Your search keyword '"Repapi E"' showing total 66 results

1. No evidence for age-related differences in mtRNA quality in the female germline

Author

Hartley, FM, Alageel, A, Appeltant, R, Gray, N, Repapi, E, Wells, D, Williams, SA, and Poulton, J

Abstract

Mitochondrial quality is implicated as a contributor to declining fertility with aging. We investigated mitochondrial transcripts in oocytes and their associated cumulus cells from mice of different ages using RNA-seq. Mice aged 3 weeks, 9 weeks, and 1 year were superovulated and 48 hr later, oocyte cumulus complexes collected by follicle puncture. We did not detect any major differences that could be attributed to aging. However, mitochondrial RNA transcripts which deviated from the consensus sequence were found at a higher frequency in cumulus cells than in their corresponding oocyte. Previous investigations have shown that variation in the sequence of mtRNA transcripts is substantial, and at least some of this can be accounted for by post-transcriptional modifications which impact base calling during sequencing. Our data would be consistent with either less post-transcriptional modification in mitochondrial RNA from oocytes than cumulus cells or with lower mtDNA mutational load.

Published

2023

2. The chromatin remodeller ATRX facilitates diverse nuclear processes, in a stochastic manner, in both heterochromatin and euchromatin

Author

Truch, J, Downes, DJ, Scott, C, Gür, ER, Telenius, JM, Repapi, E, Schwessinger, R, Gosden, M, Brown, JM, Taylor, S, Cheong, PL, Hughes, JR, Higgs, DR, and Gibbons, RJ

Subjects

Histone variants, Clinical epigenetics, X-linked Nuclear Protein, Multidisciplinary, DNA Helicases, Nuclear Proteins, General Physics and Astronomy, Chromatin remodelling, General Chemistry, Chromatin, General Biochemistry, Genetics and Molecular Biology, Euchromatin, Histones, alpha-Thalassemia, Heterochromatin, Mental Retardation, X-Linked

Abstract

The chromatin remodeller ATRX interacts with the histone chaperone DAXX to deposit the histone variant H3.3 at sites of nucleosome turnover. ATRX is known to bind repetitive, heterochromatic regions of the genome including telomeres, ribosomal DNA and pericentric repeats, many of which are putative G-quadruplex forming sequences (PQS). At these sites ATRX plays an ancillary role in a wide range of nuclear processes facilitating replication, chromatin modification and transcription. Here, using an improved protocol for chromatin immunoprecipitation, we show that ATRX also binds active regulatory elements in euchromatin. Mutations in ATRX lead to perturbation of gene expression associated with a reduction in chromatin accessibility, histone modification, transcription factor binding and deposition of H3.3 at the sequences to which it normally binds. In erythroid cells where downregulation of α-globin expression is a hallmark of ATR-X syndrome, perturbation of chromatin accessibility and gene expression occurs in only a subset of cells. The stochastic nature of this process suggests that ATRX acts as a general facilitator of cell specific transcriptional and epigenetic programmes, both in heterochromatin and euchromatin.

Published

2022

3. Transcriptomic profiling of the myeloma bone-lining niche reveals BMP signalling inhibition to improve bone disease

Author

Gooding, S, Olechnowicz, S, Morris, E, Armitage, A, Arezes, J, Frost, J, Repapi, E, Edwards, J, Ashley, N, Waugh, C, Gray, N, Martinez-Hackert, Lim, PJ, Pasricha, S-R, Knowles, H, Mead, A, Ramasamy, K, Drakesmith, A, and Edwards, C

Subjects

Cancer microenvironment, Science, Osteoclasts, Mice, Inbred Strains, Myeloma, Article, Mice, Bone Density, Bone Marrow, Osteogenesis, Cell Line, Tumor, hemic and lymphatic diseases, Animals, Humans, Femur, RNA-Seq, Bone, lcsh:Science, Adaptor Proteins, Signal Transducing, Tibia, Gene Expression Profiling, Stem Cells, Bone Morphogenetic Protein Receptors, Xenograft Model Antitumor Assays, Disease Models, Animal, Pyrimidines, Treatment Outcome, Gene Expression Regulation, Bone Morphogenetic Proteins, Pyrazoles, lcsh:Q, Bone Diseases, Multiple Myeloma, Injections, Intraperitoneal, Signal Transduction

Abstract

Multiple myeloma is an incurable, bone marrow-dwelling malignancy that disrupts bone homeostasis causing skeletal damage and pain. Mechanisms underlying myeloma-induced bone destruction are poorly understood and current therapies do not restore lost bone mass. Using transcriptomic profiling of isolated bone lining cell subtypes from a murine myeloma model, we find that bone morphogenetic protein (BMP) signalling is upregulated in stromal progenitor cells. BMP signalling has not previously been reported to be dysregulated in myeloma bone disease. Inhibition of BMP signalling in vivo using either a small molecule BMP receptor antagonist or a solubilized BMPR1a-FC receptor ligand trap prevents trabecular and cortical bone volume loss caused by myeloma, without increasing tumour burden. BMP inhibition directly reduces osteoclastogenesis, increases osteoblasts and bone formation, and suppresses bone marrow sclerostin levels. In summary we describe a novel role for the BMP pathway in myeloma-induced bone disease that can be therapeutically targeted., Multiple myeloma is a cancer of the bone marrow that can induce bone disease. Here, the authors profile the transcriptome of bone-lining cells and find a targetable role of bone morphogenetic protein (BMP) signalling in myeloma-induced bone-disease

Published

2019

4. Disruption of haematopoietic stem cell heterogeniety in a mouse model of myelproliferate neoplasm

Author

Norfo, R, Di Genua, C, Booth, C, Giustacchini, A, Povinelli, B, Gray, N, Repapi, E, Soilleux, E, Jamieson, L, Tran, N, Green, A, Jacobsen, S, and Mead, A

Published

2019

5. Bone Marrow Myelopoiesis Independently of Canonical Notch Signaling

Author

Duarte, S, Woll, P, Natalija, B, Boukarabila, H, Stenson, L, Bouriez-Jones, T, Ferry, H, Mead, A, Atkinson, D, Thongjuea, S, Jin, S, Clark, S, Chin, D, Lu-S, T, Repapi, E, Gray, N, Taylor, S, Mutvei, A, Tsoi, Y, Nerlov, C, Lendahl, U, and Jacobsen, S

Published

2019

6. A novel model of human hemopoiesis based on single cell functional and transcriptional analysis of lympho-myeloid progenitors

Author

Stoilova, B, Karamitros, D, Aboukhalil, Z, Hamey, F, Reinisch, A, Samitsch, M, Quek, L, Otto, G, Repapi, E, Doondeea, J, Usukhbayar, B, Calvo, J, Taylor, S, Goardon, N, Six, E, Pflumio, F, Porcher, C, Majeti, R, Gottgens, B, and Vyas, P

Published

2018

7. A novel model of human lympho-myeloid progenitor hierarchy based on single cell functional and transcriptional analysis

Author

Karamitros, D, Stoilova, B, Aboukhalil, Z, Reinisch, A, Hamey, F, Samitsch, M, Quek, L, Otto, G, Repapi, E, Doondeea, J, Usukhbayar, B, Calvo, J, Taylor, S, Goardon, N, Six, E, Pflumio, F, Porcher, C, Majeti, R, Gottgens, B, and Vyas, P

Abstract

Human hemopoiesis produces 10 billion new, terminally mature, blood cells daily; a production that is also rapidly responsive to external change. Dysregulation of this complex process can lead to hemopoietic and immune deficiencies and blood cancers. In humans the hemopoietic progenitor hierarchy producing lymphoid and granulocytic-monocytic (myeloid) lineages is unclear. Multiple progenitor populations give rise to lymphoid and myeloid cells but they remain incompletely characterized at the immunophenotypic, transcriptional and functional level.

Published

2018

8. Does osteogenic potential of clonal human bone marrow mesenchymal stem/stromal cells correlate with their vascular supportive ability?

Author

Merryweather-Clarke, AT, Cook, D, Lara, BJ, Hua, P, Repapi, E, Ashley, N, Lim, SY, Watt, SM, Merryweather-Clarke, AT, Cook, D, Lara, BJ, Hua, P, Repapi, E, Ashley, N, Lim, SY, and Watt, SM

Abstract

BACKGROUND: Human bone marrow-derived mesenchymal stem/stromal cells (hBM MSCs) have multiple functions, critical for skeletal formation and function. Their functional heterogeneity, however, represents a major challenge for their isolation and in developing potency and release assays to predict their functionality prior to transplantation. Additionally, potency, biomarker profiles and defining mechanisms of action in a particular clinical setting are increasing requirements of Regulatory Agencies for release of hBM MSCs as Advanced Therapy Medicinal Products for cellular therapies. Since the healing of bone fractures depends on the coupling of new blood vessel formation with osteogenesis, we hypothesised that a correlation between the osteogenic and vascular supportive potential of individual hBM MSC-derived CFU-F (colony forming unit-fibroblastoid) clones might exist. METHODS: We tested this by assessing the lineage (i.e. adipogenic (A), osteogenic (O) and/or chondrogenic (C)) potential of individual hBM MSC-derived CFU-F clones and determining if their osteogenic (O) potential correlated with their vascular supportive profile in vitro using lineage differentiation assays, endothelial-hBM MSC vascular co-culture assays and transcriptomic (RNAseq) analyses. RESULTS: Our results demonstrate that the majority of CFU-F (95%) possessed tri-lineage, bi-lineage or uni-lineage osteogenic capacity, with 64% of the CFU-F exhibiting tri-lineage AOC potential. We found a correlation between the osteogenic and vascular tubule supportive activity of CFU-F clones, with the strength of this association being donor dependent. RNAseq of individual clones defined gene fingerprints relevant to this correlation. CONCLUSIONS: This study identified a donor-dependent correlation between osteogenic and vascular supportive potential of hBM MSCs and important gene signatures that support these functions that are relevant to their bone regenerative properties.

Published

2018

9. Hepcidin is regulated by promoter-associated histone acetylation and HDAC3

Author

Pasricha, S., Lim, P., Duarte, T., Casu, C., Oosterhuis, D., Mleczko-Sanecka, K., Suciu, M., Da Silva, A., Al-Hourani, K., Arezes, J., McHugh, K., Gooding, S., Frost, J., Wray, K., Santos, A., Porto, G., Repapi, E., Gray, N., Draper, S., Ashley, N., Soilleux, E., Olinga, P., Muckenthaler, M., Hughes, J., Rivella, S., Milne, T., Armitage, A., Drakesmith, H., Pasricha, Sant-Rayn [0000-0002-5502-0434], Duarte, Tiago L [0000-0002-4901-4580], Draper, Simon J [0000-0002-9415-1357], Hughes, Jim R [0000-0002-8955-7256], Milne, Thomas A [0000-0002-0413-4271], Apollo - University of Cambridge Repository, Pharmaceutical Technology and Biopharmacy, Biopharmaceuticals, Discovery, Design and Delivery (BDDD), and Groningen Institute for Organ Transplantation (GIOT)

Subjects

Male, inorganic chemicals, congenital, hereditary, and neonatal diseases and abnormalities, Science, Amino Acid Motifs, nutritional and metabolic diseases, Acetylation, Iron Deficiencies, digestive system, Histone Deacetylases, Article, Epigenesis, Genetic, Histones, Mice, Inbred C57BL, Gene Expression Regulation, Hepcidins, hemic and lymphatic diseases, Journal Article, Animals, Humans, lcsh:Q, Promoter Regions, Genetic, lcsh:Science, Erythropoietin

Abstract

Hepcidin regulates systemic iron homeostasis. Suppression of hepcidin expression occurs physiologically in iron deficiency and increased erythropoiesis but is pathologic in thalassemia and hemochromatosis. Here we show that epigenetic events govern hepcidin expression. Erythropoiesis and iron deficiency suppress hepcidin via erythroferrone-dependent and -independent mechanisms, respectively, in vivo, but both involve reversible loss of H3K9ac and H3K4me3 at the hepcidin locus. In vitro, pan-histone deacetylase inhibition elevates hepcidin expression, and in vivo maintains H3K9ac at hepcidin-associated chromatin and abrogates hepcidin suppression by erythropoietin, iron deficiency, thalassemia, and hemochromatosis. Histone deacetylase 3 and its cofactor NCOR1 regulate hepcidin; histone deacetylase 3 binds chromatin at the hepcidin locus, and histone deacetylase 3 knockdown counteracts hepcidin suppression induced either by erythroferrone or by inhibiting bone morphogenetic protein signaling. In iron deficient mice, the histone deacetylase 3 inhibitor RGFP966 increases hepcidin, and RNA sequencing confirms hepcidin is one of the genes most differentially regulated by this drug in vivo. We conclude that suppression of hepcidin expression involves epigenetic regulation by histone deacetylase 3., Hepcidin controls systemic iron levels by inhibiting intestinal iron absorption and iron recycling. Here, Pasricha et al. demonstrate that the hepcidin-chromatin locus displays HDAC3-mediated reversible epigenetic modifications during both erythropoiesis and iron deficiency.

Published

2017

10. M1-like monocytes are a major immunological determinant of severity in previously healthy adults with life-threatening influenza

Author

Cole, SL, Dunning, J, Kok, WL, Benam, KH, Benlahrech, A, Repapi, E, Martinez, FO, Drumright, L, Powell, TJ, Bennett, M, Elderfield, R, Thomas, C, MOSAIC investigators, Dong, T, McCauley, J, Liew, FY, Taylor, S, Zambon, M, Barclay, W, Cerundolo, V, Openshaw, PJ, McMichael, AJ, Ho, LP, Wellcome Trust, Medical Research Council (MRC), Imperial College Healthcare NHS Trust- BRC Funding, National Institute for Health Research, and Commission of the European Communities

Abstract

In each influenza season, a distinct group of young, otherwise healthy individuals with no risk factors succumbs to life-threatening infection. To better understand the cause for this, we analyzed a broad range of immune responses in blood from a unique cohort of patients, comprising previously healthy individuals hospitalized with and without respiratory failure during one influenza season, and infected with one specific influenza A strain. This analysis was compared with similarly hospitalized influenza patients with known risk factors (total of n = 60 patients recruited). We found a sustained increase in a specific subset of proinflammatory monocytes, with high TNF-α expression and an M1-like phenotype (independent of viral titers), in these previously healthy patients with severe disease. The relationship between M1-like monocytes and immunopathology was strengthened using murine models of influenza, in which severe infection generated using different models (including the high-pathogenicity H5N1 strain) was also accompanied by high levels of circulating M1-like monocytes. Additionally, a raised M1/M2 macrophage ratio in the lungs was observed. These studies identify a specific subtype of monocytes as a modifiable immunological determinant of disease severity in this subgroup of severely ill, previously healthy patients, offering potential novel therapeutic avenues.

Published

2017

11. M1-like monocytes are a major immunological determinant of severity in previously healthy adults with life-threatening influenza

Author

Cole, S, Dunning, J, Kok, W, Benam, K, Benlahrech, A, Repapi, E, Martinez, F, Drumright, L, Powell, T, Bennett, M, Elderfield, R, Thomas, C, Dong, T, McCauley, J, Liew, F, Taylor, S, Zambon, M, Barclay, W, Cerundolo, V, Openshaw, P, McMichael, A, and Ho, L

Subjects

Adult, Male, Influenza A Virus, H5N1 Subtype, Tumor Necrosis Factor-alpha, Macrophages, Middle Aged, Viral Load, Monocytes, Mice, Inbred C57BL, Mice, Young Adult, Phenotype, Influenza, Human, Animals, Humans, Female, Lung, Research Article, Aged

Abstract

In each influenza season, a distinct group of young, otherwise healthy individuals with no risk factors succumbs to life-threatening infection. To better understand the cause for this, we analyzed a broad range of immune responses in blood from a unique cohort of patients, comprising previously healthy individuals hospitalized with and without respiratory failure during one influenza season, and infected with one specific influenza A strain. This analysis was compared with similarly hospitalized influenza patients with known risk factors (total of n = 60 patients recruited). We found a sustained increase in a specific subset of proinflammatory monocytes, with high TNF-α expression and an M1-like phenotype (independent of viral titers), in these previously healthy patients with severe disease. The relationship between M1-like monocytes and immunopathology was strengthened using murine models of influenza, in which severe infection generated using different models (including the high-pathogenicity H5N1 strain) was also accompanied by high levels of circulating M1-like monocytes. Additionally, a raised M1/M2 macrophage ratio in the lungs was observed. These studies identify a specific subtype of monocytes as a modifiable immunological determinant of disease severity in this subgroup of severely ill, previously healthy patients, offering potential novel therapeutic avenues., In a cohort of influenza patients, previously healthy and young patients who succumbed to life-threatening disease were defined by high levels of circulating M1-like, TNF-αhi monocytes.

Published

2017

12. MLL-AF4 binds directly to a BCL-2 specific enhancer and modulates H3K27 acetylation

Author

Godfrey, L, Kerry, J, Thorne, R, Repapi, E, Davies, JOJ, Tapia, M, Ballabio, E, Hughes, JR, Geng, H, Konopleva, M, and Milne, T

Subjects

Cancer Research, hemic and lymphatic diseases, Genetics, Cell Biology, Hematology, neoplasms, Molecular Biology

Abstract

Survival rates for children and adults carrying mutations in the Mixed Lineage Leukemia (MLL) gene continue to have a very poor prognosis. The most common MLL mutation in ALL is the t(4;11)(q21;q23) chromosome translocation that fuses MLL in frame with the AF4 gene producing MLL-AF4 and AF4-MLL fusion proteins. Previously, we demonstrated that MLL-AF4 binds to the BCL-2 gene and directly activates it through DOT1L recruitment and increased H3K79me2/3 levels. Here, we perform a detailed analysis of MLL-AF4 regulation of the entire BCL-2 family. By measuring nascent RNA production in MLL-AF4 knockdowns, we find that of all the BCL-2 family genes, MLL-AF4 directly controls the active transcription of both BCL-2 and MCL-1, and also represses BIM via binding of the polycomb group repressor 1 (PRC1) complex component CBX8. We further analyze MLL-AF4 activation of the BCL-2 gene using Capture C and identify a BCL-2 specific enhancer, consisting of two clusters of H3K27Ac at the 3’end of the gene. Loss of MLL-AF4 activity results in a reduction of H3K79me3 levels in the gene body and H3K27Ac levels at the 3’ BCL-2 enhancer, revealing a novel regulatory link between these two histone marks and MLL-AF4 mediated activation of BCL-2.

Published

2017

13. Hepcidin is regulated by promoter-associated histone acetylation and HDAC3

Author

Pasricha, S-R, Lim, PJ, Duarte, TL, Casu, C, Oosterhuis, D, Mleczko-Sanecka, K, Suciu, M, Da Silva, AR, Al-Hourani, K, Arezes, J, McHugh, K, Gooding, S, Frost, JN, Wray, K, Santos, A, Porto, G, Repapi, E, Gray, N, Draper, SJ, Ashley, N, Soilleux, E, Olinga, P, Muckenthaler, MU, Hughes, JR, Rivella, S, Milne, TA, Armitage, AE, Drakesmith, H, Pasricha, S-R, Lim, PJ, Duarte, TL, Casu, C, Oosterhuis, D, Mleczko-Sanecka, K, Suciu, M, Da Silva, AR, Al-Hourani, K, Arezes, J, McHugh, K, Gooding, S, Frost, JN, Wray, K, Santos, A, Porto, G, Repapi, E, Gray, N, Draper, SJ, Ashley, N, Soilleux, E, Olinga, P, Muckenthaler, MU, Hughes, JR, Rivella, S, Milne, TA, Armitage, AE, and Drakesmith, H

Abstract

Hepcidin regulates systemic iron homeostasis. Suppression of hepcidin expression occurs physiologically in iron deficiency and increased erythropoiesis but is pathologic in thalassemia and hemochromatosis. Here we show that epigenetic events govern hepcidin expression. Erythropoiesis and iron deficiency suppress hepcidin via erythroferrone-dependent and -independent mechanisms, respectively, in vivo, but both involve reversible loss of H3K9ac and H3K4me3 at the hepcidin locus. In vitro, pan-histone deacetylase inhibition elevates hepcidin expression, and in vivo maintains H3K9ac at hepcidin-associated chromatin and abrogates hepcidin suppression by erythropoietin, iron deficiency, thalassemia, and hemochromatosis. Histone deacetylase 3 and its cofactor NCOR1 regulate hepcidin; histone deacetylase 3 binds chromatin at the hepcidin locus, and histone deacetylase 3 knockdown counteracts hepcidin suppression induced either by erythroferrone or by inhibiting bone morphogenetic protein signaling. In iron deficient mice, the histone deacetylase 3 inhibitor RGFP966 increases hepcidin, and RNA sequencing confirms hepcidin is one of the genes most differentially regulated by this drug in vivo. We conclude that suppression of hepcidin expression involves epigenetic regulation by histone deacetylase 3.Hepcidin controls systemic iron levels by inhibiting intestinal iron absorption and iron recycling. Here, Pasricha et al. demonstrate that the hepcidin-chromatin locus displays HDAC3-mediated reversible epigenetic modifications during both erythropoiesis and iron deficiency.

Published

2017

14. Effect of 5 Genetic Variants Associated with Lung Function on the Risk of COPD, and their Joint Effects on Lung Function

Author

Soler Artigas, M, Wain, L, Repapi, E, Obeidat, M, Sayers, I, Burton, P, Johnson, T, Zhao, J, Albrecht, E, Dominiczak, A, Kerr, S, Smith, B, Cadby, G, Hui, J, Palmer, L, Hingorani, A, Wannamethee, S, Whincup, P, Ebrahim, S, Smith, G, Barroso, I, Loos, R, Wareham, N, Cooper, C, and Dennison, E

Abstract

RATIONALE: Genomic loci are associated with forced expiratory volume in one second (FEV1) or the ratio of FEV1 to forced vital capacity (FVC) in population samples, but their association with COPD has not yet been proven, nor have their combined effects on lung function and COPD been studied. OBJECTIVES: To test association with COPD of variants at five loci (TNS1, GSTCD, HTR4, AGER and THSD4) and evaluate joint effects on lung function and COPD of these SNPs, and variants at the previously reported locus near HHIP. METHODS: Sampling from 12 population-based studies (n=31,422), we obtained genotype data on 3,284 COPD cases and 17,538 controls for sentinel SNPs in TNS1, GSTCD, HTR4, AGER and THSD4. In 24,648 individuals (including 2,890 COPD cases and 13,862 controls), we additionally obtained genotypes for rs12504628 near HHIP. Each allele associated with lung function decline at these six SNPs contributed to a risk score. We studied the association of the risk score to lung function and COPD. RESULTS: Association with COPD was significant for three loci (TNS1, GSTCD, HTR4) and the previously reported HHIP locus, and suggestive and directionally consistent for AGER and TSHD4. Compared with the baseline group (7 risk alleles), carrying 10-12 risk alleles was associated with a reduction in FEV1 (β=-72.21 ml, P=3.90x10-4) and FEV1/FVC (β=-1.53%, P=6.35x10-6), and with COPD (OR=1.63, P=1.46x10-5). CONCLUSIONS: Variants in TNS1, GSTCD and HTR4 are associated with COPD. Our highest risk score category was associated with 1.6-fold higher COPD risk than the population average score.

Published

2016

15. Transforming Growth Factor β drives haemogenic endothelium programming and the transition to haematopoietic stem cells

Author

Monteiro, RMP, Pinheiro, P, Joseph, N, Peterkin, T, Koth, J, Repapi, E, Bonkhofer, F, Kirmizitas, A, and Patient, R

Abstract

Hematopoietic stem cells (HSCs) are self-renewing multipotent stem cells that generate mature blood lineages throughout life. They, together with hematopoietic progenitor cells (collectively known as HSPCs), emerge from hemogenic endothelium in the floor of the embryonic dorsal aorta by an endothelial-to-hematopoietic transition (EHT). Here we demonstrate that transforming growth factor β (TGFβ) is required for HSPC specification and that it regulates the expression of the Notch ligand Jagged1a in endothelial cells prior to EHT, in a striking parallel with the epithelial-to-mesenchymal transition (EMT). The requirement for TGFβ is two fold and sequential: autocrine via Tgfβ1a and Tgfβ1b produced in the endothelial cells themselves, followed by a paracrine input of Tgfβ3 from the notochord, suggesting that the former programs the hemogenic endothelium and the latter drives EHT. Our findings have important implications for the generation of HSPCs from pluripotent cells in vitro.

Published

2016

16. Identification of Aberrant Splicing Events in Myelodysplastic Syndrome Patients with Splicing Factor Gene Mutations

Author

Pellagatti, A., primary, Steeples, V., additional, Sharma, E., additional, Repapi, E., additional, Yip, B.H., additional, Armstrong, R.N., additional, Dolatshad, H., additional, Lockstone, H., additional, Taylor, S., additional, Giagounidis, A., additional, Vyas, P., additional, Papaemmanuil, E., additional, Woll, P., additional, Killick, S., additional, Malcovati, L., additional, Hellström-Lindberg, E., additional, Cazzola, M., additional, Smith, C.W.J., additional, and Boultwood, J., additional

Published

2017

17. P39 CTAS – a ct score to quantify disease activity in pulmonary sarcoidosis

Author

Kendrick, YK, primary, Repapi, E, additional, Helm, E, additional, Cole, SL, additional, Hoyles, R, additional, Benamore, R, additional, and Ho, LP, additional

Published

2016

18. Cryptic splicing events in the iron transporter ABCB7 and other key target genes in SF3B1-mutant myelodysplastic syndromes

Author

Dolatshad, H, primary, Pellagatti, A, additional, Liberante, F G, additional, Llorian, M, additional, Repapi, E, additional, Steeples, V, additional, Roy, S, additional, Scifo, L, additional, Armstrong, R N, additional, Shaw, J, additional, Yip, B H, additional, Killick, S, additional, Kušec, R, additional, Taylor, S, additional, Mills, K I, additional, Savage, K I, additional, Smith, C W J, additional, and Boultwood, J, additional

Published

2016

19. An integrated genomic approach for the identification and analysis of single nucleotide polymorphisms that affect cancer in humans

Author

Repapi, E, Bond, G, and Meinshausen, N

Subjects

Genetics (life sciences), Mathematical genetics and bioinformatics (statistics), Bioinformatics (life sciences)

Abstract

The identification of genetic variants such as single nucleotide polymorphisms (SNPs), which affect cancer progression, survival and response to treatments could help in the design of better prevention and treatment strategies. Genome-wide association studies (GWAS) have provided the first step of identifying SNPs associating with cancer risk. However, identifying the causal SNPs responsible for the associations has proven challenging, and GWAS have not been successful for time-to-event phenotypes such as cancer progression, due to the insurmountable obstacle of the large sample size needed. The aim of this thesis is to design and implement strategies that combine the identification of SNPs significantly associated with cancer, focusing on time-to-event phenotypes, with detailed bioinformatics analysis to allow for further experimental validation and modelling, to better understand cancer-associated genomic loci and accelerate their incorporation into the clinic. First, a methodology that utilises the Random Survival Forest is developed and combined with a bioinformatics analysis that ranks SNPs according to their potential to result in differential protein levels or activity, in order to identify SNPs that affect the progression of B-cell chronic lymphocytic leukaemia. Next, an analysis that aims to extend our understanding of the role of SNPs in mediating the cellular responses to chemotherapeutic agents is applied. SNPs that could associate with differential cellular growth responses in cancer cell line panels are identified, and their association with the differential survival of cancer patients is explored. Finally, the potential roles of SNPs in affecting the transcriptional regulation of key cancer genes resulting in differential cancer risk are assessed. First, by focusing on SNPs in an important transcription factor binding motif that has been shown to be extremely sensitive to single base pair changes (the E-box) and next, by exploring the possibility that polymorphic transcription factor binding sites could underlie the significant associations noted in cancer GWAS.

Published

2013

20. Effect of 5 Genetic Variants Associated with Lung Function on the Risk of COPD, and their Joint Effects on Lung Function

Author

Soler Artigas, M, Wain, LV, Repapi, E, Obeidat, M, Sayers, I, Burton, PR, Johnson, T, Zhao, JH, Albrecht, E, Dominiczak, AF, Kerr, SM, Smith, BH, Cadby, G, Hui, J, Palmer, LJ, Hingorani, AD, Wannamethee, SG, Whincup, PH, Ebrahim, S, Smith, GD, Barroso, I, Loos, RJ, Wareham, NJ, Cooper, C, Dennison, E, Shaheen, SO, Liu, JZ, Marchini, J, Dahgam, S, Naluai, AT, Olin, AC, Karrasch, S, Heinrich, J, Schulz, H, McKeever, TM, Pavord, ID, Heliövaara, M, Ripatti, S, Surakka, I, Blakey, JD, Kähönen, M, Britton, JR, Nyberg, F, Holloway, JW, Lawlor, DA, Morris, RW, James, AL, Jackson, CM, Hall, IP, and Tobin, MD

Subjects

respiratory tract diseases

Abstract

RATIONALE: Genomic loci are associated with forced expiratory volume in one second (FEV1) or the ratio of FEV1 to forced vital capacity (FVC) in population samples, but their association with COPD has not yet been proven, nor have their combined effects on lung function and COPD been studied. OBJECTIVES: To test association with COPD of variants at five loci (TNS1, GSTCD, HTR4, AGER and THSD4) and evaluate joint effects on lung function and COPD of these SNPs, and variants at the previously reported locus near HHIP. METHODS: Sampling from 12 population-based studies (n=31,422), we obtained genotype data on 3,284 COPD cases and 17,538 controls for sentinel SNPs in TNS1, GSTCD, HTR4, AGER and THSD4. In 24,648 individuals (including 2,890 COPD cases and 13,862 controls), we additionally obtained genotypes for rs12504628 near HHIP. Each allele associated with lung function decline at these six SNPs contributed to a risk score. We studied the association of the risk score to lung function and COPD. RESULTS: Association with COPD was significant for three loci (TNS1, GSTCD, HTR4) and the previously reported HHIP locus, and suggestive and directionally consistent for AGER and TSHD4. Compared with the baseline group (7 risk alleles), carrying 10-12 risk alleles was associated with a reduction in FEV1 (β=-72.21 ml, P=3.90x10-4) and FEV1/FVC (β=-1.53%, P=6.35x10-6), and with COPD (OR=1.63, P=1.46x10-5). CONCLUSIONS: Variants in TNS1, GSTCD and HTR4 are associated with COPD. Our highest risk score category was associated with 1.6-fold higher COPD risk than the population average score.

Published

2011

21. 16 - Identification of Aberrant Splicing Events in Myelodysplastic Syndrome Patients with Splicing Factor Gene Mutations

Author

Pellagatti, A., Steeples, V., Sharma, E., Repapi, E., Yip, B.H., Armstrong, R.N., Dolatshad, H., Lockstone, H., Taylor, S., Giagounidis, A., Vyas, P., Papaemmanuil, E., Woll, P., Killick, S., Malcovati, L., Hellström-Lindberg, E., Cazzola, M., Smith, C.W.J., and Boultwood, J.

Published

2017

22. P25 Distinct Pro-inflammatory Gene Expression Profile In Monocytes From Sarcoidosis Patients With Active Disease

Author

Crawshaw, A., primary, Kendrik, Y., additional, Repapi, E., additional, Taylor, S., additional, and Ho, L.-P., additional

Published

2014

23. A Comprehensive Evaluation of Potential Lung Function Associated Genes in the SpiroMeta General Population Sample

Author

Semple, MG, Obeidat, M, Wain, LV, Shrine, N, Kalsheker, N, Artigas, MS, Repapi, E, Burton, PR, Johnson, T, Ramasamy, A, Zhao, JH, Zhai, G, Huffman, JE, Vitart, V, Albrecht, E, Igl, W, Hartikainen, A-L, Pouta, A, Cadby, G, Hui, J, Palmer, LJ, Hadley, D, McArdle, WL, Rudnicka, AR, Barroso, I, Loos, RJF, Wareham, NJ, Mangino, M, Soranzo, N, Spector, TD, Glaeser, S, Homuth, G, Voelzke, H, Deloukas, P, Granell, R, Henderson, J, Grkovic, I, Jankovic, S, Zgaga, L, Polasek, O, Rudan, I, Wright, AF, Campbell, H, Wild, SH, Wilson, JF, Heinrich, J, Imboden, M, Probst-Hensch, NM, Gyllensten, U, Johansson, A, Zaboli, G, Mustelin, L, Rantanen, T, Surakka, I, Kaprio, J, Jarvelin, M-R, Hayward, C, Evans, DM, Koch, B, Musk, AW, Elliott, P, Strachan, DP, Tobin, MD, Sayers, I, Hall, IP, Semple, MG, Obeidat, M, Wain, LV, Shrine, N, Kalsheker, N, Artigas, MS, Repapi, E, Burton, PR, Johnson, T, Ramasamy, A, Zhao, JH, Zhai, G, Huffman, JE, Vitart, V, Albrecht, E, Igl, W, Hartikainen, A-L, Pouta, A, Cadby, G, Hui, J, Palmer, LJ, Hadley, D, McArdle, WL, Rudnicka, AR, Barroso, I, Loos, RJF, Wareham, NJ, Mangino, M, Soranzo, N, Spector, TD, Glaeser, S, Homuth, G, Voelzke, H, Deloukas, P, Granell, R, Henderson, J, Grkovic, I, Jankovic, S, Zgaga, L, Polasek, O, Rudan, I, Wright, AF, Campbell, H, Wild, SH, Wilson, JF, Heinrich, J, Imboden, M, Probst-Hensch, NM, Gyllensten, U, Johansson, A, Zaboli, G, Mustelin, L, Rantanen, T, Surakka, I, Kaprio, J, Jarvelin, M-R, Hayward, C, Evans, DM, Koch, B, Musk, AW, Elliott, P, Strachan, DP, Tobin, MD, Sayers, I, and Hall, IP

Abstract

RATIONALE: Lung function measures are heritable traits that predict population morbidity and mortality and are essential for the diagnosis of chronic obstructive pulmonary disease (COPD). Variations in many genes have been reported to affect these traits, but attempts at replication have provided conflicting results. Recently, we undertook a meta-analysis of Genome Wide Association Study (GWAS) results for lung function measures in 20,288 individuals from the general population (the SpiroMeta consortium). OBJECTIVES: To comprehensively analyse previously reported genetic associations with lung function measures, and to investigate whether single nucleotide polymorphisms (SNPs) in these genomic regions are associated with lung function in a large population sample. METHODS: We analysed association for SNPs tagging 130 genes and 48 intergenic regions (+/-10 kb), after conducting a systematic review of the literature in the PubMed database for genetic association studies reporting lung function associations. RESULTS: The analysis included 16,936 genotyped and imputed SNPs. No loci showed overall significant association for FEV(1) or FEV(1)/FVC traits using a carefully defined significance threshold of 1.3×10(-5). The most significant loci associated with FEV(1) include SNPs tagging MACROD2 (P = 6.81×10(-5)), CNTN5 (P = 4.37×10(-4)), and TRPV4 (P = 1.58×10(-3)). Among ever-smokers, SERPINA1 showed the most significant association with FEV(1) (P = 8.41×10(-5)), followed by PDE4D (P = 1.22×10(-4)). The strongest association with FEV(1)/FVC ratio was observed with ABCC1 (P = 4.38×10(-4)), and ESR1 (P = 5.42×10(-4)) among ever-smokers. CONCLUSIONS: Polymorphisms spanning previously associated lung function genes did not show strong evidence for association with lung function measures in the SpiroMeta consortium population. Common SERPINA1 polymorphisms may affect FEV(1) among smokers in the general population.

Published

2011

24. Cryptic splicing events in the iron transporter ABCB7 and other key target genes in SF3B1-mutant myelodysplastic syndromes

Author

Dolatshad, H, Pellagatti, A, Liberante, FG, Llorian, M, Repapi, E, Steeples, V, Roy, S, Scifo, L, Armstrong, RN, Shaw, J, Yip, BH, Killick, S, Kušec, R, Taylor, S, Mills, KI, Savage, KI, Smith, CWJ, and Boultwood, J

Subjects

Base Sequence, Iron, RNA Splicing, Hematopoietic Stem Cells, Phosphoproteins, 3. Good health, Mitochondria, hemic and lymphatic diseases, Myelodysplastic Syndromes, Tumor Cells, Cultured, Humans, ATP-Binding Cassette Transporters, RNA Splicing Factors, Cycloheximide

Abstract

The splicing factor SF3B1 is the most frequently mutated gene in myelodysplastic syndromes (MDS), and is strongly associated with the presence of ring sideroblasts (RS). We have performed a systematic analysis of cryptic splicing abnormalities from RNA sequencing data on hematopoietic stem cells (HSCs) of SF3B1-mutant MDS cases with RS. Aberrant splicing events in many downstream target genes were identified and cryptic 3' splice site usage was a frequent event in SF3B1-mutant MDS. The iron transporter ABCB7 is a well-recognized candidate gene showing marked downregulation in MDS with RS. Our analysis unveiled aberrant ABCB7 splicing, due to usage of an alternative 3' splice site in MDS patient samples, giving rise to a premature termination codon in the ABCB7 mRNA. Treatment of cultured SF3B1-mutant MDS erythroblasts and a CRISPR/Cas9-generated SF3B1-mutant cell line with the nonsense-mediated decay (NMD) inhibitor cycloheximide showed that the aberrantly spliced ABCB7 transcript is targeted by NMD. We describe cryptic splicing events in the HSCs of SF3B1-mutant MDS, and our data support a model in which NMD-induced downregulation of the iron exporter ABCB7 mRNA transcript resulting from aberrant splicing caused by mutant SF3B1 underlies the increased mitochondrial iron accumulation found in MDS patients with RS.

25. The U2AF1$^{S34F}$ mutation induces lineage-specific splicing alterations in myelodysplastic syndromes

Author

Yip, BH, Steeples, V, Repapi, E, Armstrong, RN, Llorian, M, Roy, S, Shaw, J, Dolatshad, H, Taylor, S, Verma, A, Bartenstein, M, Vyas, P, Cross, NC, Malcovati, L, Cazzola, M, Hellström-Lindberg, E, Ogawa, S, Smith, CW, Pellagatti, A, and Boultwood, J

Subjects

RNA Splicing, Mutation, Missense, Splicing Factor U2AF, 3. Good health, Gene Ontology, hemic and lymphatic diseases, Case-Control Studies, Myelodysplastic Syndromes, Humans, Protein Isoforms, Cell Lineage, Erythropoiesis, Cells, Cultured, Cell Proliferation, Granulocytes

Abstract

Mutations of the splicing factor-encoding gene U2AF1 are frequent in the myelodysplastic syndromes (MDS), a myeloid malignancy, and other cancers. Patients with MDS suffer from peripheral blood cytopenias, including anemia, and an increasing percentage of bone marrow myeloblasts. We studied the impact of the common U2AF1$^{S34F}$ mutation on cellular function and mRNA splicing in the main cell lineages affected in MDS. We demonstrated that U2AF1$^{S34F}$ expression in human hematopoietic progenitors impairs erythroid differentiation and skews granulomonocytic differentiation toward granulocytes. RNA sequencing of erythroid and granulomonocytic colonies revealed that U2AF1$^{S34F}$ induced a higher number of cassette exon splicing events in granulomonocytic cells than in erythroid cells. U2AF1$^{S34F}$ altered mRNA splicing of many transcripts that were expressed in both cell types in a lineage-specific manner. In hematopoietic progenitors, the introduction of isoform changes identified in the U2AF1$^{S34F}$ target genes H2AFY, encoding an H2A histone variant, and STRAP, encoding serine/threonine kinase receptor-associated protein, recapitulated phenotypes associated with U2AF1$^{S34F}$ expression in erythroid and granulomonocytic cells, suggesting a causal link. Furthermore, we showed that isoform modulation of H2AFY and STRAP rescues the erythroid differentiation defect in U2AF1$^{S34F}$ MDS cells, suggesting that splicing modulators could be used therapeutically. These data have critical implications for understanding MDS phenotypic heterogeneity and support the development of therapies targeting splicing abnormalities.

26. Fundamental period of infilled reinforced concrete frame structures

Author

Emmanouela Repapi, Constantinos C. Repapis, Panagiotis G. Asteris, Liborio Cavaleri, Asteris, P., Repapis, C., Repapi, E., and Cavaleri, L.

Subjects

Engineering, Infill wall, Modal analysis, 0211 other engineering and technologies, 020101 civil engineering, Ocean Engineering, 02 engineering and technology, reinforced concrete frame building, Span (engineering), 0201 civil engineering, Seismic analysis, regression analysi, Fundamental period, medicine, Infill, Geotechnical engineering, Safety, Risk, Reliability and Quality, Civil and Structural Engineering, 021110 strategic, defence & security studies, modal analysi, business.industry, infilled frame, Mechanical Engineering, Stiffness, Structural engineering, Building and Construction, Masonry, Geotechnical Engineering and Engineering Geology, Vibration, Settore ICAR/09 - Tecnica Delle Costruzioni, masonry, medicine.symptom, business

Abstract

The fundamental period of vibration appears to be one of the most critical parameters for the seismic design and assessment of structures. In the present paper, the results of a large-scale analytical investigation on the parameters that affect the fundamental period of reinforced concrete structures are presented. The influence of the number of storeys, the number of spans, the span length, the infill wall panel stiffness and the percentage of openings within the infill panel on the fundamental period of infilled RC frames was investigated. Based on these results, a regression analysis is applied in order to propose a new empirical equation for the estimation of the fundamental period. The derived equation is shown to have better predictive power compared with equations available in the literature.

Published

2016

27. Single cell spatial analysis reveals inflammatory foci of immature neutrophil and CD8 T cells in COVID-19 lungs.

Author

Weeratunga P, Denney L, Bull JA, Repapi E, Sergeant M, Etherington R, Vuppussetty C, Turner GDH, Clelland C, Woo J, Cross A, Issa F, de Andrea CE, Melero Bermejo I, Sims D, McGowan S, Zurke YX, Ahern DJ, Gamez EC, Whalley J, Richards D, Klenerman P, Monaco C, Udalova IA, Dong T, Antanaviciute A, Ogg G, Knight JC, Byrne HM, Taylor S, and Ho LP

Subjects

Humans, CD8-Positive T-Lymphocytes, Lung, T-Lymphocytes, Cytotoxic, Neutrophils, COVID-19

Abstract

Single cell spatial interrogation of the immune-structural interactions in COVID -19 lungs is challenging, mainly because of the marked cellular infiltrate and architecturally distorted microstructure. To address this, we develop a suite of mathematical tools to search for statistically significant co-locations amongst immune and structural cells identified using 37-plex imaging mass cytometry. This unbiased method reveals a cellular map interleaved with an inflammatory network of immature neutrophils, cytotoxic CD8 T cells, megakaryocytes and monocytes co-located with regenerating alveolar progenitors and endothelium. Of note, a highly active cluster of immature neutrophils and CD8 T cells, is found spatially linked with alveolar progenitor cells, and temporally with the diffuse alveolar damage stage. These findings offer further insights into how immune cells interact in the lungs of severe COVID-19 disease. We provide our pipeline [Spatial Omics Oxford Pipeline (SpOOx)] and visual-analytical tool, Multi-Dimensional Viewer (MDV) software, as a resource for spatial analysis., (© 2023. The Author(s).)

Published

2023

28. No evidence for age-related differences in mitochondrial RNA quality in the female germline.

Author

Hartley F, Alageel A, Appeltant R, Gray N, Repapi E, Wells D, Williams SA, and Poulton J

Subjects

Female, Animals, Mice, RNA, Mitochondrial genetics, RNA, Mitochondrial metabolism, DNA, Mitochondrial genetics, DNA, Mitochondrial metabolism, RNA genetics, RNA metabolism, Ovarian Follicle, Oocytes metabolism

Abstract

Abstract: Mitochondrial quality is implicated as a contributor to declining fertility with aging. We investigated mitochondrial transcripts in oocytes and their associated cumulus cells from mice of different ages using RNA-seq. Mice aged 3 weeks, 9 weeks, and 1 year were superovulated, and 48 h later, oocyte cumulus complexes were collected by follicle puncture. We did not detect any major differences that could be attributed to aging. However, mitochondrial RNA transcripts which deviated from the consensus sequence were found at a higher frequency in cumulus cells than in their corresponding oocyte. Previous investigations have shown that variation in the sequence of mtRNA transcripts is substantial, and at least some of this can be accounted for by post-transcriptional modifications which impact base calling during sequencing. Our data would be consistent with either less post-transcriptional modification in mitochondrial RNA from oocytes than cumulus cells or with lower mtDNA mutational load., Lay Summary: Women become less fertile as they age. Shortage of energy contributes to this, caused by a decline in the quality of mitochondria (the powerhouses of the cell) in the egg. Genes are the blueprint for the cell. They are made of DNA which is copied into an RNA message, or instructions, for making proteins. We counted differences in the RNA message of developing eggs and the cells that support them during development (cumulus cells). We compared the number of these differences in mice of different ages. These age groups represent mice had not reached puberty, those of prime reproductive age, and old mothers. We did not find any differences linked to the age of the mice. However, we did find differences between the egg and the cumulus cells. In most cases, there were lower levels of mutations in eggs than there were in cumulus cells.

Published

2022

29. IL-6 effector function of group 2 innate lymphoid cells (ILC2) is NOD2 dependent.

Author

Hardman CS, Chen YL, Salimi M, Nahler J, Corridoni D, Jagielowicz M, Fonseka CL, Johnson D, Repapi E, Cousins DJ, Barlow JL, McKenzie ANJ, Simmons A, and Ogg G

Subjects

Adult, Allergens immunology, Antigens, Dermatophagoides immunology, Humans, Immunity, Innate, Mutation, Nod2 Signaling Adaptor Protein genetics, Skin immunology, Skin microbiology, Staphylococcus aureus, Toll-Like Receptor 2 immunology, Cytokines immunology, Lymphocytes immunology, Nod2 Signaling Adaptor Protein immunology, Staphylococcal Infections immunology

Abstract

Cutaneous group 2 innate lymphoid cells (ILC2) are spatially and epigenetically poised to respond to barrier compromise and associated immunological threats. ILC2, lacking rearranged antigen-specific receptors, are primarily activated by damage-associated cytokines and respond with type 2 cytokine production. To investigate ILC2 potential for direct sensing of skin pathogens and allergens, we performed RNA sequencing of ILC2 derived from in vivo challenged human skin or blood. We detected expression of NOD2 and TLR2 by skin and blood ILC2. Stimulation of ILC2 with TLR2 agonist alone not only induced interleukin-5 (IL-5) and IL-13 expression but also elicited IL-6 expression in combination with Staphylococcus aureus muramyl dipeptide (MDP). Heat-killed skin-resident bacteria provoked an IL-6 profile in ILC2 in vitro that was notably impaired in ILC2 derived from patients with nucleotide-binding oligomerization domain-containing protein 2 (NOD2) mutations. In addition, we show that NOD2 signaling can stimulate autophagy in ILC2, which was also impaired in patients with NOD2 mutations. Here, we have identified a role for ILC2 NOD2 signaling in the differential regulation of ILC2-derived IL-6 and have reported a previously unrecognized pathway of direct ILC2 bacterial sensing., (Copyright © 2021 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.)

Published

2021

30. Multi-Modal Characterization of Monocytes in Idiopathic Pulmonary Fibrosis Reveals a Primed Type I Interferon Immune Phenotype.

Author

Fraser E, Denney L, Antanaviciute A, Blirando K, Vuppusetty C, Zheng Y, Repapi E, Iotchkova V, Taylor S, Ashley N, St Noble V, Benamore R, Hoyles R, Clelland C, Rastrick JMD, Hardman CS, Alham NK, Rigby RE, Simmons A, Rehwinkel J, and Ho LP

Subjects

Case-Control Studies, Cells, Cultured, Chemokine CCL2 blood, Flow Cytometry, Gene Expression Profiling, Humans, Idiopathic Pulmonary Fibrosis genetics, Idiopathic Pulmonary Fibrosis metabolism, Idiopathic Pulmonary Fibrosis pathology, Immunophenotyping, Interferon Type I genetics, Interleukin-6 blood, Lung metabolism, Lung pathology, Macrophage Colony-Stimulating Factor blood, Macrophages immunology, Macrophages metabolism, Monocytes metabolism, Phenotype, Receptors, IgG genetics, Receptors, IgG metabolism, Single-Cell Analysis, Idiopathic Pulmonary Fibrosis immunology, Interferon Type I metabolism, Lung immunology, Monocytes immunology

Abstract

Idiopathic pulmonary fibrosis (IPF) is the most severe form of chronic lung fibrosis. Circulating monocytes have been implicated in immune pathology in IPF but their phenotype is unknown. In this work, we determined the immune phenotype of monocytes in IPF using multi-colour flow cytometry, RNA sequencing and corresponding serum factors, and mapped the main findings to amount of lung fibrosis and single cell transcriptomic landscape of myeloid cells in IPF lungs. We show that monocytes from IPF patients displayed increased expression of CD64 (FcγR1) which correlated with amount of lung fibrosis, and an amplified type I IFN response ex vivo . These were accompanied by markedly raised CSF-1 levels, IL-6, and CCL-2 in serum of IPF patients. Interrogation of single cell transcriptomic data from human IPF lungs revealed increased proportion of CD64 hi monocytes and "transitional macrophages" with higher expression of CCL-2 and type I IFN genes. Our study shows that monocytes in IPF patients are phenotypically distinct from age-matched controls, with a primed type I IFN pathway that may contribute to driving chronic inflammation and fibrosis. These findings strengthen the potential role of monocytes in the pathogenesis of IPF., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2021 Fraser, Denney, Antanaviciute, Blirando, Vuppusetty, Zheng, Repapi, Iotchkova, Taylor, Ashley, St Noble, Benamore, Hoyles, Clelland, Rastrick, Hardman, Alham, Rigby, Simmons, Rehwinkel and Ho.)

Published

2021

31. BET inhibition disrupts transcription but retains enhancer-promoter contact.

Author

Crump NT, Ballabio E, Godfrey L, Thorne R, Repapi E, Kerry J, Tapia M, Hua P, Lagerholm C, Filippakopoulos P, Davies JOJ, and Milne TA

Subjects

CCCTC-Binding Factor metabolism, Carcinogenesis drug effects, Carcinogenesis genetics, Cell Cycle Proteins metabolism, Cell Line, Tumor, Chromatin metabolism, Chromosomal Proteins, Non-Histone metabolism, DNA-Binding Proteins metabolism, Glycols pharmacology, Histones metabolism, Humans, Leukemia genetics, Leukemia pathology, Models, Genetic, Protein Binding drug effects, Proto-Oncogene Proteins c-myc genetics, Cohesins, Enhancer Elements, Genetic, Promoter Regions, Genetic, Transcription, Genetic drug effects

Abstract

Enhancers are DNA sequences that enable complex temporal and tissue-specific regulation of genes in higher eukaryotes. Although it is not entirely clear how enhancer-promoter interactions can increase gene expression, this proximity has been observed in multiple systems at multiple loci and is thought to be essential for the maintenance of gene expression. Bromodomain and Extra-Terminal domain (BET) and Mediator proteins have been shown capable of forming phase condensates and are thought to be essential for super-enhancer function. Here, we show that targeting of cells with inhibitors of BET proteins or pharmacological degradation of BET protein Bromodomain-containing protein 4 (BRD4) has a strong impact on transcription but very little impact on enhancer-promoter interactions. Dissolving phase condensates reduces BRD4 and Mediator binding at enhancers and can also strongly affect gene transcription, without disrupting enhancer-promoter interactions. These results suggest that activation of transcription and maintenance of enhancer-promoter interactions are separable events. Our findings further indicate that enhancer-promoter interactions are not dependent on high levels of BRD4 and Mediator, and are likely maintained by a complex set of factors including additional activator complexes and, at some sites, CTCF and cohesin.

Published

2021

32. Single-cell atlas of colonic CD8 + T cells in ulcerative colitis.

Author

Corridoni D, Antanaviciute A, Gupta T, Fawkner-Corbett D, Aulicino A, Jagielowicz M, Parikh K, Repapi E, Taylor S, Ishikawa D, Hatano R, Yamada T, Xin W, Slawinski H, Bowden R, Napolitani G, Brain O, Morimoto C, Koohy H, and Simmons A

Subjects

Animals, Colon pathology, Female, Gene Expression Profiling, Humans, Intestinal Mucosa cytology, Intestinal Mucosa immunology, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, Transcriptome genetics, CD8-Positive T-Lymphocytes immunology, Colitis, Ulcerative pathology, Interleukins metabolism, Intestinal Mucosa pathology, Tumor Necrosis Factor-alpha metabolism

Abstract

Colonic antigen-experienced lymphocytes such as tissue-resident memory CD8 + T cells can respond rapidly to repeated antigen exposure. However, their cellular phenotypes and the mechanisms by which they drive immune regulation and inflammation remain unclear. Here we compiled an unbiased atlas of human colonic CD8 + T cells in health and ulcerative colitis (UC) using single-cell transcriptomics with T-cell receptor repertoire analysis and mass cytometry. We reveal extensive heterogeneity in CD8 + T-cell composition, including expanded effector and post-effector terminally differentiated CD8 + T cells. While UC-associated CD8 + effector T cells can trigger tissue destruction and produce tumor necrosis factor (TNF)-α, post-effector cells acquire innate signatures to adopt regulatory functions that may mitigate excessive inflammation. Thus, we identify colonic CD8 + T-cell phenotypes in health and UC, define their clonal relationships and characterize terminally differentiated dysfunctional UC CD8 + T cells expressing IL-26, which attenuate acute colitis in a humanized IL-26 transgenic mouse model.

Published

2020

33. Cell-intrinsic depletion of Aml1-ETO-expressing pre-leukemic hematopoietic stem cells by K-Ras activating mutation.

Author

Di Genua C, Norfo R, Rodriguez-Meira A, Wen WX, Drissen R, Booth CAG, Povinelli B, Repapi E, Gray N, Carrelha J, Kettyle LM, Jamieson L, Neo WH, Thongjuea S, Nerlov C, and Mead AJ

Subjects

Animals, Cell Proliferation genetics, Gene Expression, Gene Expression Profiling, Hematopoietic Stem Cells pathology, Humans, Mice, Mice, Transgenic, Models, Animal, Models, Biological, Precancerous Conditions genetics, Precancerous Conditions metabolism, Cell Transformation, Neoplastic genetics, Cell Transformation, Neoplastic metabolism, Core Binding Factor Alpha 2 Subunit genetics, Core Binding Factor Alpha 2 Subunit metabolism, Hematopoietic Stem Cells metabolism, Mutation, Oncogene Proteins, Fusion genetics, Oncogene Proteins, Fusion metabolism, Proto-Oncogene Proteins p21(ras) genetics, RUNX1 Translocation Partner 1 Protein genetics, RUNX1 Translocation Partner 1 Protein metabolism

Abstract

Somatic mutations in acute myeloid leukemia are acquired sequentially and hierarchically. First, pre-leukemic mutations, such as t(8;21) that encodes AML1-ETO, are acquired within the hematopoietic stem cell (HSC) compartment, while signaling pathway mutations, including KRAS activating mutations, are late events acquired during transformation of leukemic progenitor cells and are rarely detectable in HSC. This raises the possibility that signaling pathway mutations are detrimental to clonal expansion of pre-leukemic HSC. To address this hypothesis, we used conditional genetics to introduce Aml1-ETO and K-RasG12D into murine HSC, either individually or in combination. In the absence of activated Ras, Aml1-ETO-expressing HSC conferred a competitive advantage. However, activated K-Ras had a marked detrimental effect on Aml1-ETO-expressing HSC, leading to loss of both phenotypic and functional HSC. Cell cycle analysis revealed a loss of quiescence in HSC co-expressing Aml1-ETO and K-RasG12D, accompanied by an enrichment in E2F and Myc target gene expression and depletion of HSC self-renewal-associated gene expression. These findings provide a mechanistic basis for the observed absence of KRAS signaling mutations in the pre-malignant HSC compartment., (Copyright© 2019 Ferrata Storti Foundation.)

Published

2019

34. Reconstruction of the Global Neural Crest Gene Regulatory Network In Vivo.

Author

Williams RM, Candido-Ferreira I, Repapi E, Gavriouchkina D, Senanayake U, Ling ITC, Telenius J, Taylor S, Hughes J, and Sauka-Spengler T

Subjects

Animals, Genetic Heterogeneity, Vertebrates genetics, Gene Expression Regulation, Developmental genetics, Gene Regulatory Networks genetics, Neural Crest embryology, Transcriptional Activation genetics

Abstract

Precise control of developmental processes is encoded in the genome in the form of gene regulatory networks (GRNs). Such multi-factorial systems are difficult to decode in vertebrates owing to their complex gene hierarchies and dynamic molecular interactions. Here we present a genome-wide in vivo reconstruction of the GRN underlying development of the multipotent neural crest (NC) embryonic cell population. By coupling NC-specific epigenomic and transcriptional profiling at population and single-cell levels with genome/epigenome engineering in vivo, we identify multiple regulatory layers governing NC ontogeny, including NC-specific enhancers and super-enhancers, novel trans-factors, and cis-signatures allowing reverse engineering of the NC-GRN at unprecedented resolution. Furthermore, identification and dissection of divergent upstream combinatorial regulatory codes has afforded new insights into opposing gene circuits that define canonical and neural NC fates early during NC ontogeny. Our integrated approach, allowing dissection of cell-type-specific regulatory circuits in vivo, has broad implications for GRN discovery and investigation., (Copyright © 2019 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2019

35. DOT1L inhibition reveals a distinct subset of enhancers dependent on H3K79 methylation.

Author

Godfrey L, Crump NT, Thorne R, Lau IJ, Repapi E, Dimou D, Smith AL, Harman JR, Telenius JM, Oudelaar AM, Downes DJ, Vyas P, Hughes JR, and Milne TA

Subjects

Benzimidazoles pharmacology, Cell Line, Tumor, Genome-Wide Association Study, Histone-Lysine N-Methyltransferase, Histones genetics, Humans, Methylation, Methyltransferases genetics, Enhancer Elements, Genetic physiology, Gene Expression Regulation drug effects, Histones metabolism, Methyltransferases metabolism

Abstract

Enhancer elements are a key regulatory feature of many important genes. Several general features including the presence of specific histone modifications are used to demarcate potentially active enhancers. Here we reveal that putative enhancers marked with H3 lysine 79 (H3K79) di or trimethylation (me2/3) (which we name H3K79me2/3 enhancer elements or KEEs) can be found in multiple cell types. Mixed lineage leukemia gene (MLL) rearrangements (MLL-r) such as MLL-AF4 are a major cause of incurable acute lymphoblastic leukemias (ALL). Using the DOT1L inhibitor EPZ-5676 in MLL-AF4 leukemia cells, we show that H3K79me2/3 is required for maintaining chromatin accessibility, histone acetylation and transcription factor binding specifically at KEEs but not non-KEE enhancers. We go on to show that H3K79me2/3 is essential for maintaining enhancer-promoter interactions at a subset of KEEs. Together, these data implicate H3K79me2/3 as having a functional role at a subset of active enhancers in MLL-AF4 leukemia cells.

Published

2019

36. Does osteogenic potential of clonal human bone marrow mesenchymal stem/stromal cells correlate with their vascular supportive ability?

Author

Merryweather-Clarke AT, Cook D, Lara BJ, Hua P, Repapi E, Ashley N, Lim SY, and Watt SM

Subjects

Adult, Cell Proliferation, Cells, Cultured, Humans, Young Adult, Mesenchymal Stem Cells metabolism, Osteogenesis genetics

Abstract

Background: Human bone marrow-derived mesenchymal stem/stromal cells (hBM MSCs) have multiple functions, critical for skeletal formation and function. Their functional heterogeneity, however, represents a major challenge for their isolation and in developing potency and release assays to predict their functionality prior to transplantation. Additionally, potency, biomarker profiles and defining mechanisms of action in a particular clinical setting are increasing requirements of Regulatory Agencies for release of hBM MSCs as Advanced Therapy Medicinal Products for cellular therapies. Since the healing of bone fractures depends on the coupling of new blood vessel formation with osteogenesis, we hypothesised that a correlation between the osteogenic and vascular supportive potential of individual hBM MSC-derived CFU-F (colony forming unit-fibroblastoid) clones might exist., Methods: We tested this by assessing the lineage (i.e. adipogenic (A), osteogenic (O) and/or chondrogenic (C)) potential of individual hBM MSC-derived CFU-F clones and determining if their osteogenic (O) potential correlated with their vascular supportive profile in vitro using lineage differentiation assays, endothelial-hBM MSC vascular co-culture assays and transcriptomic (RNAseq) analyses., Results: Our results demonstrate that the majority of CFU-F (95%) possessed tri-lineage, bi-lineage or uni-lineage osteogenic capacity, with 64% of the CFU-F exhibiting tri-lineage AOC potential. We found a correlation between the osteogenic and vascular tubule supportive activity of CFU-F clones, with the strength of this association being donor dependent. RNAseq of individual clones defined gene fingerprints relevant to this correlation., Conclusions: This study identified a donor-dependent correlation between osteogenic and vascular supportive potential of hBM MSCs and important gene signatures that support these functions that are relevant to their bone regenerative properties.

Published

2018

37. SCL/TAL1 cooperates with Polycomb RYBP-PRC1 to suppress alternative lineages in blood-fated cells.

Author

Chagraoui H, Kristiansen MS, Ruiz JP, Serra-Barros A, Richter J, Hall-Ponselé E, Gray N, Waithe D, Clark K, Hublitz P, Repapi E, Otto G, Sopp P, Taylor S, Thongjuea S, Vyas P, and Porcher C

Subjects

Animals, Cell Differentiation physiology, Cell Line, Cell Separation methods, Embryo, Mammalian, Flow Cytometry methods, Histone Code physiology, Mesoderm cytology, Mesoderm physiology, Mice, Mouse Embryonic Stem Cells, Nuclear Proteins genetics, Polycomb Repressive Complex 1 metabolism, Polycomb-Group Proteins metabolism, RNA, Small Interfering metabolism, Repressor Proteins genetics, T-Cell Acute Lymphocytic Leukemia Protein 1 genetics, Transcription Factors genetics, Cell Lineage physiology, Gene Expression Regulation, Developmental physiology, Nuclear Proteins metabolism, Repressor Proteins metabolism, T-Cell Acute Lymphocytic Leukemia Protein 1 metabolism, Transcription Factors metabolism

Abstract

During development, it is unclear if lineage-fated cells derive from multilineage-primed progenitors and whether active mechanisms operate to restrict cell fate. Here we investigate how mesoderm specifies into blood-fated cells. We document temporally restricted co-expression of blood (Scl/Tal1), cardiac (Mesp1) and paraxial (Tbx6) lineage-affiliated transcription factors in single cells, at the onset of blood specification, supporting the existence of common progenitors. At the same time-restricted stage, absence of SCL results in expansion of cardiac/paraxial cell populations and increased cardiac/paraxial gene expression, suggesting active suppression of alternative fates. Indeed, SCL normally activates expression of co-repressor ETO2 and Polycomb-PRC1 subunits (RYBP, PCGF5) and maintains levels of Polycomb-associated histone marks (H2AK119ub/H3K27me3). Genome-wide analyses reveal ETO2 and RYBP co-occupy most SCL target genes, including cardiac/paraxial loci. Reduction of Eto2 or Rybp expression mimics Scl-null cardiac phenotype. Therefore, SCL-mediated transcriptional repression prevents mis-specification of blood-fated cells, establishing active repression as central to fate determination processes.

Published

2018

38. From Pioneer to Repressor: Bimodal foxd3 Activity Dynamically Remodels Neural Crest Regulatory Landscape In Vivo.

Author

Lukoseviciute M, Gavriouchkina D, Williams RM, Hochgreb-Hagele T, Senanayake U, Chong-Morrison V, Thongjuea S, Repapi E, Mead A, and Sauka-Spengler T

Subjects

Animals, Chromatin Assembly and Disassembly, Enhancer Elements, Genetic, Forkhead Transcription Factors genetics, Neural Crest embryology, Zebrafish, Zebrafish Proteins genetics, Forkhead Transcription Factors metabolism, Gene Expression Regulation, Developmental, Neural Crest metabolism, Zebrafish Proteins metabolism

Abstract

The neural crest (NC) is a transient embryonic stem cell-like population characterized by its multipotency and broad developmental potential. Here, we perform NC-specific transcriptional and epigenomic profiling of foxd3-mutant cells in vivo to define the gene regulatory circuits controlling NC specification. Together with global binding analysis obtained by foxd3 biotin-ChIP and single cell profiles of foxd3-expressing premigratory NC, our analysis shows that, during early steps of NC formation, foxd3 acts globally as a pioneer factor to prime the onset of genes regulating NC specification and migration by re-arranging the chromatin landscape, opening cis-regulatory elements and reshuffling nucleosomes. Strikingly, foxd3 then gradually switches from an activator to its well-described role as a transcriptional repressor and potentially uses differential partners for each role. Taken together, these results demonstrate that foxd3 acts bimodally in the neural crest as a switch from "permissive" to "repressive" nucleosome and chromatin organization to maintain multipotency and define cell fates., (Copyright © 2018 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2018

39. Impact of spliceosome mutations on RNA splicing in myelodysplasia: dysregulated genes/pathways and clinical associations.

Author

Pellagatti A, Armstrong RN, Steeples V, Sharma E, Repapi E, Singh S, Sanchi A, Radujkovic A, Horn P, Dolatshad H, Roy S, Broxholme J, Lockstone H, Taylor S, Giagounidis A, Vyas P, Schuh A, Hamblin A, Papaemmanuil E, Killick S, Malcovati L, Hennrich ML, Gavin AC, Ho AD, Luft T, Hellström-Lindberg E, Cazzola M, Smith CWJ, Smith S, and Boultwood J

Subjects

Cohort Studies, DNA Repair, Gene Expression Regulation, Humans, Myelodysplastic Syndromes epidemiology, Phosphoproteins genetics, Serine-Arginine Splicing Factors genetics, Splicing Factor U2AF genetics, Survival Analysis, Mutation, Myelodysplastic Syndromes genetics, RNA Splicing, RNA Splicing Factors genetics, Spliceosomes genetics

Abstract

SF3B1 , SRSF2 , and U2AF1 are the most frequently mutated splicing factor genes in the myelodysplastic syndromes (MDS). We have performed a comprehensive and systematic analysis to determine the effect of these commonly mutated splicing factors on pre-mRNA splicing in the bone marrow stem/progenitor cells and in the erythroid and myeloid precursors in splicing factor mutant MDS. Using RNA-seq, we determined the aberrantly spliced genes and dysregulated pathways in CD34 + cells of 84 patients with MDS. Splicing factor mutations result in different alterations in splicing and largely affect different genes, but these converge in common dysregulated pathways and cellular processes, focused on RNA splicing, protein synthesis, and mitochondrial dysfunction, suggesting common mechanisms of action in MDS. Many of these dysregulated pathways and cellular processes can be linked to the known disease pathophysiology associated with splicing factor mutations in MDS, whereas several others have not been previously associated with MDS, such as sirtuin signaling. We identified aberrantly spliced events associated with clinical variables, and isoforms that independently predict survival in MDS and implicate dysregulation of focal adhesion and extracellular exosomes as drivers of poor survival. Aberrantly spliced genes and dysregulated pathways were identified in the MDS-affected lineages in splicing factor mutant MDS. Functional studies demonstrated that knockdown of the mitosis regulators SEPT2 and AKAP8, aberrantly spliced target genes of SF3B1 and SRSF2 mutations, respectively, led to impaired erythroid cell growth and differentiation. This study illuminates the effect of the common spliceosome mutations on the MDS phenotype and provides novel insights into disease pathophysiology., (© 2018 by The American Society of Hematology.)

Published

2018

40. Canonical Notch signaling is dispensable for adult steady-state and stress myelo-erythropoiesis.

Author

Duarte S, Woll PS, Buza-Vidas N, Chin DWL, Boukarabila H, Luís TC, Stenson L, Bouriez-Jones T, Ferry H, Mead AJ, Atkinson D, Jin S, Clark SA, Wu B, Repapi E, Gray N, Taylor S, Mutvei AP, Tsoi YL, Nerlov C, Lendahl U, and Jacobsen SEW

Subjects

Animals, Immunoglobulin J Recombination Signal Sequence-Binding Protein genetics, Immunoglobulin J Recombination Signal Sequence-Binding Protein metabolism, Mice, Mice, Transgenic, Receptors, Notch genetics, Bone Marrow metabolism, Erythropoiesis, Myelopoiesis, Receptors, Notch metabolism, Signal Transduction, Stress, Physiological

Abstract

Although an essential role for canonical Notch signaling in generation of hematopoietic stem cells in the embryo and in thymic T-cell development is well established, its role in adult bone marrow (BM) myelopoiesis remains unclear. Some studies, analyzing myeloid progenitors in adult mice with inhibited Notch signaling, implicated distinct roles of canonical Notch signaling in regulation of progenitors for the megakaryocyte, erythroid, and granulocyte-macrophage cell lineages. However, these studies might also have targeted other pathways. Therefore, we specifically deleted, in adult BM, the transcription factor recombination signal-binding protein J κ (Rbpj), through which canonical signaling from all Notch receptors converges. Notably, detailed progenitor staging established that canonical Notch signaling is fully dispensable for all investigated stages of megakaryocyte, erythroid, and myeloid progenitors in steady state unperturbed hematopoiesis, after competitive BM transplantation, and in stress-induced erythropoiesis. Moreover, expression of key regulators of these hematopoietic lineages and Notch target genes were unaffected by Rbpj deficiency in BM progenitor cells., (© 2018 by The American Society of Hematology.)

Published

2018

41. Single-cell analysis reveals the continuum of human lympho-myeloid progenitor cells.

Author

Karamitros D, Stoilova B, Aboukhalil Z, Hamey F, Reinisch A, Samitsch M, Quek L, Otto G, Repapi E, Doondeea J, Usukhbayar B, Calvo J, Taylor S, Goardon N, Six E, Pflumio F, Porcher C, Majeti R, Göttgens B, and Vyas P

Subjects

Animals, Cell Lineage genetics, Cell Separation methods, Cells, Cultured, Hematopoiesis genetics, Hematopoietic Stem Cell Transplantation methods, Humans, Mice, Transplantation, Heterologous, Cell Differentiation genetics, Gene Expression Profiling methods, Lymphoid Progenitor Cells metabolism, Myeloid Progenitor Cells metabolism, Single-Cell Analysis methods

Abstract

The hierarchy of human hemopoietic progenitor cells that produce lymphoid and granulocytic-monocytic (myeloid) lineages is unclear. Multiple progenitor populations produce lymphoid and myeloid cells, but they remain incompletely characterized. Here we demonstrated that lympho-myeloid progenitor populations in cord blood - lymphoid-primed multi-potential progenitors (LMPPs), granulocyte-macrophage progenitors (GMPs) and multi-lymphoid progenitors (MLPs) - were functionally and transcriptionally distinct and heterogeneous at the clonal level, with progenitors of many different functional potentials present. Although most progenitors had the potential to develop into only one mature cell type ('uni-lineage potential'), bi- and rarer multi-lineage progenitors were present among LMPPs, GMPs and MLPs. Those findings, coupled with single-cell expression analyses, suggest that a continuum of progenitors execute lymphoid and myeloid differentiation, rather than only uni-lineage progenitors' being present downstream of stem cells.

Published

2018

42. CD1a presentation of endogenous antigens by group 2 innate lymphoid cells.

Author

Hardman CS, Chen YL, Salimi M, Jarrett R, Johnson D, Järvinen VJ, Owens RJ, Repapi E, Cousins DJ, Barlow JL, McKenzie ANJ, and Ogg G

Subjects

Adult, Antigens, CD1 immunology, Biopsy, Cytokines genetics, Cytokines immunology, Dermatitis, Atopic immunology, Female, Group IV Phospholipases A2 genetics, Group IV Phospholipases A2 immunology, Human Experimentation, Humans, Inflammation immunology, Lipids immunology, Male, Signal Transduction immunology, Skin cytology, Skin immunology, Skin pathology, Staphylococcus aureus immunology, T-Lymphocytes immunology, Toll-Like Receptors immunology, Thymic Stromal Lymphopoietin, Antigen Presentation immunology, Antigens, CD1 genetics, Hypersensitivity, Immunity, Innate, Lymphocytes immunology

Abstract

Group 2 innate lymphoid cells (ILC2) are effectors of barrier immunity, with roles in infection, wound healing, and allergy. A proportion of ILC2 express MHCII (major histocompatibility complex II) and are capable of presenting peptide antigens to T cells and amplifying the subsequent adaptive immune response. Recent studies have highlighted the importance of CD1a-reactive T cells in allergy and infection, activated by the presentation of endogenous neolipid antigens and bacterial components. Using a human skin challenge model, we unexpectedly show that human skin-derived ILC2 can express CD1a and are capable of presenting endogenous antigens to T cells. CD1a expression is up-regulated by TSLP (thymic stromal lymphopoietin) at levels observed in the skin of patients with atopic dermatitis, and the response is dependent on PLA2G4A. Furthermore, this pathway is used to sense Staphylococcus aureus by promoting Toll-like receptor-dependent CD1a-reactive T cell responses to endogenous ligands. These findings define a previously unrecognized role for ILC2 in lipid surveillance and identify shared pathways of CD1a- and PLA2G4A-dependent ILC2 inflammation amenable to therapeutic intervention., (Copyright © 2017 The Authors, some rights reserved; exclusive licensee American Association for the Advancement of Science. No claim to original U.S. Government Works.)

Published

2017

43. Hepcidin is regulated by promoter-associated histone acetylation and HDAC3.

Author

Pasricha SR, Lim PJ, Duarte TL, Casu C, Oosterhuis D, Mleczko-Sanecka K, Suciu M, Da Silva AR, Al-Hourani K, Arezes J, McHugh K, Gooding S, Frost JN, Wray K, Santos A, Porto G, Repapi E, Gray N, Draper SJ, Ashley N, Soilleux E, Olinga P, Muckenthaler MU, Hughes JR, Rivella S, Milne TA, Armitage AE, and Drakesmith H

Subjects

Acetylation, Amino Acid Motifs, Animals, Epigenesis, Genetic, Erythropoietin genetics, Erythropoietin metabolism, Hepcidins metabolism, Histone Deacetylases genetics, Histones chemistry, Humans, Iron Deficiencies, Male, Mice, Inbred C57BL, Promoter Regions, Genetic, Gene Expression Regulation, Hepcidins genetics, Histone Deacetylases metabolism, Histones metabolism

Abstract

Hepcidin regulates systemic iron homeostasis. Suppression of hepcidin expression occurs physiologically in iron deficiency and increased erythropoiesis but is pathologic in thalassemia and hemochromatosis. Here we show that epigenetic events govern hepcidin expression. Erythropoiesis and iron deficiency suppress hepcidin via erythroferrone-dependent and -independent mechanisms, respectively, in vivo, but both involve reversible loss of H3K9ac and H3K4me3 at the hepcidin locus. In vitro, pan-histone deacetylase inhibition elevates hepcidin expression, and in vivo maintains H3K9ac at hepcidin-associated chromatin and abrogates hepcidin suppression by erythropoietin, iron deficiency, thalassemia, and hemochromatosis. Histone deacetylase 3 and its cofactor NCOR1 regulate hepcidin; histone deacetylase 3 binds chromatin at the hepcidin locus, and histone deacetylase 3 knockdown counteracts hepcidin suppression induced either by erythroferrone or by inhibiting bone morphogenetic protein signaling. In iron deficient mice, the histone deacetylase 3 inhibitor RGFP966 increases hepcidin, and RNA sequencing confirms hepcidin is one of the genes most differentially regulated by this drug in vivo. We conclude that suppression of hepcidin expression involves epigenetic regulation by histone deacetylase 3.Hepcidin controls systemic iron levels by inhibiting intestinal iron absorption and iron recycling. Here, Pasricha et al. demonstrate that the hepcidin-chromatin locus displays HDAC3-mediated reversible epigenetic modifications during both erythropoiesis and iron deficiency.

Published

2017

44. The U2AF1S34F mutation induces lineage-specific splicing alterations in myelodysplastic syndromes.

Author

Yip BH, Steeples V, Repapi E, Armstrong RN, Llorian M, Roy S, Shaw J, Dolatshad H, Taylor S, Verma A, Bartenstein M, Vyas P, Cross NC, Malcovati L, Cazzola M, Hellström-Lindberg E, Ogawa S, Smith CW, Pellagatti A, and Boultwood J

Published

2017

45. Niche-mediated depletion of the normal hematopoietic stem cell reservoir by Flt3-ITD-induced myeloproliferation.

Author

Mead AJ, Neo WH, Barkas N, Matsuoka S, Giustacchini A, Facchini R, Thongjuea S, Jamieson L, Booth CAG, Fordham N, Di Genua C, Atkinson D, Chowdhury O, Repapi E, Gray N, Kharazi S, Clark SA, Bouriez T, Woll P, Suda T, Nerlov C, and Jacobsen SEW

Subjects

Animals, Anti-Inflammatory Agents, Non-Steroidal pharmacology, Bone Marrow Cells drug effects, Bone Marrow Cells metabolism, Bone Marrow Transplantation, Cells, Cultured, Etanercept pharmacology, Gene Expression Profiling methods, Hematopoietic Stem Cells drug effects, Mesenchymal Stem Cells drug effects, Mesenchymal Stem Cells metabolism, Mice, Inbred C57BL, Mice, Transgenic, Reverse Transcriptase Polymerase Chain Reaction, Single-Cell Analysis methods, Tandem Repeat Sequences genetics, Tumor Necrosis Factor-alpha antagonists & inhibitors, Tumor Necrosis Factor-alpha genetics, Tumor Necrosis Factor-alpha metabolism, Cell Proliferation genetics, Hematopoietic Stem Cells metabolism, Mutation, Stem Cell Niche genetics, fms-Like Tyrosine Kinase 3 genetics

Abstract

Although previous studies suggested that the expression of FMS-like tyrosine kinase 3 (Flt3) initiates downstream of mouse hematopoietic stem cells (HSCs), FLT3 internal tandem duplications ( FLT3 ITDs) have recently been suggested to intrinsically suppress HSCs. Herein, single-cell interrogation found Flt3 mRNA expression to be absent in the large majority of phenotypic HSCs, with a strong negative correlation between Flt3 and HSC-associated gene expression. Flt3-ITD knock-in mice showed reduced numbers of phenotypic HSCs, with an even more severe loss of long-term repopulating HSCs, likely reflecting the presence of non-HSCs within the phenotypic HSC compartment. Competitive transplantation experiments established that Flt3-ITD compromises HSCs through an extrinsically mediated mechanism of disrupting HSC-supporting bone marrow stromal cells, with reduced numbers of endothelial and mesenchymal stromal cells showing increased inflammation-associated gene expression. Tumor necrosis factor (TNF), a cell-extrinsic potent negative regulator of HSCs, was overexpressed in bone marrow niche cells from FLT3-ITD mice, and anti-TNF treatment partially rescued the HSC phenotype. These findings, which establish that Flt3-ITD-driven myeloproliferation results in cell-extrinsic suppression of the normal HSC reservoir, are of relevance for several aspects of acute myeloid leukemia biology., (© 2017 Mead et al.)

Published

2017

46. MLL-AF4 binds directly to a BCL-2 specific enhancer and modulates H3K27 acetylation.

Author

Godfrey L, Kerry J, Thorne R, Repapi E, Davies JO, Tapia M, Ballabio E, Hughes JR, Geng H, Konopleva M, and Milne TA

Subjects

Acetylation, Bcl-2-Like Protein 11 metabolism, Cell Cycle Proteins metabolism, Cell Line, Tumor, Chromatin Immunoprecipitation, Gene Expression Profiling, Gene Expression Regulation, Leukemic, High-Throughput Nucleotide Sequencing, Humans, Myeloid Cell Leukemia Sequence 1 Protein genetics, Polycomb Repressive Complex 1 metabolism, Promoter Regions, Genetic, Protein Binding, Translocation, Genetic, Enhancer Elements, Genetic, Histones metabolism, Myeloid-Lymphoid Leukemia Protein metabolism, Oncogene Proteins, Fusion metabolism, Proto-Oncogene Proteins c-bcl-2 metabolism

Abstract

Survival rates for children and adults carrying mutations in the Mixed Lineage Leukemia (MLL) gene continue to have a very poor prognosis. The most common MLL mutation in acute lymphoblastic leukemia is the t(4;11)(q21;q23) chromosome translocation that fuses MLL in-frame with the AF4 gene producing MLL-AF4 and AF4-MLL fusion proteins. Previously, we found that MLL-AF4 binds to the BCL-2 gene and directly activates it through DOT1L recruitment and increased H3K79me2/3 levels. In the study described here, we performed a detailed analysis of MLL-AF4 regulation of the entire BCL-2 family. By measuring nascent RNA production in MLL-AF4 knockdowns, we found that of all the BCL-2 family genes, MLL-AF4 directly controls the active transcription of both BCL-2 and MCL-1 and also represses BIM via binding of the polycomb group repressor 1 (PRC1) complex component CBX8. We further analyzed MLL-AF4 activation of the BCL-2 gene using Capture-C and identified a BCL-2-specific enhancer, consisting of two clusters of H3K27Ac at the 3' end of the gene. Loss of MLL-AF4 activity results in a reduction of H3K79me3 levels in the gene body and H3K27Ac levels at the 3' BCL-2 enhancer, revealing a novel regulatory link between these two histone marks and MLL-AF4-mediated activation of BCL-2., (Copyright © 2016 ISEH - International Society for Experimental Hematology. Published by Elsevier Inc. All rights reserved.)

Published

2017

47. MLL-AF4 Spreading Identifies Binding Sites that Are Distinct from Super-Enhancers and that Govern Sensitivity to DOT1L Inhibition in Leukemia.

Author

Kerry J, Godfrey L, Repapi E, Tapia M, Blackledge NP, Ma H, Ballabio E, O'Byrne S, Ponthan F, Heidenreich O, Roy A, Roberts I, Konopleva M, Klose RJ, Geng H, and Milne TA

Subjects

Binding Sites, Cell Line, Tumor, CpG Islands genetics, DNA Methylation genetics, Gene Expression Regulation, Leukemic, Genome, Human, Histone-Lysine N-Methyltransferase, Histones metabolism, Humans, Intercellular Signaling Peptides and Proteins metabolism, Lysine metabolism, Methyltransferases metabolism, Prognosis, Protein Binding, Proto-Oncogene Proteins metabolism, Enhancer Elements, Genetic genetics, Leukemia genetics, Leukemia pathology, Methyltransferases antagonists & inhibitors, Myeloid-Lymphoid Leukemia Protein metabolism, Oncogene Proteins, Fusion metabolism

Abstract

Understanding the underlying molecular mechanisms of defined cancers is crucial for effective personalized therapies. Translocations of the mixed-lineage leukemia (MLL) gene produce fusion proteins such as MLL-AF4 that disrupt epigenetic pathways and cause poor-prognosis leukemias. Here, we find that at a subset of gene targets, MLL-AF4 binding spreads into the gene body and is associated with the spreading of Menin binding, increased transcription, increased H3K79 methylation (H3K79me2/3), a disruption of normal H3K36me3 patterns, and unmethylated CpG regions in the gene body. Compared to other H3K79me2/3 marked genes, MLL-AF4 spreading gene expression is downregulated by inhibitors of the H3K79 methyltransferase DOT1L. This sensitivity mediates synergistic interactions with additional targeted drug treatments. Therefore, epigenetic spreading and enhanced susceptibility to epidrugs provides a potential marker for better understanding combination therapies in humans., (Copyright © 2017 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2017

48. CTAS: a CT score to quantify disease activity in pulmonary sarcoidosis.

Author

Benamore R, Kendrick YR, Repapi E, Helm E, Cole SL, Taylor S, and Ho LP

Subjects

Adult, Aged, Female, Humans, Male, Middle Aged, Tomography, X-Ray Computed methods, Vital Capacity physiology, Young Adult, Sarcoidosis, Pulmonary diagnostic imaging, Severity of Illness Index

Abstract

Background: A major gap in the management of sarcoidosis is the lack of accessible and objective methods to measure disease activity. Since 90% of patients have pulmonary involvement, we explored if a disease activity score based on thoracic CT scans could address this clinical issue., Methods: High-resolution CT scans from 100 consecutive patients with sarcoidosis at a regional sarcoidosis service were scored for extent of CT abnormalities known to relate to granuloma or lymphocytic infiltration from published CT-pathological studies. These individual abnormality scores were then correlated against serum ACE, sIL-2R and change in FVC to identify CT abnormalities that reflect contemporaneous disease activity. The sum of these scores, or CT A ctivity S core (CTAS), was then validated against FVC response to treatment., Findings: CT extent scores for nodularity, ground-glass opacification, interlobular septal thickening and consolidation correlated significantly with at least one of the disease activity parameters and were used to form CTAS. CTAS was found to predict FVC response to treatment at 1 year and was highly reproducible between radiologists. An abbreviated CTAS (aCTAS), constructed from presence or absence of the four CT abnormalities, also showed significant correlation with FVC response to treatment. CTAS and aCTAS also correlated with response to treatment in the fibrotic subgroup., Interpretation: CTAS provides a concept for an objective and reproducible CT scoring method to quantify disease activity in sarcoidosis. The score can potentially be used to stratify patients according to disease activity, determine response to treatment and establish if fibrotic sarcoidosis is active., Competing Interests: Competing interests: None declared., (Published by the BMJ Publishing Group Limited. For permission to use (where not already granted under a licence) please go to http://www.bmj.com/company/products-services/rights-and-licensing/.)

Published

2016

49. Transforming Growth Factor β Drives Hemogenic Endothelium Programming and the Transition to Hematopoietic Stem Cells.

Author

Monteiro R, Pinheiro P, Joseph N, Peterkin T, Koth J, Repapi E, Bonkhofer F, Kirmizitas A, and Patient R

Subjects

Animals, Animals, Genetically Modified, Cell Differentiation, Core Binding Factor Alpha 2 Subunit genetics, Epithelial-Mesenchymal Transition, Jagged-1 Protein biosynthesis, Jagged-1 Protein genetics, Morpholinos genetics, Multipotent Stem Cells cytology, Notochord embryology, Signal Transduction, Transforming Growth Factor beta1 genetics, Transforming Growth Factor beta2 genetics, Transforming Growth Factor beta3 genetics, Vascular Endothelial Growth Factor A metabolism, Zebrafish Proteins biosynthesis, Zebrafish Proteins genetics, Zebrafish Proteins metabolism, Endothelium, Vascular embryology, Hematopoietic Stem Cells cytology, Transforming Growth Factor beta1 metabolism, Transforming Growth Factor beta2 metabolism, Transforming Growth Factor beta3 metabolism, Zebrafish embryology

Abstract

Hematopoietic stem cells (HSCs) are self-renewing multipotent stem cells that generate mature blood lineages throughout life. They, together with hematopoietic progenitor cells (collectively known as HSPCs), emerge from hemogenic endothelium in the floor of the embryonic dorsal aorta by an endothelial-to-hematopoietic transition (EHT). Here we demonstrate that transforming growth factor β (TGFβ) is required for HSPC specification and that it regulates the expression of the Notch ligand Jagged1a in endothelial cells prior to EHT, in a striking parallel with the epithelial-to-mesenchymal transition (EMT). The requirement for TGFβ is two fold and sequential: autocrine via Tgfβ1a and Tgfβ1b produced in the endothelial cells themselves, followed by a paracrine input of Tgfβ3 from the notochord, suggesting that the former programs the hemogenic endothelium and the latter drives EHT. Our findings have important implications for the generation of HSPCs from pluripotent cells in vitro., (Copyright © 2016 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2016

50. A Comprehensive Analysis of the Impact of HIV on HCV Immune Responses and Its Association with Liver Disease Progression in a Unique Plasma Donor Cohort.

Author

Zhang YH, Zhao Y, Rajapaksa US, Lawrence TM, Peng YC, Liu J, Xu K, Hu K, Qin L, Liu N, Sun H, Yan HP, Repapi E, Rowland-Jones S, Thimme R, McKeating JA, and Dong T

Subjects

Adult, Aged, Antibodies, Neutralizing immunology, Antiretroviral Therapy, Highly Active, Biomarkers, China epidemiology, Coinfection, Disease Progression, Female, HIV Infections complications, HIV Infections virology, HIV-1 genetics, Hepacivirus genetics, Hepatitis C complications, Hepatitis C virology, Hepatitis C Antibodies immunology, Humans, Interferon-gamma biosynthesis, Liver Cirrhosis etiology, Liver Cirrhosis pathology, Male, Middle Aged, T-Cell Antigen Receptor Specificity immunology, T-Lymphocyte Subsets immunology, T-Lymphocyte Subsets metabolism, Viral Load, Virus Replication, Blood Donors, HIV Infections epidemiology, HIV Infections immunology, HIV-1 immunology, Hepacivirus immunology, Hepatitis C epidemiology, Hepatitis C immunology, Liver Cirrhosis epidemiology

Abstract

Objective: Human Immunodeficiency Virus (HIV) and Hepatitis C virus (HCV) co-infection is recognized as a major cause of morbidity and mortality among HIV-1 infected patients. Our understanding of the impact of HIV infection on HCV specific immune responses and liver disease outcome is limited by the heterogeneous study populations with genetically diverse infecting viruses, varying duration of infection and anti-viral treatment., Methods: Viral-specific immune responses in a cohort of 151 HCV mono- and HIV co-infected former plasma donors infected with a narrow source of virus were studied. HCV and HIV specific T cell responses were correlated with clinical data., Results: HIV-1 accelerated liver disease progression and decreased HCV specific T cell immunity. The magnitude of HCV specific T cell responses inversely correlated with lower HCV RNA load and reduced liver injury as assessed by non-invasive markers of liver fibrosis. HIV co-infection reduced the frequency of HCV specific CD4+ T cells with no detectable effect on CD8+ T cells or neutralizing antibody levels., Conclusion: Our study highlights the impact of HIV co-infection on HCV specific CD4+ T cell responses in a unique cohort of patients for both HCV and HIV and suggests a crucial role for these cells in controlling chronic HCV replication and liver disease progression.

Published

2016