Your search keyword '"Norimasa Iwanami"' showing total 63 results

1. Single-cell transcriptome analysis of medaka lymphocytes reveals absence of fully mature T cells in the thymus and the T-lineage commitment in the kidney

Author

Hiyori Sakaguchi, Masaru Matsuda, and Norimasa Iwanami

Subjects

medaka, immune system, lymphopoiesis, scRNA-seq, rag1, Immunologic diseases. Allergy, RC581-607

Abstract

The cellular and molecular mechanisms underlying lymphocyte development are diverse among teleost species. Although recent scRNA-seq analyses of zebrafish hematopoietic cells have advanced our understanding of teleost hematopoiesis, comparative studies using another genetic model, medaka, which is evolutionarily distant among teleosts, is useful for understanding commonality and species-specificity in teleosts. In order to gain insight into how different molecular and cellular mechanisms of lymphocyte development in medaka and zebrafish, we established a recombination activating gene 1 (rag1) mutant medaka, which exhibited defects in V(D)J rearrangement of lymphocyte antigen receptor genes, accordingly lacking mature B and T cells. scRNA-seq analysis of wild type and rag1 mutant lymphocytes in the thymus and kidney characterized the developing stages of T and B cells, and found that most developed cd4+cd8– and cd4–cd8+ single-positive (SP) T-cell populations are absent in the thymus, and identified lymphoid progenitor cells already committed to the T lineage in kidney, implying unique features of medaka lymphocyte development.

Published

2025

2. Author Correction: Antagonistic interactions safeguard mitotic propagation of genetic and epigenetic information in zebrafish

Author

Divine-Fondzenyuy Lawir, Cristian Soza-Ried, Norimasa Iwanami, Iliana Siamishi, Göran O. Bylund, Connor O´Meara, Katarzyna Sikora, Benoît Kanzler, Erik Johansson, Michael Schorpp, Pierre Cauchy, and Thomas Boehm

Subjects

Biology (General), QH301-705.5

Published

2024

3. Author Correction: Genetic landscape of T cells identifies synthetic lethality for T-ALL

Author

Connor P. O’Meara, Lucia Guerri, Divine-Fondzenyuy Lawir, Fernando Mateos, Mary Iconomou, Norimasa Iwanami, Cristian Soza-Ried, Katarzyna Sikora, Iliana Siamishi, Orlando Giorgetti, Sarah Peter, Michael Schorpp, and Thomas Boehm

Subjects

Biology (General), QH301-705.5

Published

2024

4. Antagonistic interactions safeguard mitotic propagation of genetic and epigenetic information in zebrafish

Author

Divine-Fondzenyuy Lawir, Cristian Soza-Ried, Norimasa Iwanami, Iliana Siamishi, Göran O. Bylund, Connor O´Meara, Katarzyna Sikora, Benoît Kanzler, Erik Johansson, Michael Schorpp, Pierre Cauchy, and Thomas Boehm

Subjects

Biology (General), QH301-705.5

Abstract

Abstract The stability of cellular phenotypes in developing organisms depends on error-free transmission of epigenetic and genetic information during mitosis. Methylation of cytosine residues in genomic DNA is a key epigenetic mark that modulates gene expression and prevents genome instability. Here, we report on a genetic test of the relationship between DNA replication and methylation in the context of the developing vertebrate organism instead of cell lines. Our analysis is based on the identification of hypomorphic alleles of dnmt1, encoding the DNA maintenance methylase Dnmt1, and pole1, encoding the catalytic subunit of leading-strand DNA polymerase epsilon holoenzyme (Pole). Homozygous dnmt1 mutants exhibit genome-wide DNA hypomethylation, whereas the pole1 mutation is associated with increased DNA methylation levels. In dnmt1/pole1 double-mutant zebrafish larvae, DNA methylation levels are restored to near normal values, associated with partial rescue of mutant-associated transcriptional changes and phenotypes. Hence, a balancing antagonism between DNA replication and maintenance methylation buffers against replicative errors contributing to the robustness of vertebrate development.

Published

2024

5. Tnpo3 controls splicing of the pre-mRNA encoding the canonical TCR α chain of iNKT cells

Author

Norimasa Iwanami, Andreas S. Richter, Katarzyna Sikora, and Thomas Boehm

Subjects

Science

Abstract

Abstract Unconventional T cells, such as innate natural killer T cells (iNKT) cells, are an important part of vertebrate immune defences. iNKT recognise glycolipids through a T cell receptor (TCR) that is composed of a semi-invariant TCR α chain, paired with a restricted set of TCR β chains. Here, we show that splicing of the cognate Trav11-Traj18-Trac pre-mRNA encoding the characteristic Vα14Jα18 variable region of this semi-invariant TCR depends on the presence of Tnpo3. The Tnpo3 gene encodes a nuclear transporter of the β-karyopherin family whose cargo includes various splice regulators. The block of iNKT cell development in the absence of Tnpo3 can be overcome by transgenic provision of a rearranged Trav11-Traj18-Trac cDNA, indicating that Tnpo3 deficiency does not interfere with the development of iNKT cells per se. Our study thus identifies a role for Tnpo3 in regulating the splicing of the pre-mRNA encoding the cognate TCRα chain of iNKT cells.

Published

2023

6. Maturation of the medaka immune system depends on reciprocal interactions between the microbiota and the intestinal tract

Author

Hiyori Sakaguchi, Yuna Sato, Ryo Matsumoto, Joe Gomikawa, Namie Yoshida, Tomohiro Suzuki, Masaru Matsuda, and Norimasa Iwanami

Subjects

medaka, microbiota, immune system, germ-free, SCID, Immunologic diseases. Allergy, RC581-607

Abstract

The interactions between the host immune system and intestinal microorganisms have been studied in many animals, including fish. However, a detailed analysis has not been performed in medaka, an established fish model for biological studies. Here, we investigated the effect of immunodeficiency on the microbiota composition and the effect of gut bacteria on intestinal epithelial development and immune responses in medaka. Chronological analysis of the intestinal microbiota of interleukin 2 receptor subunit gamma (il2rg) mutant medaka showed a gradual decrease in the evenness of operational taxonomic units, mainly caused by the increased abundance of the Aeromonadaceae family. Exposure of wild-type medaka to high doses of an intestine-derived opportunistic bacterium of the Aeromonadaceae family induced an inflammatory response, suggesting a harmful effect on adult il2rg mutants. In addition, we established germ-free conditions in larval medaka and observed large absorptive vacuoles in intestinal epithelial cells, indicating a block in epithelial maturation. Transcriptome analysis revealed a decrease in the expression of genes involved in the defense response, including the antimicrobial peptide gene hepcidin, whose expression is induced by lipopolysaccharide stimulation in normal larvae. These results show that reciprocal interactions between the microbiome and the intestinal tract are required for the maturation of the medaka immune system.

Published

2023

7. Clonal dynamics underlying the skewed CD4/CD8 ratio of mouse thymocytes revealed by TCR-independent barcoding

Author

Norimasa Iwanami, Malte Petersen, Dagmar Diekhoff, and Thomas Boehm

Subjects

Biology (General), QH301-705.5

Abstract

CRSIPR-mediated barcoding of pre-TCR-expressing T cells is used to investigate the clonal dynamics of thymic T cells and reveals new fundamental understanding of how the skewed CD4/CD8 ratio arises during thymic selection.

Published

2022

8. Limits to in vivo fate changes of epithelia in thymus and parathyroid by ectopic expression of transcription factors Gcm2 and Foxn1

Author

Daisuke Nagakubo, Mayumi Hirakawa, Norimasa Iwanami, and Thomas Boehm

Subjects

Medicine, Science

Abstract

Abstract The development of the parathyroid and the thymus from the third pharyngeal pouch depends on the activities of the Gcm2 and Foxn1 transcription factors, respectively, whose expression domains sharply demarcate two regions in the developing third pharyngeal pouch. Here, we have generated novel mouse models to examine whether ectopic co-expression of Gcm2 in the thymic epithelium and of Foxn1 in the parathyroid perturbs the establishment of organ fates in vivo. Expression of Gcm2 in the thymic rudiment does not activate a parathyroid-specific expression programme, even in the absence of Foxn1 activity. Co-expression of Foxn1 in the parathyroid fails to impose thymopoietic capacity. We conclude that the actions of Foxn1 and Gcm2 transcription factors are cell context-dependent and that they each require permissive transcription factor landscapes in order to successfully interfere with organ-specific cell fate.

Published

2022

9. Genetic landscape of T cells identifies synthetic lethality for T-ALL

Author

Connor P. O’Meara, Lucia Guerri, Divine-Fondzenyuy Lawir, Fernando Mateos, Mary Iconomou, Norimasa Iwanami, Cristian Soza-Ried, Katarzyna Sikora, Iliana Siamishi, Orlando Giorgetti, Sarah Peter, Michael Schorpp, and Thomas Boehm

Subjects

Biology (General), QH301-705.5

Abstract

Abstract To capture the global gene network regulating the differentiation of immature T cells in an unbiased manner, large-scale forward genetic screens in zebrafish were conducted and combined with genetic interaction analysis. After ENU mutagenesis, genetic lesions associated with failure of T cell development were identified by meiotic recombination mapping, positional cloning, and whole genome sequencing. Recessive genetic variants in 33 genes were identified and confirmed as causative by additional experiments. The mutations affected T cell development but did not perturb the development of an unrelated cell type, growth hormone-expressing somatotrophs, providing an important measure of cell-type specificity of the genetic variants. The structure of the genetic network encompassing the identified components was established by a subsequent genetic interaction analysis, which identified many instances of positive (alleviating) and negative (synthetic) genetic interactions. Several examples of synthetic lethality were subsequently phenocopied using combinations of small molecule inhibitors. These drugs not only interfered with normal T cell development, but also elicited remission in a model of T cell acute lymphoblastic leukaemia. Our findings illustrate how genetic interaction data obtained in the context of entire organisms can be exploited for targeted interference with specific cell types and their malignant derivatives.

Published

2021

10. Transgenerational inheritance of impaired larval T cell development in zebrafish

Author

Norimasa Iwanami, Divine-Fondzenyuy Lawir, Katarzyna Sikora, Connor O´Meara, Kohei Takeshita, Michael Schorpp, and Thomas Boehm

Subjects

Science

Abstract

Evidence for transgenerational inheritance of epigenetic information in vertebrates is scarce. Here the authors report that homozygous dnmt1 mutant zebrafish are essentially normal, with the exception of impaired lymphopoiesis, with impaired larval (but not adult) T cell development being transmitted to subsequent generations by genotypically wildtype fish.

Published

2020

11. Epigenetic Protection of Vertebrate Lymphoid Progenitor Cells by Dnmt1

Author

Norimasa Iwanami, Kohei Takeshita, Divine-Fondzenyuy Lawir, Isao Suetake, Shoji Tajima, Katarzyna Sikora, Inês Trancoso, Connor ÓMeara, Iliana Siamishi, Yousuke Takahama, Makoto Furutani-Seiki, Hisato Kondoh, Yasushige Yonezawa, Michael Schorpp, and Thomas Boehm

Subjects

Molecular Genetics, Phenotyping, Transcriptomics, Science

Abstract

Summary: DNA methylation is a universal epigenetic mechanism involved in regulation of gene expression and genome stability. The DNA maintenance methylase DNMT1 ensures that DNA methylation patterns are faithfully transmitted to daughter cells during cell division. Because loss of DNMT1 is lethal, a pan-organismic analysis of DNMT1 function is lacking. We identified new recessive dnmt1 alleles in medaka and zebrafish and, guided by the structures of mutant proteins, generated a recessive variant of mouse Dnmt1. Each of the three missense mutations studied here distorts the catalytic pocket and reduces enzymatic activity. Because all three DNMT1 mutant animals are viable, it was possible to examine their phenotypes throughout life. The consequences of genome-wide hypomethylation of DNA of somatic tissues in the Dnmt1 mutants are surprisingly mild but consistently affect the development of the lymphoid lineage. Our findings indicate that developing lymphocytes in vertebrates are sensitive to perturbations of DNA maintenance methylation.

Published

2020

12. Lymphocyte-Specific Function of the DNA Polymerase Epsilon Subunit Pole3 Revealed by Neomorphic Alleles

Author

Iliana Siamishi, Norimasa Iwanami, Thomas Clapes, Eirini Trompouki, Connor P. O’Meara, and Thomas Boehm

Subjects

DNA polymerase epsilon, T cell, B cell, lymphopoiesis, non-replicative function, Biology (General), QH301-705.5

Abstract

Summary: Immunodeficiencies are typically caused by loss-of-function mutations in lymphocyte-specific genes. Occasionally, mutations in ubiquitous general-purpose factors, including those affecting essential components of the DNA polymerase epsilon (POLE) holoenzyme, have cell-type-specific consequences. POLE3, one of the four components of the POLE holoenzyme, features a histone fold domain and a unique acidic C terminus, making it a particularly attractive candidate mediating cell type-specific activities of POLE. Mice lacking Pole3 survive up to late embryonic stages, indicating that this subunit is dispensable for DNA replication. The phenotypes of viable hypomorphic and neomorphic alleles are surprisingly tissue restricted and reveal a stage-specific function of the histone fold domain of Pole3 during T and B cell development. Gradual introduction of positively charged residues into the acidic C terminus leads to peripheral lymphopenia of increasing severity. Our findings serve as a paradigm to understand the molecular basis of cell-type-specific non-replicative functions of the ubiquitous POLE complex.

Published

2020

13. Correction: WDR55 Is a Nucleolar Modulator of Ribosomal RNA Synthesis, Cell Cycle Progression, and Teleost Organ Development.

Author

Norimasa Iwanami, Tomokazu Higuchi, Yumi Sasano, Toshinobu Fujiwara, Vu Q. Hoa, Minoru Okada, Sadiqur R. Talukder, Sanae Kunimatsu, Jie Li, Fumi Saito, Chitralekha Bhattacharya, Angabin Matin, Takashi Sasaki, Nobuyoshi Shimizu, Hiroshi Mitani, Heinz Himmelbauer, Akihiro Momoi, Hisato Kondoh, Makoto Furutani-Seiki, and Yousuke Takahama

Subjects

Genetics, QH426-470

Published

2008

14. WDR55 is a nucleolar modulator of ribosomal RNA synthesis, cell cycle progression, and teleost organ development.

Author

Norimasa Iwanami, Tomokazu Higuchi, Yumi Sasano, Toshinobu Fujiwara, Vu Q Hoa, Minoru Okada, Sadiqur R Talukder, Sanae Kunimatsu, Jie Li, Fumi Saito, Chitralekha Bhattacharya, Angabin Matin, Takashi Sasaki, Nobuyoshi Shimizu, Hiroshi Mitani, Heinz Himmelbauer, Akihiro Momoi, Hisato Kondoh, Makoto Furutani-Seiki, and Yousuke Takahama

Subjects

Genetics, QH426-470

Abstract

The thymus is a vertebrate-specific organ where T lymphocytes are generated. Genetic programs that lead to thymus development are incompletely understood. We previously screened ethylnitrosourea-induced medaka mutants for recessive defects in thymus development. Here we report that one of those mutants is caused by a missense mutation in a gene encoding the previously uncharacterized protein WDR55 carrying the tryptophan-aspartate-repeat motif. We find that WDR55 is a novel nucleolar protein involved in the production of ribosomal RNA (rRNA). Defects in WDR55 cause aberrant accumulation of rRNA intermediates and cell cycle arrest. A mutation in WDR55 in zebrafish also leads to analogous defects in thymus development, whereas WDR55-null mice are lethal before implantation. These results indicate that WDR55 is a nuclear modulator of rRNA synthesis, cell cycle progression, and embryonic organogenesis including teleost thymus development.

Published

2008

15. The Hox code responsible for the patterning of the anterior vertebrae in zebrafish.

Author

Akiteru Maeno, Rina Koita, Hidemichi Nakazawa, Renka Fujii, Kazuya Yamada, Sae Oikawa, Taisei Tani, Mizuki Ishizaka, Koumi Satoh, Atsuki Ishizu, Takumi Sugawara, Urara Adachi, Morimichi Kikuchi, Norimasa Iwanami, Masaru Matsuda, and Akinori Kawamura

Subjects

SPINE, HOMEOBOX genes, THORACIC vertebrae, ACTINOPTERYGII, X-ray computed microtomography, BRACHYDANIO, MICE

Abstract

The vertebral column is a characteristic structure of vertebrates. Genetic studies in mice have shown that Hox-mediated patterning plays a key role in specifying discrete anatomical regions of the vertebral column. Expression pattern analyses in several vertebrate embryos have provided correlative evidence that the anterior boundaries of Hox expression coincide with distinct anatomical vertebrae. However, because functional analyses have been limited to mice, it remains unclear which Hox genes actually function in vertebral patterning in other vertebrates. In this study, various zebrafish Hox mutants were generated for loss-of-function phenotypic analysis to functionally decipher the Hox code responsible for the zebrafish anterior vertebrae between the occipital and thoracic vertebrae. We found that Hox genes in HoxB- and HoxC-related clusters participate in regulating the morphology of the zebrafish anterior vertebrae. In addition, medaka hoxc6a was found to be responsible for anterior vertebral identity, as in zebrafish. Based on phenotypic similarities with Hoxc6 knockout mice, our results suggest that the Hox patterning system, including at least Hoxc6, may have been functionally established in the vertebral patterning of the common ancestor of ray-finned and lobe-finned fishes. [ABSTRACT FROM AUTHOR]

Published

2024

16. Teleost Hox code defines regional identities competent for the formation of dorsal and anal fins.

Author

Urara Adachi, Rina Koita, Akira Seto, Akiteru Maeno, Atsuki Ishizu, Sae Oikawa, Taisei Tani, Mizuki Ishizaka, Kazuya Yamada, Koumi Satoh, Hidemichi Nakazawa, Hiroyuki Furudate, Koichi Kawakami, Norimasa Iwanami, Masaru Matsuda, and Akinori Kawamura

Subjects

HOMEOBOX genes, GENE regulatory networks, FRAMESHIFT mutation, ORYZIAS latipes, TETRAPODS

Abstract

The dorsal and anal fins can vary widely in position and length along the anterior-posterior axis in teleost fishes. However, the molecular mechanisms underlying the diversification of these fins remain unknown. Here, we used genetic approaches in zebrafish and medaka, in which the relative positions of the dorsal and anal fins are opposite, to demonstrate the crucial role of hox genes in the patterning of the teleost posterior body, including the dorsal and anal fins. By the CRISPR-Cas9-induced frameshift mutations and positional cloning of spontaneous dorsalfinless medaka, we show that various hox mutants exhibit the absence of dorsal or anal fins, or a stepwise posterior extension of these fins, with vertebral abnormalities. Our results indicate that multiple hox genes, primarily from hoxc-related clusters, encompass the regions responsible for the dorsal and anal fin formation along the anterior-posterior axis. These results further suggest that shifts in the anterior boundaries of hox expression which vary among fish species, lead to diversification in the position and size of the dorsal and anal fins, similar to how modulations in Hox expression can alter the number of anatomically distinct vertebrae in tetrapods. Furthermore, we show that hox genes responsible for dorsal fin formation are different between zebrafish and medaka. Our results suggest that a novel mechanism has occurred during teleost evolution, in which the gene network responsible for fin formation might have switched to the regulation downstream of other hox genes, leading to the remarkable diversity in the dorsal fin position. [ABSTRACT FROM AUTHOR]

Published

2024

17. Limits to in vivo fate changes of epithelia in thymus and parathyroid by ectopic expression of transcription factors Gcm2 and Foxn1

Author

Daisuke, Nagakubo, Mayumi, Hirakawa, Norimasa, Iwanami, and Thomas, Boehm

Subjects

Parathyroid Glands, Mice, Multidisciplinary, Animals, Nuclear Proteins, Cell Differentiation, Forkhead Transcription Factors, Thymus Gland, Epithelium, Ectopic Gene Expression, Transcription Factors

Abstract

The development of the parathyroid and the thymus from the third pharyngeal pouch depends on the activities of the Gcm2 and Foxn1 transcription factors, respectively, whose expression domains sharply demarcate two regions in the developing third pharyngeal pouch. Here, we have generated novel mouse models to examine whether ectopic co-expression of Gcm2 in the thymic epithelium and of Foxn1 in the parathyroid perturbs the establishment of organ fates in vivo. Expression of Gcm2 in the thymic rudiment does not activate a parathyroid-specific expression programme, even in the absence of Foxn1 activity. Co-expression of Foxn1 in the parathyroid fails to impose thymopoietic capacity. We conclude that the actions of Foxn1 and Gcm2 transcription factors are cell context-dependent and that they each require permissive transcription factor landscapes in order to successfully interfere with organ-specific cell fate.

Published

2022

18. Evolutionarily conserved role of hps1 in melanin production and blood coagulation in medaka fish

Author

Norimasa Iwanami, Yuka Ozaki, Hiyori Sakaguchi, Yuko Watanabe, Qi Meng, Kyoka Matsumoto, Tomohiro Suzuki, Kiyotaka Hitomi, and Masaru Matsuda

Subjects

Mammals, Melanins, Albinism, Oryzias, Membrane Proteins, Hemorrhagic Disorders, Mice, Hermanski-Pudlak Syndrome, Mutation, Genetics, Animals, Humans, Molecular Biology, Blood Coagulation, Genetics (clinical)

Abstract

Hermansky–Pudlak syndrome is an autosomal recessive disease characterized by albinism, visual impairment, and blood platelet dysfunction. One of the genes responsible for Hermansky–Pudlak syndrome, hps1, regulates organelle biogenesis and thus plays important roles in melanin production, blood clotting, and the other organelle-related functions in humans and mice. However, the function of hps1 in other species remains poorly understood. In this study, we discovered albino medaka fish during the maintenance of a wild-derived population and identified hps1 as the responsible gene using positional cloning. In addition to the specific absence of melanophore pigmentation, the hps1 mutant showed reduced blood coagulation, suggesting that hps1 is involved in clotting caused by both mammalian platelets and fish thrombocytes. Together, the findings of our study demonstrate that hps1 has an evolutionarily conserved role in melanin production and blood coagulation. In addition, our study presents a useful vertebrate model for understanding the molecular mechanisms of Hermansky–Pudlak syndrome.

Published

2022

19. Transgenerational inheritance of impaired larval T cell development in zebrafish

Author

Michael Schorpp, Norimasa Iwanami, Thomas Boehm, Connor O Meara, Divine-Fondzenyuy Lawir, Kohei Takeshita, and Katarzyna Sikora

Subjects

0301 basic medicine, Male, Embryology, Somatic cell, T-Lymphocytes, General Physics and Astronomy, Epigenesis, Genetic, Animals, Genetically Modified, 0302 clinical medicine, lcsh:Science, Zebrafish, Genetics, Multidisciplinary, Lymphopoiesis, Cell Differentiation, Spermatozoa, medicine.anatomical_structure, Larva, DNA methylation, embryonic structures, Epigenetics, Female, DNA (Cytosine-5-)-Methyltransferase 1, Epigenetic memory, T cell, Science, Immunology, Genes, Recessive, Biology, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, medicine, Animals, Allele, Gene, Alleles, fungi, General Chemistry, Regulatory-Associated Protein of mTOR, DNA Methylation, Zebrafish Proteins, biology.organism_classification, 030104 developmental biology, Differentially methylated regions, Core Binding Factor Alpha 3 Subunit, Mutation, lcsh:Q, 030217 neurology & neurosurgery

Abstract

Evidence for transgenerational inheritance of epigenetic information in vertebrates is scarce. Aberrant patterns of DNA methylation in gametes may set the stage for transmission into future generations. Here, we describe a viable hypomorphic allele of dnmt1 in zebrafish that causes widespread demethylation of CpG dinucleotides in sperm and somatic tissues. We find that homozygous mutants are essentially normal, with the exception of drastically impaired lymphopoiesis, affecting both larval and adult phases of T cell development. The phenotype of impaired larval (but not adult) T cell development is transmitted to subsequent generations by genotypically wildtype fish. We further find that about 200 differentially methylated regions in sperm DNA of transmitting and non-transmitting males, including hypermethylated sites associated with runx3 and rptor genes, whose reduced activities are associated with impaired larval T cell development. Our results indicate a particular sensitivity of larval T cell development to transgenerationally inherited epimutations., Evidence for transgenerational inheritance of epigenetic information in vertebrates is scarce. Here the authors report that homozygous dnmt1 mutant zebrafish are essentially normal, with the exception of impaired lymphopoiesis, with impaired larval (but not adult) T cell development being transmitted to subsequent generations by genotypically wildtype fish.

Published

2020

20. Tnpo3 enables EBF1 function in conditions of antagonistic Notch signaling

Author

Marc Bayer, Sören Boller, Senthilkumar Ramamoothy, Nikolay Zolotarev, Pierre Cauchy, Norimasa Iwanami, Gerhard Mittler, Thomas Boehm, and Rudolf Grosschedl

Subjects

Mice, Receptors, Notch, Genetics, Trans-Activators, Animals, Glutamic Acid, Immunoglobulins, Cell Lineage, Karyopherins, beta Karyopherins, Chromatin, Developmental Biology, Transcription Factors

Abstract

Transcription factor EBF1 (early B cell factor 1) acts as a key regulator of B cell specification. The transcriptional network in which EBF1 operates has been extensively studied; however, the regulation of EBF1 function remains poorly defined. By mass spectrometric analysis of proteins associated with endogenous EBF1 in pro-B cells, we identified the nuclear import receptor Transportin-3 (Tnpo3) and found that it interacts with the immunoglobulin-like fold domain of EBF1. We delineated glutamic acid 271 of EBF1 as a critical residue for the association with Tnpo3. EBF1E271A showed normal nuclear localization; however, it had an impaired B cell programming ability in conditions of Notch signaling, as determined by retroviral transduction of Ebf1−/− progenitors. By RNA-seq analysis of EBF1E271A-expressing progenitors, we found an up-regulation of T lineage determinants and down-regulation of early B genes, although similar chromatin binding of EBF1E271A and EBF1wt was detected in pro-B cells expressing activated Notch1. B lineage-specific inactivation of Tnpo3 in mice resulted in a block of early B cell differentiation, accompanied by a down-regulation of B lineage genes and up-regulation of T and NK lineage genes. Taken together, our observations suggest that Tnpo3 ensures B cell programming by EBF1 in nonpermissive conditions.

Published

2022

21. A small fish model for quantitative analysis of radiation effects using visualized thymus responses in GFP transgenic medaka

Author

Takako Maruyama-Hayakawa, Norimasa Iwanami, Kazutaka Doi, Bing Wang, and Kouichi Maruyama

Subjects

Radiological and Ultrasound Technology, Transgene, Green Fluorescent Proteins, Oryzias, Dose-Response Relationship, Radiation, Thymus Gland, Biology, Radiation, 030218 nuclear medicine & medical imaging, Green fluorescent protein, Cell biology, Animals, Genetically Modified, Lethal Dose 50, 03 medical and health sciences, 0302 clinical medicine, Fluorescent light, In vivo, 030220 oncology & carcinogenesis, Animals, %22">Fish , Radiology, Nuclear Medicine and imaging, Quantitative analysis (chemistry)

Abstract

Purpose: The aim of this study was to establish a new method of real-time, in vivo detection of radiation damage and recovery.Methods: The thymus was observed under fluorescent light in a g...

Published

2019

22. Antigen receptor repertoires of one of the smallest known vertebrates

Author

Vydianathan Ravi, Heok Hui Tan, Orlando Bruno Giorgetti, Thomas Boehm, Boon-Hui Tay, Connor P. O'Meara, Byrappa Venkatesh, Aravind Prasad, Nisha E. Pillai, Michael Schorpp, Prashant Shingate, and Norimasa Iwanami

Subjects

animal structures, Immunology, Receptors, Antigen, T-Cell, Adaptive Immunity, Biology, 03 medical and health sciences, 0302 clinical medicine, Immune system, biology.animal, Genetics, Animals, natural sciences, Research Articles, 030304 developmental biology, Mammals, 0303 health sciences, Multidisciplinary, T-cell receptor, Fishes, Vertebrate, SciAdv r-articles, respiratory system, biology.organism_classification, Acquired immune system, Paedocypris, Evolutionary biology, Vertebrates, biology.protein, Immunocompetence, Antibody, Clone (B-cell biology), 030215 immunology, circulatory and respiratory physiology, Research Article

Abstract

The antigen receptor repertoires of one of the smallest vertebrates are organized in a fractal manner., The rules underlying the structure of antigen receptor repertoires are not yet fully defined, despite their enormous importance for the understanding of adaptive immunity. With current technology, the large antigen receptor repertoires of mice and humans cannot be comprehensively studied. To circumvent the problems associated with incomplete sampling, we have studied the immunogenetic features of one of the smallest known vertebrates, the cyprinid fish Paedocypris sp. “Singkep” (“minifish”). Despite its small size, minifish has the key genetic facilities characterizing the principal vertebrate lymphocyte lineages. As described for mammals, the frequency distributions of immunoglobulin and T cell receptor clonotypes exhibit the features of fractal systems, demonstrating that self-similarity is a fundamental property of antigen receptor repertoires of vertebrates, irrespective of body size. Hence, minifish achieve immunocompetence via a few thousand lymphocytes organized in robust scale-free networks, thereby ensuring immune reactivity even when cells are lost or clone sizes fluctuate during immune responses.

Published

2021

23. Epigenetic Protection of Vertebrate Lymphoid Progenitor Cells by Dnmt1

Author

Michael Schorpp, Shoji Tajima, Yasushige Yonezawa, Iliana Siamishi, Connor P. O'Meara, Hisato Kondoh, Makoto Furutani-Seiki, Norimasa Iwanami, Isao Suetake, Yousuke Takahama, Katarzyna Sikora, Kohei Takeshita, Thomas Boehm, Divine-Fondzenyuy Lawir, and Inês Trancoso

Subjects

0301 basic medicine, Cell division, Mutant, 02 engineering and technology, Biology, environment and public health, Article, Molecular Genetics, 03 medical and health sciences, chemistry.chemical_compound, DNA Maintenance, Epigenetics, Allele, lcsh:Science, Transcriptomics, Regulation of gene expression, Multidisciplinary, urogenital system, 021001 nanoscience & nanotechnology, Cell biology, 030104 developmental biology, chemistry, Phenotyping, DNA methylation, embryonic structures, lcsh:Q, 0210 nano-technology, DNA

Abstract

Summary DNA methylation is a universal epigenetic mechanism involved in regulation of gene expression and genome stability. The DNA maintenance methylase DNMT1 ensures that DNA methylation patterns are faithfully transmitted to daughter cells during cell division. Because loss of DNMT1 is lethal, a pan-organismic analysis of DNMT1 function is lacking. We identified new recessive dnmt1 alleles in medaka and zebrafish and, guided by the structures of mutant proteins, generated a recessive variant of mouse Dnmt1. Each of the three missense mutations studied here distorts the catalytic pocket and reduces enzymatic activity. Because all three DNMT1 mutant animals are viable, it was possible to examine their phenotypes throughout life. The consequences of genome-wide hypomethylation of DNA of somatic tissues in the Dnmt1 mutants are surprisingly mild but consistently affect the development of the lymphoid lineage. Our findings indicate that developing lymphocytes in vertebrates are sensitive to perturbations of DNA maintenance methylation., Graphical Abstract, Highlights • Genetic screens identified recessive viable missense alleles of dnmt1 in teleosts • A viable mouse Dnmt1 mutant generated by structure-guided precision mutagenesis • Missense mutations distort the catalytic pocket and reduce enzymatic activity • DNA hypomethylation consistently affects development of the lymphoid lineage, Molecular Genetics; Phenotyping; Transcriptomics

Published

2020

24. Lymphocyte-Specific Function of the DNA Plymerase Epsilon Subunit Pole3 Revealed by Neomorphic Alleles

Author

Eirini Trompouki, Iliana Siamishi, Connor P. O'Meara, Norimasa Iwanami, Thomas Clapes, and Thomas Boehm

Subjects

DNA Replication, 0301 basic medicine, Protein subunit, DNA polymerase epsilon, Mice, Transgenic, Biology, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, medicine, Animals, Lymphocytes, lcsh:QH301-705.5, Gene, Alleles, B cell, DNA Polymerase III, non-replicative function, C-terminus, DNA replication, T cell, lymphopoiesis, DNA Polymerase II, Phenotype, Cell biology, 030104 developmental biology, medicine.anatomical_structure, lcsh:Biology (General), Mutation, Histone fold, 030217 neurology & neurosurgery

Abstract

Summary: Immunodeficiencies are typically caused by loss-of-function mutations in lymphocyte-specific genes. Occasionally, mutations in ubiquitous general-purpose factors, including those affecting essential components of the DNA polymerase epsilon (POLE) holoenzyme, have cell-type-specific consequences. POLE3, one of the four components of the POLE holoenzyme, features a histone fold domain and a unique acidic C terminus, making it a particularly attractive candidate mediating cell type-specific activities of POLE. Mice lacking Pole3 survive up to late embryonic stages, indicating that this subunit is dispensable for DNA replication. The phenotypes of viable hypomorphic and neomorphic alleles are surprisingly tissue restricted and reveal a stage-specific function of the histone fold domain of Pole3 during T and B cell development. Gradual introduction of positively charged residues into the acidic C terminus leads to peripheral lymphopenia of increasing severity. Our findings serve as a paradigm to understand the molecular basis of cell-type-specific non-replicative functions of the ubiquitous POLE complex.

Published

2020

25. Cytidine deaminase 2 is required for VLRB antibody gene assembly in lampreys

Author

Danièle Vassaux, Connor P. O'Meara, Michael Schorpp, Norimasa Iwanami, Thomas Boehm, Ryo Morimoto, Inês Trancoso, Stephen J. Holland, Guillaume Evanno, Ahmed Souissi, Orlando Bruno Giorgetti, Max Planck Institute of Immunobiology and Epigenetics (MPI-IE), Max-Planck-Gesellschaft, Écologie et santé des écosystèmes (ESE), AGROCAMPUS OUEST, Institut national d'enseignement supérieur pour l'agriculture, l'alimentation et l'environnement (Institut Agro)-Institut national d'enseignement supérieur pour l'agriculture, l'alimentation et l'environnement (Institut Agro)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE), National Center for Geriatrics and Gerontology, and Research Institute

Subjects

0301 basic medicine, Immunoglobulin gene, biology, Somatic cell, Immunology, General Medicine, Cytidine deaminase, biology.organism_classification, Germline, 3. Good health, Cell biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, Lampetra, [SDE]Environmental Sciences, biology.protein, medicine, Antibody, Gene, 030217 neurology & neurosurgery, B cell

Abstract

International audience; The antibodies of jawless vertebrates consist of leucine-rich repeat arrays encoded by somatically assembled VLRB genes. It is unknown how the incomplete germline VLRB loci are converted into functional antibody genes during B lymphocyte development in lampreys. In Lampetra planeri larvae lacking the cytidine deaminase CDA2 gene, VLRB assembly fails, whereas the T lineage-associated VLRA and VLRC antigen receptor gene assemblies occur normally. Thus, CDA2 acts in a B cell lineage-specific fashion to support the somatic diversification of VLRB antibody genes. CDA2 is closely related to activation-induced cytidine deaminase (AID), which is essential for the elaboration of immunoglobulin gene repertoires in jawed vertebrates. Our results thus identify a convergent mechanism of antigen receptor gene assembly and diversification that independently evolved in the two sister branches of vertebrates.

Published

2020

26. Evolutionary transition from degenerate to nonredundant cytokine signaling networks supporting intrathymic T cell development

Author

Thomas Boehm, Norimasa Iwanami, Iliana Siamishi, Michael Schorpp, Isabell Hess, Divine-Fondzenyuy Lawir, and Katarzyna Sikora

Subjects

0301 basic medicine, medicine.medical_treatment, T cell, 03 medical and health sciences, 0302 clinical medicine, Immunology and Inflammation, network structure, thymus, evolution, medicine, Interleukin-7 receptor, Zebrafish, Gene, Multidisciplinary, biology, Biological Sciences, biology.organism_classification, medicine.disease, zebrafish, Cell biology, Thymocyte, 030104 developmental biology, Cytokine, medicine.anatomical_structure, Immune disorder, cytokine signaling, Signal transduction, 030215 immunology

Abstract

Significance In mammals, intrathymic T cell development strictly depends on the activity of the IL-7 cytokine signaling pathway, leading to catastrophic immunodeficiency when even 1 of the components in the pathway fails. Here we report the unexpected observation that the development of T cells in the thymus of the teleost Danio rerio (zebrafish) is instead supported by the collective actions of several cytokine signaling pathways, with IL-7 signaling playing only a minor role. This finding suggests that during the course of evolution, a degenerate network was converted into a state of precarious brittleness, possibly because some of the evolutionarily ancient constitutive cytokine pathways had to be repurposed to meet increased demands for sophisticated regulation during the mammalian immune response., In mammals, T cell development critically depends on the IL-7 cytokine signaling pathway. Here we describe the identification of the zebrafish ortholog of mammalian IL-7 based on chromosomal localization, deduced protein sequence, and expression patterns. To examine the biological role of il7 in teleosts, we generated an il7 allele lacking most of its coding exons using CRISPR/Cas9-based mutagenesis. il7-deficient animals are viable and exhibit no obvious signs of immune disorder. With respect to intrathymic T cell development, il7 deficiency is associated with only a mild reduction of thymocyte numbers, contrasting with a more pronounced impairment of T cell development in il7r-deficient fish. Genetic interaction studies between il7 and il7r mutants, and il7 and crlf2(tslpr) mutants suggest the contribution of additional, as-yet unidentified cytokines to intrathymic T cell development. Such activities were also ascertained for other cytokines, such as il2 and il15, collectively indicating that in contrast to the situation in mammals, T cell development in the thymus of teleosts is driven by a degenerate multicomponent network of γc cytokines; this explains why deficiencies of single components have little detrimental effect. In contrast, the dependence on a single cytokine in the mammalian thymus has catastrophic consequences in cases of congenital deficiencies in genes affecting the IL-7 signaling pathway. We speculate that the transition from a degenerate to a nonredundant cytokine network supporting intrathymic T cell development emerged as a consequence of repurposing evolutionarily ancient constitutive cytokine pathways for regulatory functions in the mammalian peripheral immune system.

Published

2019

27. Cytidine deaminase 2 is required for

Author

Ryo, Morimoto, Connor P, O'Meara, Stephen J, Holland, Inês, Trancoso, Ahmed, Souissi, Michael, Schorpp, Danièle, Vassaux, Norimasa, Iwanami, Orlando B, Giorgetti, Guillaume, Evanno, and Thomas, Boehm

Subjects

Receptors, Antigen, Cytidine Deaminase, Animals, Antibodies, Monoclonal, Lampreys

Abstract

The antibodies of jawless vertebrates consist of leucine-rich repeat arrays encoded by somatically assembled

Published

2019

28. Expansions, diversification, and interindividual copy number variations of AID/APOBEC family cytidine deaminase genes in lampreys

Author

L. Aravind, Inês Trancoso, Elena N. Temereva, Mani Larijani, Michael Schorpp, Stephen J. Holland, Lakshminarayan M. Iyer, Heather Fifield, Prashant Shingate, Norimasa Iwanami, Fumiaki Sugahara, Guillaume Evanno, Sarah Peter, Lesley M. Berghuis, Justin J. King, Byrappa Venkatesh, Thomas Boehm, Shigeru Kuratani, Christine Strohmeier, Katarzyna Sikora, Emma M Quinlan, Max Planck Institute of Immunobiology and Epigenetics (MPI-IE), Max-Planck-Gesellschaft, Memorial University of Newfoundland, National Center for Biotechnology Information, National Library of Medicine, National Institutes of Health, Université du Luxembourg (Uni.lu), Hyogo College of Medicine, Partenaires INRAE, Laboratory for evolutionary morphology, Kobe University, International Institute of Molecular and Cell Biology, Biological Faculty, St Petersburg State University (SPbU), Écologie et santé des écosystèmes (ESE), Institut National de la Recherche Agronomique (INRA)-AGROCAMPUS OUEST, and Institut national d'enseignement supérieur pour l'agriculture, l'alimentation et l'environnement (Institut Agro)-Institut national d'enseignement supérieur pour l'agriculture, l'alimentation et l'environnement (Institut Agro)

Subjects

0301 basic medicine, DNA Copy Number Variations, Protein Conformation, [SDV]Life Sciences [q-bio], APOBEC-1 Deaminase, education, Sequence Homology, Somatic hypermutation, 03 medical and health sciences, chemistry.chemical_compound, Immunology and Inflammation, 0302 clinical medicine, Cytidine Deaminase, biology.animal, antigen receptor diversification, evolution, Animals, RNA-editing enzymes, Amino Acid Sequence, Lymphocytes, Gene conversion, Copy-number variation, Gene, Genetics, DNA-editing enzymes, Multidisciplinary, Whole Genome Sequencing, biology, Lamprey, High-Throughput Nucleotide Sequencing, Lampreys, Vertebrate, Cytidine, Cytidine deaminase, Biological Sciences, biology.organism_classification, Receptors, Antigen, 030104 developmental biology, PNAS Plus, chemistry, jawless vertebrate, 030217 neurology & neurosurgery

Abstract

Significance Cytidine deaminases of the AID/APOBEC family mutate the genetic material of pathogens or contribute to the generation and diversification of antibody repertoires in jawed vertebrates. In the extant jawless vertebrate, the lamprey, two members of the AID/APOBEC family are implicated in the somatic diversification of variable lymphocyte receptor (VLR) repertoires. We discovered an unexpected diversity of cytidine deaminase genes within and among lamprey species. The cytidine deaminases with features comparable to jawed vertebrate AID are always present, suggesting that they are involved in essential processes, such as VLR assembly. In contrast, other genes show a remarkable copy number variation, like the APOBEC3 genes in mammals. This suggests an unexpected similarity in functional deployment of AID/APOBEC cytidine deaminases across all vertebrates., Cytidine deaminases of the AID/APOBEC family catalyze C-to-U nucleotide transitions in mRNA or DNA. Members of the APOBEC3 branch are involved in antiviral defense, whereas AID contributes to diversification of antibody repertoires in jawed vertebrates via somatic hypermutation, gene conversion, and class switch recombination. In the extant jawless vertebrate, the lamprey, two members of the AID/APOBEC family are implicated in the generation of somatic diversity of the variable lymphocyte receptors (VLRs). Expression studies linked CDA1 and CDA2 genes to the assembly of VLRA/C genes in T-like cells and the VLRB genes in B-like cells, respectively. Here, we identify and characterize several CDA1-like genes in the larvae of different lamprey species and demonstrate that these encode active cytidine deaminases. Structural comparisons of the CDA1 variants highlighted substantial differences in surface charge; this observation is supported by our finding that the enzymes require different conditions and substrates for optimal activity in vitro. Strikingly, we also found that the number of CDA-like genes present in individuals of the same species is variable. Nevertheless, irrespective of the number of different CDA1-like genes present, all lamprey larvae have at least one functional CDA1-related gene encoding an enzyme with predicted structural and chemical features generally comparable to jawed vertebrate AID. Our findings suggest that, similar to APOBEC3 branch expansion in jawed vertebrates, the AID/APOBEC family has undergone substantial diversification in lamprey, possibly indicative of multiple distinct biological roles.

Published

2018

29. A missense mutation in zbtb17 blocks the earliest steps of T cell differentiation in zebrafish

Author

Michael Schorpp, Thomas Boehm, Divine-Fondzenyuy Lawir, and Norimasa Iwanami

Subjects

0301 basic medicine, Genetics, Zinc finger, Multidisciplinary, biology, T-Lymphocytes, T cell, Mutant, Mutation, Missense, Cell Differentiation, Zebrafish Proteins, biology.organism_classification, Article, 03 medical and health sciences, 030104 developmental biology, medicine.anatomical_structure, T cell differentiation, Transcriptional regulation, medicine, Animals, Missense mutation, Gene, Zebrafish, Transcription Factors

Abstract

T cells are an evolutionarily conserved feature of the adaptive immune systems of vertebrates. Comparative studies using evolutionarily distant species hold great promise for unraveling the genetic landscape underlying this process. To this end, we used ENU mutagenesis to generate mutant zebrafish with specific aberrations in early T cell development. Here, we describe the identification of a recessive missense mutation in the transcriptional regulator zbtb17 (Q562K), which affects the ninth zinc finger module of the protein. Homozygous mutant fish exhibit an early block of intrathymic T cell development, as a result of impaired thymus colonization owing to reduced expression of the gene encoding the homing receptor ccr9a, and inefficient T cell differentiation owing to reduced expression of socs1a. Our results reveal the zbtb17-socs1 axis as an evolutionarily conserved central regulatory module of early T cell development of vertebrates.

Published

2017

30. Studying the adaptive immune system in zebrafish by transplantation of hematopoietic precursor cells

Author

Isabel Hess, Michael Schorpp, Norimasa Iwanami, and Thomas Boehm

Subjects

0301 basic medicine, Mutation, biology, Cell growth, Acquired immune system, biology.organism_classification, medicine.disease_cause, Cell biology, Transplantation, 03 medical and health sciences, Haematopoiesis, 030104 developmental biology, Immune system, Precursor cell, Immunology, medicine, Zebrafish

Abstract

Traditionally, transplantation has been a major experimental procedure to study the development and function of hematopoietic and immune systems. Here, we describe the use of a zebrafish strain lacking definitive hematopoiesis (cmybI181N) for interspecific analysis of hematopoietic and immune cell development. Without conditioning prior to transplantation, allogeneic and xenogeneic hematopoietic progenitor cells stably engraft in adult zebrafish homozygous for the cmyb mutation. This unique animal model can be used to genetically and functionally disentangle universal and species-specific contributions of the microenvironment to hematopoietic progenitor cell maintenance and development.

Published

2017

31. Ethylnitrosourea-induced thymus-defective mutants identify roles of KIAA1440, TRRAP, and SKIV2L2 in teleost organ development

Author

Norimasa Iwanami, Hisato Kondoh, Minoru Okada, Yousuke Takahama, Yasuhito Seo, Makoto Furutani-Seiki, Takashi Sasaki, Vu Q. Hoa, Nobuyoshi Shimizu, and Hiroshi Mitani

Subjects

Positional cloning, Organogenesis, Oryzias, Molecular Sequence Data, Immunology, Mutant, Mutagenesis (molecular biology technique), Thymus Gland, Germ layer, Biology, Gene expression, Animals, Immunology and Allergy, Gene, Adaptor Proteins, Signal Transducing, Genetics, Base Sequence, Nuclear Proteins, Exons, biology.organism_classification, Alternative Splicing, Ethylnitrosourea, Mutation, RNA Helicases

Abstract

The thymus is an organ where T lymphocytes develop. Thymus development requires interactions of cells derived from three germ layers. However, the molecular mechanisms that control thymus development are not fully understood. To identify the genes that regulate thymus development, we previously carried out a large-scale screening for ethylnitrosourea-induced mutagenesis using medaka, Oryzias latipes, and established a panel of recessive thymus-lacking mutants. Here we report the identification of three genes responsible for these mutations. We found that the mutations in KIAA1440, TRRAP, and SKIV2L2 caused the defects in distinct steps of thymus development. We also found that these genes were widely expressed in many organs and that the mutations in these genes caused defects in the development of various other organs. These results enabled us to identify previously unknown roles of widely expressed genes in medaka organ development. The possible reasons why thymus-defective teleost mutants could be used to identify widely expressed genes and future strategies to increase the likelihood of identifying genes that specifically regulate thymus development are discussed.

Published

2009

32. Noninvasive Intravital Imaging of Thymocyte Dynamics in Medaka

Author

Vu Q. Hoa, Jie Li, Norimasa Iwanami, Makoto Furutani-Seiki, and Yousuke Takahama

Subjects

Pathology, medicine.medical_specialty, Genes, RAG-1, T-Lymphocytes, Transgene, Green Fluorescent Proteins, Molecular Sequence Data, Immunology, Oryzias, Motility, Thymus Gland, Biology, Recombination-activating gene, Animals, Genetically Modified, Cell Movement, medicine, Animals, Immunology and Allergy, Primordium, Receptor, Homeodomain Proteins, Microscopy, Video, Laser Scanning Cytometry, Cell biology, Thymocyte, Microscopy, Fluorescence, Lymphoid Progenitor Cells, Preclinical imaging

Abstract

In vivo imaging of thymocytes has not been accomplished due to their localization deep within opaque body and high susceptibility to surgical stress. To overcome these problems, medaka is useful because of transparency and ex-uterine development. We report the noninvasive detection of thymocytes in transgenic medaka that express fluorescent protein under the control of immature-lymphocyte-specific rag1. We show that lymphoid progenitor cells colonize the thymus primordium in an anterior-to-posterior orientation-specific manner, revealing that extrathymic anterior components guide prevascular thymus colonization. We also show that developing thymocytes acquire “random walk motility” along with the expression of Ag receptors and coreceptors, suggesting that thymocyte walking is initiated at the developmental stage for repertoire selection. Thus, transgenic medaka enables real-time intravital imaging of thymocytes without surgical invasion.

Published

2007

33. Cellular and molecular events during early thymus development

Author

Georg A. Holländer, Yousuke Takahama, Norimasa Iwanami, Jason Gill, Saulius Zuklys, and Cunlan Liu

Subjects

Cell type, Stromal cell, Pharyngeal pouch, T-Lymphocytes, Lymphocyte, Immunology, Thymus Gland, Biology, Mice, Immune system, Precursor cell, DiGeorge syndrome, DiGeorge Syndrome, medicine, Animals, Humans, Paired Box Transcription Factors, Immunology and Allergy, Transcription factor, Homeodomain Proteins, Intracellular Signaling Peptides and Proteins, Gene Expression Regulation, Developmental, Nuclear Proteins, Forkhead Transcription Factors, Hematopoietic Stem Cells, medicine.disease, Cell biology, medicine.anatomical_structure, Protein Tyrosine Phosphatases, T-Box Domain Proteins

Abstract

Summary: The thymic stromal compartment consists of several cell types that collectively enable the attraction, survival, expansion, migration, and differentiation of T-cell precursors. The thymic epithelial cells constitute the most abundant cell type of the thymic microenvironment and can be differentiated into morphologically, phenotypically, and functionally separate subpopulations of the postnatal thymus. All thymic epithelial cells are derived from the endodermal lining of the third pharyngeal pouch. Very soon after the formation of a thymus primordium and prior to its vascularization, thymic epithelial cells orchestrate the first steps of intrathymic T-cell development, including the attraction of lymphoid precursor cells to the thymic microenvironment. The correct segmentation of pharyngeal epithelial cells and their subsequent crosstalk with cells in the pharyngeal arches are critical prerequisites for the formation of a thymus anlage. Mutations in several transcription factors and their target genes have been informative to detail some of the complex mechanisms that control the development of the thymus anlage. This review highlights recent findings related to the genetic control of early thymus organogenesis and provides insight into the molecular basis by which lymphocyte precursors are attracted to the thymus.

Published

2006

34. Peptide-induced immune protection of CD8+ T cell-deficient mice against Friend retrovirus-induced disease

Author

Norimasa Iwanami, Masaaki Miyazawa, Hiroyuki Kawabata, Hideaki Matsukuma, Haruo Matsumura, Hiroyuki Abe, Atsuko Niwa, Nobutada Tabata, Sachiyo Tsuji-Kawahara, and Hirohide Uenishi

Subjects

CD4-Positive T-Lymphocytes, T cell, Immunology, Epitopes, T-Lymphocyte, CD8-Positive T-Lymphocytes, Biology, Antibodies, Viral, Mice, Immune system, Bone Marrow, medicine, Animals, Immunology and Allergy, Cytotoxic T cell, Antigen-presenting cell, Mice, Knockout, B-Lymphocytes, Mice, Inbred BALB C, Leukemia, Experimental, Friend virus, Vaccination, Gene Products, env, Viral Vaccines, General Medicine, Acquired immune system, biology.organism_classification, Virology, Friend murine leukemia virus, B-1 cell, Tumor Virus Infections, medicine.anatomical_structure, biology.protein, Antibody, Spleen, Retroviridae Infections

Abstract

CD8 1 CTLs and virus-neutralizing antibodies have been associated with spontaneous and vaccine-induced immune control of retroviral infections. We previously showed that a single immunization with an env gene-encoded CD4 1 T cell epitope protected mice against fatal Friend retrovirus infection. Here, we analyzed immune cell components required for the peptide-induced anti-retroviral protection. Mice lacking CD8 1 T cells were nevertheless protected against Friend virus infection, while mice lacking B cells were not. Virus-producing cells both in the spleen and bone marrow decreased rapidly in their number and became undetectable by 4 weeks after infection in the majority of the peptide-immunized animals even in the absence of CD8 1 T cells. In the vaccinated animals the production and class switching of virus-neutralizing and anti-leukemia cell antibodies were facilitated; however, virus-induced erythroid cell expansion was suppressed before neutralizing antibodies became detectable in the serum. Further, the numbers of virus-producing cells in the spleen and bone marrow in the early stage of the infection were smaller in the peptide-immunized than in unimmunized control mice in the absence of B cells. Thus, peptide immunization facilitates both early cellular and late humoral immune responses that lead to the effective control of the retrovirus-induced disease, but CD8 1 T cells are not crucial for the elimination of virus-infected cells in the peptide-primed animals.

Published

2005

35. Mutations affecting gonadal development in Medaka, Oryzias latipes

Author

Tomomi Watanabe, Hisato Kondoh, Norimasa Iwanami, Toshiyuki Yamanaka, Chikako Morinaga, Takao Sasado, Katsutoshi Niwa, Takeshi Tomonaga, Hiroki Yoda, Ai Shinomiya, Hiroshi Suwa, Sanae Kunimatsu, Yasuko Okamoto, Yukihiro Hirose, Akihito Yasuoka, Makoto Furutani-Seiki, Thorsten Henrich, Minoru Tanaka, and Tomonori Deguchi

Subjects

Genetics, Male, endocrine system, Embryology, Gonad, Sexual differentiation, biology, Somatic cell, Oryzias, Mutant, biology.organism_classification, Molecular biology, medicine.anatomical_structure, Germ Cells, Phenotype, Mutation, medicine, Animals, Female, Development of the gonads, Gonads, Gene, Germ cell, Developmental Biology

Abstract

A gonad is formed from germ cells and somatic mesodermal cells through their interactions. Its development is coupled with the determination and differentiation of the sex and sex-associated traits. We carried out a large-scale screening of Medaka mutants in which gonadal development is affected. Screening was performed on larvae at 8 days posthatching for abnormal abundance and/or distribution of germ cells detected by the in situ hybridization for olvas (Medaka vasa). We describe here 16 mutants of 13 genes, which are classified into four groups. Group 1, consisting of four mutants of three genes kon, tot) characterised by an increase in germ cell number. An adult tot homozygote fish has the characteristic feature of possessing hypertrophic gonads filled with immature oocytes. Group 2, represented by a single gene (zen) mutant characterized by a gradual loss of germ cells. Group 3, consisting of four mutants of distinct genes (eko, eki, sht, ano) showing irregular clustering of germ cells. Group 4, consisting of seven mutants of five genes (arr, hyo, mzr, hdr, fbk) showing fragmented clusters of germ cells. In some mutants belonging to Groups 1, 3 and 4, the expression level of ftz-f1 (sf-1/Ad4BP) in gonadal somatic cells significantly decreased, suggesting that interaction between somatic and germ cells is affected.

Published

2004

36. Mutations affecting liver development and function in Medaka, Oryzias latipes, screened by multiple criteria

Author

Yukihiro Hirose, Akihito Yasuoka, Hiroshi Nishina, Felix Loosli, Hiroshi Suwa, Clemens Grabher, Katsutoshi Niwa, Satoshi Asaka, Hiroki Yoda, Takao Sasado, Kota Saito, Rebecca Quiring, Matthias Carl, Sanae Kunimatsu, Keiko Abe, Daiju Kitagawa, Tomonori Deguchi, Chikako Morinaga, Thorsten Henrich, Masakazu Osakada, Sylke Winkler, Tomomi Watanabe, Ryumei Kurashige, Katsuhito Takahashi, Yousuke Takahama, Hisato Kondoh, Joachim Wittbrodt, Toshiaki Katada, Norimasa Iwanami, Makoto Furutani-Seiki, and Filippo Del Bene

Subjects

Genetics, Mutation, Embryology, Liver morphogenesis, Endoderm, Mutant, Oryzias, Gallbladder, Mutagenesis (molecular biology technique), Biology, Lipid Metabolism, medicine.disease_cause, Phenotype, Complementation, Liver, Endoderm formation, medicine, Animals, Gene, In Situ Hybridization, Body Patterning, Developmental Biology

Abstract

We report here mutations affecting various aspects of liver development and function identified by multiple assays in a systematic mutagenesis screen in Medaka. The 22 identified recessive mutations assigned to 19 complementation groups fell into five phenotypic groups. Group 1, showing defective liver morphogenesis, comprises mutations in four genes, which may be involved in the regulation of growth or patterning of the gut endoderm. Group 2 comprises mutations in three genes that affect the laterality of the liver; in kendama mutants of this group, the laterality of the heart and liver is uncoupled and randomized. Group 3 includes mutations in three genes altering bile color, indicative of defects in hemoglobin-bilirubin metabolism and globin synthesis. Group 4 consists of mutations in three genes, characterized by a decrease in the accumulation of fluorescent metabolite of a phospholipase A(2) substrate, PED6, in the gall bladder. Lipid metabolism or the transport of lipid metabolites may be affected by these mutations. Mutations in Groups 3 and 4 may provide animal models for relevant human diseases. Group 5 mutations in six genes affect the formation of endoderm, endodermal rods and hepatic bud from which the liver develops. These Medaka mutations, identified by morphological and metabolite marker screens, should provide clues to understanding molecular mechanisms underlying formation of a functional liver.

Published

2004

37. Identification of radiation-sensitive mutants in the Medaka, Oryzias latipes

Author

Chikako Morinaga, Hiroki Yoda, Tomonori Deguchi, Hiroshi Mitani, Hisato Kondoh, Akihiro Shima, Akihito Yasuoka, Thorsten Hennrich, Masakazu Osakada, Katsutoshi Niwa, Yukihiro Hirose, Takao Sasado, Atsuko Shimada, Makoto Furutani-Seiki, Norimasa Iwanami, Nozomi Kogure, Sanae Kunimatsu, Hiroshi Suwa, Tomomi Watanabe, Takeshi Todo, and Kouichi Aizawa

Subjects

Tail, Genome instability, Embryology, Time Factors, animal structures, DNA Repair, DNA repair, Oryzias, Mutant, Apoptosis, Radiation Tolerance, Genomic Instability, Midblastula, Animals, biology, Embryo, Gastrula, biology.organism_classification, Molecular biology, Double Strand Break Repair, Comet assay, Gamma Rays, Mutation, embryonic structures, Comet Assay, Developmental Biology

Abstract

We screened populations of N-ethyl-N-nitrosourea (ENU)-mutagenized Medaka, (Oryzias latipes) for radiation-sensitive mutants to investigate the mechanism of genome stability induced by ionizing radiation in developing embryos. F3 embryos derived from male founders that were homozygous for induced the mutations were irradiated with gamma-rays at the organogenesis stage (48hpf) at a dose that did not cause malformation in wild-type embryos. We screened 2130 F2 pairs and identified three types of mutants with high incidence of radiation-induced curly tailed (ric) malformations using a low dose of irradiation. The homozygous strain from one of these mutants, ric1, which is highly fertile and easy to breed, was established and characterized related to gamma-irradiation response. The ric1 strain also showed higher incidence of malformation and lower hatchability compared to the wild-type CAB strain after gamma-irradiation at the morula and pre-early gastrula stages. We found that the decrease in hatching success after gamma-irradiation, depends on the maternal genotype at the ric1 locus. Terminal deoxynucleotidyl transferase-mediated deoxy-UTP nick end-labeling assays showed a high frequency of apoptosis in the ric1 embryos immediately after gamma-irradiation at the pre-early gastrula stage but apoptotic cells were not observed before midblastula transition (MBT). The neutral comet assay revealed that the ric1 mutant has a defect in the rapid repair of DNA double-strand breaks induced by gamma-rays. These results suggest that RIC1 is involved in the DNA double strand break repair in embryos from morula to organogenesis stages, and unrepaired DNA double strand breaks in ric1 trigger apoptosis after MBT. These results support the use of the ric1 strain for investigating various biological consequences of DNA double strand breaks in vivo and for sensitive monitoring of genotoxicity related to low dose radiation.

Published

2004

38. Mutations affecting thymus organogenesis in Medaka, Oryzias latipes

Author

Sanae Kunimatsu, Tomonori Deguchi, Rie Takei, Thorsten Henrich, Chikako Morinaga, Yousuke Takahama, Yukihiro Hirose, Takao Sasado, Katsutoshi Niwa, Akihito Yasuoka, Hiroki Yoda, Osamu Ohara, Hisato Kondoh, Norimasa Iwanami, Yuko Ishikura, Hiroshi Suwa, Makoto Furutani-Seiki, and Jie Li

Subjects

Genetics, Embryology, biology, Genes, RAG-1, Lymphocyte, Oryzias, Mutant, Gene Expression, Gene Expression Regulation, Developmental, Mutagenesis (molecular biology technique), Organogenesis, Thymus Gland, T lymphocyte, biology.organism_classification, Recombination-activating gene, Cell biology, Branchial Region, medicine.anatomical_structure, Mutation, medicine, Animals, Pharyngeal arch, Developmental Biology

Abstract

The thymus is an organ for T lymphocyte maturation and is indispensable for the establishment of a highly developed immune system in vertebrates. In order to genetically dissect thymus organogenesis, we carried out a large-scale mutagenesis screening for Medaka mutations affecting recombination activating gene 1 (rag1) expression in the developing thymus. We identified 24 mutations, defining at least 13 genes, which led to a marked reduction of rag1 expression in the thymus. As thymus development depends on pharyngeal arches, we classified those mutations into three classes according to the defects in the pharyngeal arches. Class 1 mutants had no or slight morphological abnormalities in the pharyngeal arches, implying that the mutations may include defects in such thymus-specific events as lymphocyte development and thymic epithelial cell maturation. Class 2 mutants had abnormally shaped pharyngeal arches. Class 3 mutants showed severely attenuated pharyngeal arch development. In Class 2 and Class 3 mutants, the defects in thymus development may be due to abnormal pharyngeal arch development. Those mutations are expected to be useful for identifying the molecular mechanisms underlying thymus organogenesis.

Published

2004

39. Mutations affecting retina development in Medaka

Author

Felix Loosli, Rebecca Quiring, Hiroshi Suwa, Harun Elmasri, Caroline Iquel, Chikako Morinaga, Sanae Kunimatsu, Katsutoshi Niwa, Christoph Winkler, Clemens Grabher, Yukihiro Hirose, Annette Krone, Thorsten Henrich, Filippo Del Bene, Tomonori Deguchi, Beate Wittbrodt, Matthias Carl, Sylke Winkler, Akihito Yasuoka, Takao Sasado, Masakazu Osakada, Juan Ramón Martínez-Morales, Hisato Kondoh, Martina Rembold, Joachim Wittbrodt, Tomomi Watanabe, Makoto Furutani-Seiki, Hiroki Yoda, Norimasa Iwanami, Roche, Japan Science and Technology Agency, Company of Biologists, Boehringer Ingelheim Fonds, Marie Curie Memorial Foundation, German Research Foundation, and European Commission

Subjects

Embryology, genetic structures, Teleost, Mutant, Oryzias, Mutagenesis (molecular biology technique), Genes, Recessive, Biology, Optic cup (anatomical), medicine.disease_cause, Eye, Retina, Optic vesicle formation, medicine, Animals, Genetics, Mutation, Pigmentation, Cell Differentiation, Large scale, Optic vesicle, eye diseases, Medaka, medicine.anatomical_structure, Mutagenesis, sense organs, Neural plate, Developmental Biology

Abstract

12 páginas, 5 figuras, 1 tabla.-- et al., In a large scale mutagenesis screen of Medaka we identified 60 recessive zygotic mutations that affect retina development. Based on the onset and type of phenotypic abnormalities, the mutants were grouped into five categories: the first includes 11 mutants that are affected in neural plate and optic vesicle formation. The second group comprises 15 mutants that are impaired in optic vesicle growth. The third group includes 18 mutants that are affected in optic cup development. The fourth group contains 13 mutants with defects in retinal differentiation. 12 of these have smaller eyes, whereas one mutation results in enlarged eyes. The fifth group consists of three mutants with defects in retinal pigmentation. The collection of mutants will be used to address the molecular genetic mechanisms underlying vertebrate eye formation., This work was supported by the Roche Research Foundation (F.L.) the Japanese Agency for Science and Technology (JST) (R.Q., M.C., S.W.), the Company of Biologists Ltd (F.D.B.), the Boehringer Ingelheim Foundation (C.G.), the Marie Curie Foundation (J-R. M-M.) and through grants from the DFG, EC (J.W) and HFSP (H.K, J.W.).

Published

2004

40. A systematic genome-wide screen for mutations affecting organogenesis in Medaka, Oryzias latipes

Author

Katsutoshi Niwa, Harun Elmasri, Toshiaki Katada, Norimasa Iwanami, Makoto Furutani-Seiki, Yasuko Okamoto, Tomonori Deguchi, Noboru Nakajima, Akihito Yasuoka, Yukihiro Hirose, Yousuke Takahama, Clemens Grabher, Ai Shinomiya, Yasuko Kota, Sanae Kunimatsu, Hisato Kondoh, Hiroshi Mitani, Akihiro Momoi, Tomomi Watanabe, Rebecca Quiring, Katsuhito Takahashi, Hiroshi Nishina, Toshiyuki Yamanaka, Joachim Wittbrodt, Hiroki Yoda, Takeshi Todo, Hiroshi Suwa, Kota Saito, Daiju Kitagawa, Sylke Winkler, Keiko Abe, Chikako Morinaga, Matthias Carl, Satoshi Asaka, Thorsten Henrich, Minoru Tanaka, Filippo Del Bene, Takao Sasado, Masakazu Osakada, Mirana Ramialison, Christoph Winkler, and Felix Loosli

Subjects

Embryology, animal structures, DNA repair, Oryzias, Organogenesis, Mutagenesis (molecular biology technique), Thymus Gland, Eye, Radiation Tolerance, Prosencephalon, Animals, Zebrafish, Gene, Genetics, biology, fungi, biology.organism_classification, Phenotype, Germ cell migration, Germ Cells, Somites, Research Design, embryonic structures, Mutation, Nerve tract, Developmental Biology

Abstract

A large-scale mutagenesis screen was performed in Medaka to identify genes acting in diverse developmental processes. Mutations were identified in homozygous F3 progeny derived from ENU-treated founder males. In addition to the morphological inspection of live embryos, other approaches were used to detect abnormalities in organogenesis and in specific cellular processes, including germ cell migration, nerve tract formation, sensory organ differentiation and DNA repair. Among 2031 embryonic lethal mutations identified, 312 causing defects in organogenesis were selected for further analyses. From these, 126 mutations were characterized genetically and assigned to 105 genes. The similarity of the development of Medaka and zebrafish facilitated the comparison of mutant phenotypes, which indicated that many mutations in Medaka cause unique phenotypes so far unrecorded in zebrafish. Even when mutations of the two fish species cause a similar phenotype such as one-eyed-pinhead or parachute, more genes were found in Medaka than in zebrafish that produced the same phenotype when mutated. These observations suggest that many Medaka mutants represent new genes and, therefore, are important complements to the collection of zebrafish mutants that have proven so valuable for exploring genomic function in development.

Published

2004

41. Mutations affecting retinotectal axonal pathfinding in Medaka, Oryzias latipes

Author

Tomomi Watanabe, Hiroshi Suwa, Joachim Wittbrodt, Norimasa Iwanami, Yukihiro Hirose, Tomonori Deguchi, Hisato Kondoh, Sanae Kunimatsu, Toshiyuki Yamanaka, Thorsten Henrich, Hiroki Yoda, Makoto Furutani-Seiki, Yasuko Okamoto, Chikako Morinaga, Masakazu Osakada, Takao Sasado, Katsutoshi Niwa, and Akihito Yasuoka

Subjects

Superior Colliculi, Embryology, Oryzias, Mutant, Biology, Eye, medicine.disease_cause, Retinal ganglion, chemistry.chemical_compound, medicine, Animals, Zebrafish, Mutation, Retina, fungi, Optic Nerve, Retinal, Anatomy, biology.organism_classification, Phenotype, Axons, eye diseases, Cell biology, medicine.anatomical_structure, nervous system, chemistry, Optic Chiasm, sense organs, Tectum, Developmental Biology

Abstract

We screened for mutations affecting retinotectal axonal projection in Medaka, Oryzias latipes. In wild-type Medaka embryos, all the axons of retinal ganglion cells (RGCs) project to the contralateral tectum, such that the topological relationship of the retinal field is maintained. We labeled RGC axons using DiI/DiO at the nasodorsal and temporoventral positions of the retina, and screened for mutations affecting the pattern of stereotypic projections to the tectum. By screening 184 mutagenized haploid genomes, seven mutations in five genes causing defects in axonal pathfinding were identified, whereas mutations affecting the topographic projection of RGC axons were not found. The mutants were grouped into two classes according to their phenotypes. In mutants of Class I, a subpopulation of the RGC axons branched out either immediately after leaving the eye or after reaching the midline, and this axonal subpopulation projected to the ipsilateral tectum. In mutants of Class II, subpopulations of RGC axons branched out after crossing the midline and projected aberrantly. These mutants will provide clues to understanding the functions of genes essential for axonal pathfinding, which may be conserved or partly divergent among vertebrates.

Published

2004

42. Genetic dissection of the formation of the forebrain in Medaka, Oryzias latipes

Author

Satoshi Asaka, Chritoph Winkler, Hiroshi Suwa, Chikako Morinaga, Sylke Winkler, Masakazu Osakada, Takao Sasado, Kota Saito, Thorsten Henrich, Akihito Yasuoka, Sanae Kunimatsu, Felix Loosli, Hiroshi Nishina, Rebecca Quiring, Katsutoshi Niwa, Akihiro Momoi, Harun Elmasri, Hiroki Yoda, Yukihiro Hirose, Toshiaki Katada, Norimasa Iwanami, Tomonori Deguchi, Tomomi Watanabe, Matthias Carl, Makoto Furutani-Seiki, Filippo Del Bene, Daiju Kitagawa, Clemens Grabher, Joachim Wittbrodt, and Hisato Kondoh

Subjects

Genetics, Mutation, Embryology, biology, Mutant, Oryzias, medicine.disease_cause, biology.organism_classification, Phenotype, Diencephalon, Prosencephalon, Forebrain, medicine, biology.protein, Animals, Sonic hedgehog, Zebrafish, Gene, Developmental Biology

Abstract

The forebrain, consisting of the telencephalon and diencephalon, is essential for processing sensory information. To genetically dissect formation of the forebrain in vertebrates, we carried out a systematic screen for mutations affecting morphogenesis of the forebrain in Medaka. Thirty-three mutations defining 25 genes affecting the morphological development of the forebrain were grouped into two classes. Class 1 mutants commonly showing a decrease in forebrain size, were further divided into subclasses 1A to 1D. Class 1A mutation (1 gene) caused an early defect evidenced by the lack of bf1 expression, Class 1B mutations (6 genes) patterning defects revealed by the aberrant expression of regional marker genes, Class 1C mutation (1 gene) a defect in a later stage, and Class 1D (3 genes) a midline defect analogous to the zebrafish one-eyed pinhead mutation. Class 2 mutations caused morphological abnormalities in the forebrain without considerably affecting its size, Class 2A mutations (6 genes) caused abnormalities in the development of the ventricle, Class 2B mutations (2 genes) severely affected the anterior commissure, and Class 2C (6 genes) mutations resulted in a unique forebrain morphology. Many of these mutants showed the compromised sonic hedgehog expression in the zona-limitans-intrathalamica (zli), arguing for the importance of this structure as a secondary signaling center. These mutants should provide important clues to the elucidation of the molecular mechanisms underlying forebrain development, and shed new light on phylogenically conserved and divergent functions in the developmental process.

Published

2004

43. Mutations affecting early distribution of primordial germ cells in Medaka (Oryzias latipes) embryo

Author

Katsutoshi Niwa, Yasuko Kota, Yukihiro Hirose, Akihito Yasuoka, Hiroki Yoda, Tomonori Deguchi, Hiroshi Suwa, Yasuko Okamoto, Thorsten Henrich, Masakazu Osakada, Minoru Tanaka, Toshiyuki Yamanaka, Takao Sasado, Makoto Furutani-Seiki, Ai Shinomiya, Sanae Kunimatsu, Norimasa Iwanami, Chikako Morinaga, Hisato Kondoh, and Tomomi Watanabe

Subjects

Male, Genetics, endocrine system, Embryology, biology, urogenital system, Oryzias, fungi, Cell migration, Embryo, In situ hybridization, biology.organism_classification, Phenotype, Germ Cells, medicine.anatomical_structure, Mutation, embryonic structures, medicine, Animals, Female, Ploidy, Yolk sac, Developmental Biology, Genetic screen

Abstract

The development of germ cells has been intensively studied in Medaka (Oryzias latipes). We have undertaken a large-scale screen to identify mutations affecting the development of primordial germ cells (PGCs) in Medaka. Embryos derived from mutagenized founder fish were screened for an abnormal distribution or number of PGCs at embryonic stage 27 by RNA in situ hybridization for the Medaka vasa homologue (olvas). At this stage, PGCs coalesce into two bilateral vasa-expressing foci in the ventrolateral regions of the trunk after their migration and group organization. Nineteen mutations were identified from a screen corresponding to 450 mutagenized haploid genomes. Eleven of the mutations caused altered PGC distribution. Most of these alterations were associated with morphological abnormalities and could be grouped into four phenotypic classes: Class 1, PGCs dispersed into bilateral lines; Class 2, PGCs dispersed in a region more medial than that in Class 1; Class 3, PGCs scattered laterally and over the yolk sac area; and Class 4, PGCs clustered in a single median focus. Eight mutations caused a decrease in the number of PGCs. This decrease was observed in the offspring of heterozygous mothers, indicating the contribution of a maternal factor in determining PGC abundance. Taken together, these mutations should prove useful in identifying molecular mechanisms underlying the early PGC development and migration.

Published

2004

44. Novel regulators of lymphopoiesis identified using forward genetic screens in zebrafish

Author

Michael Schorpp, Cristian Soza-Ried, Norimasa Iwanami, Iliana Siamishi, and Thomas Boehm

Subjects

Genetics, Cancer Research, Cell Biology, Hematology, Lymphopoiesis, Biology, biology.organism_classification, Molecular Biology, Zebrafish, Genetic screen

Published

2017

45. Zebrafish as a model for understanding the evolution of the vertebrate immune system and human primary immunodeficiency

Author

Norimasa Iwanami

Subjects

Cancer Research, T-Lymphocytes, Population, Computational biology, Immune system, biology.animal, Genetics, medicine, Animals, Humans, education, Molecular Biology, Zebrafish, education.field_of_study, B-Lymphocytes, biology, Lymphopoiesis, Immunologic Deficiency Syndromes, Vertebrate, Cell Biology, Hematology, biology.organism_classification, medicine.disease, Phenotype, Biological Evolution, Reverse genetics, Immune System, Models, Animal, Primary immunodeficiency, Genetic screen

Abstract

Zebrafish is an important vertebrate model that provides the opportunity for the combination of genetic interrogation with advanced live imaging in the analysis of complex developmental and physiologic processes. Among the many advances that have been achieved using the zebrafish model, it has had a great impact on immunology. Here, I discuss recent work focusing on the genetic underpinnings of the development and function of lymphocytes in fish. Lymphocytes play critical roles in vertebrate-specific acquired immune systems of jawless and jawed fish. The unique opportunities afforded by the ability to carry out forward genetic screens and the rapidly evolving armamentarium of reverse genetics in fish usher in a new immunologic research that complements the traditional models of chicken and mouse. Recent work has greatly increased our understanding of the molecular components of the zebrafish immune system, identifying evolutionarily conserved and fish-specific functions of immune-related genes. Interestingly, some of the genes whose mutations underlie the phenotypes in immunodeficient zebrafish were also identified in immunodeficient human patients. In addition, because of the generally conserved structure and function of immune facilities, the zebrafish also provides a versatile model to examine the functional consequences of genetic variants in immune-relevant genes in the human population. Thus, I propose that genetic approaches using the zebrafish hold great potential for a better understanding of molecular mechanisms of human primary immunodeficiencies and the evolution of vertebrate immune systems.

Published

2014

46. Zebrafish model for allogeneic hematopoietic cell transplantation not requiring preconditioning

Author

Norimasa Iwanami, Isabell Hess, Thomas Boehm, and Michael Schorpp

Subjects

Lymphocyte, Mutation, Missense, Stem cell factor, Models, Biological, Chimera (genetics), Proto-Oncogene Proteins c-myb, medicine, Animals, Humans, Transplantation, Homologous, Gene, Zebrafish, Multidisciplinary, biology, Hematopoietic Stem Cell Transplantation, Biological Sciences, Zebrafish Proteins, biology.organism_classification, Hematopoietic Stem Cells, Molecular biology, Cell biology, Hematopoiesis, Transplantation, Haematopoiesis, medicine.anatomical_structure, Amino Acid Substitution, Stem cell

Abstract

Recent work on vertebrate hematopoiesis has uncovered the presence of deeply rooted similarities between fish and mammals at molecular and cellular levels. Although small animal models such as zebrafish are ideally suited for genetic and chemical screens, the study of cellular aspects of hematopoietic development in lower vertebrates is severely hampered by the complex nature of their histocompatibility-determining genes. Hence, even when hosts are sublethally irradiated before hematopoietic cell transplantation, stable and long-term reconstitution by allogeneic stem cells often fails. Here, we describe the unexpected observation that transplantation and maintenance of allogeneic hematopoietic stem cells in zebrafish homozygous for the c-myb t25127 allele, carrying a missense mutation (Ile181Asn) in the DNA binding domain can be achieved without prior conditioning. Using this model, we examined several critical parameters of zebrafish hematopoiesis in a near-physiological setting. Limiting dilution analysis suggests that the kidney marrow of adult zebrafish harbors about 10 transplantable hematopoietic stem cells; this tissue also contains thymus-settling precursors that colonize the thymic rudiment within days after transplantation and initiate robust T-cell development. We also demonstrate that c-myb mutants can be stably reconstituted with hematopoietic cells carrying specific genetic defects in lymphocyte development, exemplifying one of the many potential uses of this model in experimental hematology.

Published

2013

47. Evolution of the immune system in the lower vertebrates

Author

Isabell Hess, Thomas Boehm, and Norimasa Iwanami

Subjects

Lymphoid Tissue, animal diseases, Lineage (evolution), chemical and pharmacologic phenomena, Adaptive Immunity, Evolution, Molecular, Fish Diseases, Immune system, Phylogenetics, biology.animal, Genetics, Animals, Humans, Molecular Biology, Genetics (clinical), Coevolution, Phylogeny, biology, Lamprey, Fishes, Immunologic Deficiency Syndromes, Vertebrate, biochemical phenomena, metabolism, and nutrition, Acquired immune system, biology.organism_classification, Evolutionary biology, Immune System, Immunology, bacteria, Hagfish

Abstract

The evolutionary emergence of vertebrates was accompanied by the invention of adaptive immunity. This is characterized by extraordinarily diverse repertoires of somatically assembled antigen receptors and the facility of antigen-specific memory, leading to more rapid and efficient secondary immune responses. Adaptive immunity emerged twice during early vertebrate evolution, once in the lineage leading to jawless fishes (such as lamprey and hagfish) and, independently, in the lineage leading to jawed vertebrates (comprising the overwhelming majority of extant vertebrates, from cartilaginous fishes to mammals). Recent findings on the immune systems of jawless and jawed fishes (here referred to as lower vertebrates) impact on the identification of general principles governing the structure and function of adaptive immunity and its coevolution with innate defenses. The discovery of conserved features of adaptive immunity will guide attempts to generate synthetic immunological functionalities and thus provide new avenues for intervening with faulty immune functions in humans.

Published

2012

48. Genetic evidence for an evolutionarily conserved role of IL-7 signaling in T cell development of zebrafish

Author

Cristian Soza-Ried, Nico Riffel, Norimasa Iwanami, Isabell Hess, Thomas Boehm, Fernando Mateos, and Michael Schorpp

Subjects

Genetics, Receptors, Interleukin-7, biology, Positional cloning, T cell, Interleukin-7, T-Lymphocytes, Immunology, Lymphocyte differentiation, Thymus Gland, biology.organism_classification, Evolution, Molecular, medicine.anatomical_structure, Organ Specificity, Mutation, medicine, Immunology and Allergy, Animals, Signal transduction, Cytokine receptor, Janus kinase, Zebrafish, B cell, Signal Transduction

Abstract

In mammals, the cytokine IL-7 is a key regulator of various aspects of lymphocyte differentiation and homeostasis. Because of the difficulty of identifying cytokine homologs in lower vertebrates and the paucity of assay systems and reagents, the degree of functional conservation of cytokine signaling pathways, particularly those pertaining to lymphocyte development, is unclear. In this article, we report on the analysis and characterization of three zebrafish mutants with severely impaired thymopoiesis. The identification of affected genes by positional cloning revealed components of the IL-7 signaling pathway. A presumptive null allele of the zebrafish homolog of the IL-7Rα–chain causes substantially reduced cellularity of the thymus but spares B cell development in the kidney. Likewise, nonsense mutations in the zebrafish homologs of janus kinases JAK1 and JAK3 preferentially affect T cell development. The functional interactions of the cytokine receptor components were examined in the three groups of fish hetero- or homozygous for either il7r and jak1, il7r and jak3, or jak1 and jak3 mutations. The differential effects on T cell development arising from the different genotypes could be explained on the basis of the known structure of the mammalian IL-7R complex. Because IL-7 signaling appears to be a universal requirement for T cell development in vertebrates, the mutants described in this article represent alternative animal models of human immunodeficiency syndromes amenable to large-scale genetic and chemical screens.

Published

2011

49. Cover Picture: Eur. J. Immunol. 9/09

Author

Takashi Sasaki, Vu Q. Hoa, Makoto Furutani-Seiki, Norimasa Iwanami, Nobuyoshi Shimizu, Hiroshi Mitani, Yasuhito Seo, Yousuke Takahama, Hisato Kondoh, and Minoru Okada

Subjects

Evolutionary biology, Immunology, Immunology and Allergy, Cover (algebra), Organ development, Biology

Abstract

This cover is specifically designed to celebrate the 2nd European Congress of Immunology (www.eci-berlin2009.com), to be held September 13–16, 2009 in Berlin. The cover consists of a collage of images from Iwanami et al. (pp 2606–2616) with Berlin's historic Bradenburg Gate, Brandenburger Tor, in the forefront (image of the Brandenburg Gate r ImageState'. Iwanami et al.'s elegant study shows that, in addition, to defective thymus development, teleosts with mutations in KIAA1440, TRRAP, and SKIV2L2 also exhibit defective development of multiple organs, thus identifying previously unknown roles of these genes in organ development.

Published

2009

50. Mutations affecting the formation of posterior lateral line system in Medaka, Oryzias latipes

Author

Katsutoshi Niwa, Hisato Kondoh, Sanae Kunimatsu, Yukihiro Hirose, Akihito Yasuoka, Yoshiko Aihara, Thorsten Henrich, Norimasa Iwanami, Hiroki Yoda, Keiko Abe, Chikako Morinaga, Makoto Furutani-Seiki, Takao Sasado, Tomonori Deguchi, and Hiroshi Suwa

Subjects

Genetics, Embryology, Mutation, animal structures, biology, Sensory Receptor Cells, Oryzias, Lateral line, Mutant, Embryo, medicine.disease_cause, biology.organism_classification, Cell biology, embryonic structures, medicine, Animals, Primordium, Peripheral Nerves, Growth cone, Gene, Developmental Biology

Abstract

We performed a systematic screen for mutations affecting the trajectory of axons visualized by immunohistochemical staining of Medaka embryos with anti-acetylated tubulin antibody. Among the mutations identified, yanagi (yan) and kazura (kaz) mutations caused specific defects in projection of the posterior lateral line (PLL) nerve. In yan and kaz mutant embryos, the PLL nerve main bundle was misrouted ventrally and dorsally or anteriorly. Medaka semaphorin3A, sdf1, and cxcr4 cDNA fragments were cloned to allow analysis of these mutants. There were no changes in semaphorin3A or sdf1 expression in mutant embryos, suggesting that the tissues expressing semaphorin3A or sdf1 that are involved in PLL nerve guidance are present in these mutant embryos. Double staining revealed that the mislocated PLL primordium and growth cone of the ectopically projected PLL nerve were always colocalized in both yan and kaz mutant embryos, suggesting that migration of PLL primordia and PLL nerve growth cones are not uncoupled in these mutants. Although homozygous yan larvae showed incomplete migration of the PLL primordium along the anteroposterior axis, ventral proneuromast migration was complete, suggesting that ventral migration of the proneuromast does not require the signaling affected in yan mutants. In addition to the PLL system, the distribution of primordial germ cells (PGCs) was also affected in both yan and kaz mutant embryos, indicating that yan and kaz genes are required for the migration of both PLL primordia and PGCs. Genetic linkage analysis indicated that kaz is linked to cxcr4, but yan is not linked to sdf1 or cxcr4. These mutations will provide genetic clues to investigate the molecular mechanism underlying formation of the PLL system.

Published

2003