Your search keyword '"Grimes, H. Leighton"' showing total 29 results

1. Essential role of a ThPOK autoregulatory loop in the maintenance of mature CD4 + T cell identity and function.

Author

Basu J, Reis BS, Peri S, Zha J, Hua X, Ge L, Ferchen K, Nicolas E, Czyzewicz P, Cai KQ, Tan Y, Fuxman Bass JI, Walhout AJM, Grimes HL, Grivennikov SI, Mucida D, and Kappes DJ

Subjects

Animals, Cell Differentiation immunology, Colitis immunology, Colitis prevention & control, DNA-Binding Proteins genetics, Disease Models, Animal, Female, Intestinal Mucosa cytology, Intestinal Mucosa immunology, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, T-Lymphocytes, Helper-Inducer immunology, T-Lymphocytes, Regulatory immunology, Transcription Factors genetics, Transcription, Genetic genetics, DNA-Binding Proteins metabolism, Intraepithelial Lymphocytes cytology, T-Lymphocytes, Helper-Inducer cytology, T-Lymphocytes, Regulatory cytology, Transcription Factors metabolism

Abstract

The transcription factor ThPOK (encoded by the Zbtb7b gene) controls homeostasis and differentiation of mature helper T cells, while opposing their differentiation to CD4 + intraepithelial lymphocytes (IELs) in the intestinal mucosa. Thus CD4 IEL differentiation requires ThPOK transcriptional repression via reactivation of the ThPOK transcriptional silencer element (Sil ThPOK ). In the present study, we describe a new autoregulatory loop whereby ThPOK binds to the Sil ThPOK to maintain its own long-term expression in CD4 T cells. Disruption of this loop in vivo prevents persistent ThPOK expression, leads to genome-wide changes in chromatin accessibility and derepresses the colonic regulatory T (T reg ) cell gene expression signature. This promotes selective differentiation of naive CD4 T cells into GITR lo PD-1 lo CD25 lo (Triple lo ) T reg cells and conversion to CD4 + IELs in the gut, thereby providing dominant protection from colitis. Hence, the ThPOK autoregulatory loop represents a key mechanism to physiologically control ThPOK expression and T cell differentiation in the gut, with potential therapeutic relevance., (© 2021. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published

2021

2. Lsd1 as a therapeutic target in Gfi1-activated medulloblastoma.

Author

Lee C, Rudneva VA, Erkek S, Zapatka M, Chau LQ, Tacheva-Grigorova SK, Garancher A, Rusert JM, Aksoy O, Lea R, Mohammad HP, Wang J, Weiss WA, Grimes HL, Pfister SM, Northcott PA, and Wechsler-Reya RJ

Subjects

Animals, Antibiotics, Antineoplastic therapeutic use, Cell Proliferation drug effects, Cerebellar Neoplasms genetics, Cerebellar Neoplasms therapy, DNA-Binding Proteins genetics, Doxorubicin therapeutic use, Gene Expression Regulation, Neoplastic, HEK293 Cells, Histone Demethylases genetics, Humans, Medulloblastoma genetics, Medulloblastoma therapy, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, SCID, NIH 3T3 Cells, Neoplasm Transplantation, Oncogenic Viruses, Retroviridae, Transcription Factors genetics, Carcinogenesis drug effects, Cerebellar Neoplasms pathology, DNA-Binding Proteins metabolism, Histone Demethylases metabolism, Medulloblastoma pathology, Transcription Factors metabolism

Abstract

Drugs that modify the epigenome are powerful tools for treating cancer, but these drugs often have pleiotropic effects, and identifying patients who will benefit from them remains a major clinical challenge. Here we show that medulloblastomas driven by the transcription factor Gfi1 are exquisitely dependent on the enzyme lysine demethylase 1 (Kdm1a/Lsd1). We demonstrate that Lsd1 physically associates with Gfi1, and that these proteins cooperate to inhibit genes involved in neuronal commitment and differentiation. We also show that Lsd1 is essential for Gfi1-mediated transformation: Gfi1 proteins that cannot recruit Lsd1 are unable to drive tumorigenesis, and genetic ablation of Lsd1 markedly impairs tumor growth in vivo. Finally, pharmacological inhibitors of Lsd1 potently inhibit growth of Gfi1-driven tumors. These studies provide important insight into the mechanisms by which Gfi1 contributes to tumorigenesis, and identify Lsd1 inhibitors as promising therapeutic agents for Gfi1-driven medulloblastoma.

Published

2019

3. SKI controls MDS-associated chronic TGF-β signaling, aberrant splicing, and stem cell fitness.

Author

Muench DE, Ferchen K, Velu CS, Pradhan K, Chetal K, Chen X, Weirauch MT, Colmenares C, Verma A, Salomonis N, and Grimes HL

Subjects

DNA-Binding Proteins metabolism, Gene Expression Regulation, Hematopoietic Stem Cells metabolism, Humans, MicroRNAs genetics, MicroRNAs metabolism, Myelodysplastic Syndromes metabolism, Myelodysplastic Syndromes pathology, Proto-Oncogene Proteins metabolism, RNA, Messenger genetics, DNA-Binding Proteins genetics, Gene Deletion, Hematopoietic Stem Cells pathology, Myelodysplastic Syndromes genetics, Proto-Oncogene Proteins genetics, RNA Splicing, Signal Transduction, Transforming Growth Factor beta metabolism

Abstract

The transforming growth factor beta (TGF-β) signaling pathway controls hematopoietic stem cell (HSC) behavior in the marrow niche; however, TGF-β signaling becomes chronic in early-stage myelodysplastic syndrome (MDS). Although TGF-β signaling normally induces negative feedback, in early-stage MDS, high levels of microRNA-21 (miR-21) contribute to chronic TGF-β signaling. We found that a TGF-β signal-correlated gene signature is sufficient to identify an MDS patient population with abnormal RNA splicing (eg, CSF3R ) independent of splicing factor mutations and coincident with low HNRNPK activity. Levels of SKI messenger RNA (mRNA) encoding a TGF-β antagonist are sufficient to identify these patients. However, MDS patients with high SKI mRNA and chronic TGF-β signaling lack SKI protein because of miR-21 activity. To determine the impact of SKI loss, we examined murine Ski -/- HSC function. First, competitive HSC transplants revealed a profound defect in stem cell fitness (competitive disadvantage) but not specification, homing, or multilineage production. Aged recipients of Ski -/- HSCs exhibited mild phenotypes similar to phenotypes in those with macrocytic anemia. Second, blastocyst complementation revealed a dramatic block in Ski -/- hematopoiesis in the absence of transplantation. Similar to SKI- high MDS patient samples, Ski -/- HSCs strikingly upregulated TGF-β signaling and deregulated expression of spliceosome genes (including Hnrnpk ). Moreover, novel single-cell splicing analyses demonstrated that Ski -/- HSCs and high levels of SKI expression in MDS patient samples share abnormal alternative splicing of common genes (including those that encode splicing factors). We conclude that miR-21-mediated loss of SKI activates TGF-β signaling and alternative splicing to impair the competitive advantage of normal HSCs (fitness), which could contribute to selection of early-stage MDS-genic clones., (© 2018 by The American Society of Hematology.)

Published

2018

4. Obesity alters the long-term fitness of the hematopoietic stem cell compartment through modulation of Gfi1 expression.

Author

Lee JM, Govindarajah V, Goddard B, Hinge A, Muench DE, Filippi MD, Aronow B, Cancelas JA, Salomonis N, Grimes HL, and Reynaud D

Subjects

Animals, DNA-Binding Proteins deficiency, Disease Models, Animal, Gene Expression Regulation, Hematopoiesis genetics, Hematopoiesis physiology, Hematopoietic Stem Cell Transplantation, Hematopoietic Stem Cells pathology, Mice, Mice, Congenic, Mice, Inbred C57BL, Mice, Obese, Mice, Transgenic, Obesity pathology, Oxidative Stress, Transcription Factors deficiency, Up-Regulation, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Hematopoietic Stem Cells metabolism, Obesity genetics, Obesity metabolism, Transcription Factors genetics, Transcription Factors metabolism

Abstract

Obesity is a chronic organismal stress that disrupts multiple systemic and tissue-specific functions. In this study, we describe the impact of obesity on the activity of the hematopoietic stem cell (HSC) compartment. We show that obesity alters the composition of the HSC compartment and its activity in response to hematopoietic stress. The impact of obesity on HSC function is progressively acquired but persists after weight loss or transplantation into a normal environment. Mechanistically, we establish that the oxidative stress induced by obesity dysregulates the expression of the transcription factor Gfi1 and that increased Gfi1 expression is required for the abnormal HSC function induced by obesity. These results demonstrate that obesity produces durable changes in HSC function and phenotype and that elevation of Gfi1 expression in response to the oxidative environment is a key driver of the altered HSC properties observed in obesity. Altogether, these data provide phenotypic and mechanistic insight into durable hematopoietic dysregulations resulting from obesity., (© 2018 Lee et al.)

Published

2018

5. Enhancer hijacking activates GFI1 family oncogenes in medulloblastoma.

Author

Northcott PA, Lee C, Zichner T, Stütz AM, Erkek S, Kawauchi D, Shih DJ, Hovestadt V, Zapatka M, Sturm D, Jones DT, Kool M, Remke M, Cavalli FM, Zuyderduyn S, Bader GD, VandenBerg S, Esparza LA, Ryzhova M, Wang W, Wittmann A, Stark S, Sieber L, Seker-Cin H, Linke L, Kratochwil F, Jäger N, Buchhalter I, Imbusch CD, Zipprich G, Raeder B, Schmidt S, Diessl N, Wolf S, Wiemann S, Brors B, Lawerenz C, Eils J, Warnatz HJ, Risch T, Yaspo ML, Weber UD, Bartholomae CC, von Kalle C, Turányi E, Hauser P, Sanden E, Darabi A, Siesjö P, Sterba J, Zitterbart K, Sumerauer D, van Sluis P, Versteeg R, Volckmann R, Koster J, Schuhmann MU, Ebinger M, Grimes HL, Robinson GW, Gajjar A, Mynarek M, von Hoff K, Rutkowski S, Pietsch T, Scheurlen W, Felsberg J, Reifenberger G, Kulozik AE, von Deimling A, Witt O, Eils R, Gilbertson RJ, Korshunov A, Taylor MD, Lichter P, Korbel JO, Wechsler-Reya RJ, and Pfister SM

Subjects

Animals, Child, Chromosomes, Human, Pair 9 genetics, DNA-Binding Proteins metabolism, Humans, Medulloblastoma classification, Medulloblastoma pathology, Mice, Proto-Oncogene Proteins metabolism, Repressor Proteins metabolism, Transcription Factors metabolism, DNA-Binding Proteins genetics, Enhancer Elements, Genetic genetics, Genomic Structural Variation genetics, Medulloblastoma genetics, Oncogenes genetics, Proto-Oncogene Proteins genetics, Repressor Proteins genetics, Transcription Factors genetics

Abstract

Medulloblastoma is a highly malignant paediatric brain tumour currently treated with a combination of surgery, radiation and chemotherapy, posing a considerable burden of toxicity to the developing child. Genomics has illuminated the extensive intertumoral heterogeneity of medulloblastoma, identifying four distinct molecular subgroups. Group 3 and group 4 subgroup medulloblastomas account for most paediatric cases; yet, oncogenic drivers for these subtypes remain largely unidentified. Here we describe a series of prevalent, highly disparate genomic structural variants, restricted to groups 3 and 4, resulting in specific and mutually exclusive activation of the growth factor independent 1 family proto-oncogenes, GFI1 and GFI1B. Somatic structural variants juxtapose GFI1 or GFI1B coding sequences proximal to active enhancer elements, including super-enhancers, instigating oncogenic activity. Our results, supported by evidence from mouse models, identify GFI1 and GFI1B as prominent medulloblastoma oncogenes and implicate 'enhancer hijacking' as an efficient mechanism driving oncogene activation in a childhood cancer.

Published

2014

6. Growth factor independence 1 antagonizes a p53-induced DNA damage response pathway in lymphoblastic leukemia.

Author

Khandanpour C, Phelan JD, Vassen L, Schütte J, Chen R, Horman SR, Gaudreau MC, Krongold J, Zhu J, Paul WE, Dührsen U, Göttgens B, Grimes HL, and Möröy T

Subjects

Animals, Humans, Lymphoma, B-Cell genetics, Lymphoma, B-Cell mortality, Mice, Mice, Inbred C57BL, Mice, Knockout, Mutation genetics, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma genetics, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma mortality, Proto-Oncogene Proteins c-bcl-2 metabolism, Receptor, Notch1 genetics, Xenograft Model Antitumor Assays, Apoptosis, DNA Damage genetics, DNA-Binding Proteins physiology, Lymphoma, B-Cell pathology, Precursor T-Cell Lymphoblastic Leukemia-Lymphoma pathology, Transcription Factors physiology, Tumor Suppressor Protein p53 physiology

Abstract

Most patients with acute lymphoblastic leukemia (ALL) fail current treatments highlighting the need for better therapies. Because oncogenic signaling activates a p53-dependent DNA damage response and apoptosis, leukemic cells must devise appropriate countermeasures. We show here that growth factor independence 1 (Gfi1) can serve such a function because Gfi1 ablation exacerbates p53 responses and lowers the threshold for p53-induced cell death. Specifically, Gfi1 restricts p53 activity and expression of proapoptotic p53 targets such as Bax, Noxa (Pmaip1), and Puma (Bbc3). Subsequently, Gfi1 ablation cures mice from leukemia and limits the expansion of primary human T-ALL xenografts in mice. This suggests that targeting Gfi1 could improve the prognosis of patients with T-ALL or other lymphoid leukemias., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

7. Growth factor independent-1 maintains Notch1-dependent transcriptional programming of lymphoid precursors.

Author

Phelan JD, Saba I, Zeng H, Kosan C, Messer MS, Olsson HA, Fraszczak J, Hildeman DA, Aronow BJ, Möröy T, and Grimes HL

Subjects

Animals, Cell Lineage, Gene Expression Regulation, Leukemic immunology, Gene Regulatory Networks, Hematopoietic Stem Cells cytology, Hematopoietic Stem Cells metabolism, Humans, Lymphocytes cytology, Lymphocytes metabolism, Mice, T-Lymphocytes immunology, DNA-Binding Proteins genetics, Receptor, Notch1 genetics, Signal Transduction genetics, T-Lymphocytes cytology, Transcription Factors genetics

Abstract

Growth factor independent 1 (Gfi1) is a transcriptional repressor originally identified as a gene activated in T-cell leukemias induced by Moloney-murine-leukemia virus infection. Notch1 is a transmembrane receptor that is frequently mutated in human T-cell acute lymphoblastic leukemia (T-ALL). Gfi1 is an important factor in the initiation and maintenance of lymphoid leukemias and its deficiency significantly impedes Notch dependent initiation of T-ALL in animal models. Here, we show that immature hematopoietic cells require Gfi1 to competently integrate Notch-activated signaling. Notch1 activation coupled with Gfi1 deficiency early in T-lineage specification leads to a dramatic loss of T-cells, whereas activation in later stages leaves development unaffected. In Gfi1 deficient multipotent precursors, Notch activation induces lethality and is cell autonomous. Further, without Gfi1, multipotent progenitors do not maintain Notch1-activated global expression profiles typical for T-lineage precursors. In agreement with this, we find that both lymphoid-primed multipotent progenitors (LMPP) and early T lineage progenitors (ETP) do not properly form or function in Gfi1(-/-) mice. These defects correlate with an inability of Gfi1(-/-) progenitors to activate lymphoid genes, including IL7R, Rag1, Flt3 and Notch1. Our data indicate that Gfi1 is required for hematopoietic precursors to withstand Notch1 activation and to maintain Notch1 dependent transcriptional programming to determine early T-lymphoid lineage identity., Competing Interests: Dr. H. Leighton Grimes is an Associate Editor at PLOS Genetics. Otherwise, the authors have declared that no relevant competing interests exist.

Published

2013

8. The human GFI136N variant induces epigenetic changes at the Hoxa9 locus and accelerates K-RAS driven myeloproliferative disorder in mice.

Author

Khandanpour C, Krongold J, Schütte J, Bouwman F, Vassen L, Gaudreau MC, Chen R, Calero-Nieto FJ, Diamanti E, Hannah R, Meyer SE, Grimes HL, van der Reijden BA, Jansen JH, Patel CV, Peeters JK, Löwenberg B, Dührsen U, Göttgens B, and Möröy T

Subjects

Animals, Cluster Analysis, DNA-Binding Proteins metabolism, Gene Expression Profiling, Gene Expression Regulation, Genetic Predisposition to Disease, Hematopoiesis genetics, Histones metabolism, Humans, Mice, Mice, Transgenic, Myeloid Progenitor Cells metabolism, Myeloid Progenitor Cells pathology, Myeloproliferative Disorders metabolism, Myeloproliferative Disorders mortality, Proto-Oncogene Proteins p21(ras) metabolism, Transcription Factors metabolism, DNA-Binding Proteins genetics, Epigenesis, Genetic, Homeodomain Proteins genetics, Myeloproliferative Disorders genetics, Proto-Oncogene Proteins p21(ras) genetics, Transcription Factors genetics

Abstract

The coding single nucleotide polymorphism GFI136N in the human gene growth factor independence 1 (GFI1) is present in 3%-7% of whites and increases the risk for acute myeloid leukemia (AML) by 60%. We show here that GFI136N, in contrast to GFI136S, lacks the ability to bind to the Gfi1 target gene that encodes the leukemia-associated transcription factor Hoxa9 and fails to initiate histone modifications that regulate HoxA9 expression. Consistent with this, AML patients heterozygous for the GFI136N variant show increased HOXA9 expression compared with normal controls. Using ChipSeq, we demonstrate that GFI136N specific epigenetic changes are also present in other genes involved in the development of AML. Moreover, granulomonocytic progenitors, a bone marrow subset from which AML can arise in humans and mice, show a proliferative expansion in the presence of the GFI136N variant. In addition, granulomonocytic progenitors carrying the GFI136N variant allele have altered gene expression patterns and differ in their ability to grow after transplantation. Finally, GFI136N can accelerate a K-RAS driven fatal myeloproliferative disease in mice. Our data suggest that the presence of a GFI136N variant allele induces a preleukemic state in myeloid precursors by deregulating the expression of Hoxa9 and other AML-related genes.

Published

2012

9. Gfi1 expressed in bone marrow stromal cells is a novel osteoblast suppressor in patients with multiple myeloma bone disease.

Author

D'Souza S, del Prete D, Jin S, Sun Q, Huston AJ, Kostov FE, Sammut B, Hong CS, Anderson JL, Patrene KD, Yu S, Velu CS, Xiao G, Grimes HL, Roodman GD, and Galson DL

Subjects

3T3 Cells, Animals, Blotting, Western, Bone Marrow Cells metabolism, Bone Marrow Cells pathology, Bone Neoplasms genetics, Bone Neoplasms pathology, Cell Line, Tumor, Core Binding Factor Alpha 1 Subunit genetics, Core Binding Factor Alpha 1 Subunit metabolism, DNA-Binding Proteins genetics, Female, Gene Expression, Humans, Interleukin-7 metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, SCID, Multiple Myeloma genetics, Multiple Myeloma pathology, Osteoblasts pathology, RNA Interference, Reverse Transcriptase Polymerase Chain Reaction, Stromal Cells pathology, Transcription Factors genetics, Tumor Necrosis Factor-alpha metabolism, Bone Neoplasms metabolism, DNA-Binding Proteins metabolism, Multiple Myeloma metabolism, Osteoblasts metabolism, Stromal Cells metabolism, Transcription Factors metabolism

Abstract

Protracted inhibition of osteoblast (OB) differentiation characterizes multiple myeloma (MM) bone disease and persists even when patients are in long-term remission. However, the underlying pathophysiology for this prolonged OB suppression is unknown. Therefore, we developed a mouse MM model in which the bone marrow stromal cells (BMSCs) remained unresponsive to OB differentiation signals after removal of MM cells. We found that BMSCs from both MM-bearing mice and MM patients had increased levels of the transcriptional repressor Gfi1 compared with controls and that Gfi1 was a novel transcriptional repressor of the critical OB transcription factor Runx2. Trichostatin-A blocked the effects of Gfi1, suggesting that it induces epigenetic changes in the Runx2 promoter. MM-BMSC cell-cell contact was not required for MM cells to increase Gfi1 and repress Runx2 levels in MC-4 before OBs or naive primary BMSCs, and Gfi1 induction was blocked by anti-TNF-α and anti-IL-7 antibodies. Importantly, BMSCs isolated from Gfi1(-/-) mice were significantly resistant to MM-induced OB suppression. Strikingly, siRNA knockdown of Gfi1 in BMSCs from MM patients significantly restored expression of Runx2 and OB differentiation markers. Thus, Gfi1 may have an important role in prolonged MM-induced OB suppression and provide a new therapeutic target for MM bone disease.

Published

2011

10. Zinc finger protein Gfi1 controls the endotoxin-mediated Toll-like receptor inflammatory response by antagonizing NF-kappaB p65.

Author

Sharif-Askari E, Vassen L, Kosan C, Khandanpour C, Gaudreau MC, Heyd F, Okayama T, Jin J, Rojas ME, Grimes HL, Zeng H, and Möröy T

Subjects

Animals, Base Sequence, Cell Line, DNA genetics, DNA metabolism, DNA Primers genetics, DNA-Binding Proteins antagonists & inhibitors, DNA-Binding Proteins deficiency, DNA-Binding Proteins genetics, Humans, Immunity, Innate drug effects, Inflammation etiology, Lipopolysaccharides toxicity, Macrophages immunology, Macrophages metabolism, Mice, Mice, Inbred C57BL, Mice, Knockout, Promoter Regions, Genetic, RNA, Messenger genetics, RNA, Messenger metabolism, Shock, Septic etiology, Shock, Septic immunology, Shock, Septic metabolism, Signal Transduction, Transcription Factors antagonists & inhibitors, Transcription Factors deficiency, Transcription Factors genetics, Transcriptional Activation, Tumor Necrosis Factor-alpha genetics, Zinc Fingers, DNA-Binding Proteins metabolism, Inflammation immunology, Inflammation metabolism, Toll-Like Receptors metabolism, Transcription Factor RelA antagonists & inhibitors, Transcription Factors metabolism

Abstract

Endotoxin (bacterial lipopolysaccharide [LPS]) causes fatal septic shock via the Toll-like receptor 4 (TLR-4) protein present on innate immunity effector cells, which activates nuclear factor kappa B (NF-kappaB), inducing proinflammatory cytokines, including tumor necrosis factor alpha (TNF-alpha). An early step in this process involves nuclear sequestration of the p65-RelA NF-kappaB subunit, enabling transcriptional activation of target inflammatory cytokine genes. Here, we analyzed the role of the nuclear zinc finger protein Gfi1 in the TLR response using primary bone marrow-derived macrophages. We show that upon LPS stimulation, expression of Gfi1 is induced with kinetics similar to those of nuclear translocation of p65 and that Gfi1 interacts with p65 and inhibits p65-mediated transcriptional transactivation by interfering with p65 binding to target gene promoter DNA. Gfi1-deficient macrophages show abnormally high mRNA levels of the TNF-alpha gene and many other p65 target genes and a higher rate of TNF promoter occupancy by p65 than wild-type cells after LPS stimulation, suggesting that Gfi1 functions as an antagonist of NF-kappaB activity at the level of promoter binding. Our findings identify a new function of Gfi1 as a general negative regulator of the endotoxin-initiated innate immune responses, including septic shock and possibly other severe inflammatory diseases.

Published

2010

11. Gfi1-cells and circuits: unraveling transcriptional networks of development and disease.

Author

Phelan JD, Shroyer NF, Cook T, Gebelein B, and Grimes HL

Subjects

Animals, DNA-Binding Proteins genetics, Gene Regulatory Networks, Hematopoiesis genetics, Hematopoietic Stem Cells metabolism, Humans, Leukemia genetics, Leukemia physiopathology, Neutropenia genetics, Neutropenia physiopathology, Signal Transduction genetics, Transcription Factors genetics, DNA-Binding Proteins physiology, Hematopoiesis physiology, Hematopoietic Stem Cells physiology, Signal Transduction physiology, Transcription Factors physiology

Abstract

Purpose of Review: The review will integrate current knowledge of transcriptional circuits whose dysregulation leads to autoimmunity, neutropenia and leukemia., Recent Findings: Growth factor independent-1 (Gfi1) is a transcriptional repressor with essential roles in controlling hematopoietic stem cell biology, myeloid and lymphoid differentiation and lymphocyte effector functions. Recent work has suggested that Gfi1 competes or collaborates with other transcription factors to modulate transcription programs and lineage decisions., Summary: Gfi1 is central to several transcriptional circuits whose dysregulation leads to abnormal or malignant hematopoiesis. These functional relationships are conserved from Drosophila development. Such conserved pathways represent central oncogenic or 'gatekeeper' pathways that are pivotal to understanding the process of cellular transformation, and illustrate key targets for clinical intervention.

Published

2010

12. Contributions to neutropenia from PFAAP5 (N4BP2L2), a novel protein mediating transcriptional repressor cooperation between Gfi1 and neutrophil elastase.

Author

Salipante SJ, Rojas ME, Korkmaz B, Duan Z, Wechsler J, Benson KF, Person RE, Grimes HL, and Horwitz MS

Subjects

Animals, Carrier Proteins genetics, Carrier Proteins metabolism, Cell Differentiation, Cell Proliferation, Chromatin Immunoprecipitation, Genes, Reporter, HL-60 Cells, Hematopoietic Stem Cells cytology, Hematopoietic Stem Cells physiology, Humans, Leukocyte Elastase genetics, Neutropenia genetics, RNA, Small Interfering genetics, RNA, Small Interfering metabolism, Repressor Proteins genetics, Transcription, Genetic, Tumor Suppressor Proteins genetics, Tumor Suppressor Proteins metabolism, Two-Hybrid System Techniques, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Gene Expression Regulation, Leukocyte Elastase metabolism, Neutropenia metabolism, Repressor Proteins metabolism, Transcription Factors genetics, Transcription Factors metabolism

Abstract

"Neutropenia" refers to deficient numbers of neutrophils, the most abundant type of white blood cell. Two main forms of inherited neutropenia are cyclic neutropenia, in which neutrophil counts oscillate with a 21-day frequency, and severe congenital neutropenia, in which static neutropenia may evolve at times into leukemia. Mutations of ELA2, encoding the protease neutrophil elastase, can cause both disorders. Among other genes, severe congenital neutropenia can also result from mutations affecting the transcriptional repressor Gfi1, one of whose genetic targets is ELA2, suggesting that the two act through similar mechanisms. In order to identify components of a common pathway regulating neutrophil production, we conducted yeast two-hybrid screens with Gfi1 and neutrophil elastase and detected a novel protein, PFAAP5 (also known as N4BP2L2), interacting with both. Expression of PFAAP5 allows neutrophil elastase to potentiate the repression of Gfi1 target genes, as determined by reporter assays, RNA interference, chromatin immunoprecipitation, and impairment of neutrophil differentiation in HSCs with PFAAP5 depletion, thus delineating a mechanism through which neutrophil elastase could regulate its own synthesis. Our findings are consistent with theoretical models of cyclic neutropenia proposing that its periodicity can be explained through disturbance of a feedback circuit in which mature neutrophils inhibit cell proliferation, thereby homeostatically regulating progenitor populations.

Published

2009

13. Gfi1 integrates progenitor versus granulocytic transcriptional programming.

Author

Horman SR, Velu CS, Chaubey A, Bourdeau T, Zhu J, Paul WE, Gebelein B, and Grimes HL

Subjects

Animals, Cell Differentiation genetics, Cells, Cultured, DNA-Binding Proteins genetics, Embryonic Development genetics, Gene Expression Regulation, Developmental, Genetic Predisposition to Disease, Granulocyte Precursor Cells metabolism, Granulocytes metabolism, Homeodomain Proteins genetics, Homeodomain Proteins metabolism, Leukemia genetics, Mice, Mice, Inbred C57BL, Mice, Knockout, Myeloid Ecotropic Viral Integration Site 1 Protein, Neoplasm Proteins genetics, Neoplasm Proteins metabolism, Pre-B-Cell Leukemia Transcription Factor 1, Transcription Factors genetics, Transcription Factors metabolism, Transcription, Genetic physiology, DNA-Binding Proteins physiology, Granulocyte Precursor Cells physiology, Granulocytes physiology, Transcription Factors physiology

Abstract

In patients with severe congenital neutropenia (SCN) and mice with growth factor independent-1 (Gfi1) loss of function, arrested myeloid progenitors accumulate, whereas terminal granulopoiesis is blocked. One might assume that Gfi-null progenitors accumulate because they lack the ability to differentiate. Instead, our data indicate that Gfi1 loss of function deregulates 2 separable transcriptional programs, one of which controls the accumulation and lineage specification of myeloid progenitors, but not terminal granulopoiesis. We demonstrate that Gfi1 directly represses HoxA9, Pbx1, and Meis1 during normal myelopoiesis. Gfi1-/- progenitors exhibit elevated levels of HoxA9, Pbx1 and Meis1, exaggerated HoxA9-Pbx1-Meis1 activity, and progenitor transformation in collaboration with oncogenic K-Ras. Limiting HoxA9 alleles corrects, in a dose-dependent manner, in vivo and in vitro phenotypes observed with loss of Gfi1 in myeloid progenitor cells but did not rescue Gfi1-/- blocked granulopoiesis. Thus, Gfi1 integrates 2 events during normal myeloid differentiation; the suppression of a HoxA9-Pbx1-Meis1 progenitor program and the induction of a granulopoietic transcription program.

Published

2009

14. Gfi1 regulates miR-21 and miR-196b to control myelopoiesis.

Author

Velu CS, Baktula AM, and Grimes HL

Subjects

Animals, Bone Marrow Transplantation, Chromatin Immunoprecipitation, Colony-Forming Units Assay, Electrophoretic Mobility Shift Assay, Female, Flow Cytometry, Gene Expression Profiling, Granulocyte Colony-Stimulating Factor pharmacology, Granulocytes cytology, Granulocytes physiology, Hematopoietic Stem Cells, Immunoblotting, Male, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Mice, Knockout, MicroRNAs physiology, Oligonucleotide Array Sequence Analysis, RNA, Small Interfering pharmacology, Bone Marrow physiology, DNA-Binding Proteins physiology, MicroRNAs genetics, Myelopoiesis physiology, Transcription Factors physiology

Abstract

The zinc finger protein growth factor independent-1 (Gfi1) is a transcriptional repressor that is critically required for normal granulocytic differentiation. GFI1 loss-of-function mutations are found in some patients with severe congenital neutropenia (SCN). The SCN-associated GFI1-mutant proteins act as dominant negatives to block granulopoiesis through selective deregulation of a subset of GFI1 target genes. Here we show that Gfi1 is a master regulator of microRNAs, and that deregulated expression of these microRNAs recapitulates a Gfi1 loss-of-function block to granulocyte colony-stimulating factor (G-CSF)-stimulated granulopoiesis. Specifically, bone marrow cells from a GFI1-mutant SCN patient and Gfi1(-/-) mice display deregulated expression of miR-21 and miR-196B expression. Flow cytometric analysis and colony assays reveal that the overexpression or depletion of either miR induces changes in myeloid development. However, coexpression of miR-21 and miR-196b (as seen in Gfi1(-/-) mice and a GFI1N382S SCN patient) completely blocks G-CSF-induced granulopoiesis. Thus, our results not only identify microRNAs whose regulation is required during myelopoiesis, but also provide an example of synergy in microRNA biologic activity and illustrate potential mechanisms underlying SCN disease pathogenesis.

Published

2009

15. Ajuba functions as a histone deacetylase-dependent co-repressor for autoregulation of the growth factor-independent-1 transcription factor.

Author

Montoya-Durango DE, Velu CS, Kazanjian A, Rojas ME, Jay CM, Longmore GD, and Grimes HL

Subjects

Cell Line, Cell Survival, DNA-Binding Proteins genetics, Homeodomain Proteins genetics, Humans, LIM Domain Proteins, Protein Binding, Transcription Factors genetics, DNA-Binding Proteins metabolism, Down-Regulation, Histone Deacetylases metabolism, Homeodomain Proteins metabolism, Transcription Factors metabolism

Abstract

Growth factor independent-1 (Gfi1) is a zinc finger protein with a SNAG-transcriptional repressor domain. Ajuba is a LIM domain protein that shuttles between the cytoplasm and the nucleus. Ajuba functions as a co-repressor for synthetic Gfi1 SNAG-repressor domain-containing constructs, but a role for Ajuba co-repression of the cognate DNA bound Gfi1 protein has not been defined. Co-immunoprecipitation of synthetic and endogenous proteins and co-elution with gel filtration suggest that an endogenous Ajuba.Gfi1.HDAC multiprotein complex is possible. Active histone deacetylase activity co-immunoprecipitates with Ajuba or Gfi1, and both proteins depend upon histone deacetylases for full transcriptional repression activity. Ajuba LIM domains directly bind to Gfi1, but the association is not SNAG domain-dependent. ChIP analysis and reciprocal knockdown experiments suggest that Ajuba selectively functions as a co-repressor for Gfi1 autoregulation. The data suggest that Ajuba is utilized as a corepressor selectively on Gfi1 target genes.

Published

2008

16. Mutations in growth factor independent-1 associated with human neutropenia block murine granulopoiesis through colony stimulating factor-1.

Author

Zarebski A, Velu CS, Baktula AM, Bourdeau T, Horman SR, Basu S, Bertolone SJ, Horwitz M, Hildeman DA, Trent JO, and Grimes HL

Subjects

Animals, Cell Differentiation genetics, Cell Lineage, Electrophoretic Mobility Shift Assay, Flow Cytometry, Hematopoietic Stem Cells cytology, Humans, Immunoblotting, Immunoprecipitation, Mice, Mutation, Neutropenia congenital, Reverse Transcriptase Polymerase Chain Reaction, Transcription, Genetic, DNA-Binding Proteins genetics, Granulocytes cytology, Hematopoiesis genetics, Macrophage Colony-Stimulating Factor metabolism, Neutropenia genetics, Transcription Factors genetics

Abstract

Severe congenital neutropenia (SCN) is characterized by a deficiency of mature neutrophils, leading to recurrent bacterial and fungal infections. Although mutations in Elastase-2, neutrophil (ELA2) predominate in human SCN, mutation of Ela2 in mice does not recapitulate SCN. The growth factor independent-1 (GFI1) transcription factor regulates ELA2. Mutations in GFI1 are associated with human SCN, and genetic deletion of Gfi1 results in murine neutropenia. We examined whether human SCN-associated GFI1N382S mutant proteins are causal in SCN and found that GFI1 functions as a rate-limiting granulopoietic molecular switch. The N382S mutation inhibited GFI1 DNA binding and resulted in a dominant-negative block to murine granulopoiesis. Moreover, Gfi1N382S selectively derepressed the monopoietic cytokine CSF1 and its receptor. Gfi1N382S-expressing Csf1-/- cells formed neutrophils. These results reveal a common transcriptional program that underlies both human and murine myelopoiesis, and that is central to the pathogenesis of SCN associated with mutations in GFI1. This shared transcriptional pathway may provide new avenues for understanding SCN caused by mutations in other genes and for clinical intervention into human neutropenias.

Published

2008

17. Epigenetic regulation of protein-coding and microRNA genes by the Gfi1-interacting tumor suppressor PRDM5.

Author

Duan Z, Person RE, Lee HH, Huang S, Donadieu J, Badolato R, Grimes HL, Papayannopoulou T, and Horwitz MS

Subjects

Cell Cycle physiology, Cell Line, DNA-Binding Proteins genetics, Hematopoiesis physiology, Histone Deacetylase 1, Histone Deacetylases genetics, Histone Deacetylases metabolism, Histone Methyltransferases, Histone-Lysine N-Methyltransferase metabolism, Humans, MicroRNAs metabolism, Molecular Sequence Data, Neutropenia genetics, Neutropenia metabolism, Promoter Regions, Genetic, Protein Methyltransferases, RNA Interference, Transcription Factors genetics, Transcription, Genetic, Two-Hybrid System Techniques, Zinc Fingers, DNA-Binding Proteins metabolism, Epigenesis, Genetic, Gene Expression Regulation, MicroRNAs genetics, Transcription Factors metabolism

Abstract

Gfi1 transcriptionally governs hematopoiesis, and its mutations produce neutropenia. In an effort to identify Gfi1-interacting proteins and also to generate new candidate genes causing neutropenia, we performed a yeast two-hybrid screen with Gfi1. Among other Gfi1-interacting proteins, we identified a previously uncharacterized member of the PR domain-containing family of tumor suppressors, PRDM5. PRDM5 has 16 zinc fingers, and we show that it acts as a sequence-specific, DNA binding transcription factor that targets hematopoiesis-associated protein-coding and microRNA genes, including many that are also targets of Gfi1. PRDM5 epigenetically regulates transcription similarly to Gfi1: it recruits the histone methyltransferase G9a and class I histone deacetylases to its target gene promoters and demonstrates repressor activity on synthetic reporters; on endogenous target genes, however, it functions as an activator, in addition to a repressor. Interestingly, genes that PRDM5 activates, as opposed to those it represses, are also targets of Gfi1, suggesting a competitive mechanism through which two repressors could cooperate in order to become transcriptional activators. In neutropenic patients, we identified PRDM5 protein sequence variants perturbing transcriptional function, suggesting a potentially important role in hematopoiesis.

Published

2007

18. Loss of GFI1 impairs pulmonary neuroendorine cell proliferation, but the neuroendocrine phenotype has limited impact on post-naphthalene airway repair.

Author

Linnoila RI, Jensen-Taubman S, Kazanjian A, and Grimes HL

Subjects

Animals, Apoptosis, Carcinoma, Small Cell chemically induced, Cell Differentiation, DNA-Binding Proteins genetics, Lung Neoplasms chemically induced, Mice, Mice, Knockout, Phenotype, Regeneration, Respiratory Mucosa pathology, Stem Cells cytology, Transcription Factors genetics, Carcinoma, Small Cell pathology, Cell Proliferation drug effects, DNA-Binding Proteins physiology, Environmental Pollutants toxicity, Lung pathology, Lung Neoplasms pathology, Naphthalenes toxicity, Neurosecretory Systems pathology, Transcription Factors physiology

Abstract

Naphthalene exposure kills lung airway epithelial (Clara) cells, but is rapidly followed by Clara cell reconstitution coincident with proliferation of pulmonary neuroendocrine cells (PNEC). Although a role for mature PNEC in the reconstitution process has been excluded, the reconstituting progenitor cells have been suggested to enter a transient neuroendocrine (NE) differentiation phase before differentiating to Clara cells. Furthermore, these progenitors were suggested to be the target population for transformation to a NE tumor; small cell lung cancer (SCLC). Although the NE phenotype is central to SCLC oncogenesis, the relevance of NE differentiation to post naphthalene reconstitution remains to be determined. The Growth factor independent-1 (Gfi1) transcription factor is expressed in SCLC and is required for the NE differentiation of PNEC. Gfi1(-/-) mice display a 70% reduction in airway cells that express NE markers, and cells that stain for NE markers show weak expression of some markers. Therefore, to determine the relevance of the NE phenotype to post-naphthalene reconstitution, we examined post-naphthalene reconstitution in Gfi1(-/-) mice. Our analyses indicate that the post-naphthalene regeneration process includes both airway epithelial proliferation and apoptosis. Gfi1 deletion lowered both airway epithelial proliferation and apoptosis; however, the post-naphthalene rate of increase in growth and apoptosis was not significantly different between Gfi1(-/-) mice and wild-type littermates. Moreover, the timing and extent of CC10+ cell regeneration was unaffected by Gfi1 deletion. These data suggest that neither Gfi1 nor the NE phenotype play a dominant role in the regeneration process. However, the few Gfi1(-/-) cells capable of NE differentiation show a significant reduction in post-naphthalene proliferation. The modest proliferation seen in Gfi1(-/-) NE cells is consistent with the previously proposed role for Gfi1 in controlling neuroendocrine cancer growth.

Published

2007

19. The growth factor independence-1 transcription factor: new functions and new insights.

Author

Kazanjian A, Gross EA, and Grimes HL

Subjects

Animals, DNA-Binding Proteins genetics, Hematopoiesis genetics, Humans, Mice, Neurons, Afferent metabolism, Neurosecretory Systems metabolism, Neutropenia genetics, Neutropenia metabolism, Oncogene Proteins genetics, Organ Specificity, Transcription Factors genetics, Tumor Suppressor Proteins genetics, DNA-Binding Proteins metabolism, Oncogene Proteins metabolism, Transcription Factors metabolism, Tumor Suppressor Proteins metabolism

Abstract

The growth factor independence-1 (Gfi1) transcription factor is required for proper development of neuroendocrine cells, sensory neurons, and blood. Patients with mutations in Gfi1 exhibit severe congenital neutropenia (SCN) or non-immune chronic idiopathic neutropenia of adults. Gfi1 was initially described as an oncoprotein that mediates tumor progression in a mouse model of leukemia; however, recent data suggest that Gfi1 may act as either an oncogene or an anti-proliferative tumor suppressor gene depending on the cell type. Here we review the latest literature on Gfi1, and emphasize its role in the hematopoietic, sensory and neuroendocrine systems.

Published

2006

20. Gfi1 coordinates epigenetic repression of p21Cip/WAF1 by recruitment of histone lysine methyltransferase G9a and histone deacetylase 1.

Author

Duan Z, Zarebski A, Montoya-Durango D, Grimes HL, and Horwitz M

Subjects

Cell Line, Tumor, Cell Proliferation, Cyclin-Dependent Kinase Inhibitor p21 biosynthesis, Cyclin-Dependent Kinase Inhibitor p21 metabolism, DNA-Binding Proteins genetics, Histocompatibility Antigens genetics, Histone Deacetylase 1, Histone Deacetylases genetics, Histone-Lysine N-Methyltransferase genetics, Histones metabolism, Humans, Methylation, Promoter Regions, Genetic genetics, Protein Binding, Repressor Proteins genetics, Transcription Factors genetics, Transcription, Genetic genetics, Cyclin-Dependent Kinase Inhibitor p21 genetics, DNA-Binding Proteins metabolism, Epigenesis, Genetic, Histocompatibility Antigens metabolism, Histone Deacetylases metabolism, Histone-Lysine N-Methyltransferase metabolism, Repressor Proteins metabolism, Transcription Factors metabolism

Abstract

The growth factor independent 1 (Gfi1) transcriptional regulator oncoprotein plays a crucial role in hematopoietic, inner ear, and pulmonary neuroendocrine cell development and governs cell processes as diverse as self-renewal of hematopoietic stem cells, proliferation, apoptosis, differentiation, cell fate specification, and oncogenesis. However, the molecular basis of its transcriptional functions has remained elusive. Here we show that Gfi1 recruits the histone lysine methyltransferase G9a and the histone deacetylase 1 (HDAC1) in order to modify the chromatin of genes targeted for repression by Gfi1. G9a and HDAC1 are both in a repressive complex assembled by Gfi1. Endogenous Gfi1 colocalizes with G9a, HDAC1, and K9-dimethylated histone H3. Gfi1 associates with G9a and HDAC1 on the promoter of the cell cycle regulator p21Cip/WAF1, resulting in an increase in K9 dimethylation at histone H3. Silencing of Gfi1 expression in myeloid cells reverses G9a and HDAC1 recruitment to p21Cip/WAF1 and elevates its expression. These findings highlight the role of epigenetics in the regulation of development and oncogenesis by Gfi1.

Published

2005

21. Identification of growth factor independent-1 (GFI1) as a repressor of 25-hydroxyvitamin D 1-alpha hydroxylase (CYP27B1) gene expression in human prostate cancer cells.

Author

Dwivedi PP, Anderson PH, Omdahl JL, Grimes HL, Morris HA, and May BK

Subjects

5' Flanking Region genetics, Binding Sites genetics, DNA Mutational Analysis, Enhancer Elements, Genetic, Humans, Male, Nuclear Proteins metabolism, Promoter Regions, Genetic genetics, Prostatic Neoplasms metabolism, Sequence Deletion, 25-Hydroxyvitamin D3 1-alpha-Hydroxylase genetics, DNA-Binding Proteins metabolism, Gene Expression Regulation, Neoplastic, Prostatic Neoplasms genetics, Repressor Proteins metabolism, Transcription Factors metabolism

Abstract

The hormone 1,25-dihydroxyvitamin D (1,25D) may play a protective role in prostate cancer. 25-hydroxyvitamin D 1-alpha hydroxylase (CYP27B1) is the enzyme responsible for the regulation of cellular 1,25D levels. CYP27B1 is substantially repressed in prostate cancer cells. We have investigated the molecular basis for this inhibition. First, we identify a repressive region between -997 and -1200 in the human CYP27B1 promoter following transient transfection analysis in the prostate cancer cell lines DU145, PC3 and LNCaP. Next, we demonstrate a role for the transcription factor growth factor independent-1 (GFI1) in the repression of CYP27B1. Electrophoretic mobility assays with nuclear extracts from prostate cancer cell lines established binding of GFI1 to the sequence 5'-TGGTACAATCATAACTCACTGCAG-3' present at -997 to -1200 in the repressive region. Site directed mutagenesis of the core GFI1 binding sequence (5'-AATC-3') substantially increased while forced expression of GFI1 decreased the expression of the CYP27B1 reporter construct. Importantly, GFI1 repression is dependent on an intact GFI1 binding site in the -997 to -1200 region. GFI1 is an oncoprotein known to form a large protein complex with co-repressors that recruit histone deacetylases. We propose that the formation of such a repressive complex on the inhibitory domain of the CYP27B1 gene in prostate cancer cells could lead to silencing of either the nearby enhancer or proximal promoter domains and lead to cancer progression by reducing local production of 1,25D. These studies provide the basis for a more detailed understanding of CYP27B1 repression in prostate cancer cells and could provide a novel insight in future diagnosis and treatment.

Published

2005

22. Growth factor independence-1 is expressed in primary human neuroendocrine lung carcinomas and mediates the differentiation of murine pulmonary neuroendocrine cells.

Author

Kazanjian A, Wallis D, Au N, Nigam R, Venken KJ, Cagle PT, Dickey BF, Bellen HJ, Gilks CB, and Grimes HL

Subjects

Animals, Carcinoma, Neuroendocrine genetics, Carcinoma, Small Cell genetics, Cell Differentiation, Cell Extracts pharmacology, Cell Line, Tumor, DNA-Binding Proteins genetics, Female, Humans, Lung drug effects, Lung Neoplasms genetics, Mice, Neoplasm Transplantation, Neurosecretory Systems drug effects, Pregnancy, Transcription Factors genetics, Transfection, Transplantation, Heterologous, Carcinoma, Neuroendocrine metabolism, Carcinoma, Small Cell metabolism, DNA-Binding Proteins biosynthesis, Lung cytology, Lung Neoplasms metabolism, Neurosecretory Systems cytology, Transcription Factors biosynthesis

Abstract

Human small cell lung cancers might be derived from pulmonary cells with a neuroendocrine phenotype. They are driven to proliferate by autocrine and paracrine neuropeptide growth factor stimulation. The molecular basis of the neuroendocrine phenotype of lung carcinomas is relatively unknown. The Achaete-Scute Homologue-1 (ASH1) transcription factor is critically required for the formation of pulmonary neuroendocrine cells and is a marker for human small cell lung cancers. The Drosophila orthologues of ASH1 (Achaete and Scute) and the growth factor independence-1 (GFI1) oncoprotein (Senseless) genetically interact to inhibit Notch signaling and specify fly sensory organ development. Here, we show that GFI1, as with ASH1, is expressed in neuroendocrine lung cancer cell lines and that GFI1 in lung cancer cell lines functions as a DNA-binding transcriptional repressor protein. Forced expression of GFI1 potentiates tumor formation of small-cell lung carcinoma cells. In primary human lung cancer specimens, GFI1 expression strongly correlates with expression of ASH1, the neuroendocrine growth factor gastrin-releasing peptide, and neuroendocrine markers synaptophysin and chromogranin A (P < 0.0000001). GFI1 colocalizes with chromogranin A and calcitonin-gene-related peptide in embryonic and adult murine pulmonary neuroendocrine cells. In addition, mice with a mutation in GFI1 display abnormal development of pulmonary neuroendocrine cells, indicating that GFI1 is important for neuroendocrine differentiation.

Published

2004

23. Targeted transcriptional repression of Gfi1 by GFI1 and GFI1B in lymphoid cells.

Author

Doan LL, Porter SD, Duan Z, Flubacher MM, Montoya D, Tsichlis PN, Horwitz M, Gilks CB, and Grimes HL

Subjects

Animals, Base Sequence, Cell Line, Cells, Cultured, Conserved Sequence genetics, DNA genetics, DNA metabolism, Humans, Jurkat Cells, Mice, Molecular Sequence Data, Promoter Regions, Genetic genetics, Protein Binding, Proto-Oncogene Proteins genetics, RNA, Messenger genetics, RNA, Messenger metabolism, Rats, Repressor Proteins genetics, Response Elements genetics, Sequence Homology, Nucleic Acid, Thymus Gland cytology, DNA-Binding Proteins genetics, DNA-Binding Proteins metabolism, Gene Expression Regulation, Proto-Oncogene Proteins metabolism, Repressor Proteins metabolism, T-Lymphocytes metabolism, Thymus Gland metabolism, Transcription Factors, Transcription, Genetic

Abstract

Growth factor independence-1 (GFI1) and GFI1B are closely related, yet differentially expressed transcriptional repressors with nearly identical DNA binding domains. GFI1 is upregulated in the earliest thymocyte precursors, while GFI1B expression is restricted to T lymphopoiesis stages coincident with activation. Transgenic expression of GFI1 potentiates T-cell activation, while forced GFI1B expression decreases activation. Both mice and humans with mutant Gfi1 display lymphoid abnormalities. Here we describe autoregulation of Gfi1 in primary mouse thymocytes and a human T-cell line. GFI1 binding to cis-element sequences conserved between rat, mouse and human Gfi1 mediates direct and potent transcriptional repression. In addition, dramatic regulation of Gfi1 can also be mediated by GFI1B. These data provide the first example of a gene directly targeted by GFI1 and GFI1B. Moreover, they support a role for auto- and trans-regulation of Gfi1 by GFI1 and GFI1B in maintaining the normal expression patterns of Gfi1, and suggest that GFI1B may indirectly affect T-cell activation through repression of Gfi1.

Published

2004

24. Gfi-1 attaches to the nuclear matrix, associates with ETO (MTG8) and histone deacetylase proteins, and represses transcription using a TSA-sensitive mechanism.

Author

McGhee L, Bryan J, Elliott L, Grimes HL, Kazanjian A, Davis JN, and Meyers S

Subjects

Cells, Cultured, DNA-Binding Proteins chemistry, Enzyme Inhibitors metabolism, Enzyme Inhibitors pharmacology, Genes, Reporter genetics, Histone Deacetylase Inhibitors, Humans, Hydroxamic Acids pharmacology, Intermediate Filaments metabolism, Luminescent Proteins metabolism, Microscopy, Fluorescence, Proto-Oncogene Proteins metabolism, RUNX1 Translocation Partner 1 Protein, Repressor Proteins chemistry, Transcription, Genetic physiology, Transfection, DNA-Binding Proteins metabolism, Histone Deacetylases metabolism, Hydroxamic Acids metabolism, Nuclear Matrix metabolism, Repressor Proteins metabolism, Transcription Factors metabolism

Abstract

Gfi-1 and Gfi-1B can repress transcription and play important roles in hematopoietic cell survival and differentiation. Although these proteins are known to bind DNA through a C-terminal zinc-finger domain and may require an N-terminal SNAG domain (SNAIL/Gfi-1) to repress transcription, the mechanism by which Gfi-1 and Gfi-1B act is unknown. A first step towards understanding the mechanism by which these proteins repress transcription is to identify interacting proteins that could contribute to transcriptional repression. ETO (also termed MTG8), was first identified through its involvement in the (8;21) translocation associated with acute myelogenous leukemia. It attaches to the nuclear matrix and associates with histone deacetylases and the co-repressors N-CoR, SMRT, and mSin3A, and may act as a co-repressor for site-specific transcriptions factors. In this report we demonstrate that Gfi-1 interacts with ETO and related proteins both in vitro and in vivo and with histone deacetylase proteins in vivo. We observed that a portion of Gfi-1 and Gfi-1B associated with the nuclear matrix, as is the case with ETO. Moreover, Gfi-1 and ETO co-localize to punctate subnuclear structures. When co-expressed in mammalian cells, Gfi-1 associates with histone deacetylse-1 (HDAC-1), HDAC-2, and HDAC-3. These data identify ETO as a partner for Gfi-1 and Gfi-1B, and suggest that Gfi-1 proteins repress transcription through recruitment of histone deacetylase-containing complexes., (Copyright 2003 Wiley-Liss, Inc.)

Published

2003

25. Mutations in proto-oncogene GFI1 cause human neutropenia and target ELA2.

Author

Person RE, Li FQ, Duan Z, Benson KF, Wechsler J, Papadaki HA, Eliopoulos G, Kaufman C, Bertolone SJ, Nakamoto B, Papayannopoulou T, Grimes HL, and Horwitz M

Subjects

Adult, Aged, Child, Preschool, Chromosomes immunology, Colony-Forming Units Assay, Female, Humans, Infant, Luciferases metabolism, Male, Neutropenia blood, Neutropenia etiology, Neutrophils enzymology, Pedigree, Precipitin Tests, Promoter Regions, Genetic, Proto-Oncogene Mas, Reverse Transcriptase Polymerase Chain Reaction, Zinc Fingers, DNA-Binding Proteins genetics, Leukocyte Elastase genetics, Mutation, Missense, Neutropenia genetics, Transcription Factors

Abstract

Mice lacking the transcriptional repressor oncoprotein Gfi1 are unexpectedly neutropenic. We therefore screened GFI1 as a candidate for association with neutropenia in affected individuals without mutations in ELA2 (encoding neutrophil elastase), the most common cause of severe congenital neutropenia (SCN; ref. 3). We found dominant negative zinc finger mutations that disable transcriptional repressor activity. The phenotype also includes immunodeficient lymphocytes and production of a circulating population of myeloid cells that appear immature. We show by chromatin immunoprecipitation, gel shift, reporter assays and elevated expression of ELA2 in vivo in neutropenic individuals that GFI1 represses ELA2, linking these two genes in a common pathway involved in myeloid differentiation.

Published

2003

26. The zinc finger transcription factor Gfi1, implicated in lymphomagenesis, is required for inner ear hair cell differentiation and survival.

Author

Wallis D, Hamblen M, Zhou Y, Venken KJ, Schumacher A, Grimes HL, Zoghbi HY, Orkin SH, and Bellen HJ

Subjects

Animals, Basic Helix-Loop-Helix Transcription Factors, Behavior, Animal physiology, Cell Differentiation genetics, Cell Survival genetics, Cochlea cytology, Cochlea embryology, DNA-Binding Proteins genetics, Ear, Inner cytology, Ear, Inner embryology, Gene Expression Regulation, Developmental, Hair Cells, Auditory, Inner metabolism, Mice, Mice, Mutant Strains, Neurons cytology, Neurons metabolism, Organ of Corti ultrastructure, Transcription Factors genetics, Zinc Fingers, DNA-Binding Proteins metabolism, Hair Cells, Auditory, Inner cytology, Lymphoma genetics, Transcription Factors metabolism

Abstract

Gfi1 was first identified as causing interleukin 2-independent growth in T cells and lymphomagenesis in mice. Much work has shown that Gfi1 and Gfi1b, a second mouse homolog, play pivotal roles in blood cell lineage differentiation. However, neither Gfi1 nor Gfi1b has been implicated in nervous system development, even though their invertebrate homologues, senseless in Drosophila and pag-3 in C. elegans are expressed and required in the nervous system. We show that Gfi1 mRNA is expressed in many areas that give rise to neuronal cells during embryonic development in mouse, and that Gfi1 protein has a more restricted expression pattern. By E12.5 Gfi1 mRNA is expressed in both the CNS and PNS as well as in many sensory epithelia including the developing inner ear epithelia. At later developmental stages, Gfi1 expression in the ear is refined to the hair cells and neurons throughout the inner ear. Gfi1 protein is expressed in a more restricted pattern in specialized sensory cells of the PNS, including the eye, presumptive Merkel cells, the lung and hair cells of the inner ear. Gfi1 mutant mice display behavioral defects that are consistent with inner ear anomalies, as they are ataxic, circle, display head tilting behavior and do not respond to noise. They have a unique inner ear phenotype in that the vestibular and cochlear hair cells are differentially affected. Although Gfi1-deficient mice initially specify inner ear hair cells, these hair cells are disorganized in both the vestibule and cochlea. The outer hair cells of the cochlea are improperly innervated and express neuronal markers that are not normally expressed in these cells. Furthermore, Gfi1 mutant mice lose all cochlear hair cells just prior to and soon after birth through apoptosis. Finally, by five months of age there is also a dramatic reduction in the number of cochlear neurons. Hence, Gfi1 is expressed in the developing nervous system, is required for inner ear hair cell differentiation, and its loss causes programmed cell death.

Published

2003

27. The miR-23a~27a~24-2 microRNA cluster buffers transcription and signaling pathways during hematopoiesis.

Author

Kurkewich, Jeffrey L., Hansen, Justin, Klopfenstein, Nathan, Zhang, Helen, Wood, Christian, Boucher, Austin, Hickman, Joseph, Muench, David E., Grimes, H. Leighton, and Dahl, Richard

Subjects

MICRORNA, CELLULAR signal transduction, HEMATOPOIESIS, GENETIC overexpression, KNOCKOUT mice

Abstract

MicroRNA cluster mirn23a has previously been shown to promote myeloid development at the expense of lymphoid development in overexpression and knockout mouse models. This polarization is observed early in hematopoietic development, with an increase in common lymphoid progenitors (CLPs) and a decrease in all myeloid progenitor subsets in adult bone marrow. The pool size of multipotential progenitors (MPPs) is unchanged; however, in this report we observe by flow cytometry that polarized subsets of MPPs are changed in the absence of mirn23a. Additionally, in vitro culture of MPPs and sorted MPP transplants showed that these cells have decreased myeloid and increased lymphoid potential in vitro and in vivo. We investigated the mechanism by which mirn23a regulates hematopoietic differentiation and observed that mirn23a promotes myeloid development of hematopoietic progenitors through regulation of hematopoietic transcription factors and signaling pathways. Early transcription factors that direct the commitment of MPPs to CLPs (Ikzf1, Runx1, Satb1, Bach1 and Bach2) are increased in the absence of mirn23a miRNAs as well as factors that commit the CLP to the B cell lineage (FoxO1, Ebf1, and Pax5). Mirn23a appears to buffer transcription factor levels so that they do not stochastically reach a threshold level to direct differentiation. Intriguingly, mirn23a also inversely regulates the PI3 kinase (PI3K)/Akt and BMP/Smad signaling pathways. Pharmacological inhibitor studies, coupled with dominant active/dominant negative biochemical experiments, show that both signaling pathways are critical to mirn23a’s regulation of hematopoietic differentiation. Lastly, consistent with mirn23a being a physiological inhibitor of B cell development, we observed that the essential B cell transcription factor EBF1 represses expression of mirn23a. In summary, our data demonstrates that mirn23a regulates a complex array of transcription and signaling pathways to modulate adult hematopoiesis. [ABSTRACT FROM AUTHOR]

Published

2017

28. MEF2C and EBF1 Co-regulate B Cell-Specific Transcription

Author

Li Chai, Matthew Davis, Nikki R. Kong, Astar Winoto, Robert Tjian, and Grimes, H Leighton

Subjects

0301 basic medicine, Cancer Research, B Cells, Myeloid, Transcription, Genetic, Cellular differentiation, Gene Expression, Biochemistry, p38 Mitogen-Activated Protein Kinases, White Blood Cells, Animal Cells, Medicine and Health Sciences, 2.1 Biological and endogenous factors, MEF2C, Myeloid Cells, Aetiology, Phosphorylation, Genetics (clinical), Cancer, B-Lymphocytes, MEF2 Transcription Factors, Stem Cells, Cell Differentiation, Hematology, HNF1B, Enzymes, Haematopoiesis, Protein Transport, medicine.anatomical_structure, Blood, 293T cells, Cell lines, Stem Cell Research - Nonembryonic - Non-Human, Cellular Types, Oxidoreductases, Biological cultures, Luciferase, Transcription, Research Article, Subcellular Fractions, Transcriptional Activation, lcsh:QH426-470, Precursor Cells, Immune Cells, 1.1 Normal biological development and functioning, Immunology, DNA transcription, Biology, Histone Deacetylases, Cell Line, 03 medical and health sciences, Genetic, Underpinning research, DNA-binding proteins, medicine, Genetics, Humans, Immunoprecipitation, Gene Regulation, Cell Lineage, Progenitor cell, Antibody-Producing Cells, Molecular Biology, Transcription factor, Ecology, Evolution, Behavior and Systematics, B-Lymphoid, Blood Cells, Precursor Cells, B-Lymphoid, Biology and Life Sciences, Proteins, Cell Biology, Hematopoietic Stem Cells, Stem Cell Research, Regulatory Proteins, Research and analysis methods, lcsh:Genetics, 030104 developmental biology, Enzymology, Cancer research, Trans-Activators, IRF8, Transcription Factors, Developmental Biology

Abstract

Hematopoietic stem cells are capable of self-renewal or differentiation along three main lineages: myeloid, erythroid, and lymphoid. One of the earliest lineage decisions for blood progenitor cells is whether to adopt the lymphoid or myeloid fate. Previous work had shown that myocyte enhancer factor 2C (MEF2C) is indispensable for the lymphoid fate decision, yet the specific mechanism of action remained unclear. Here, we have identified early B cell factor-1 (EBF1) as a co-regulator of gene expression with MEF2C. A genome-wide survey of MEF2C and EBF1 binding sites identified a subset of B cell-specific genes that they target. We also determined that the p38 MAPK pathway activates MEF2C to drive B cell differentiation. Mef2c knockout mice showed reduced B lymphoid-specific gene expression as well as increased myeloid gene expression, consistent with MEF2C’s role as a lineage fate regulator. This is further supported by interaction between MEF2C and the histone deacetylase, HDAC7, revealing a likely mechanism to repress the myeloid transcription program. This study thus elucidates both activation and repression mechanisms, identifies regulatory partners, and downstream targets by which MEF2C regulates lymphoid-specific differentiation., Author Summary B cells comprise important defense systems against infections in animals. Generating B cells requires the interplay of signals received by a blood stem cell and the ability of this cell to turn on or off gene expression, the latter of which is regulated largely by transcription factors. Despite the characterization of many transcription factors and their functions in B cell differentiation, there still remains an incomplete understanding of how these molecules work together and the hierarchy involved in cell lineage determination. Mis-regulation by transcription factors can lead to many blood disorders such as leukemias and lymphomas, making the discovery of the missing links in transcription regulation important. This study places the transcription factor MEF2C at the node of the complex gene expression network that determines the B cell fate. We identified many new transcriptional targets of MEF2C, elucidated the signal to activate its function, as well as offered insights on how MEF2C can balance its dual role to both turn on and off gene expression. In summary, this study contributed to understanding the important molecular network underlying the generation of B cells.

Published

2016

29. Identification of growth factor independent-1 (GFI1) as a repressor of 25-hydroxyvitamin D 1-alpha hydroxylase (CYP27B1) gene expression in human prostate cancer cells

Author

H. Leighton Grimes, John L. Omdahl, Brian K. May, Paul H. Anderson, Howard A. Morris, Prem P. Dwivedi, Morris, Howard Arthur, Dwivedi, Prem, Anderson, P.H, Omdahl, John, Grimes, H. Leighton, and May, Brian

Subjects

Male, Cancer Research, 5' Flanking Region, Endocrinology, Diabetes and Metabolism, DNA Mutational Analysis, Clinical Sciences, Repressor, Biology, Prostate cancer, Endocrinology, DU145, LNCaP, medicine, Humans, Enhancer, Promoter Regions, Genetic, Transcription factor, Sequence Deletion, 25-Hydroxyvitamin D3 1-alpha-Hydroxylase, Binding Sites, Cancer, Nuclear Proteins, Prostatic Neoplasms, medicine.disease, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, Repressor Proteins, Enhancer Elements, Genetic, Oncology, Cancer cell, Cancer research, Transcription Factors

Abstract

The hormone 1,25-dihydroxyvitamin D (1,25D) may play a protective role in prostate cancer. 25-hydroxyvitamin D 1-alpha hydroxylase (CYP27B1) is the enzyme responsible for the regulation of cellular 1,25D levels. CYP27B1 is substantially repressed in prostate cancer cells. We have investigated the molecular basis for this inhibition. First, we identify a repressive region between -997 and -1200 in the human CYP27B1 promoter following transient transfection analysis in the prostate cancer cell lines DU145, PC3 and LNCaP. Next, we demonstrate a role for the transcription factor growth factor independent-1 (GFI1) in the repression of CYP27B1. Electrophoretic mobility assays with nuclear extracts from prostate cancer cell lines established binding of GFI1 to the sequence 5'-TGGTACAATCATAACTCACTGCAG-3' present at -997 to -1200 in the repressive region. Site directed mutagenesis of the core GFI1 binding sequence (5'-AATC-3') substantially increased while forced expression of GFI1 decreased the expression of the CYP27B1 reporter construct. Importantly, GFI1 repression is dependent on an intact GFI1 binding site in the -997 to -1200 region. GFI1 is an oncoprotein known to form a large protein complex with co-repressors that recruit histone deacetylases. We propose that the formation of such a repressive complex on the inhibitory domain of the CYP27B1 gene in prostate cancer cells could lead to silencing of either the nearby enhancer or proximal promoter domains and lead to cancer progression by reducing local production of 1,25D. These studies provide the basis for a more detailed understanding of CYP27B1 repression in prostate cancer cells and could provide a novel insight in future diagnosis and treatment.

Published

2005