Your search keyword '"Achim Leutz"' showing total 134 results

1. Arginine methylation of the p30 C/EBPα oncoprotein regulates progenitor proliferation and myeloid differentiation

Author

Linh T. Nguyen, Karin Zimmermann, Elisabeth Kowenz-Leutz, Dorothea Dörr, Anja Schütz, Jörg Schönheit, Alexander Mildner, and Achim Leutz

Subjects

biochemistry, cell biology, transcriptomics, Science

Abstract

Summary: The transcription factor CCAAT enhancer binding protein alpha (C/EBPα) is a master regulator of myelopoiesis. CEBPA encodes a long (p42) and a truncated (p30) protein isoform from a single mRNA. Mutations that abnormally enhance expression of p30 are associated with acute myelogenous leukemia (AML). We show by mutational analysis that three highly conserved arginine residues in the p30 C/EBPα N-terminus, previously found to be methylated, are involved in myeloid lineage commitment, progenitor proliferation, and differentiation. The conservative amino acid substitution with lysine that retains the amino acid side chain charge enhanced progenitor proliferation, while a non-conservative substitution with uncharged side chains (alanine, leucine) impaired proliferation and enhanced granulopoiesis. Analysis of protein interactions suggested that arginine methylation of p30 C/EBPα differentially determines interactions with SWI/SNF and MLL complexes. Pharmacological targeting of p30 C/EBPα arginine methylation may have clinical relevance in myeloproliferative and inflammatory diseases, in neutropenia, and in leukemic stem cells.

Published

2024

2. Carm1-arginine methylation of the transcription factor C/EBPα regulates transdifferentiation velocity

Author

Guillem Torcal Garcia, Elisabeth Kowenz-Leutz, Tian V Tian, Antonis Klonizakis, Jonathan Lerner, Luisa De Andres-Aguayo, Valeriia Sapozhnikova, Clara Berenguer, Marcos Plana Carmona, Maria Vila Casadesus, Romain Bulteau, Mirko Francesconi, Sandra Peiro, Philipp Mertins, Kenneth Zaret, Achim Leutz, and Thomas Graf

Subjects

cell fate, transcription factor, gene regulation, blood cell differentiation, lineage choice, transdifferentiation, Medicine, Science, Biology (General), QH301-705.5

Abstract

Here, we describe how the speed of C/EBPα-induced B cell to macrophage transdifferentiation (BMT) can be regulated, using both mouse and human models. The identification of a mutant of C/EBPα (C/EBPαR35A) that greatly accelerates BMT helped to illuminate the mechanism. Thus, incoming C/EBPα binds to PU.1, an obligate partner expressed in B cells, leading to the release of PU.1 from B cell enhancers, chromatin closing and silencing of the B cell program. Released PU.1 redistributes to macrophage enhancers newly occupied by C/EBPα, causing chromatin opening and activation of macrophage genes. All these steps are accelerated by C/EBPαR35A, initiated by its increased affinity for PU.1. Wild-type C/EBPα is methylated by Carm1 at arginine 35 and the enzyme’s perturbations modulate BMT velocity as predicted from the observations with the mutant. Increasing the proportion of unmethylated C/EBPα in granulocyte/macrophage progenitors by inhibiting Carm1 biases the cell’s differentiation toward macrophages, suggesting that cell fate decision velocity and lineage directionality are closely linked processes.

Published

2023

3. Immune cell C/EBPβ deficiency is associated with hepatic mononuclear defects and spontaneous hepatitis but not steatohepatitis induced liver fibrosis

Author

Itay Moshkovits, Ayelet Kaminitz, Debby Reuveni, Metsada Pasmanik‐Chor, Eli Brazowski, Alexander Mildner, Achim Leutz, and Ehud Zigmond

Subjects

cells, molecules, monocytes/macrophages, transcription factors, Immunologic diseases. Allergy, RC581-607

Abstract

Abstract Background CCAAT/enhancer‐binding protein β (C/EBPβ) is a transcription factor known to be involved in macrophage differentiation and function, steatohepatitis and liver fibrosis. Methods Immune restricted C/EBPβ deficient and control mice were investigated in steady‐state and in the CDA‐HFD steatohepatitis model. Mice were assessed for weight change, liver biochemical profile, histology and hepatic phagocytes composition. Results Flow cytometry analysis of hepatic nonparenchymal cells revealed reduced numbers of hepatic monocytes and Kupffer cells and an increase in hepatic MHC class II positive myeloid cells in immune cells restricted C/EBPβ deficient mice. Immune‐restricted C/EBPβ deficiency resulted in decreased weight gain and appearance of mild spontaneous liver inflammation. Nevertheless, In the CDA‐HFD steatohepatitis model, immune restricted C/EBPβ deficient and proficient mice exhibit similar grade of hepatic steatosis, liver enzymes levels and fibrosis stage. Conclusions Immune‐restricted C/EBPβ deficiency leads to significant alteration in hepatic mononuclear phagocytes composition associated with spontaneous mild hepatitis. Steatohepatitis associated fibrosis is not dependent on C/EBPβ expression by immune cells.

Published

2022

4. Tongue immune compartment analysis reveals spatial macrophage heterogeneity

Author

Ekaterini Maria Lyras, Karin Zimmermann, Lisa Katharina Wagner, Dorothea Dörr, Christoph SN Klose, Cornelius Fischer, Steffen Jung, Simon Yona, Avi-Hai Hovav, Werner Stenzel, Steffen Dommerich, Thomas Conrad, Achim Leutz, and Alexander Mildner

Subjects

Tongue, macrophages, single cell sequencing, cell development, Medicine, Science, Biology (General), QH301-705.5

Abstract

The tongue is a unique muscular organ situated in the oral cavity where it is involved in taste sensation, mastication, and articulation. As a barrier organ, which is constantly exposed to environmental pathogens, the tongue is expected to host an immune cell network ensuring local immune defence. However, the composition and the transcriptional landscape of the tongue immune system are currently not completely defined. Here, we characterised the tissue-resident immune compartment of the murine tongue during development, health and disease, combining single-cell RNA-sequencing with in situ immunophenotyping. We identified distinct local immune cell populations and described two specific subsets of tongue-resident macrophages occupying discrete anatomical niches. Cx3cr1+ macrophages were located specifically in the highly innervated lamina propria beneath the tongue epidermis and at times in close proximity to fungiform papillae. Folr2+ macrophages were detected in deeper muscular tissue. In silico analysis indicated that the two macrophage subsets originate from a common proliferative precursor during early postnatal development and responded differently to systemic LPS in vivo. Our description of the under-investigated tongue immune system sets a starting point to facilitate research on tongue immune-physiology and pathology including cancer and taste disorders.

Published

2022

5. PRISMA and BioID disclose a motifs-based interactome of the intrinsically disordered transcription factor C/EBPα

Author

Evelyn Ramberger, Valeria Sapozhnikova, Elisabeth Kowenz-Leutz, Karin Zimmermann, Nathalie Nicot, Petr V. Nazarov, Daniel Perez-Hernandez, Ulf Reimer, Philipp Mertins, Gunnar Dittmar, and Achim Leutz

Subjects

Proteomics, Omics, Transcriptomics, Science

Abstract

Summary: C/EBPα represents a paradigm intrinsically disordered transcription factor containing short linear motifs and post-translational modifications (PTM). Unraveling C/EBPα protein interaction networks is a prerequisite for understanding the multi-modal functions of C/EBPα in hematopoiesis and leukemia. Here, we combined arrayed peptide matrix screening (PRISMA) with BioID to generate an in vivo validated and isoform specific interaction map of C/EBPα. The myeloid C/EBPα interactome comprises promiscuous and PTM-regulated interactions with protein machineries involved in gene expression, epigenetics, genome organization, DNA replication, RNA processing, and nuclear transport. C/EBPα interaction hotspots coincide with homologous conserved regions of the C/EBP family that also score as molecular recognition features. PTMs alter the interaction spectrum of C/EBP-motifs to configure a multi-valent transcription factor hub that interacts with multiple co-regulatory components, including BAF/SWI-SNF or Mediator complexes. Combining PRISMA and BioID is a powerful strategy to systematically explore the PTM-regulated interactomes of intrinsically disordered transcription factors.

Published

2021

6. PRISMA: Protein Interaction Screen on Peptide Matrix Reveals Interaction Footprints and Modifications- Dependent Interactome of Intrinsically Disordered C/EBPβ

Author

Gunnar Dittmar, Daniel Perez Hernandez, Elisabeth Kowenz-Leutz, Marieluise Kirchner, Günther Kahlert, Radoslaw Wesolowski, Katharina Baum, Maria Knoblich, Maria Hofstätter, Arnaud Muller, Jana Wolf, Ulf Reimer, and Achim Leutz

Subjects

Science

Abstract

Summary: CCAAT enhancer-binding protein beta (C/EBPβ) is a pioneer transcription factor that specifies cell differentiation. C/EBPβ is intrinsically unstructured, a molecular feature common to many proteins involved in signal processing and epigenetics. The structure of C/EBPβ differs depending on alternative translation initiation and multiple post-translational modifications (PTM). Mutation of distinct PTM sites in C/EBPβ alters protein interactions and cell differentiation, suggesting that a C/EBPβ PTM indexing code determines epigenetic outcomes. Herein, we systematically explored the interactome of C/EBPβ using an array technique based on spot-synthesized C/EBPβ-derived linear tiling peptides with and without PTM, combined with mass spectrometric proteomic analysis of protein interactions. We identified interaction footprints of ∼1,300 proteins in nuclear extracts, many with chromatin modifying, chromatin remodeling, and RNA processing functions. The results suggest that C/EBPβ acts as a multi-tasking molecular switchboard, integrating signal-dependent modifications and structural plasticity to orchestrate interactions with numerous protein complexes directing cell fate and function. : Proteomics; Systems Biology; Transcriptomics Subject Areas: Proteomics, Systems Biology, Transcriptomics

Published

2019

7. The C/EBPβ LIP isoform rescues loss of C/EBPβ function in the mouse

Author

Valérie Bégay, Christian Baumeier, Karin Zimmermann, Arnd Heuser, and Achim Leutz

Subjects

Medicine, Science

Abstract

Abstract The transcription factor C/EBPβ regulates hematopoiesis, bone, liver, fat, and skin homeostasis, and female reproduction. C/EBPβ protein expression from its single transcript occurs by alternative in-frame translation initiation at consecutive start sites to generate three isoforms, two long (LAP*, LAP) and one truncated (LIP), with the same C-terminal bZip dimerization domain. The long C/EBPβ isoforms are considered gene activators, whereas the LIP isoform reportedly acts as a dominant-negative repressor. Here, we tested the putative repressor functions of the C/EBPβ LIP isoform in mice by comparing monoallelic WT or LIP knockin mice with Cebpb knockout mice, in combination with monoallelic Cebpa mice. The C/EBPβ LIP isoform was sufficient to function in coordination with C/EBPα in murine development, adipose tissue and sebocyte differentiation, and female fertility. Thus, the C/EBPβ LIP isoform likely has more physiological functions than its currently known role as a dominant-negative inhibitor, which are more complex than anticipated.

Published

2018

8. C/EBP-Induced Transdifferentiation Reveals Granulocyte-Macrophage Precursor-like Plasticity of B Cells

Author

Branko Cirovic, Jörg Schönheit, Elisabeth Kowenz-Leutz, Jelena Ivanovska, Christine Klement, Nina Pronina, Valérie Bégay, and Achim Leutz

Subjects

hematopoiesis, leukemia, differentiation, stem cell, progenitor, lineage switch, Medicine (General), R5-920, Biology (General), QH301-705.5

Abstract

The lymphoid-myeloid transdifferentiation potentials of members of the C/EBP family (C/EBPα, β, δ, and ε) were compared in v-Abl-immortalized primary B cells. Conversion of B cells to macrophages was readily induced by the ectopic expression of any C/EBP, and enhanced by endogenous C/EBPα and β activation. High transgene expression of C/EBPβ or C/EBPε, but not of C/EBPα or C/EBPδ, also induced the formation of granulocytes. Granulocytes and macrophages emerged in a mutually exclusive manner. C/EBPβ-expressing B cells produced granulocyte-macrophage progenitor (GMP)-like progenitors when subjected to selective pressure to eliminate lymphoid cells. The GMP-like progenitors remained self-renewing and cytokine-independent, and continuously produced macrophages and granulocytes. In addition to their suitability to study myelomonocytic lineage bifurcation, lineage-switched GMP-like progenitors could reflect the features of the lympho-myeloid lineage switch observed in leukemic progression.

Published

2017

9. Author Correction: Loss-of-function uORF mutations in human malignancies

Author

Julia Schulz, Nancy Mah, Martin Neuenschwander, Tabea Kischka, Richard Ratei, Peter M. Schlag, Esmeralda Castaños-Vélez, Iduna Fichtner, Per-Ulf Tunn, Carsten Denkert, Oliver Klaas, Wolfgang E. Berdel, Jens P. von Kries, Wojciech Makalowski, Miguel A. Andrade-Navarro, Achim Leutz, and Klaus Wethmar

Subjects

Medicine, Science

Abstract

An amendment to this paper has been published and can be accessed via a link at the top of the paper.

Published

2021

10. Hacking cell differentiation: transcriptional rerouting in reprogramming, lineage infidelity and metaplasia

Author

Gonçalo Regalo and Achim Leutz

Subjects

carcinogenesis, haematopoiesis, metaplasia, transcription factor, trans‐differentiation, Medicine (General), R5-920, Genetics, QH426-470

Abstract

Abstract Initiating neoplastic cell transformation events are of paramount importance for the comprehension of regeneration and vanguard oncogenic processes but are difficult to characterize and frequently clinically overlooked. In epithelia, pre‐neoplastic transformation stages are often distinguished by the appearance of phenotypic features of another differentiated tissue, termed metaplasia. In haemato/lymphopoietic malignancies, cell lineage ambiguity is increasingly recorded. Both, metaplasia and biphenotypic leukaemia/lymphoma represent examples of dysregulated cell differentiation that reflect a history of trans‐differentiation and/or epigenetic reprogramming. Here we compare the similarity between molecular events of experimental cell trans‐differentiation as an emerging therapeutic concept, with lineage confusion, as in metaplasia and dysplasia forecasting tumour development.

Published

2013

11. PU.1 Level-Directed Chromatin Structure Remodeling at the Irf8 Gene Drives Dendritic Cell Commitment

Author

Jörg Schönheit, Christiane Kuhl, Marie Luise Gebhardt, Francisco Fernández Klett, Pia Riemke, Marina Scheller, Gang Huang, Ronald Naumann, Achim Leutz, Carol Stocking, Josef Priller, Miguel A. Andrade-Navarro, and Frank Rosenbauer

Subjects

Biology (General), QH301-705.5

Abstract

Dendritic cells (DCs) are essential regulators of immune responses; however, transcriptional mechanisms that establish DC lineage commitment are poorly defined. Here, we report that the PU.1 transcription factor induces specific remodeling of the higher-order chromatin structure at the interferon regulatory factor 8 (Irf8) gene to initiate DC fate choice. An Irf8 reporter mouse enabled us to pinpoint an initial progenitor stage at which DCs separate from other myeloid lineages in the bone marrow. In the absence of Irf8, this progenitor undergoes DC-to-neutrophil reprogramming, indicating that DC commitment requires an active, Irf8-dependent escape from alternative myeloid lineage potential. Mechanistically, myeloid Irf8 expression depends on high PU.1 levels, resulting in local chromosomal looping and activation of a lineage- and developmental-stage-specific cis-enhancer. These data delineate PU.1 as a concentration-dependent rheostat of myeloid lineage selection by controlling long-distance contacts between regulatory elements and suggest that specific higher-order chromatin remodeling at the Irf8 gene determines DC differentiation.

Published

2013

12. Lymphoid to myeloid cell trans-differentiation is determined by C/EBPβ structure and post-translational modifications.

Author

Bilyana Stoilova, Elisabeth Kowenz-Leutz, Marina Scheller, and Achim Leutz

Subjects

Medicine, Science

Abstract

The transcription factor C/EBPβ controls differentiation, proliferation, and functionality of many cell types, including innate immune cells. A detailed molecular understanding of how C/EBPβ directs alternative cell fates remains largely elusive. A multitude of signal-dependent post-translational modifications (PTMs) differentially affect the protean C/EBPβ functions. In this study we apply an assay that converts primary mouse B lymphoid progenitors into myeloid cells in order to answer the question how C/EBPβ regulates (trans-) differentiation and determines myeloid cell fate. We found that structural alterations and various C/EBPβ PTMs determine the outcome of trans-differentiation of lymphoid into myeloid cells, including different types of monocytes/macrophages, dendritic cells, and granulocytes. The ability of C/EBPβ to recruit chromatin remodeling complexes is required for the granulocytic trans-differentiation outcome. These novel findings reveal that PTMs and structural plasticity of C/EBPβ are adaptable modular properties that integrate and rewire epigenetic functions to direct differentiation to diverse innate immune system cells, which are crucial for the organism survival.

Published

2013

13. Regulation of adipocyte 11β-hydroxysteroid dehydrogenase type 1 (11β-HSD1) by CCAAT/enhancer-binding protein (C/EBP) β isoforms, LIP and LAP.

Author

Cristina L Esteves, Val Kelly, Valérie Bégay, Tak Y Man, Nicholas M Morton, Achim Leutz, Jonathan R Seckl, and Karen E Chapman

Subjects

Medicine, Science

Abstract

11β-Hydroxysteroid dehydrogenase type 1 (11β-HSD1) catalyses intracellular regeneration of active glucocorticoids, notably in liver and adipose tissue. 11β-HSD1 is increased selectively in adipose tissue in human obesity, a change implicated in the pathogenesis of metabolic syndrome. With high fat (HF)-feeding, adipose tissue 11β-HSD1 is down-regulated in mice, plausibly to counteract metabolic disease. Transcription of 11β-HSD1 is directly regulated by members of the CCAAT/enhancer binding protein (C/EBP) family. Here we show that while total C/EBPβ in adipose tissue is unaltered by HF diet, the ratio of the C/EBPβ isoforms liver-enriched inhibitor protein (LIP) and liver-enriched activator protein (LAP) (C/EBPβ-LIP:LAP) is increased in subcutaneous adipose. This may cause changes in 11β-HSD1 expression since genetically modified C/EBPβ((+/L)) mice, with increased C/EBPβ-LIP:LAP ratio, have decreased subcutaneous adipose 11β-HSD1 mRNA levels, whereas C/EBPβ(ΔuORF) mice, with decreased C/EBPβ-LIP:LAP ratio, show increased subcutaneous adipose 11β-HSD1. C/EBPβ-LIP:LAP ratio is regulated by endoplasmic reticulum (ER) stress and mTOR signalling, both of which are altered in obesity. In 3T3-L1 adipocytes, 11β-HSD1 mRNA levels were down-regulated following induction of ER stress by tunicamycin but were up-regulated following inhibition of mTOR by rapamycin. These data point to a central role for C/EBPβ and its processing to LIP and LAP in transcriptional regulation of 11β-HSD1 in adipose tissue. Down-regulation of 11β-HSD1 by increased C/EBPβ-LIP:LAP in adipocytes may be part of a nutrient-sensing mechanism counteracting nutritional stress generated by HF diet.

Published

2012

14. Eukaryotic initiation factor 2α phosphorylation is required for B-cell maturation and function in mice

Author

Nina Mielke, Rolf Schwarzer, Cornelis F. Calkhoven, Randal J. Kaufman, Bernd Dörken, Achim Leutz, and Franziska Jundt

Subjects

Diseases of the blood and blood-forming organs, RC633-647.5

Abstract

Background The control of translation initiation is a crucial component in the regulation of gene expression. The eukaryotic initiation factor 2α (eIF2α) mediates binding of the initiator transfer-messenger-RNA to the AUG initiation codon, and thus controls a rate-limiting step in translation initiation. Phosphorylation of eIF2α at serine 51 is linked to cellular stress response and attenuates translation initiation. The biochemistry of translation inhibition mediated by eIF2α phosphorylation is well characterized, yet the physiological importance in hematopoiesis remains only partially known.Design and Methods Using hematopoietic stem cells carrying a non-phosphorylatable mutant form of eIF2α (eIF2αAA), we examined the efficiency of reconstitution in wild-type and B-cell-deficient microMT C57BL/6 recipients in two independent models.Results We provide evidence that phosphorylation-deficient eIF2α mutant hematopoietic stem cells may repopulate lethally irradiated mice but have a defect in the development and maintenance of newly formed B cells in the bone marrow and of naïve follicular B cells in the periphery. The mature B-cell compartment is markedly reduced in bone marrow, spleen and peripheral blood, and B-cell receptor-mediated proliferation in vitro and serum immunoglobulin secretion in vivo are impaired.Conclusions The data suggest that regulation of translation through eIF2α phosphorylation is dispensable in hematopoietic reconstitution but essential during late B-cell development.

Published

2011

15. Carm1 regulates the speed of C/EBPα-induced transdifferentiation by a cofactor stealing mechanism

Author

Guillem Torcal Garcia, Elisabeth Kowenz-Leutz, Tian V. Tian, Antonios Klonizakis, Jonathan Lerner, Luisa de Andrés-Aguayo, Clara Berenguer, Marcos Plana-Carmona, Maria Vila-Casadesús, Romain Bulteau, Mirko Francesconi, Sandra Peiró, Kenneth S. Zaret, Achim Leutz, and Thomas Graf

Abstract

Cell fate decisions are driven by lineage-restricted transcription factors but how they are regulated is incompletely understood. The C/EBPα-induced B cell to macrophage transdifferentiation (BMT) is a powerful system to address this question. Here we describe that C/EBPα with a single arginine mutation (C/EBPαR35A) induces a dramatically accelerated BMT in mouse and human cells. Changes in the expression of lineage-restricted genes occur as early as within 1 hour compared to 18 hours with the wild type. Mechanistically C/EBPαR35Aexhibits an increased affinity for PU.1, a bi-lineage transcription factor required for C/EBPα-induced BMT. The complex induces more rapid chromatin accessibility changes and an enhanced relocation (stealing) of PU.1 from B cell to myeloid gene regulatory elements. Arginine 35 is methylated by Carm1 and inhibition of the enzyme accelerates BMT, similar to the mutant. Our data suggest that the relative proportions of methylated and unmethylated C/EBPα in a bipotent progenitor can determine the velocity of cell fate choice and lineage directionality.

Published

2022

16. C/EBPβ regulates lipid metabolism and Pparg isoform 2 expression in alveolar macrophages

Author

Dorothea Dörr, Benedikt Obermayer, January Mikolaj Weiner, Karin Zimmermann, Chiara Anania, Lisa Katharina Wagner, Ekaterini Maria Lyras, Valeriia Sapozhnikova, David Lara-Astiaso, Felipe Prósper, Roland Lang, Darío G. Lupiáñez, Dieter Beule, Uta E. Höpken, Achim Leutz, and Alexander Mildner

Subjects

Immunology, General Medicine

Abstract

Pulmonary alveolar proteinosis (PAP) is a syndrome characterized by accumulation of surfactant lipoproteins within the lung alveoli. Alveolar macrophages (AMs) are crucial for surfactant clearance, and their differentiation depends on colony-stimulating factor 2 (CSF2), which regulates the establishment of an AM-characteristic gene regulatory network. Here, we report that the transcription factor CCAAT/enhancer binding protein β (C/EBPβ) is essential for the development of the AM identity, as demonstrated by transcriptome and chromatin accessibility analysis. Furthermore, C/EBPβ-deficient AMs showed severe defects in proliferation, phagocytosis, and lipid metabolism, collectively resulting in a PAP-like syndrome. Mechanistically, the long C/EBPβ protein variants LAP* and LAP together with CSF2 signaling induced the expression of Pparg isoform 2 but not Pparg isoform 1, a molecular regulatory mechanism that was also observed in other CSF2-primed macrophages. These results uncover C/EBPβ as a key regulator of AM cell fate and shed light on the molecular networks controlling lipid metabolism in macrophages.

Published

2022

17. Author response: Tongue immune compartment analysis reveals spatial macrophage heterogeneity

Author

Ekaterini Maria Lyras, Karin Zimmermann, Lisa Katharina Wagner, Dorothea Dörr, Christoph SN Klose, Cornelius Fischer, Steffen Jung, Simon Yona, Avi-Hai Hovav, Werner Stenzel, Steffen Dommerich, Thomas Conrad, Achim Leutz, and Alexander Mildner

Published

2022

18. The transcription factor C/EBPβ orchestrates dendritic cell maturation and functionality under homeostatic and malignant conditions

Author

Uta E. Höpken, Annika Graband, Lutz Menzel, Myroslav Zapukhlyak, Georg Lenz, Michael Grau, Achim Leutz, Armin Rehm, Martin Janz, and Florian Scholz

Subjects

Male, T-Lymphocytes, chemical and pharmacologic phenomena, Mice, Transgenic, Cell fate determination, Monocytes, Cell Line, Mice, Tumor Microenvironment, Animals, Humans, Protein Isoforms, E2F1, E2F, Transcription factor, Cyclin-dependent kinase 1, Multidisciplinary, Chemistry, CCAAT-Enhancer-Binding Protein-beta, TOR Serine-Threonine Kinases, Cell Differentiation, Dendritic Cells, Dendritic cell, Biological Sciences, Cell cycle, Cell biology, Mice, Inbred C57BL, Gene Expression Regulation, Female, Signal transduction, Signal Transduction, Transcription Factors

Abstract

Dendritic cell (DC) maturation is a prerequisite for the induction of adaptive immune responses against pathogens and cancer. Transcription factor (TF) networks control differential aspects of early DC progenitor versus late-stage DC cell fate decisions. Here, we identified the TF C/EBPβ as a key regulator for DC maturation and immunogenic functionality under homeostatic and lymphoma-transformed conditions. Upon cell-specific deletion of C/EBPβ in CD11c(+)MHCII(hi) DCs, gene expression profiles of splenic C/EBPβ(−/−) DCs showed a down-regulation of E2F cell cycle target genes and associated proliferation signaling pathways, whereas maturation signatures were enriched. Total splenic DC cell numbers were modestly increased but differentiation into cDC1 and cDC2 subsets were unaltered. The splenic CD11c(+)MHCII(hi)CD64(+) DC compartment was also increased, suggesting that C/EBPβ deficiency favors the expansion of monocytic-derived DCs. Expression of C/EBPβ could be mimicked in LAP/LAP* isoform knockin DCs, whereas the short isoform LIP supported a differentiation program similar to deletion of the full-length TF. In accordance with E2F1 being a negative regulator of DC maturation, C/EBPβ(−/−) bone marrow-derived DCs matured much faster enabling them to activate and polarize T cells stronger. In contrast to a homeostatic condition, lymphoma-exposed DCs exhibited an up-regulation of the E2F transcriptional pathways and an impaired maturation. Pharmacological blockade of C/EBPβ/mTOR signaling in human DCs abrogated their protumorigenic function in primary B cell lymphoma cocultures. Thus, C/EBPβ plays a unique role in DC maturation and immunostimulatory functionality and emerges as a key factor of the tumor microenvironment that promotes lymphomagenesis.

Published

2020

19. Cxcl10+ monocytes define a pathogenic subset in the central nervous system during autoimmune neuroinflammation

Author

Chiara Medaglia, Ido Amit, Lisa Katharina Wagner, Matthias Mack, Alexander Mildner, Hanjie Li, Steffen Jung, Amir Giladi, Dorothea Dörr, Simon Yona, Anat Shemer, Achim Leutz, and Franziska Paul

Subjects

0301 basic medicine, Myeloid, Monocyte, Multiple sclerosis, Immunology, Dendritic cell, Biology, medicine.disease, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Immune system, medicine, Immunology and Allergy, CXCL10, Progenitor cell, Neuroinflammation, 030215 immunology

Abstract

Multiple sclerosis (MS) is characterized by pathological inflammation that results from the recruitment of lymphoid and myeloid immune cells from the blood into the brain. Due to subset heterogeneity, defining the functional roles of the various cell subsets in acute and chronic stages of MS has been challenging. Here, we used index and transcriptional single-cell sorting to characterize the mononuclear phagocytes that infiltrate the central nervous system from the periphery in mice with experimentally induced autoimmune encephalomyelitis, a model of MS. We identified eight monocyte and three dendritic cell subsets at acute and chronic disease stages in which the defined transcriptional programs pointed toward distinct functions. Monocyte-specific cell ablation identified Cxcl10+ and Saa3+ monocytic subsets with a pathogenic potential. Transfer experiments with different monocyte and precursor subsets indicated that these Cxcl10+ and Saa3+ pathogenic cells were not derived from Ly6C+ monocytes but from early myeloid cell progenitors. These results suggest that blocking specific pathogenic monocytic subsets, including Cxcl10+ and Saa3+ monocytes, could be used for targeted therapeutic interventions.

Published

2020

20. Author Correction: Loss-of-function uORF mutations in human malignancies

Author

Miguel A. Andrade-Navarro, Peter M. Schlag, Wolfgang E. Berdel, Tabea Kischka, Achim Leutz, Jens Peter von Kries, Oliver Klaas, Klaus Wethmar, Esmeralda Castaños-Vélez, Richard Ratei, Nancy Mah, Carsten Denkert, Martin Neuenschwander, Wojciech Makalowski, Iduna Fichtner, Per-Ulf Tunn, and Julia Schulz

Subjects

Receptor, EphB1, Carcinogenesis, Science, MEDLINE, MAP Kinase Kinase 6, Bioinformatics, Open Reading Frames, Genes, Reporter, Cell Line, Tumor, Neoplasms, Proto-Oncogenes, Humans, Medicine, Author Correction, Luciferases, Peptide Chain Initiation, Translational, Loss function, Multidisciplinary, business.industry, Published Erratum, High-Throughput Nucleotide Sequencing, Protein-Tyrosine Kinases, Neoplasm Proteins, HEK293 Cells, Mutation, Codon, Terminator, 5' Untranslated Regions, business, Genome-Wide Association Study

Abstract

Ribosome profiling revealed widespread translational activity at upstream open reading frames (uORFs) and validated uORF-mediated translational control as a commonly repressive mechanism of gene expression. Translational activation of proto-oncogenes through loss-of-uORF mutations has been demonstrated, yet a systematic search for cancer-associated genetic alterations in uORFs is lacking. Here, we applied a PCR-based, multiplex identifier-tagged deep sequencing approach to screen 404 uORF translation initiation sites of 83 human tyrosine kinases and 49 other proto-oncogenes in 308 human malignancies. We identified loss-of-function uORF mutations in EPHB1 in two samples derived from breast and colon cancer, and in MAP2K6 in a sample of colon adenocarcinoma. Both mutations were associated with enhanced translation, suggesting that loss-of-uORF-mediated translational induction of the downstream main protein coding sequence may have contributed to carcinogenesis. Computational analysis of whole exome sequencing datasets of 464 colon adenocarcinomas subsequently revealed another 53 non-recurrent somatic mutations functionally deleting 22 uORF initiation and 31 uORF termination codons, respectively. These data provide evidence for somatic mutations affecting uORF initiation and termination codons in human cancer. The insufficient coverage of uORF regions in current whole exome sequencing datasets demands for future genome-wide analyses to ultimately define the contribution of uORF-mediated translational deregulation in oncogenesis.

Published

2021

21. A comprehensive motifs-based interactome of the C/EBPα transcription factor

Author

Karin Zimmermann, Nathalie Nicot, Evelyn Ramberger, Daniel Pérez-Hernández, Valeria Sapozhnikova, Gunnar Dittmar, Achim Leutz, Elisabeth Kowenz-Leutz, Philipp Mertins, Ulf Reimer, and Petr V. Nazarov

Subjects

Gene isoform, Chemistry, DNA replication, Short linear motif, Computational biology, Intrinsically disordered proteins, Proteomics, Transcription factor, Interactome, Protein–protein interaction

Abstract

The pioneering transcription factor C/EBPα coordinates cell fate and cell differentiation. C/EBPα represents an intrinsically disordered protein with multiple short linear motifs and extensive post-translational side chain modifications (PTM), reflecting its modularity and functional plasticity. Here, we combined arrayed peptide matrix screening (PRISMA) with biotin ligase proximity labeling proteomics (BioID) to generate a linear, isoform specific and PTM-dependent protein interaction map of C/EBPα in myeloid cells. The C/EBPα interactome comprises promiscuous and PTM-regulated interactions with protein machineries involved in gene expression, epigenetics, genome organization, DNA replication, RNA processing, and nuclear transport as the basis of functional C/EBPα plasticity. Protein interaction hotspots were identified that coincide with homologous conserved regions of the C/EBP family and revealed interaction motifs that score as molecular recognition features (MoRF). PTMs alter the interaction spectrum of multi-valent C/EBP-motifs to configure a multimodal transcription factor hub that allows interaction with multiple co-regulatory components, including BAF/SWI-SNF or Mediator complexes. Combining PRISMA and BioID acts as a powerful strategy to systematically explore the interactomes of intrinsically disordered proteins and their PTM-regulated, multimodal capacity.Key pointsIntegration of proximity labeling and arrayed peptide screen proteomics refines the interactome of C/EBPα isoformsHotspots of protein interactions in C/EBPα mostly occur in conserved short linear motifsInteractions of the BAF/SWI-SNF complex with C/EBPα are modulated by arginine methylation and isoform statusThe integrated experimental strategy suits systematic interactome studies of intrinsically disordered proteins

Published

2020

22. C/EBPβ-Dependent Epigenetic Memory Induces Trained Immunity in Hematopoietic Stem Cells

Author

Orit Matcovitch-Natan, Bérengère de Laval, Sandrine Sarrazin, Caroline Huber, Julien Maurizio, Eyal David, Susanne Reinhardt, Gregory Gimenez, Bertrand Nadel, Christophe Bordi, Prashanth K. Kandalla, Achim Leutz, Gabriel Brisou, Louise Simonnet, Alexander Mildner, Ido Amit, Michael H. Sieweke, Centre d'Immunologie de Marseille - Luminy (CIML), Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS)-Aix Marseille Université (AMU), Inovarion, Institute of Anatomy and Center for Regenerative Therapies, TU Dresden (CRTD), Max Delbrück Center for Molecular Medicine [Berlin] (MDC), Helmholtz-Gemeinschaft = Helmholtz Association, Weizmann Institute of Science [Rehovot, Israël], Biotechnology Center, and Center for Regenerative Therapies Dresden (CRTD), Technische Universität Dresden = Dresden University of Technology (TU Dresden), Institut de Microbiologie de la Méditerranée (IMM), Aix Marseille Université (AMU)-Centre National de la Recherche Scientifique (CNRS), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), ANR-17-CE15-0007,HSCmemory,Exploration de l'existence d'une fonction et d'une mémoire immunitaire au niveau de la Cellules Souche Hématopoïétique.(2017), and ANR-18-CE12-0019,Epromoters,Contrôle de la réponse au stress par une nouvelle classe de promoteurs à activité enhancer(2018)

Subjects

Epigenomics, Myeloid, [SDV]Life Sciences [q-bio], Secondary infection, Biology, Epigenesis, Genetic, 03 medical and health sciences, 0302 clinical medicine, Immune system, Immunity, Genetics, medicine, Humans, ComputingMilieux_MISCELLANEOUS, 030304 developmental biology, Myelopoiesis, 0303 health sciences, Innate immune system, CCAAT-Enhancer-Binding Protein-beta, Cell Biology, biochemical phenomena, metabolism, and nutrition, Hematopoietic Stem Cells, Immunity, Innate, 3. Good health, Cell biology, Haematopoiesis, medicine.anatomical_structure, 030220 oncology & carcinogenesis, bacteria, Molecular Medicine, Stem cell, 030217 neurology & neurosurgery

Abstract

Summary Hematopoietic stem cells (HSCs) maintain life-long production of immune cells and can directly respond to infection, but sustained effects on the immune response remain unclear. We show that acute immune stimulation with lipopolysaccharide (LPS) induced only transient changes in HSC abundance, composition, progeny, and gene expression, but persistent alterations in accessibility of specific myeloid lineage enhancers occurred, which increased responsiveness of associated immune genes to secondary stimulation. Functionally, this was associated with increased myelopoiesis of pre-exposed HSCs and improved innate immunity against the gram-negative bacterium P. aeruginosa. The accessible myeloid enhancers were enriched for C/EBPβ targets, and C/EBPβ deletion erased the long-term inscription of LPS-induced epigenetic marks and gene expression. Thus, short-term immune signaling can induce C/EBPβ-dependent chromatin accessibility, resulting in HSC-trained immunity, during secondary infection. This establishes a mechanism for how infection history can be epigenetically inscribed in HSCs as an integral memory function of innate immunity.

Published

2020

23. Loss-of-function uORF mutations in human malignancies

Author

Iduna Fichtner, Carsten Denkert, Richard Ratei, Nancy Mah, Oliver Klaas, Martin Neuenschwander, Tabea Kischka, Achim Leutz, Julia Schulz, Klaus Wethmar, Wojciech Makalowski, Esmeralda Castaños-Vélez, Jens Peter von Kries, Per-Ulf Tunn, Miguel A. Andrade-Navarro, Peter M. Schlag, and Wolfgang E. Berdel

Subjects

0301 basic medicine, Cancer Research, Multidisciplinary, lcsh:R, lcsh:Medicine, Computational biology, Biology, medicine.disease_cause, Deep sequencing, Article, 03 medical and health sciences, Open reading frame, 030104 developmental biology, medicine, Translational Activation, lcsh:Q, Ribosome profiling, Technology Platforms, Carcinogenesis, lcsh:Science, Gene, Exome sequencing, Loss function

Abstract

Ribosome profiling revealed widespread translational activity at upstream open reading frames (uORFs) and validated uORF-mediated translational control as a commonly repressive mechanism of gene expression. Translational activation of proto-oncogenes through loss-of-uORF mutations has been demonstrated, yet a systematic search for cancer-associated genetic alterations in uORFs is lacking. Here, we applied a PCR-based, multiplex identifier-tagged deep sequencing approach to screen 404 uORF translation initiation sites of 83 human tyrosine kinases and 49 other proto-oncogenes in 308 human malignancies. We identified loss-of-function uORF mutations in EPHB1 in two samples derived from breast and colon cancer, and in MAP2K6 in a sample of colon adenocarcinoma. Both mutations were associated with enhanced translation, suggesting that loss-of-uORF-mediated translational induction of the downstream main protein coding sequence may have contributed to carcinogenesis. Computational analysis of whole exome sequencing datasets of 464 colon adenocarcinomas subsequently revealed another 53 non-recurrent somatic mutations functionally deleting 22 uORF initiation and 31 uORF termination codons, respectively. These data provide evidence for somatic mutations affecting uORF initiation and termination codons in human cancer. The insufficient coverage of uORF regions in current whole exome sequencing datasets demands for future genome-wide analyses to ultimately define the contribution of uORF-mediated translational deregulation in oncogenesis.

Published

2018

24. Cxcl10

Author

Amir, Giladi, Lisa Katharina, Wagner, Hanjie, Li, Dorothea, Dörr, Chiara, Medaglia, Franziska, Paul, Anat, Shemer, Steffen, Jung, Simon, Yona, Matthias, Mack, Achim, Leutz, Ido, Amit, and Alexander, Mildner

Subjects

Central Nervous System, Phagocytes, Serum Amyloid A Protein, Encephalomyelitis, Autoimmune, Experimental, Multiple Sclerosis, Autoimmunity, Cell Differentiation, Mice, Transgenic, Dendritic Cells, Monocytes, Chemokine CXCL10, Mice, Inbred C57BL, Mice, Animals, Humans, Female, Neurogenic Inflammation, Single-Cell Analysis, Cells, Cultured, Transcription Factors

Abstract

Multiple sclerosis (MS) is characterized by pathological inflammation that results from the recruitment of lymphoid and myeloid immune cells from the blood into the brain. Due to subset heterogeneity, defining the functional roles of the various cell subsets in acute and chronic stages of MS has been challenging. Here, we used index and transcriptional single-cell sorting to characterize the mononuclear phagocytes that infiltrate the central nervous system from the periphery in mice with experimentally induced autoimmune encephalomyelitis, a model of MS. We identified eight monocyte and three dendritic cell subsets at acute and chronic disease stages in which the defined transcriptional programs pointed toward distinct functions. Monocyte-specific cell ablation identified Cxcl10

Published

2019

25. PRISMA: Protein Interaction Screen on Peptide Matrix reveals interaction footprints and modifications- dependent interactome of intrinsically disordered C/EBPb

Author

Gunnar, Dittmar, Daniel Perez, Hernandez, Elisabeth, Kowenz-Leutz, Marieluise, Kirchner, Günther, Kahlert, Radoslaw, Wesolowski, Katharina, Baum, Maria, Knoblich, Maria, Hofstätter, Arnaud, Muller, Jana, Wolf, Ulf, Reimer, and Achim, Leutz

Subjects

Proteomics, Cancer Research, Systems Biology, lcsh:Q, Technology Platforms, Transcriptomics, lcsh:Science, Article

Abstract

Summary CCAAT enhancer-binding protein beta (C/EBPβ) is a pioneer transcription factor that specifies cell differentiation. C/EBPβ is intrinsically unstructured, a molecular feature common to many proteins involved in signal processing and epigenetics. The structure of C/EBPβ differs depending on alternative translation initiation and multiple post-translational modifications (PTM). Mutation of distinct PTM sites in C/EBPβ alters protein interactions and cell differentiation, suggesting that a C/EBPβ PTM indexing code determines epigenetic outcomes. Herein, we systematically explored the interactome of C/EBPβ using an array technique based on spot-synthesized C/EBPβ-derived linear tiling peptides with and without PTM, combined with mass spectrometric proteomic analysis of protein interactions. We identified interaction footprints of ∼1,300 proteins in nuclear extracts, many with chromatin modifying, chromatin remodeling, and RNA processing functions. The results suggest that C/EBPβ acts as a multi-tasking molecular switchboard, integrating signal-dependent modifications and structural plasticity to orchestrate interactions with numerous protein complexes directing cell fate and function., Graphical Abstract, Highlights • PRISMA yields a high-resolution SLiM- and PTM-based C/EBPβ interactome • Disclosure of intrinsically disordered protein hub functions and interaction networks • New connections between C/EBPβ and RNA processing, transcription elongation, MLL, NuRD • C/EBPβ interaction with TLE3 is regulated by arginine methylation, Proteomics; Systems Biology; Transcriptomics

Published

2019

26. 216. CLASSICAL MONOCYTES PROMOTE CRESCENT FORMATION AND NECROSIS IN ANCA-ASSOCIATED NECROTIZING CRESCENTIC GLOMERULONEPHRITIS

Author

Adrian Schreiber, Achim Leutz, Alexander Mildner, Ralph Kettritz, and Anthony Rousselle

Subjects

Pathology, medicine.medical_specialty, Necrosis, Rheumatology, business.industry, Necrotizing crescentic glomerulonephritis, medicine, Pharmacology (medical), medicine.symptom, business, Idiopathic crescentic glomerulonephritis

Published

2019

27. Publisher Correction: Cxcl10+ monocytes define a pathogenic subset in the central nervous system during autoimmune neuroinflammation

Author

Hanjie Li, Dorothea Dörr, Lisa Katharina Wagner, Matthias Mack, Amir Giladi, Steffen Jung, Ido Amit, Anat Shemer, Chiara Medaglia, Simon Yona, Alexander Mildner, Franziska Paul, and Achim Leutz

Subjects

medicine.anatomical_structure, business.industry, Immunology, Central nervous system, medicine, Immunology and Allergy, CXCL10, business, Neuroscience, Neuroinflammation

Published

2020

28. Author Correction: Cxcl10+ monocytes define a pathogenic subset in the central nervous system during autoimmune neuroinflammation

Author

Alexander Mildner, Chiara Medaglia, Simon Yona, Dorothea Dörr, Anat Shemer, Amir Giladi, Lisa Katharina Wagner, Matthias Mack, Ido Amit, Franziska Paul, Steffen Jung, Achim Leutz, and Hanjie Li

Subjects

medicine.anatomical_structure, business.industry, Immunology, Central nervous system, Immunology and Allergy, Medicine, CXCL10, business, Neuroscience, Neuroinflammation

Published

2020

29. Protein Interaction Screen on Peptide Matrix (PRISMA) reveals interaction footprints and the PTM-dependent interactome of intrinsically disordered C/EBPβ

Author

Jana Wolf, Daniel Pérez-Hernández, Maria Knoblich, Arnaud Muller, E. Kowenz-Leutz, Ulf Reimer, Marieluise Kirchner, Günther Kahlert, Radoslaw Wesolowski, Achim Leutz, Katharina Baum, and Gunnar Dittmar

Subjects

Chemistry, Cellular differentiation, Epigenetics, Computational biology, Cell fate determination, Interactome, Transcription factor, Function (biology), Protein–protein interaction, Chromatin

Abstract

SummaryCCAAT enhancer binding protein beta (C/EBPβ) is a pioneer transcription factor that specifies cell differentiation. C/EBPβ is intrinsically unstructured, a molecular feature common to many proteins involved in signal processing and epigenetics. The structure of C/EBPβ differs depending on alternative translation start site usage and multiple post-translational modifications (PTM). Mutation of distinct PTM sites in C/EBPβ alters designated protein interactions and cell differentiation, suggesting a C/EBPβ PTM indexing code determines epigenetic outcomes. Herein, we systematically explored the interactome of C/EBPβ using an array of spot-synthesised C/EBPβ-derived linear tiling peptides with and without PTM, combined with mass spectrometric proteomic analysis of protein interactions. We identified interaction footprints of ~1300 proteins in nuclear cell extracts, many with chromatin modifying, remodelling and RNA processing functions. The results suggest C/EBPβ acts as a multi-tasking molecular switchboard, integrating signal-dependent modifications and structural plasticity to orchestrate interactions with numerous protein complexes directing cell fate and function.HighlightsPeptide array based interaction proteomics map SLiM and PTM dependent C/EBPβ interactomeNovel links between C/EBPβ, RNA processing, transcription elongation, MLL, NuRD were revealedC/EBPβ structure organizes modular hub function for gene regulatory machineryPRISMA is suitable to resolve protein interactions and networks based on intrinsically disordered proteins

Published

2017

30. Deficiency in <scp>mTORC</scp> 1‐controlled C/ <scp>EBP</scp> β ‐ <scp>mRNA</scp> translation improves metabolic health in mice

Author

Tobias Ackermann, Gertrud Kortman, Götz Hartleben, Zhao-Qi Wang, Julia von Maltzahn, Nahum Sonenberg, Achim Leutz, Michael Kiehntopf, Christine Müller, Sabrina Eichwald, Cornelis F. Calkhoven, and Laura M Zidek

Subjects

Calorie restriction, P70-S6 Kinase 1, Translation (biology), mTORC1, Biology, Biochemistry, Open reading frame, Enhancer binding, Ribosomal protein s6, Upstream open reading frame, Genetics, biological phenomena, cell phenomena, and immunity, Molecular Biology

Abstract

The mammalian target of rapamycin complex 1 (mTORC1) is a central regulator of physiological adaptations in response to changes in nutrient supply. Major downstream targets of mTORC1 signalling are the mRNA translation regulators p70 ribosomal protein S6 kinase 1 (S6K1p70) and the 4E-binding proteins (4E-BPs). However, little is known about vertebrate mRNAs that are specifically controlled by mTORC1 signalling and are engaged in regulating mTORC1-associated physiology. Here, we show that translation of the CCAAT/enhancer binding protein beta (C/EBPβ) mRNA into the C/EBPβ-LIP isoform is suppressed in response to mTORC1 inhibition either through pharmacological treatment or through calorie restriction. Our data indicate that the function of 4E-BPs is required for suppression of LIP. Intriguingly, mice lacking the cis-regulatory upstream open reading frame (uORF) in the C/EBPβ-mRNA, which is required for mTORC1-stimulated translation into C/EBPβ-LIP, display an improved metabolic phenotype with features also found under calorie restriction. Thus, our data suggest that translational adjustment of C/EBPβ-isoform expression is one of the key processes that direct metabolic adaptation in response to changes in mTORC1 activity.

Published

2015

31. A High Content Screening Assay for Evaluation of Biomaterial-Mediated Cell Fusion Processes

Author

Andreas Lendlein, Manfred Gossen, Axel T. Neffe, Benjamin F. Pierce, J Görs, Bart Rijckaert, Jeske J. Smink, Achim Leutz, T. Gebauer, and Toralf Roch

Subjects

Cell fusion, Materials science, Polymers and Plastics, Organic Chemistry, Biomaterial, Condensed Matter Physics, Regenerative medicine, Bone resorption, Cell biology, medicine.anatomical_structure, Tissue engineering, Osteoclast, High-content screening, Materials Chemistry, medicine, Bone regeneration

Abstract

Summary Biomaterials are of increasing importance in regenerative medicine and entail delivery systems in somatic cell therapies, matrices for tissue engineering or tissue regeneration. The evaluation of biomaterial induced biological effects remains a key issue in clinical application. Cell-based assays for potential cytotoxic and immunological responses have been developed but are often inadequate to address cell-type specific responses to biomaterials. To quantitatively monitor attachment, survival, proliferation and fusion-controlled differentiation of osteoclasts (bone resorbing cells), a High Content Screening (HCS) assay has been developed based on osteoclast differentiation of the murine monocytic cell line RAW 264.7. This assay was applied to investigate the influence of degradation products of polymers from gelatin and lysine diisocyanate, which display tailorable mechanical properties and have potential as biomaterials. The data show that the degradation products inhibit formation of multinuclear osteoclasts and suggest a potential support of bone regeneration by suppression of bone resorption.

Published

2014

32. uORFdb—a comprehensive literature database on eukaryotic uORF biology

Author

Miguel A. Andrade-Navarro, Adriano Barbosa-Silva, Achim Leutz, and Klaus Wethmar

Subjects

I. Nucleic acid sequence, structure and regulation, Five prime untranslated region, RNA Stability, Nonsense-mediated decay, Biology, computer.software_genre, Mice, Open Reading Frames, Upstream open reading frame, Genetics, Animals, Humans, Coding region, Disease, RNA, Messenger, ORFS, Promoter Regions, Genetic, Gene, Internet, Database, Genetic Variation, Translation (biology), Nonsense Mediated mRNA Decay, Alternative Splicing, Open reading frame, Protein Biosynthesis, Databases, Nucleic Acid, Ribosomes, computer

Abstract

Approximately half of all human transcripts contain at least one upstream translational initiation site that precedes the main coding sequence (CDS) and gives rise to an upstream open reading frame (uORF). We generated uORFdb, publicly available at http://cbdm.mdc-berlin.de/tools/uorfdb, to serve as a comprehensive literature database on eukaryotic uORF biology. Upstream ORFs affect downstream translation by interfering with the unrestrained progression of ribosomes across the transcript leader sequence. Although the first uORF-related translational activity was observed >30 years ago, and an increasing number of studies link defective uORF-mediated translational control to the development of human diseases, the features that determine uORF-mediated regulation of downstream translation are not well understood. The uORFdb was manually curated from all uORF-related literature listed at the PubMed database. It categorizes individual publications by a variety of denominators including taxon, gene and type of study. Furthermore, the database can be filtered for multiple structural and functional uORF-related properties to allow convenient and targeted access to the complex field of eukaryotic uORF biology.

Published

2013

33. PU.1 Level-Directed Chromatin Structure Remodeling at the Irf8 Gene Drives Dendritic Cell Commitment

Author

Josef Priller, Carol Stocking, Miguel A. Andrade-Navarro, Frank Rosenbauer, Francisco Fernández Klett, Gang Huang, Marie Luise Gebhardt, Pia Riemke, Marina Scheller, Achim Leutz, Jörg Schönheit, Ronald Naumann, and Christiane Kuhl

Subjects

Cancer Research, Lineage (genetic), Myeloid, Bone Marrow Cells, Biology, General Biochemistry, Genetics and Molecular Biology, Chromatin remodeling, Mice, Proto-Oncogene Proteins, medicine, Animals, Humans, Cell Lineage, Myeloid Cells, Promoter Regions, Genetic, lcsh:QH301-705.5, Transcription factor, Cells, Cultured, Mice, Knockout, Base Sequence, Cell Differentiation, Dendritic Cells, Dendritic cell, Chromatin Assembly and Disassembly, Chromatin, Mice, Inbred C57BL, medicine.anatomical_structure, lcsh:Biology (General), Interferon Regulatory Factors, Trans-Activators, Cancer research, IRF8, Reprogramming

Abstract

SummaryDendritic cells (DCs) are essential regulators of immune responses; however, transcriptional mechanisms that establish DC lineage commitment are poorly defined. Here, we report that the PU.1 transcription factor induces specific remodeling of the higher-order chromatin structure at the interferon regulatory factor 8 (Irf8) gene to initiate DC fate choice. An Irf8 reporter mouse enabled us to pinpoint an initial progenitor stage at which DCs separate from other myeloid lineages in the bone marrow. In the absence of Irf8, this progenitor undergoes DC-to-neutrophil reprogramming, indicating that DC commitment requires an active, Irf8-dependent escape from alternative myeloid lineage potential. Mechanistically, myeloid Irf8 expression depends on high PU.1 levels, resulting in local chromosomal looping and activation of a lineage- and developmental-stage-specific cis-enhancer. These data delineate PU.1 as a concentration-dependent rheostat of myeloid lineage selection by controlling long-distance contacts between regulatory elements and suggest that specific higher-order chromatin remodeling at the Irf8 gene determines DC differentiation.

Published

2013

34. DNA methylation protects hematopoietic stem cell multipotency from myeloerythroid restriction

Author

Marco Prinz, Christiane Kuhl, Elena Mancini, Shabnam Kharazi, Ann-Marie Bröske, Rudolf Jaenisch, Andreas Enns, Miguel A. Andrade-Navarro, Sten Eirik W. Jacobsen, Frank Rosenbauer, Matthew R. Huska, Lena Vockentanz, Achim Leutz, Marina Scheller, and Claus Nerlov

Subjects

DNA (Cytosine-5-)-Methyltransferase 1, Cell Survival, Cellular differentiation, Biology, DNA methyltransferase, Epigenesis, Genetic, Mice, Erythroid Cells, Genetics, medicine, Animals, Homeostasis, Cell Lineage, Epigenetics, DNA (Cytosine-5-)-Methyltransferases, Leukemia, Multipotent Stem Cells, Hematopoietic stem cell, Cell Differentiation, DNA Methylation, Hematopoietic Stem Cells, Molecular biology, Cell biology, Hematopoiesis, medicine.anatomical_structure, Gene Expression Regulation, Multipotent Stem Cell, DNA methylation, Neoplastic Stem Cells, Stem cell, Reprogramming

Abstract

DNA methylation is a dynamic epigenetic mark that undergoes extensive changes during differentiation of self-renewing stem cells. However, whether these changes are the cause or consequence of stem cell fate remains unknown. Here, we show that alternative functional programs of hematopoietic stem cells (HSCs) are governed by gradual differences in methylation levels. Constitutive methylation is essential for HSC self-renewal but dispensable for homing, cell cycle control and suppression of apoptosis. Notably, HSCs from mice with reduced DNA methyltransferase 1 activity cannot suppress key myeloerythroid regulators and thus can differentiate into myeloerythroid, but not lymphoid, progeny. A similar methylation dosage effect controls stem cell function in leukemia. These data identify DNA methylation as an essential epigenetic mechanism to protect stem cells from premature activation of predominant differentiation programs and suggest that methylation dynamics determine stem cell functions in tissue homeostasis and cancer.

Published

2016

35. Comprehensive translational control of tyrosine kinase expression by upstream open reading frames

Author

Enrique M. Muro, Sweta Talyan, Miguel A. Andrade-Navarro, Achim Leutz, Klaus Wethmar, and Julia Schulz

Subjects

0301 basic medicine, Cancer Research, Five prime untranslated region, Kozak consensus sequence, Short Communication, Biology, medicine.disease_cause, Proto-Oncogene Mas, Gene Expression Regulation, Enzymologic, 03 medical and health sciences, Open Reading Frames, Eukaryotic translation, Upstream open reading frame, Genetics, medicine, Humans, Gene Regulatory Networks, Molecular Biology, Mutation, Gene Expression Profiling, Translation (biology), Protein-Tyrosine Kinases, Open reading frame, 030104 developmental biology, HEK293 Cells, Protein Biosynthesis, Human genome, HeLa Cells

Abstract

Post-transcriptional control has emerged as a major regulatory event in gene expression and often occurs at the level of translation initiation. Although overexpression or constitutive activation of tyrosine kinases (TKs) through gene amplification, translocation or mutation are well-characterized oncogenic events, current knowledge about translational mechanisms of TK activation is scarce. Here, we report the presence of translational cis-regulatory upstream open reading frames (uORFs) in the majority of transcript leader sequences of human TK mRNAs. Genetic ablation of uORF initiation codons in TK transcripts resulted in enhanced translation of the associated downstream main protein-coding sequences (CDSs) in all cases studied. Similarly, experimental removal of uORF start codons in additional non-TK proto-oncogenes, and naturally occurring loss-of-uORF alleles of the c-met proto-oncogene (MET) and the kinase insert domain receptor (KDR), was associated with increased CDS translation. Based on genome-wide sequence analyses we identified polymorphisms in 15.9% of all human genes affecting uORF initiation codons, associated Kozak consensus sequences or uORF-related termination codons. Together, these data suggest a comprehensive role of uORF-mediated translational control and delineate how aberrant induction of proto-oncogenes through loss-of-function mutations at uORF initiation codons may be involved in the etiology of cancer. We provide a detailed map of uORFs across the human genome to stimulate future research on the pathogenic role of uORFs.

Published

2016

36. Tal1 regulates osteoclast differentiation through suppression of the master regulator of cell fusion DC‐STAMP

Author

Joachim R. Göthert, Nadine Courtial, Olga N. Kuvardina, Achim Leutz, Jeske J. Smink, and Jörn Lausen

Subjects

musculoskeletal diseases, Medizin, Regulator, Gene Expression, Osteoclasts, Mice, Transgenic, Nerve Tissue Proteins, Biology, Biochemistry, Bone and Bones, Cell Fusion, Mice, Osteoclast, Proto-Oncogene Proteins, Basic Helix-Loop-Helix Transcription Factors, Genetics, medicine, Animals, RNA, Small Interfering, Promoter Regions, Genetic, Molecular Biology, Transcription factor, Cells, Cultured, T-Cell Acute Lymphocytic Leukemia Protein 1, Regulation of gene expression, Microphthalmia-Associated Transcription Factor, Binding Sites, Cell fusion, Base Sequence, Membrane Proteins, Cell Differentiation, Microphthalmia-associated transcription factor, Hematopoiesis, medicine.anatomical_structure, Gene Knockdown Techniques, Trans-Activators, Cancer research, Bone Remodeling, Stem cell, Biotechnology, TAL1

Abstract

The balance between bone-forming osteoblasts and bone-resorbing osteoclasts is crucial to bone homeostasis, an equilibrium that is disturbed in many bone diseases. The transcription factor Tal1 is involved in the establishment of hematopoietic stem cells in the embryo and is a master regulator of hematopoietic gene expression in the adult. Here, we show that Tal1 is expressed in osteoclasts and that loss of Tal1 in osteoclast progenitors leads to altered expression of >1200 genes. We found that DC-STAMP, a key regulator of osteoclast cell fusion, is a direct target gene of Tal1 and show that Tal1 represses DC-STAMP expression by counteracting the activating function of the transcription factors PU.1 and MITF. The identification of Tal1 as a factor involved in cell fusion contributes to the understanding of osteoclast-associated diseases, including osteoporosis.—Courtial, N., Smink, J. J., Kuvardina, O. N., Leutz, A., Gothert, J. R., Lausen, J. Tal1 regulates osteoclast differentiation through suppression ...

Published

2011

37. Crosstalk between phosphorylation and multi-site arginine/lysine methylation in C/EBPs

Author

Ole Pless, Achim Leutz, Elisabeth Kowenz-Leutz, Gunnar Dittmar, and Michael Lappe

Subjects

Arginine, Molecular Sequence Data, Lysine, Biology, Methylation, Biochemistry, Chromatin remodeling, Cell Physiological Phenomena, Gene expression, CCAAT-Enhancer-Binding Protein-alpha, Genetics, Animals, Humans, Protein Isoforms, Histone code, Amino Acid Sequence, Point-of-View, Phosphorylation, Binding Sites, Sequence Homology, Amino Acid, CCAAT-Enhancer-Binding Protein-beta, Crosstalk (biology), Mutation, Female, Biotechnology

Abstract

C/EBPs are implied in an amazing number of cellular functions: C/EBPs regulate tissue and cell type specific gene expression, proliferation, and differentiation control. C/EBPs assist in energy metabolism, female reproduction, innate immunity, inflammation, senescence, and the development of neoplasms. How can C/EBPs fulfill so many functions? Here we discuss that C/EBPs are extensively modified by methylation of arginine and lysine side chains and that regulated methylation profoundly affects the activity of C/EBPs.

Published

2011

38. Targets of the Tal1 Transcription Factor in Erythrocytes

Author

Fransisca Leonard, Ole Pless, Benjamin Koch, Olga N. Kuvardina, Achim Leutz, and Jörn Lausen

Subjects

Cellular differentiation, GATA2, Cell Biology, Ubiquitin-conjugating enzyme, Biology, Biochemistry, Molecular biology, Chromatin, Cell biology, Erythropoiesis, Molecular Biology, Chromatin immunoprecipitation, Transcription factor, TAL1

Abstract

The Tal1 transcription factor is essential for the development of the hematopoietic system and plays a role during definitive erythropoiesis in the adult. Despite the importance of Tal1 in erythropoiesis, only a small number of erythroid differentiation target genes are known. A chromatin precipitation and cloning approach was established to uncover novel Tal1 target genes in erythropoiesis. The BirA tag/BirA ligase biotinylation system in combination with streptavidin chromatin precipitation (Strep-CP) was used to co-precipitate genomic DNA bound to Tal1. Tal1 was found to bind in the vicinity of 31 genes including the E2-ubiquitin conjugase UBE2H gene. Binding of Tal1 to UBE2H was confirmed by chromatin immunoprecipitation. UBE2H expression is increased during erythroid differentiation of hCD34+ cells. Tal1 expression activated UBE2H expression, whereas Tal1 knock-down reduced UBE2H expression and ubiquitin transfer activity. This study identifies parts of the ubiquitinylation machinery as a cellular target downstream of the transcription factor Tal1 and provides novel insights into Tal1-regulated erythropoiesis.

Published

2010

39. C/EBPβΔuORF mice—a genetic model for uORF-mediated translational control in mammals

Author

Valérie Bégay, Bernd Dörken, Achim Leutz, Klaus Wethmar, Volker Wiesenthal, Katrin Zaragoza, Cornelis F. Calkhoven, and Jeske J. Smink

Subjects

Male, Biology, medicine.disease_cause, Upstream ORF, liver regeneration, C/EBPb, cell cycle, translational control, Transcriptome, Mice, Open Reading Frames, Research Communication, Eukaryotic translation, Genetic model, Genetics, medicine, Animals, Gene, Regulation of gene expression, Mutation, CCAAT-Enhancer-Binding Protein-beta, Cell Cycle, Translation (biology), Open reading frame, Gene Expression Regulation, Liver, Models, Animal, Female, Developmental Biology

Abstract

Upstream ORFs (uORFs) are translational control elements found predominantly in transcripts of key regulatory genes. No mammalian genetic model exists to experimentally validate the physiological relevance of uORF-regulated translation initiation. We report that mice deficient for the CCAAT/enhancer-binding protein β (C/EBPβ) uORF initiation codon fail to initiate translation of the autoantagonistic LIP (liver inhibitory protein) C/EBPβ isoform. C/EBPβΔuORF mice show hyperactivation of acute-phase response genes, persistent repression of E2F-regulated genes, delayed and blunted S-phase entry of hepatocytes after partial hepatectomy, and impaired osteoclast differentiation. These data and the widespread prevalence of uORFs in mammalian transcriptomes suggest a comprehensive role of uORF-regulated translation in (patho)physiology.

Published

2010

40. Crosstalk between C/EBPβ phosphorylation, arginine methylation, and SWI/SNF/Mediator implies an indexing transcription factor code

Author

Achim Leutz, Maria Knoblich, Gunnar Dittmar, Ole Pless, and Elisabeth Kowenz-Leutz

Subjects

Protein-Arginine N-Methyltransferases, CARM1, Chromosomal Proteins, Non-Histone, Molecular Sequence Data, chromatin remodelling, Biology, Arginine, Methylation, General Biochemistry, Genetics and Molecular Biology, Article, Transactivation, Mice, Animals, Epigenetics, Amino Acid Sequence, signalling, Phosphorylation, Molecular Biology, Transcription factor, Regulation of gene expression, General Immunology and Microbiology, Ccaat-enhancer-binding proteins, General Neuroscience, CCAAT-Enhancer-Binding Protein-beta, differentiation, Molecular biology, SWI/SNF, post-translational modification, histone code, biological phenomena, cell phenomena, and immunity, hormones, hormone substitutes, and hormone antagonists, Signal Transduction, Transcription Factors

Abstract

Cellular signalling cascades regulate the activity of transcription factors that convert extracellular information into gene regulation. C/EBPbeta is a ras/MAPkinase signal-sensitive transcription factor that regulates genes involved in metabolism, proliferation, differentiation, immunity, senescence, and tumourigenesis. The protein arginine methyltransferase 4 PRMT4/CARM1 interacts with C/EBPbeta and dimethylates a conserved arginine residue (R3) in the C/EBPbeta N-terminal transactivation domain, as identified by mass spectrometry of cell-derived C/EBPbeta. Phosphorylation of the C/EBPbeta regulatory domain by ras/MAPkinase signalling abrogates the interaction between C/EBPbeta and PRMT4/CARM1. Differential proteomic screening, protein interaction studies, and mutational analysis revealed that methylation of R3 constraines interaction with SWI/SNF and Mediator complexes. Mutation of the R3 methylation site alters endogenous myeloid gene expression and adipogenic differentiation. Thus, phosphorylation of the transcription factor C/EBPbeta couples ras signalling to arginine methylation and regulates the interaction of C/EBPbeta with epigenetic gene regulatory protein complexes during cell differentiation.

Published

2010

41. Rapamycin and the transcription factor C/EBPβ as a switch in osteoclast differentiation: implications for lytic bone diseases

Author

Achim Leutz and Jeske J. Smink

Subjects

Gene isoform, medicine.medical_specialty, Bone density, Osteoporosis, Osteoclasts, Review, Biology, Bone remodeling, Osteoclast, Internal medicine, Enhancer binding, Drug Discovery, medicine, Animals, Humans, Genetics(clinical), Rapamycin, Transcription factor, Genetics (clinical), PI3K/AKT/mTOR pathway, Cancer, Sirolimus, Medicine(all), Leukemia, CCAAT-Enhancer-Binding Protein-beta, Cell Differentiation, medicine.disease, MafB, Cell biology, Endocrinology, medicine.anatomical_structure, C/EBPβ, Molecular Medicine, Bone Diseases

Abstract

Lytic bone diseases and in particular osteoporosis are common age-related diseases characterized by enhanced bone fragility due to loss of bone density. Increasingly, osteoporosis poses a major global health-care problem due to the growth of the elderly population. Recently, it was found that the gene regulatory transcription factor CCAAT/enhancer binding protein beta (C/EBPbeta) is involved in bone metabolism. C/EBPbeta occurs as different protein isoforms of variable amino terminal length, and regulation of the C/EBPbeta isoform ratio balance was found to represent an important factor in osteoclast differentiation and bone homeostasis. Interestingly, adjustment of the C/EBPbeta isoform ratio by the process of translational control is downstream of the mammalian target of rapamycin kinase (mTOR), a sensor of the nutritional status and a target of immunosuppressive and anticancer drugs. The findings imply that modulating the process of translational control of C/EBPbeta isoform expression could represent a novel therapeutic approach in osteolytic bone diseases, including cancer and infection-induced bone loss.

Published

2009

42. Functional interaction of CCAAT/enhancer-binding-protein-α basic region mutants with E2F transcription factors and DNA

Author

Elisabeth Kowenz-Leutz, Qingbin Liu, Udo Heinemann, Anja Schuetz, Maria Knoblich, and Achim Leutz

Subjects

0301 basic medicine, Models, Molecular, Mutant, Molecular Sequence Data, Biophysics, Biology, Biochemistry, Protein Structure, Secondary, 03 medical and health sciences, Transactivation, Mice, Structural Biology, Genetics, E2F1, Animals, Humans, Protein Interaction Domains and Motifs, Amino Acid Sequence, E2F, Molecular Biology, Transcription factor, Cells, Cultured, Ccaat-enhancer-binding proteins, Sequence Homology, Amino Acid, Point mutation, DNA, Molecular biology, E2F Transcription Factors, 030104 developmental biology, HEK293 Cells, CCAAT-Enhancer-Binding Proteins, Mutant Proteins, Protein Binding

Abstract

The transcription factor CCAAT/enhancer-binding protein α (C/EBPα) regulates cell cycle arrest and terminal differentiation of neutrophils and adipocytes. Mutations in the basic leucine zipper domain (bZip) of C/EBPα are associated with acute myeloid leukemia. A widely used murine transforming C/EBPα basic region mutant (BRM2) entails two bZip point mutations (I294A/R297A). BRM2 has been discordantly described as defective for DNA binding or defective for interaction with E2F. We have separated the two BRM2 mutations to shed light on the intertwined reciprocity between C/EBPα-E2F-DNA interactions. Both, C/EBPα I294A and R297A retain transactivation capacity and interaction with E2F-DP. The C/EBPα R297A mutation destabilized DNA binding, whereas the C/EBPα I294A mutation enhanced binding to DNA. The C/EBPα R297A mutant, like BRM2, displayed enhanced interaction with E2F-DP but failed to repress E2F-dependent transactivation although both mutants were readily suppressed by E2F1 for transcription through C/EBP cis-regulatory sites. In contrast, the DNA binding enhanced C/EBPα I294A mutant displayed increased repression of E2F-DP mediated transactivation and resisted E2F-DP mediated repression. Thus, the efficient repression of E2F dependent S-phase genes and the activation of differentiation genes reside in the balanced DNA binding capacity of C/EBPα.

Published

2015

43. Lymphoid cell growth and transformation are suppressed by a key regulatory element of the gene encoding PU.1

Author

Christoph Plass, Daniel G. Tenen, Björn Hackanson, Linda K. Clayton, Joseph R. Tumang, Koichi Akashi, Bronwyn M. Owens, Achim Leutz, Ulrich Steidl, Katharina Wagner, Marina Scheller, Li Yu, Hiromi Iwasaki, Chunhui Liu, Frank Rosenbauer, Thomas L. Rothstein, and Jeffery L. Kutok

Subjects

T cell, Repressor, Mice, Transgenic, Mice, SCID, Thymus Gland, Regulatory Sequences, Nucleic Acid, Biology, Lymphoma, T-Cell, medicine.disease_cause, Mice, Proto-Oncogene Proteins, Genetics, medicine, Animals, Lymphocytes, Promoter Regions, Genetic, Enhancer, Transcription factor, beta Catenin, Regulation of gene expression, B-Lymphocytes, Stem Cells, Wnt signaling pathway, DNA Methylation, Molecular biology, Wnt Proteins, Cell Transformation, Neoplastic, medicine.anatomical_structure, Gene Expression Regulation, DNA methylation, Trans-Activators, Thy-1 Antigens, TCF Transcription Factors, Carcinogenesis, Signal Transduction

Abstract

Tight regulation of transcription factors, such as PU.1, is crucial for generation of all hematopoietic lineages. We previously reported that mice with a deletion of an upstream regulatory element (URE) of the gene encoding PU.1 (Sfpi1) developed acute myeloid leukemia. Here we show that the URE has an essential role in orchestrating the dynamic PU.1 expression pattern required for lymphoid development and tumor suppression. URE deletion ablated B2 cells but stimulated growth of B1 cells in mice. The URE was a PU.1 enhancer in B cells but a repressor in T cell precursors. TCF transcription factors coordinated this repressor function and linked PU.1 to Wnt signaling. Failure of appropriate PU.1 repression in T cell progenitors with URE deletion disrupted differentiation and induced thymic transformation. Genome-wide DNA methylation assessment showed that epigenetic silencing of selective tumor suppressor genes completed PU.1-initiated transformation of lymphoid progenitors with URE deletion. These results elucidate how a single transcription factor, PU.1, through the cell context-specific activity of a key cis-regulatory element, affects the development of multiple cell lineages and can induce cancer.

Published

2005

44. A rapamycin derivative (everolimus) controls proliferation through down-regulation of truncated CCAAT enhancer binding protein {beta} and NF-{kappa}B activity in Hodgkin and anaplastic large cell lymphomas

Author

Franziska Jundt, Nina Raetzel, Cornelis F. Calkhoven, Andreas Lietz, Stephan Mathas, Katharina Kley, Achim Leutz, Bernd Dörken, Christine Müller, and Stem Cell Aging Leukemia and Lymphoma (SALL)

Subjects

Lymphoma, Transplantation, Heterologous, Immunology, Down-Regulation, Mice, SCID, Biology, SCID, Biochemistry, Cell Line, Mice, Mice, Inbred NOD, Cell Line, Tumor, hemic and lymphatic diseases, medicine, Large B-Cell, Animals, Humans, Everolimus, Anaplastic large-cell lymphoma, Transcription factor, PI3K/AKT/mTOR pathway, Cell Proliferation, Sirolimus, Transplantation, Heterologous, Tumor, Cell growth, CCAAT-Enhancer-Binding Protein-beta, Cell Cycle, NF-kappa B, Cell Biology, Hematology, Cell cycle, medicine.disease, NFKB1, Molecular biology, Hodgkin Disease, Diffuse, Inbred NOD, Lymphoma, Large B-Cell, Diffuse, medicine.drug

Abstract

The immunosuppressive macrolide rapamycin and its derivative everolimus (SDZ RAD, RAD) inhibit the mammalian target of rapamycin (mTOR) signaling pathway. In this study, we provide evidence that RAD has profound antiproliferative activity in vitro and in NOD/SCID mice in vivo against Hodgkin lymphoma (HL) and anaplastic large cell lymphoma (ALCL) cells. Moreover, we identified 2 molecular mechanisms that showed how RAD exerts antiproliferative effects in HL and ALCL cells. RAD down-regulated the truncated isoform of the transcription factor CCAAT enhancer binding protein β (C/EBPβ), which is known to disrupt terminal differentiation and induce a transformed phenotype. Furthermore, RAD inhibited constitutive nuclear factor κB (NF-κB) activity, which is a critical survival factor of HL cells. Pharmacologic inhibition of the mTOR pathway by RAD therefore interferes with essential proliferation and survival pathways in HL and ALCL cells and might serve as a novel treatment option. (Blood. 2005;106: 1801-1807)

Published

2005

45. Essential Requirement of CCAAT/Enhancer Binding Proteins in Embryogenesis

Author

Achim Leutz, Jeske J. Smink, and Valérie Bégay

Subjects

Genetic Markers, Placenta, Gene Expression, In situ hybridization, Biology, Fetal Development, Mice, Pregnancy, Enhancer binding, Gene expression, CCAAT-Enhancer-Binding Protein-alpha, Animals, Cell Growth and Development, Fetal Death, Molecular Biology, Transcription factor, reproductive and urinary physiology, In Situ Hybridization, Mice, Knockout, Base Sequence, Ccaat-enhancer-binding proteins, CCAAT-Enhancer-Binding Protein-beta, Embryogenesis, Embryo, DNA, Cell Biology, Molecular biology, embryonic structures, Female, Haploinsufficiency

Abstract

The CCAAT/enhancer binding proteins C/EBPalpha and C/EBPbeta are related transcription factors that are important for the function of various organs in the postnatal mouse. Gene replacement and tissue culture experiments have suggested partial redundancy of both transcription factors. Here we show that mouse embryos deficient of both C/EBPalpha and C/EBPbeta (C/EBPalphabeta(-/-)) die between embryonic day 10 (E10) and E11 and display defective placentas. In situ hybridization revealed that C/EBPalpha and C/EBPbeta are coexpressed in the chorionic plate at E9.5 and later in the trophoblasts of the labyrinthine layer. In C/EBPalphabeta(-/-) placentas, allantoic blood vessels invaded the chorion; however, vessel expansion and development of the labyrinthine layer was impaired. Furthermore, a single copy of either C/EBPalpha in the absence of C/EBPbeta or C/EBPbeta in the absence of C/EBPalpha is sufficient to complete development, suggesting complementation of these C/EBPs during embryogenesis. A single copy of C/EBPalpha in the absence of C/EBPbeta, however, fails to rescue survival after birth, suggesting haploinsufficiency of C/EBPalpha in newborns. Our data thus reveal novel essential, redundant, and dosage dependent functions of C/EBPs.

Published

2004

46. Ras Induces Mediator Complex Exchange on C/EBPβ

Author

Elisabeth Kowenz-Leutz, Xianming Mo, Hong Xu, and Achim Leutz

Subjects

Transcriptional Activation, MAPK/ERK pathway, Transcription, Genetic, MAP Kinase Signaling System, Protein Conformation, Recombinant Fusion Proteins, Repressor, Apoptosis, RNA polymerase II, Biology, MED1, Transactivation, Mediator, Genes, Reporter, Humans, Transcription factor, Molecular Biology, Glutathione Transferase, Models, Genetic, CCAAT-Enhancer-Binding Protein-beta, Cell Biology, Cyclin-Dependent Kinase 8, Precipitin Tests, Molecular biology, Chromatin, Cyclin-Dependent Kinases, Protein Structure, Tertiary, Enzyme Activation, Mutation, Trans-Activators, ras Proteins, biology.protein, RNA, Cyclin-dependent kinase 8, RNA Polymerase II, HeLa Cells, Protein Binding, Signal Transduction

Abstract

C/EBPbeta is an intrinsically repressed transcription factor that regulates genes involved in differentiation, proliferation, tumorigenesis, and apoptosis. C/EBPbeta acts as a repressor that is turned into an activator by the Ras oncoprotein through phosphorylation of a MAPK site. C/EBPbeta activation is accompanied by a conformational change. Active and repressive C/EBPbeta interacts with multisubunit Mediator complexes through the CRSP130/Sur2 subunit. The CRSP130/Sur2 subunit is common to two distinct types of Mediator complexes, characterized by CRSP70 and CDK8 proteins as transcriptionally active and inactive Mediator, respectively. Knockdown of CRSP130/Sur2 prevents Mediator binding and transactivation through C/EBPbeta. Oncogenic Ras signaling or activating mutations in C/EBPbeta selects the transcriptionally active Mediator complex that also associates with RNA polymerase II. These results show that a Ras-induced structural alteration of C/EBPbeta determines differential gene activation through selective interaction with distinct Mediator complexes.

Published

2004

47. Über Ortungs- und Navigationsverfahren bei Tieren : Ein komplexes natürliches Ortungs- und Navigationsverfahren dargestellt am Beispiel der Honigbiene

Author

Achim Leutz and Achim Leutz

Subjects

Social sciences, Humanities

Published

2013

48. Distinct changes in gene expression induced by A-Myb, B-Myb and c-Myb proteins

Author

John J. Rushton, Xianming Mo, Lisa M. Davis, Wanli Lei, Achim Leutz, and Scott A. Ness

Subjects

Cancer Research, Cell Cycle Proteins, Biology, Adenoviridae, Proto-Oncogene Proteins c-myb, Transcription (biology), Proto-Oncogene Proteins, Gene expression, Genetics, Humans, MYB, Breast, Molecular Biology, Transcription factor, Cells, Cultured, Cell Line, Transformed, Oligonucleotide Array Sequence Analysis, Regulation of gene expression, Reporter gene, Epithelial Cells, Promoter, DNA-Binding Proteins, Gene Expression Regulation, Trans-Activators, Keratins, Female, DNA microarray

Abstract

The c-Myb, A-Myb and B-Myb transcription factors have nearly identical DNA-binding domains, activate the same reporter gene constructs in animal cells, but have different biological roles. The Myb proteins are often coexpressed in the same cells, raising questions about whether they activate similar or distinct gene expression profiles, and whether they cooperate or compete in regulating the same promoters. Here, recombinant adenoviruses were used to express each protein in human mammary cells, and then microarray assays were used to assess global changes in gene expression. Each Myb protein induced a unique and specific set of changes, displaying activities far more complex than revealed by standard reporter gene assays. These results have important implications for the roles of various Myb proteins in normal and transformed human cells, for regulatory pathways that might modify their activities and for the importance of acquired mutations that may qualitatively alter their functions in tumors.

Published

2003

49. The Conserved Mynd Domain of BS69 Binds Cellular and Oncoviral Proteins through a Common PXLXP Motif

Author

Stéphane Ansieau and Achim Leutz

Subjects

Transcriptional Activation, DNA, Complementary, Transcription, Genetic, Recombinant Fusion Proteins, viruses, Amino Acid Motifs, Molecular Sequence Data, Cell Cycle Proteins, Plasma protein binding, Transfection, Binding, Competitive, Biochemistry, DNA-binding protein, Adenoviridae, Conserved sequence, Viral Proteins, Protein structure, Transcription (biology), Two-Hybrid System Techniques, Basic Helix-Loop-Helix Transcription Factors, Animals, Humans, Amino Acid Sequence, Caenorhabditis elegans, Molecular Biology, Peptide sequence, Conserved Sequence, Glutathione Transferase, Genetics, Sequence Homology, Amino Acid, biology, Cell Biology, biology.organism_classification, Precipitin Tests, Protein Structure, Tertiary, Cell biology, DNA-Binding Proteins, Epstein-Barr Virus Nuclear Antigens, Adenovirus E1A Proteins, Carrier Proteins, Peptides, Co-Repressor Proteins, Gene Deletion, HeLa Cells, Plasmids, Protein Binding, Transcription Factors

Abstract

BS69 is a transcriptional co-repressor protein and a potential tumor suppressor that binds to the adenoviral oncoprotein E1A. We show that the C-terminal Mynd domain of BS69 (amino acids 516-561) or the closely related Mynd domains of the Caenorhabditis elegans proteins Bra-1 and Bra-2 bind not only to E1A but also to the Epstein-Barr virus EBNA2 oncoprotein and the Myc-related cellular protein MGA. Interaction depends on intact PXLXP motifs present in all three proteins. Moreover, viral proteins compete for binding of BS69 to MGA in a PXLXP-dependent fashion. Because deletions in E1A or EBNA2 that cover the PXLXP motifs are non-transforming, our observations suggest a role for BS69 in cell growth control that is reminiscent of abrogation of the Rb function by various oncoproteins.

Published

2002

50. Genomic Characterization of Murine Monocytes Reveals C/EBPβ Transcription Factor Dependence of Ly6C − Cells

Author

Franziska Paul, Jörg Schönheit, Eyal David, Josef Priller, David Lara-Astiaso, Steffen Jung, Ido Amit, Erika Lorenzo-Vivas, Louise Chappell-Maor, Alexander Mildner, Amir Giladi, and Achim Leutz

Subjects

Male, 0301 basic medicine, Cellular differentiation, Immunology, Population, Bone Marrow Cells, Monocyte-Macrophage Precursor Cells, Biology, Monocytes, Epigenesis, Genetic, Immunophenotyping, Mice, 03 medical and health sciences, 0302 clinical medicine, Nuclear Receptor Subfamily 4, Group A, Member 1, medicine, Animals, Antigens, Ly, Cluster Analysis, Immunology and Allergy, Promoter Regions, Genetic, Enhancer, education, Transcription factor, Mice, Knockout, education.field_of_study, CCAAT-Enhancer-Binding Protein-beta, Gene Expression Profiling, Monocyte, High-Throughput Nucleotide Sequencing, Cell Differentiation, Genomics, Molecular biology, Transplantation, Phenotype, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, Gene Expression Regulation, Monocyte differentiation, Female, Biomarkers, 030217 neurology & neurosurgery, Protein Binding

Abstract

Monocytes are circulating, short-lived mononuclear phagocytes, which in mice and man comprise two main subpopulations. Murine Ly6C+ monocytes display developmental plasticity and are recruited to complement tissue-resident macrophages and dendritic cells on demand. Murine vascular Ly6C- monocytes patrol the endothelium, act as scavengers, and support vessel wall repair. Here we characterized population and single cell transcriptomes, as well as enhancer and promoter landscapes of the murine monocyte compartment. Single cell RNA-seq and transplantation experiments confirmed homeostatic default differentiation of Ly6C+ into Ly6C- monocytes. The main two subsets were homogeneous, but linked by a more heterogeneous differentiation intermediate. We show that monocyte differentiation occurred through de novo enhancer establishment and activation of pre-established (poised) enhancers. Generation of Ly6C- monocytes involved induction of the transcription factor C/EBPβ and C/EBPβ-deficient mice lacked Ly6C- monocytes. Mechanistically, C/EBPβ bound the Nr4a1 promoter and controlled expression of this established monocyte survival factor.

Published

2017