients may require intermittent transfusion therapy especially during intercurrent illness. Most pregnancies in which the foetus is known to have the haemoglobin Bart's hydrops foetalis syndrome are terminated due to the increased risk of both maternal and foetal morbidity.

Published

2010

169. Distinct factors control histone variant H3.3 localization at specific genomic regions.

Author

Goldberg AD, Banaszynski LA, Noh KM, Lewis PW, Elsaesser SJ, Stadler S, Dewell S, Law M, Guo X, Li X, Wen D, Chapgier A, DeKelver RC, Miller JC, Lee YL, Boydston EA, Holmes MC, Gregory PD, Greally JM, Rafii S, Yang C, Scambler PJ, Garrick D, Gibbons RJ, Higgs DR, Cristea IM, Urnov FD, Zheng D, and Allis CD

Subjects

Animals, Binding Sites, Cell Cycle Proteins genetics, Cell Cycle Proteins metabolism, Embryonic Stem Cells metabolism, Genome, Histone Chaperones genetics, Histone Chaperones metabolism, Histones genetics, Histones metabolism, Mice, Mice, Inbred C57BL, Telomere metabolism, Transcription Factors genetics, Transcription Factors metabolism, Transcription Initiation Site, Histones analysis, Telomere chemistry

Abstract

The incorporation of histone H3 variants has been implicated in the epigenetic memory of cellular state. Using genome editing with zinc-finger nucleases to tag endogenous H3.3, we report genome-wide profiles of H3 variants in mammalian embryonic stem cells and neuronal precursor cells. Genome-wide patterns of H3.3 are dependent on amino acid sequence and change with cellular differentiation at developmentally regulated loci. The H3.3 chaperone Hira is required for H3.3 enrichment at active and repressed genes. Strikingly, Hira is not essential for localization of H3.3 at telomeres and many transcription factor binding sites. Immunoaffinity purification and mass spectrometry reveal that the proteins Atrx and Daxx associate with H3.3 in a Hira-independent manner. Atrx is required for Hira-independent localization of H3.3 at telomeres and for the repression of telomeric RNA. Our data demonstrate that multiple and distinct factors are responsible for H3.3 localization at specific genomic locations in mammalian cells., ((c) 2010 Elsevier Inc. All rights reserved.)

Published

2010

170. Adventitious changes in long-range gene expression caused by polymorphic structural variation and promoter competition.

Author

Lower KM, Hughes JR, De Gobbi M, Henderson S, Viprakasit V, Fisher C, Goriely A, Ayyub H, Sloane-Stanley J, Vernimmen D, Langford C, Garrick D, Gibbons RJ, and Higgs DR

Subjects

Chromosomes, Human, Pair 16, Humans, Regulatory Sequences, Nucleic Acid, Telomere, alpha-Globins genetics, Gene Expression, Polymorphism, Single Nucleotide, Promoter Regions, Genetic

Abstract

It is well established that all of the cis-acting sequences required for fully regulated human alpha-globin expression are contained within a region of approximately 120 kb of conserved synteny. Here, we show that activation of this cluster in erythroid cells dramatically affects expression of apparently unrelated and noncontiguous genes in the 500 kb surrounding this domain, including a gene (NME4) located 300 kb from the alpha-globin cluster. Changes in NME4 expression are mediated by physical cis-interactions between this gene and the alpha-globin regulatory elements. Polymorphic structural variation within the globin cluster, altering the number of alpha-globin genes, affects the pattern of NME4 expression by altering the competition for the shared alpha-globin regulatory elements. These findings challenge the concept that the genome is organized into discrete, insulated regulatory domains. In addition, this work has important implications for our understanding of genome evolution, the interpretation of genome-wide expression, expression-quantitative trait loci, and copy number variant analyses.

Published

2009

171. Polycomb response elements in vertebrates.

Author

Garrick D, De Gobbi M, Gibbons R, and Higgs DR

Published

2009

172. The changing face of homozygous sickle cell disease: 102 patients over 60 years.

Author

Serjeant GR, Serjeant BE, Mason KP, Hambleton IR, Fisher C, and Higgs DR

Subjects

Aged, Aged, 80 and over, Female, Fetal Hemoglobin, Homozygote, Humans, Jamaica epidemiology, Longitudinal Studies, Male, Pregnancy, Pregnancy Complications, Hematologic, Retrospective Studies, beta-Globins genetics, Anemia, Sickle Cell complications, Anemia, Sickle Cell genetics, Anemia, Sickle Cell mortality

Abstract

Earlier reports on homozygous sickle cell (SS) disease have been biased by severely affected cases. The Jamaican clinic which seeks to avoid such bias has 102 patients surviving beyond 60 years. The objective of this study was to examine the features of elderly cases and assess factors determining survival and the behaviour of this disease with advancing age. A retrospective review of all cases and prospective assessment in survivors was conducted at The Sickle Cell Clinic at the University of the West Indies, Kingston, Jamaica previously operated by the MRC Laboratories. All patients with SS disease born prior to December 31, 1943 who would, by January 2004, have passed their 60th birthday were traced and their current status ascertained. The molecular and clinical features were assessed and observations on the clinical behaviour of the disease and of haematology and biochemistry are presented. Of the 102 patients, 58 had died, four had emigrated and 40 were alive, resident in Jamaica and aged 60-87 years. Survival was associated with female gender and higher foetal haemoglobin but not with alpha-thalassaemia or beta-globin haplotype. A tendency to familial clustering among elderly survivors did not reach statistical significance. Painful crises ameliorated with age and there was a benign course in pregnancy. Mean haemoglobin levels fell with age and were generally associated with rising creatinine levels indicating the importance of renal failure. Elderly survivors present some features of intrinsic mildness but also manifest age-related amelioration of painful crises and falling haemoglobin levels from progressive renal damage.

Published

2009

173. The regulatory interplay of CpG islands and nucleosome remodeling at mammalian primary response genes.

Author

Garrick D, De Gobbi M, Gibbons R, and Higgs DR

Published

2009

174. XNP/ATRX at sites of nucleosome replacement.

Author

Garrick D, De Gobbi M, Gibbons R, and Higgs DR

Published

2009

175. CTCF, cohesin and higher-order chromatin structure.

Author

Garrick D, De Gobbi M, Gibbons R, and Higgs DR

Published

2009

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

Author

Vernimmen D, Marques-Kranc F, Sharpe JA, Sloane-Stanley JA, Wood WG, Wallace HA, Smith AJ, and Higgs DR

Subjects

Animals, Base Sequence, Cell Line, Cells, Cultured, DNA Probes genetics, Erythropoiesis genetics, Female, Gene Regulatory Networks, Humans, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Multigene Family, Promoter Regions, Genetic, Regulatory Elements, Transcriptional, Chromosomes, Human genetics, alpha-Globins genetics

Abstract

Previous studies in the mouse have shown that high levels of alpha-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 alpha cluster and their interactions with the alpha-globin promoter. All of these elements interact with the alpha-globin gene in an erythroid-specific manner. These results were confirmed in a mouse model of human alpha 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 alpha-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 alpha-globin cluster during erythropoiesis provides a simple and tractable model to understand the mechanisms underlying long-range gene regulation.

Published

2009

177. Alpha zero-thalassemia due to recombination between the alpha 1-globin gene and an AluI repeat

Author

Nicholls, RD, Higgs, DR, Clegg, JB, and Weatherall, DJ

Abstract

A form of alpha zero-thalassemia found in subjects of Mediterranean origin has been analyzed by gene mapping and DNA sequencing. Homozygotes have the hemoglobin Bart's hydrops fetalis syndrome, while compound heterozygotes for this defect and alpha+-thalassemia have hemoglobin H disease. It results from a deletion that removes 20.5 kilobases of DNA from within the alpha-globin gene cluster. Sequence data from the regions adjacent to the breakpoint indicate that the recombination event that caused this deletion occurred between the alpha 1-gene and an unusual AluI sequence located between the embryonic zeta genes.

Published

1985

178. The polyadenylation site mutation in the alpha-globin gene cluster

Author

Thein, SL, Wallace, RB, Pressley, L, Clegg, JB, Weatherall, DJ, and Higgs, DR

Abstract

In a previous study, we described a form of nondeletion alpha- thalassemia (alpha T Saudi alpha) found in subjects of Saudi Arabian origin. In the current study, using synthetic oligoprobe hybridization and restriction enzyme analysis, we have demonstrated that the molecular basis of alpha T Saudi alpha is due solely to a single base mutation (AATAAA----AATAAG) in the polyadenylation signal of the alpha 2 gene and that the frameshift mutation in codon 14 of the linked alpha 1 gene is the result of a cloning artefact. The alpha 2 polyadenylation signal mutation occurs in other Middle Eastern and the Mediterranean populations and is responsible for the clinical phenotype of Hb H disease in some Saudi Arabian individuals with five alpha genes (alpha T Saudi alpha/(alpha alpha alpha)T Saudi). Evidence suggests that the (alpha alpha alpha)T Saudi haplotype has arisen as a result of a recombination between two misaligned chromosomes bearing the alpha T Saudi alpha defect.

Published

1988

179. The cellular basis for different fetal hemoglobin levels among sickle cell individuals with two, three, and four alpha-globin genes

Author

Dover, GJ, Chang, VT, Boyer, SH, Serjeant, GR, Antonarakis, S, and Higgs, DR

Abstract

Fetal hemoglobin (HbF) levels vary widely among individuals with sickle cell anemia (SS). Previous studies have suggested that HbF levels in SS individuals with alpha-thalassemia (two or three functional alpha- globin genes) are lower than HbF levels in SS individuals with four normal alpha-globin genes. Using immunocytochemical techniques, we studied F cell production as measured by % F reticulocytes, the amount of HbF per F cell, and the preferential survival of F cells versus non- F cells in 51 subjects with four alpha genes, 32 subjects with three alpha genes, and 18 subjects with two alpha genes. Comparison between alpha-globin gene groups was performed for the total sample as well as for a subset of 82 individuals who had replicate samples and a further subset of 39 age-matched individuals. %HbF levels were 6.8, 4.9, and 4.5 percent for the total four-, three-, and two-alpha-globin-gene groups, respectively. The percentage of F reticulocytes, percentage HbF per F cell, and the enrichment ratio (% F cell/% F reticulocytes) did not change significantly with alpha-globin gene number. Moreover, no correlation existed between alpha-globin gene number and the absolute number of F cells in any group studied. However, there was a strong inverse correlation (r = -0.407, P = .0001) between non-F cell levels (1.7 +/- 2, 2.2 +/- 5, 3.0 +/- 1.0 X 10(12)/L) and decreasing alpha- globin gene number. These data suggest that falling HbF levels among SS individuals with lessened numbers of alpha-globin genes reflect prolonged survival of non-F cells and are not due to intrinsic differences in F cell production or in the amount of HbF per F cell. The improved survival of non-F cells in SS alpha-thalassemia is presumed to be due to the lower MCHC observed in such individuals.

Published

1987

180. Human embryonic zeta-globin chains in fetal and newborn blood

Author

Chui, DH, Mentzer, WC, Patterson, M, Iarocci, TA, Embury, SH, Perrine, SP, Mibashan, RS, and Higgs, DR

Abstract

A sensitive and specific radioimmunoassay (RIA) for human embryonic zeta-globin chains was used to study normal fetal blood and newborn cord blood as well as cord blood from newborns with alpha-thalassemias. From 17 weeks until 37 weeks of gestation, zeta-globin chains were present in almost all fetal and cord blood samples (0.27% +/- 0.15% in samples of weeks 17 through 30; 0.14% +/- 0.11% in samples of weeks 31 through 37). zeta-Globin chains were present in greater than 80% of cord blood hemolysates from normal, full-term newborns (0.15% +/- 0.11%) as well as from 16 near-term newborns of diabetic mothers (0.13% +/- 0.13%). zeta-Globin chains were not detected in normal infants aged 3 months to 2 years. In cord blood hemolysates from alpha-thalassemic newborns, the levels of zeta-globin chain content varied from very high to undetectable levels. Gene mapping of the zeta-alpha-globin gene cluster was performed in 12 newborns in whom cord blood zeta-globin chains had been determined. Newborns who were carriers of alpha- thalassemia-1 due to the (--SEA/) deletion had very high levels of zeta- globin chains (greater than 1.5%).

Published

1989

181. A review of the molecular genetics of the human alpha-globin gene cluster

Author

Higgs, DR, Vickers, MA, Wilkie, AO, Pretorius, IM, Jarman, AP, and Weatherall, DJ

Published

1989

182. Alpha thalassemia and the hematology of homozygous sickle cell disease in childhood

Author

Stevens, MC, Maude, GH, Beckford, M, Grandison, Y, Mason, K, Taylor, B, Serjeant, BE, Higgs, DR, Teal, H, and Weatherall, DJ

Abstract

alpha Thalassemia modifies the hematologic expression of homozygous sickle cell (SS) disease, resulting in increased total hemoglobin and HbA2 and decreased HbF, mean cell volume, reticulocytes, irreversibly sickled cells, and bilirubin levels. The age at which these changes develop in children with SS disease is unknown. Ascertainment of globin gene status in a large representative sample of children with SS disease has afforded an opportunity to study the hematologic indices in nine children homozygous for alpha thalassemia 2 (two-gene group), 90 children heterozygous for alpha thalassemia 2 (three-gene group), and 167 children with a normal alpha globin gene complement (four-gene group). The two-gene group had significantly lower mean cell volumes from birth, higher red cell counts from one month, lower reticulocytes from three months, and higher HbA2 levels from one year, as compared with the four-gene group. Children with three genes had intermediate indices but resembled more closely the four-gene group. Differences in total hemoglobin or in fetal hemoglobin between the groups were not apparent by eight years of age. The most characteristic differences of the two-gene group were the raised proportional HbA2 level and low mean cell volume, the latter having some predictive value for alpha thalassemia status at birth.

Published

1986

183. The alpha thalassaemias.

Author

Higgs DR and Weatherall DJ

Subjects

Genetic Variation, Genetics, Population, Genotype, Hemoglobins genetics, Humans, Mental Retardation, X-Linked genetics, Neural Tube Defects genetics, Phenotype, Tropical Medicine, alpha-Globins genetics, alpha-Thalassemia epidemiology, alpha-Thalassemia genetics

Abstract

Recent work in the alpha thalassaemia field has started to provide some indication of the mechanisms involved in the very high frequency of the different forms of alpha thalassaemia among the populations of tropical countries, and, at the same time, is starting to define at least some of the mechanisms for its remarkable phenotypic heterogeneity. These diseases continue to provide extremely valuable models for the better understanding of the regulation of the alpha globin genes, and for human molecular pathology in general. The much less common disorders, ATR-16 and ATR-X are also providing valuable information about the spectrum of molecular lesions associated with different forms of mental retardation and about the molecular mechanisms involved in their varying phenotypes.

Published

2009

184. The role of X-inactivation in the gender bias of patients with acquired alpha-thalassaemia and myelodysplastic syndrome (ATMDS).

Author

Haas PS, Roy NB, Gibbons RJ, Deville MA, Fisher C, Schwabe M, Bissé E, van Dorsselaer A, Higgs DR, and Lübbert M

Subjects

Aged, Cross-Sectional Studies, DNA Helicases genetics, DNA Methylation, DNA Mutational Analysis methods, Epigenesis, Genetic, Female, Humans, Male, Middle Aged, Mutation, Myelodysplastic Syndromes pathology, Nuclear Proteins genetics, Sex Distribution, X-linked Nuclear Protein, alpha-Thalassemia pathology, Myelodysplastic Syndromes genetics, X Chromosome Inactivation, alpha-Thalassemia genetics

Abstract

Alpha thalassaemia myelodysplastic syndrome (ATMDS) is an unusual complication of chronic myeloid malignancy that is associated with a striking red cell phenotype. It represents an acquired form of alpha-thalassaemia that most commonly arises in the context of myelodysplasia. It has recently been shown that this condition occurs in association with somatic mutations of a known X-encoded trans-acting regulator of alpha globin gene (HBA) expression, ATRX. There is an unexplained, strong male preponderance of individuals with the ATMDS phenotype with a >5:1 male-female ratio and furthermore, all the somatic ATRX mutations described to date have been in males. Here we report the identification, in a single centre, of two females with ATMDS and mutations in the ATRX gene, proving that ATMDS associated with such mutations may occur, albeit rarely, in females. It seemed possible that females might be less likely to develop ATMDS if the inactivated copy of the ATRX gene (ATRX) became progressively re-activated throughout life. This study ruled out this hypothesis by investigating the pattern of ATRX inactivation in a cross-sectional analysis of normal females at ages ranging from newborn to 90 years.

Published

2009

185. The role of molecular diagnostic testing for hemoglobinopathies and thalassemias.

Author

Sabath DE

Subjects

Pregnancy, Female, Child, Humans, Prenatal Diagnosis methods, Molecular Diagnostic Techniques, beta-Globins genetics, beta-Thalassemia diagnosis, beta-Thalassemia genetics, Hemoglobinopathies diagnosis, Hemoglobinopathies genetics, alpha-Thalassemia genetics

Abstract

Hemoglobin disorders are among the most common genetic diseases worldwide. Molecular diagnosis is helpful in cases where the diagnosis is uncertain and for genetic counseling. Protein-based diagnostic techniques are frequently adequate for initial diagnosis. Molecular genetic testing is pursued in some cases, particularly when a definitive diagnosis is not possible and especially for the purpose of assessing genetic risk for couples wanting to have children. The expertise available in the clinical hematology laboratory is essential for the diagnosis of patients with hemoglobin abnormalities. Initial diagnoses are made using protein-based techniques such as electrophoresis and chromatography. Based on these findings, genetic risk to an individual's offspring can be assessed. In the setting of β-thalassemia and other β-globin disorders, coincident α-thalassemia may be difficult to diagnose, which can have potentially serious consequences. In addition, unusual forms of β-thalassemia caused by deletions in the β-globin locus cannot be definitively characterized using standard techniques. Molecular diagnostic testing has an important role in the diagnosis of hemoglobin disorders and is important in the setting of genetic counseling. Molecular testing also has a role in prenatal diagnosis to identify fetuses affected by severe hemoglobinopathies and thalassemias., (© 2023 John Wiley & Sons Ltd.)

Published

2023

186. Hematopoietic cell transplantation for congenital dyserythropoietic anemia IV caused by compound heterozygous KLF1 mutations.

Author

Yang K, Nie W, Huang Q, Liao G, Xiao J, and Yin X

Subjects

Humans, Mutation, Anemia, Dyserythropoietic, Congenital genetics, Anemia, Dyserythropoietic, Congenital therapy, Hematopoietic Stem Cell Transplantation

Published

2023

187. "Double-hit" ineffective erythropoiesis-concurrent β-thalassemia with α-gene triplication and myelodysplastic syndrome with SF3B1 mutation.

Author

Chen PH, Gorshein E, Tormey C, Siddon AJ, and Perincheri S

Subjects

Humans, Erythropoiesis genetics, Mutation, RNA Splicing Factors genetics, Phosphoproteins genetics, beta-Thalassemia genetics, Myelodysplastic Syndromes genetics

Published

2023

188. Neuronal death resulting from targeted disruption of the Snf2 protein ATRX is mediated by p53.

Author

Seah C, Levy MA, Jiang Y, Mokhtarzada S, Higgs DR, Gibbons RJ, and Bérubé NG

Subjects

Animals, Animals, Newborn, Bromodeoxyuridine metabolism, Cell Death drug effects, Cell Death genetics, Cell Differentiation genetics, Cell Movement genetics, Cell Proliferation, DNA Helicases deficiency, Embryo, Mammalian, Female, Gene Expression Regulation, Developmental genetics, Hippocampus embryology, Hippocampus metabolism, Homeodomain Proteins metabolism, Male, Mice, Mice, Transgenic, Mutation, Neurons drug effects, Nuclear Proteins deficiency, Pregnancy, Signal Transduction genetics, Stem Cells physiology, Tumor Suppressor Protein p53 genetics, Tumor Suppressor Proteins metabolism, X-linked Nuclear Protein, gamma-Aminobutyric Acid metabolism, DNA Helicases metabolism, Neurons physiology, Nuclear Proteins metabolism, Prosencephalon cytology, Tumor Suppressor Protein p53 physiology

Abstract

ATRX, a chromatin remodeling protein of the Snf2 family, participates in diverse cellular functions including regulation of gene expression and chromosome alignment during mitosis and meiosis. Mutations in the human gene cause alpha thalassemia mental retardation, X-linked (ATR-X) syndrome, a rare disorder characterized by severe cognitive deficits, microcephaly and epileptic seizures. Conditional inactivation of the Atrx gene in the mouse forebrain leads to neonatal lethality and defective neurogenesis manifested by increased cell death and reduced cellularity in the developing neocortex and hippocampus. Here, we show that Atrx-null forebrains do not generate dentate granule cells due to a reduction in precursor cell number and abnormal migration of differentiating granule cells. In addition, fewer GABA-producing interneurons are generated that migrate from the ventral telencephalon to the cortex and hippocampus. Staining for cleaved caspase 3 demonstrated increased apoptosis in both the hippocampal hem and basal telencephalon concurrent with p53 pathway activation. Elimination of the tumor suppressor protein p53 in double knock-out mice rescued cell death in the embryonic telencephalon but only partially ameliorated the Atrx-null phenotypes at birth. Together, these findings show that ATRX deficiency leads to p53-dependent neuronal apoptosis which is responsible for some but not all of the phenotypic consequences of ATRX deficiency in the forebrain.

Published

2008

189. The role of the polycomb complex in silencing alpha-globin gene expression in nonerythroid cells.

Author

Garrick D, De Gobbi M, Samara V, Rugless M, Holland M, Ayyub H, Lower K, Sloane-Stanley J, Gray N, Koch C, Dunham I, and Higgs DR

Subjects

Base Sequence, Cell Line, Cells, Cultured, DNA-Binding Proteins antagonists & inhibitors, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Embryonic Stem Cells metabolism, Enhancer of Zeste Homolog 2 Protein, HeLa Cells, Histone Deacetylases metabolism, Humans, Pluripotent Stem Cells metabolism, Polycomb Repressive Complex 2, Polycomb-Group Proteins, RNA Interference, RNA, Small Interfering genetics, Transcription Factors antagonists & inhibitors, Transcription Factors genetics, Transcription Factors metabolism, Gene Silencing, Globins genetics, Repressor Proteins metabolism

Abstract

Although much is known about globin gene activation in erythroid cells, relatively little is known about how these genes are silenced in nonerythroid tissues. Here we show that the human alpha- and beta-globin genes are silenced by fundamentally different mechanisms. The alpha-genes, which are surrounded by widely expressed genes in a gene dense region of the genome, are silenced very early in development via recruitment of the Polycomb (PcG) complex. By contrast, the beta-globin genes, which lie in a relatively gene-poor chromosomal region, are not bound by this complex in nonerythroid cells. The PcG complex seems to be recruited to the alpha-cluster by sequences within the CpG islands associated with their promoters; the beta-globin promoters do not lie within such islands. Chromatin associated with the alpha-globin cluster is modified by histone methylation (H3K27me3), and silencing in vivo is mediated by the localized activity of histone deacetylases (HDACs). The repressive (PcG/HDAC) machinery is removed as hematopoietic progenitors differentiate to form erythroid cells. The alpha- and beta-globin genes thus illustrate important, contrasting mechanisms by which cell-specific hematopoietic genes (and tissue-specific genes in general) may be silenced.

Published

2008

190. Good news for the aging population?

Author

Vyas P and Higgs DR

Published

2008

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

Author

Rugless MJ, Fisher CA, Old JM, Sloane-Stanley J, Ayyub H, Higgs DR, and Garrick D

Subjects

Adult, Cells, Cultured, Child, Chromatin genetics, Chromatin metabolism, Chromosomes, Human, Pair 16 genetics, Female, Gene Expression, Globins metabolism, Humans, Male, Phenotype, RNA Polymerase II metabolism, DNA Replication, Gene Deletion, Globins genetics, Multigene Family

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

192. Association between active genes occurs at nuclear speckles and is modulated by chromatin environment.

Author

Brown JM, Green J, das Neves RP, Wallace HA, Smith AJ, Hughes J, Gray N, Taylor S, Wood WG, Higgs DR, Iborra FJ, and Buckle VJ

Subjects

Animals, Anion Exchange Protein 1, Erythrocyte genetics, Anion Exchange Protein 1, Erythrocyte metabolism, Cell Nucleus metabolism, Gene Expression Regulation, Globins genetics, Humans, In Situ Hybridization, Fluorescence, Mice, Multigene Family, Blood Cells physiology, Chromatin metabolism, Chromosomes metabolism, Erythropoiesis genetics, Intranuclear Inclusion Bodies metabolism, Transcription, Genetic

Abstract

Genes on different chromosomes can be spatially associated in the nucleus in several transcriptional and regulatory situations; however, the functional significance of such associations remains unclear. Using human erythropoiesis as a model, we show that five cotranscribed genes, which are found on four different chromosomes, associate with each other at significant but variable frequencies. Those genes most frequently in association lie in decondensed stretches of chromatin. By replacing the mouse alpha-globin gene cluster in situ with its human counterpart, we demonstrate a direct effect of the regional chromatin environment on the frequency of association, whereas nascent transcription from the human alpha-globin gene appears unaffected. We see no evidence that cotranscribed erythroid genes associate at shared transcription foci, but we do see stochastic clustering of active genes around common nuclear SC35-enriched speckles (hence the apparent nonrandom association between genes). Thus, association between active genes may result from their location on decondensed chromatin that enables clustering around common nuclear speckles.

Published

2008

193. Genetic complexity in sickle cell disease.

Author

Higgs DR and Wood WG

Subjects

Anemia, Sickle Cell complications, Anemia, Sickle Cell epidemiology, Anemia, Sickle Cell metabolism, Fetal Hemoglobin genetics, Globins genetics, Humans, Pain complications, Pain epidemiology, Pain genetics, Pain metabolism, Polymorphism, Single Nucleotide genetics, Quantitative Trait Loci genetics, Anemia, Sickle Cell genetics

Published

2008

194. Switching genes on and off in haemopoiesis.

Author

Garrick D, De Gobbi M, Lynch M, and Higgs DR

Subjects

Animals, Erythroid Cells cytology, Erythroid Cells metabolism, Globins genetics, Humans, Polycomb-Group Proteins, Protein Binding, Repressor Proteins metabolism, Signal Transduction, Hematopoiesis genetics

Abstract

At present, the molecular mechanisms by which stem cells commit to and differentiate towards specific lineages are poorly characterized, and will need to be better understood before stem cells can be exploited fully in experimental and clinical settings. Transcriptional regulation, the ability to turn genes on and off, lies at the heart of these processes of lineage commitment and specification. We have focused on fully understanding how these decisions are made at a single mammalian gene locus, the alpha-globin genes, which become up-regulated in a tissue- and developmental-stage specific manner during haemopoiesis. The studies summarized in the present article have revealed that complete regulation of this gene cluster involves not only activating mechanisms in expressing erythroid cells, but also repressing mechanisms, involving the Polycomb complex and histone deacetylases which are present in non-erythroid tissues. Taken together, these observations provide a well-characterized model of how gene expression is fully regulated during the transition from stem cells through lineage commitment and terminal differentiation.

Published

2008

195. A new dawn for stem-cell therapy.

Author

Higgs DR

Subjects

Animals, Disease Models, Animal, Embryonic Stem Cells, Hematopoietic Stem Cells cytology, Histocompatibility Testing, Humans, Mice, Transduction, Genetic, Anemia, Sickle Cell therapy, Cellular Reprogramming, Fibroblasts cytology, Hematopoietic Stem Cell Transplantation, Pluripotent Stem Cells cytology

Published

2008

196. Population analysis of the alpha hemoglobin stabilizing protein (AHSP) gene identifies sequence variants that alter expression and function.

Author

dos Santos CO, Zhou S, Secolin R, Wang X, Cunha AF, Higgs DR, Kwiatkowski JL, Thein SL, Gallagher PG, Costa FF, and Weiss MJ

Subjects

Amino Acid Substitution, DNA blood, DNA genetics, Gene Expression Regulation, Genome, Human, Genotype, Humans, Phylogeny, Promoter Regions, Genetic, Thalassemia genetics, Blood Proteins genetics, Genetic Variation, Molecular Chaperones genetics, Polymorphism, Single Nucleotide, beta-Thalassemia genetics

Abstract

Alpha-hemoglobin stabilizing protein (AHSP) is a potential modifier of beta-thalassemia by virtue of its ability to detoxify excess free alpha-globin. However, examination of patients with beta-thalassemia from a few geographic regions failed to identify obvious AHSP mutations. We extended these studies by analyzing AHSP gene sequences in 366 anonymous individuals from five different areas of the world. We detected numerous polymorphisms comprising 18 different haplotypes and two rare missense mutations. Two sequence variations produce functional effects in laboratory assays. First, a rare missense mutation in a Brazilian/Mediterranean cohort converts asparagine to isoleucine at position 75 of AHSP protein and impairs its ability to inhibit reactive oxygen species production by alpha-hemoglobin. Second, a high-frequency polymorphism in intron 1 of the AHSP gene (12391 G>A) alters an Oct-1 transcription factor binding site previously shown to be important for optimal gene expression. The 12391A polymorphism impairs Oct-1 binding and inhibits the ability of AHSP regulatory sequences to activate expression of a linked luciferase reporter. Although structural mutations predicted to alter AHSP protein function or ablate its activity are rare, the 12391 G>A SNP is common and represents a potential mechanism through which genetically determined variations in AHSP expression could influence beta-thalassemia.

Published

2008

197. Long-range regulation of alpha-globin gene expression.

Author

Higgs DR, Vernimmen D, and Wood B

Subjects

Animals, Evolution, Molecular, Gene Order physiology, Hematopoiesis genetics, Humans, Models, Biological, Multigene Family genetics, Multigene Family physiology, Regulatory Sequences, Nucleic Acid genetics, Transcription Factors metabolism, Transcription Factors physiology, Gene Expression Regulation physiology, Globins genetics, Regulatory Sequences, Nucleic Acid physiology

Abstract

Over the past 20 years, there has been an increasing awareness that gene expression can be regulated by multiple cis-acting sequences located at considerable distances (10-1000 kb) from the genes they control. Detailed investigation of a few specialized mammalian genes, including the genes controlling the synthesis of hemoglobin, provide important models to understand how such long-range regulatory elements act. In general, these elements contain a high density of evolutionarily conserved, transcription factor-binding sites and in many ways resemble the upstream regulatory elements found adjacent to the promoters of genes in simpler organisms, differing only in the distance over which they act. We have investigated in detail how the remote regulatory elements of the alpha-globin cluster become activated as hematopoietic stem cells (HSCs) undergo commitment, lineage specification, and differentiation to form red blood cells. In turn, we have addressed how, during this process, the upstream elements control the correct spatial and temporal expression from the alpha-gene promoter which lies approximately 60 kb downstream of these elements. At present too few loci have been studied to determine whether there are general principles underlying long-range regulation but some common themes are emerging.

Published

2008

198. Tissue-specific histone modification and transcription factor binding in alpha globin gene expression.

Author

De Gobbi M, Anguita E, Hughes J, Sloane-Stanley JA, Sharpe JA, Koch CM, Dunham I, Gibbons RJ, Wood WG, and Higgs DR

Subjects

Acetylation, Animals, Cells, Cultured, Chromosomes, Human, Pair 16, Enhancer Elements, Genetic, Erythroblasts immunology, Gene Expression Regulation, Humans, K562 Cells, Methylation, Mice, Promoter Regions, Genetic, T-Lymphocytes cytology, Telomere, Globins genetics, Histones metabolism, Transcription Factors metabolism, Transcription, Genetic genetics

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 alpha globin genes and 9 widely expressed genes flanking the alpha 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 alpha 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

199. Prevalence of erythrocyte haemoglobin H inclusions in unselected patients with clonal myeloid disorders.

Author

Steensma DP, Porcher JC, Hanson CA, Lathrop CL, Hoyer JD, Lasho TA, Tefferi A, and Higgs DR

Subjects

Acute Disease, Aged, Erythrocyte Indices, Erythrocytes chemistry, Female, Hemoglobin H analysis, Humans, Leukemia, Myeloid blood, Leukemia, Myeloid complications, Male, Middle Aged, Myelodysplastic Syndromes blood, Myeloproliferative Disorders blood, Prospective Studies, Myelodysplastic Syndromes complications, Myeloproliferative Disorders complications, alpha-Thalassemia etiology

Abstract

Patients with clonal myeloid disorders, especially myelodysplastic syndromes (MDS), may acquire alpha-thalassaemia. To estimate the prevalence of this erythrocyte phenotype, we examined brilliant cresyl blue-stained blood smears from 201 patients with neoplastic myeloid disorders and 282 controls (195 non-clonal anaemia, 62 with medical illnesses without anaemia and 25 healthy persons). Haemoglobin H inclusions were detected in 8/100 patients with MDS (8%) and 2/81 (2.5%) patients with myeloproliferative disorders, but in none of the acute leukaemia patients or controls. We conclude that the emergence of thalassaemic clones may be relatively common in the disordered marrow milieu of MDS.

Published

2007

200. Structural consequences of disease-causing mutations in the ATRX-DNMT3-DNMT3L (ADD) domain of the chromatin-associated protein ATRX.

Author

Argentaro A, Yang JC, Chapman L, Kowalczyk MS, Gibbons RJ, Higgs DR, Neuhaus D, and Rhodes D

Subjects

Amino Acid Sequence, Amino Acid Substitution, Cell Transformation, Viral, Herpesvirus 4, Human, Humans, Lymphocytes virology, Models, Molecular, Molecular Sequence Data, Nuclear Magnetic Resonance, Biomolecular, Protein Structure, Secondary, Protein Structure, Tertiary, Sequence Alignment, Static Electricity, Structure-Activity Relationship, Surface Properties, X-linked Nuclear Protein, Chromatin metabolism, DNA Helicases chemistry, DNA Helicases genetics, Nuclear Proteins chemistry, Nuclear Proteins genetics, Point Mutation genetics

Abstract

The chromatin-associated protein ATRX was originally identified because mutations in the ATRX gene cause a severe form of syndromal X-linked mental retardation associated with alpha-thalassemia. Half of all of the disease-associated missense mutations cluster in a cysteine-rich region in the N terminus of ATRX. This region was named the ATRX-DNMT3-DNMT3L (ADD) domain, based on sequence homology with a family of DNA methyltransferases. Here, we report the solution structure of the ADD domain of ATRX, which consists of an N-terminal GATA-like zinc finger, a plant homeodomain finger, and a long C-terminal alpha-helix that pack together to form a single globular domain. Interestingly, the alpha-helix of the GATA-like finger is exposed and highly basic, suggesting a DNA-binding function for ATRX. The disease-causing mutations fall into two groups: the majority affect buried residues and hence affect the structural integrity of the ADD domain; another group affects a cluster of surface residues, and these are likely to perturb a potential protein interaction site. The effects of individual point mutations on the folding state and stability of the ADD domain correlate well with the levels of mutant ATRX protein in patients, providing insights into the molecular pathophysiology of ATR-X syndrome.

Published

2007