Your search keyword '"Hironori Hojo"' showing total 92 results

51. Antxr1, Which is a Target of Runx2, Regulates Chondrocyte Proliferation and Apoptosis

Author

Hironori Hojo, Shinsuke Ohba, Xin Qin, Toshihisa Komori, Hisato Komori, Brad St. Croix, Carolina A. Yoshida, Qing Jiang, Kei Yamana, and Viviane K. S. Kawata-Matsuura

Subjects

Male, Core Binding Factor Alpha 1 Subunit, lcsh:Chemistry, Mice, Osteogenesis, Runx2, Femur, lcsh:QH301-705.5, Spectroscopy, Mice, Knockout, Microfilament Proteins, apoptosis, Osteoblast, Cell Differentiation, General Medicine, GAPO syndrome, Computer Science Applications, Cell biology, Up-Regulation, RUNX2, medicine.anatomical_structure, Female, Genetically modified mouse, musculoskeletal diseases, Receptors, Cell Surface, Biology, Catalysis, Chondrocyte, Article, Inorganic Chemistry, Chondrocytes, Downregulation and upregulation, medicine, Animals, Physical and Theoretical Chemistry, Molecular Biology, Endochondral ossification, Skeleton, Cell Proliferation, Antxr1, Tibia, Organic Chemistry, Endothelial Cells, medicine.disease, Mice, Inbred C57BL, Cartilage, lcsh:Biology (General), lcsh:QD1-999, Apoptosis, Mutation, Transcriptome, chondrocyte proliferation

Abstract

Antxr1/Tem8 is highly expressed in tumor endothelial cells and is a receptor for anthrax toxin. Mutation of Antxr1 causes GAPO syndrome, which is characterized by growth retardation, alopecia, pseudo-anodontia, and optic atrophy. However, the mechanism underlying the growth retardation remains to be clarified. Runx2 is essential for osteoblast differentiation and chondrocyte maturation and regulates chondrocyte proliferation through Ihh induction. In the search of Runx2 target genes in chondrocytes, we found that Antxr1 expression is upregulated by Runx2. Antxr1 was highly expressed in cartilaginous tissues and was directly regulated by Runx2. In skeletal development, the process of endochondral ossification proceeded similarly in wild-type and Antxr1&ndash, /&ndash, mice. However, the limbs of Antxr1&ndash, mice were shorter than those of wild-type mice from embryonic day 16.5 due to the reduced chondrocyte proliferation. Chondrocyte-specific Antxr1 transgenic mice exhibited shortened limbs, although the process of endochondral ossification proceeded as in wild-type mice. BrdU-uptake and apoptosis were both increased in chondrocytes, and the apoptosis-high regions were mineralized. These findings indicated that Antxr1, of which the expression is regulated by Runx2, plays an important role in chondrocyte proliferation and that overexpression of Antxr1 causes chondrocyte apoptosis accompanied by matrix mineralization.

Published

2020

52. Induction and expansion of human PRRX1

Author

Daisuke, Yamada, Masahiro, Nakamura, Tomoka, Takao, Shota, Takihira, Aki, Yoshida, Shunsuke, Kawai, Akihiro, Miura, Lu, Ming, Hiroyuki, Yoshitomi, Mai, Gozu, Kumi, Okamoto, Hironori, Hojo, Naoyuki, Kusaka, Ryosuke, Iwai, Eiji, Nakata, Toshifumi, Ozaki, Junya, Toguchida, and Takeshi, Takarada

Subjects

Homeodomain Proteins, Pluripotent Stem Cells, Tissue Engineering, Polymers, Cell Culture Techniques, Collagen Diseases, Cell Differentiation, Mesenchymal Stem Cells, Mice, SCID, Culture Media, Receptor, Platelet-Derived Growth Factor beta, Mice, Chondrocytes, Mice, Inbred NOD, Animals, Humans, Thy-1 Antigens, Chondrogenesis

Abstract

Current protocols for the differentiation of human pluripotent stem cells (hPSCs) into chondrocytes do not allow for the expansion of intermediate progenitors so as to prospectively assess their chondrogenic potential. Here we report a protocol that leverages PRRX1-tdTomato reporter hPSCs for the selective induction of expandable and ontogenetically defined PRRX1

Published

2020

53. Generation of orthotopically functional salivary gland from embryonic stem cells

Author

Osamu Ohara, Shinsuke Ohba, Kenji Hata, Yusuke Kawashima, Hironori Hojo, Takashi Tsuji, Junichi Tanaka, Miho Ogawa, Ichiro Saito, Rika Yasuhara, Takayoshi Sakai, Shiro Nakamura, Kenji Mishima, Tomio Inoue, Koki Takamatsu, Toshiyuki Fukada, Riko Nishimura, Yo Mabuchi, and Tarou Irie

Subjects

0301 basic medicine, Exocrine gland, animal structures, Science, Saliva secretion, General Physics and Astronomy, Ectoderm, Biology, Regenerative medicine, General Biochemistry, Genetics and Molecular Biology, Salivary Glands, Article, 03 medical and health sciences, Mice, stomatognathic system, medicine, Animals, Humans, Induced pluripotent stem cell, lcsh:Science, Cells, Cultured, Multidisciplinary, Salivary gland, Gene Expression Profiling, Mouth Mucosa, Mouse Embryonic Stem Cells, General Chemistry, Embryonic stem cell, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, medicine.anatomical_structure, HEK293 Cells, embryonic structures, Female, lcsh:Q, Morphogen, Transcription Factors

Abstract

Organoids generated from pluripotent stem cells are used in the development of organ replacement regenerative therapy by recapitulating the process of organogenesis. These processes are strictly regulated by morphogen signalling and transcriptional networks. However, the precise transcription factors involved in the organogenesis of exocrine glands, including salivary glands, remain unknown. Here, we identify a specific combination of two transcription factors (Sox9 and Foxc1) responsible for the differentiation of mouse embryonic stem cell-derived oral ectoderm into the salivary gland rudiment in an organoid culture system. Following orthotopic transplantation into mice whose salivary glands had been removed, the induced salivary gland rudiment not only showed a similar morphology and gene expression profile to those of the embryonic salivary gland rudiment of normal mice but also exhibited characteristics of mature salivary glands, including saliva secretion. This study suggests that exocrine glands can be induced from pluripotent stem cells for organ replacement regenerative therapy., Functional salivary glands have not been generated from embryonic stem cells (mESCs) to date. Here the authors demonstrate directed in vitro differentiation of mESCs to oral ectoderm and salivary gland rudiments that form mature, functional salivary glands after orthotopic transplantation.

Published

2018

54. Identification of the gene-regulatory landscape in skeletal development and potential links to skeletal regeneration

Author

Shinsuke Ohba, Hironori Hojo, and Ung-il Chung

Subjects

0301 basic medicine, Skeletal development, Biomedical Engineering, Gene regulatory network, Computational biology, Biology, Regenerative medicine, Gene regulatory networks, Epigenetic regulation, Biomaterials, 03 medical and health sciences, Epigenetics, lcsh:QH573-671, Enhancer, Gene, Transcription factor, Genetics, lcsh:R5-920, lcsh:Cytology, Osteoblast, Chondrocyte, Chromatin, RUNX2, 030104 developmental biology, Transcriptional regulators, lcsh:Medicine (General), Developmental Biology

Abstract

A class of gene-regulatory elements called enhancers are the main mediators controlling quantitative, temporal and spatial gene expressions. In the course of evolution, the enhancer landscape of higher organisms such as mammals has become quite complex, exerting biological functions precisely and coordinately. In mammalian skeletal development, the master transcription factors Sox9, Runx2 and Sp7/Osterix function primarily through enhancers on the genome to achieve specification and differentiation of skeletal cells. Recently developed genome-scale analyses have shed light on multiple layers of gene regulations, uncovering not only the primary mode of actions of these transcription factors on skeletal enhancers, but also the relation of the epigenetic landscape to three-dimensional chromatin architecture. Here, we review findings on the emerging framework of gene-regulatory networks involved in skeletal development. We further discuss the power of genome-scale analyses to provide new insights into genetic diseases and regenerative medicine in skeletal tissues.

Published

2017

55. An Emerging Regulatory Landscape for Skeletal Development

Author

Andrew P. McMahon, Shinsuke Ohba, and Hironori Hojo

Subjects

Mammals, 0301 basic medicine, Genome, Organogenesis, Gene regulatory network, Gene Expression Regulation, Developmental, Vertebrate, Biology, Bioinformatics, Article, 03 medical and health sciences, 030104 developmental biology, Evolutionary biology, biology.animal, Genetics, Transcriptional regulation, Animals, Gene Regulatory Networks, Gene, Skeleton, Signal Transduction

Abstract

Skeletal development creates the physical framework that shapes our body and its actions. In the past two decades, genetic studies have provided important insights into the molecular processes at play, including the roles of signaling pathways and transcriptional effectors that coordinate an orderly, progressive emergence and expansion of distinct cartilage and bone cell fates in an invariant temporal and spatial pattern for any given skeletal element within that specific vertebrate species. Genome-scale studies have provided additional layers of understanding, moving from individual genes to the gene regulatory landscape, integrating regulatory information through cis-regulatory modules into cell type-specific gene regulatory programs. This review discusses our current understanding of the transcriptional control of mammalian skeletal development, focusing on recent genome-scale studies.

Published

2016

56. Local administration of a hedgehog agonist accelerates fracture healing in a mouse model

Author

Tsuyoshi Takato, Hailati Aini, Shinsuke Ohba, Miki Kashiwagi, Yoshiaki Kitaura, Ung-il Chung, Yujiro Maeda, and Hironori Hojo

Subjects

Male, 0301 basic medicine, Bone density, Callus formation, Biophysics, 030209 endocrinology & metabolism, Thiophenes, Bone healing, Biology, Biochemistry, Chondrocyte, Mice, 03 medical and health sciences, Chondrocytes, Imaging, Three-Dimensional, 0302 clinical medicine, Bone Density, medicine, Animals, Hedgehog Proteins, Proliferation Marker, Bony Callus, Molecular Biology, Fracture Healing, Cyclohexylamines, fungi, food and beverages, Osteoblast, X-Ray Microtomography, Cell Biology, Anatomy, musculoskeletal system, Cell biology, Mice, Inbred C57BL, Tibial Fractures, body regions, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Callus, Smoothened

Abstract

Bone fracture healing is processed through multiple biological stages including the transition from cartilaginous callus to bony callus formation. Because of its specific, temporal and indispensable functions demonstrated by mouse genetic studies, Hedgehog (Hh) signaling is one of the most potent signaling pathways involved in these processes, but the effect of Hh-signaling activation by small compounds on the repair process had not yet been addressed. Here we examined therapeutic effects of local and one shot-administration of the Hh agonist known as smoothened agonist (SAG) on bone fracture healing in a mouse model. A quantitative analysis with three-dimensional micro-computed tomography showed that SAG administration increased the size of both the cartilaginous callus and bony callus at 14 days after the surgery. A histological analysis showed that SAG administration increased the number of cells expressing a proliferation marker and a chondrocyte marker in cartilaginous callus as well as the cells expressing an osteoblast marker in bony callus. These results indicate that the SAG administration resulted in an enhancement of callus formation during bone fracture healing, which is at least in part mediated by an increase in chondrocyte proliferation in cartilaginous callus and the promotion of bone formation in bony callus. Therapeutic strategies with a SAG-mediated protocol may thus be useful for the treatment of bone fractures.

Published

2016

57. Sp7/Osterix Is Restricted to Bone-Forming Vertebrates where It Acts as a Dlx Co-factor in Osteoblast Specification

Author

Hironori Hojo, Lick Pui Lai, Andrew P. McMahon, Shinsuke Ohba, and Xinjun He

Subjects

0301 basic medicine, Genetically modified mouse, Article, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, Osteogenesis, biology.animal, medicine, Animals, Amino Acid Sequence, Gene Knock-In Techniques, Nucleotide Motifs, Enhancer, Molecular Biology, Homeodomain Proteins, Zinc finger, Genetics, chemistry.chemical_classification, Genome, Osteoblasts, Base Sequence, biology, Reproducibility of Results, Vertebrate, Osteoblast, DNA, Cell Biology, DLX5, AT Rich Sequence, Biological Evolution, Amino acid, Enhancer Elements, Genetic, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, chemistry, Sp7 Transcription Factor, Vertebrates, Bone forming, 030217 neurology & neurosurgery, Transcription Factors, Developmental Biology

Abstract

In extant species, bone formation is restricted to vertebrate species. Sp7/Osterix is a key transcriptional determinant of bone-secreting osteoblasts. We performed Sp7 chromatin immunoprecipitation sequencing analysis identifying a large set of predicted osteoblast enhancers and validated a subset of these in cell culture and transgenic mouse assays. Sp family members bind GC-rich target sequences through their zinc finger domain. Several lines of evidence suggest that Sp7 acts differently, engaging osteoblast targets in Dlx-containing regulatory complexes bound to AT-rich motifs. Amino acid differences in the Sp7 zinc finger domain reduce Sp7's affinity for the Sp family consensus GC-box target; Dlx5 binding maps to this domain of Sp7. The data support a model in which Dlx recruitment of Sp7 to osteoblast enhancers underlies Sp7-directed osteoblast specification. Because an Sp7-like zinc finger variant is restricted to vertebrates, the emergence of an Sp7 member within the Sp family was likely closely coupled to the evolution of bone-forming vertebrates.

Published

2016

58. Gene regulatory landscape in osteoblast differentiation

Author

Shinsuke Ohba and Hironori Hojo

Subjects

0301 basic medicine, Histology, Physiology, Endocrinology, Diabetes and Metabolism, Population, Gene regulatory network, 030209 endocrinology & metabolism, Computational biology, Biology, Cell fate determination, Gene regulatory networks, 03 medical and health sciences, Epigenome, 0302 clinical medicine, Osteogenesis, Transcriptional regulation, Epigenetics, Enhancer, education, Gene, education.field_of_study, Osteoblasts, Cell Differentiation, Gene regulatory landscape, 030104 developmental biology, Gene Expression Regulation, Transcriptional regulators, Signal Transduction

Abstract

The development of osteoblasts, a bone-forming cell population, occurs in conjunction with development of the skeleton, which creates our physical framework and shapes the body. In the past two decades, genetic studies have uncovered the molecular framework of this process?namely, transcriptional regulators and signaling pathways coordinate the cell fate determination and differentiation of osteoblasts in a spatial and temporal manner. Recently emerging genome-wide studies provide additional layers of understanding of the gene regulatory landscape during osteoblast differentiation, allowing us to gain novel insight into the modes of action of the key regulators, functional interaction among the regulator-bound enhancers, epigenetic regulations, and the complex nature of regulatory inputs. In this review, we summarize current understanding of the transcriptional regulation in osteoblasts, in terms of the gene regulatory landscape., Bone, 137, art.no.115458; 2020

Published

2020

59. Insights into Gene Regulatory Networks in Chondrocytes

Author

Shinsuke Ohba and Hironori Hojo

Subjects

Gene regulatory network, Review, Computational biology, Genome, Catalysis, Inorganic Chemistry, Chondrocytes, chondrogenesis, Animals, Humans, Gene Regulatory Networks, Physical and Theoretical Chemistry, Molecular Biology, Gene, Transcription factor, Spectroscopy, biology, Organic Chemistry, High-Throughput Nucleotide Sequencing, General Medicine, Chondrogenesis, Computer Science Applications, Chromatin, Histone, next-generation sequencers, biology.protein, Function (biology), Transcription Factors, Sox9

Abstract

Chondrogenesis is a key developmental process that molds the framework of our body and generates the skeletal tissues by coupling with osteogenesis. The developmental processes are well-coordinated by spatiotemporal gene expressions, which are hardwired with gene regulatory elements. Those elements exist as thousands of modules of DNA sequences on the genome. Transcription factors function as key regulatory proteins by binding to regulatory elements and recruiting cofactors. Over the past 30 years, extensive attempts have been made to identify gene regulatory mechanisms in chondrogenesis, mainly through biochemical approaches and genetics. More recently, newly developed next-generation sequencers (NGS) have identified thousands of gene regulatory elements on a genome scale, and provided novel insights into the multiple layers of gene regulatory mechanisms, including the modes of actions of transcription factors, post-translational histone modifications, chromatin accessibility, the concept of pioneer factors, and three-dimensional chromatin architecture. In this review, we summarize the studies that have improved our understanding of the gene regulatory mechanisms in chondrogenesis, from the historical studies to the more recent works using NGS. Finally, we consider the future perspectives, including efforts to improve our understanding of the gene regulatory landscape in chondrogenesis and potential applications to the treatment of chondrocyte-related diseases.

Published

2019

60. Distinct Transcriptional Programs Underlie Sox9 Regulation of the Mammalian Chondrocyte

Author

Xinjun He, Hironori Hojo, Andrew P. McMahon, and Shinsuke Ohba

Subjects

Transcriptional Activation, endocrine system, Chromatin Immunoprecipitation, Core Binding Factor Alpha 1 Subunit, SOX9, Biology, Genome, General Biochemistry, Genetics and Molecular Biology, Chondrocyte, Article, chemistry.chemical_compound, Mice, Chondrocytes, Transcriptional regulation, medicine, Animals, Humans, Enhancer, Gene, lcsh:QH301-705.5, Cells, Cultured, Genetics, Mice, Inbred ICR, SOX9 Transcription Factor, Sequence Analysis, DNA, Chromatin, medicine.anatomical_structure, chemistry, lcsh:Biology (General), Gene Expression Regulation, embryonic structures, DNA

Abstract

SummarySox9 encodes an essential transcriptional regulator of chondrocyte specification and differentiation. When Sox9 nuclear activity was compared with markers of chromatin organization and transcriptional activity in primary chondrocytes, we identified two distinct categories of target association. Class I sites cluster around the transcriptional start sites of highly expressed genes with no chondrocyte-specific signature. Here, Sox9 association reflects protein-protein association with basal transcriptional components. Class II sites highlight evolutionarily conserved active enhancers that direct chondrocyte-related gene activity through the direct binding of Sox9 dimer complexes to DNA. Sox9 binds through sites with sub-optimal binding affinity; the number and grouping of enhancers into super-enhancer clusters likely determines the levels of target gene expression. Interestingly, comparison of Sox9 action in distinct chondrocyte lineages points to similar regulatory strategies. In addition to providing insights into Sox family action, our comprehensive identification of the chondrocyte regulatory genome will facilitate the study of skeletal development and human disease.

Published

2015

61. Signaling pathways regulating the specification and differentiation of the osteoblast lineage

Author

Shinsuke Ohba, Hironori Hojo, and Ung-il Chung

Subjects

lcsh:R5-920, Signaling pathways, Specification and differentiation, lcsh:Cytology, Regeneration (biology), Mesenchymal stem cell, Osteoblast lineage, Biomedical Engineering, Wnt signaling pathway, Osteoblast, Review Article, Biology, Bone morphogenetic protein, Cell biology, Biomaterials, medicine.anatomical_structure, Transcription factors, medicine, lcsh:QH573-671, Signal transduction, lcsh:Medicine (General), Bone regeneration, Transcription factor, Developmental Biology

Abstract

Tissue engineering is an approach to the regeneration of tissues that uses a combination of cell sources, signaling factors and scaffolds. Among these three components, signaling factors for bone regeneration have not yet been established, and it is necessary to better understand osteoblast progenitors as a target cells. Several lines of evidence have revealed that, during bone formation, mesenchymal cells are specified and differentiate into osteoblasts through several stages of precursors. The osteoblast lineage is defined by the expression of stage-specific transcription factors. The specification and differentiation are organized by a variety of signaling pathways including hedgehog (Hh), Wnt, Notch, bone morphogenetic protein (BMP) and transforming growth factor-beta (TGFβ). In this review we integrate the known functions of these signaling pathways and discuss future tasks to gain a better understanding of the signaling network in osteogenesis for tissue engineering.

Published

2015

62. The regulation of Smpd3 expression in skeletal tissues and its role in fracture healing

Author

Garthiga Manickam, Monzur Murshed, Jingjing Li, Amjad Javed, and Hironori Hojo

Subjects

Expression (architecture), General Medicine, Bone healing, Biology, Cell biology, Skeletal tissue

Published

2017

63. Three-dimensional system enabling the maintenance and directed differentiation of pluripotent stem cells under defined conditions

Author

Shinsuke Ohba, Alexander C. Lichtler, Kosuke Kanke, Hironori Hojo, Denise Zujur, and Ung-il Chung

Subjects

Pluripotent Stem Cells, 0301 basic medicine, Mesoderm, endocrine system diseases, organoid, Cellular differentiation, Cell Culture Techniques, 02 engineering and technology, Embryoid body, Biology, digestive system, bone, Osteocytes, Mice, 03 medical and health sciences, Directed differentiation, Osteogenesis, three-dimensional culture, medicine, Animals, pluripotent stem cell, Induced pluripotent stem cell, Research Articles, Multidisciplinary, Tissue Scaffolds, digestive, oral, and skin physiology, SciAdv r-articles, Cell Differentiation, Cell Biology, Anatomy, 021001 nanoscience & nanotechnology, Embryonic stem cell, digestive system diseases, Cell biology, 030104 developmental biology, medicine.anatomical_structure, embryonic structures, osteoblast, Endoderm, Stem cell, 0210 nano-technology, Research Article

Abstract

A three-dimensional culture system enables maintenance of pluripotent stem cells (PSCs) and formation of PSC-derived organoids., The development of in vitro models for the maintenance and differentiation of pluripotent stem cells (PSCs) is an active area of stem cell research. The strategies used so far are based mainly on two-dimensional (2D) cultures, in which cellular phenotypes are regulated by soluble factors. We show that a 3D culture system with atelocollagen porous scaffolds can significantly improve the outcome of the current platforms intended for the maintenance and lineage specification of mouse PSCs (mPSCs). Unlike 2D conditions, the 3D conditions maintained the undifferentiated state of mouse embryonic stem cells (mESCs) without exogenous stimulation and also supported endoderm, mesoderm, and ectoderm differentiation of mESCs under serum-free conditions. Moreover, 3D mPSC–derived mesodermal cells showed accelerated osteogenic differentiation, giving rise to functional osteoblast-osteocyte populations within calcified structures. The present strategy offers a 3D platform suitable for the formation of organoids that mimic in vivo organs containing various cell types, and it may be adaptable to the generation of ectoderm-, mesoderm-, and endoderm-derived tissues when combined with appropriate differentiation treatments.

Published

2017

64. Identification of a chondrocyte-specific Indian Hedgehog enhancer and SOX9-mediated mechanisms of the enhancer activation

Author

Shinsuke Ohba, Hironori Hojo, Akira Yamakawa, and Ung-il Chung

Subjects

Indian hedgehog, medicine.anatomical_structure, Rheumatology, biology, Biomedical Engineering, medicine, Orthopedics and Sports Medicine, Identification (biology), SOX9, biology.organism_classification, Enhancer, Chondrocyte, Cell biology

Published

2018

65. Repair of rabbit segmental femoral defects by using a combination of tetrapod-shaped calcium phosphate granules and basic fibroblast growth factor-binding ion complex gel

Author

Nobuyuki Shimohata, Shinsuke Ohba, Sungjin Choi, I-Li Liu, Hiroyuki Koyama, Nobuo Sasaki, Ryohei Nishimura, Muneki Honnami, Ung-il Chung, Wataru Kamimura, Hironori Hojo, Manabu Mochizuki, and Tetsushi Taguchi

Subjects

Calcium Phosphates, Male, Materials science, Basic fibroblast growth factor, Long bone, Biophysics, chemistry.chemical_element, Bioengineering, Calcium, Fibroblast growth factor, Biomaterials, Neovascularization, chemistry.chemical_compound, Implants, Experimental, Osteogenesis, medicine, Animals, Humans, Bone formation, Femur, Bone regeneration, Ions, Wound Healing, X-Ray Microtomography, Molecular biology, Polypropylene mesh, medicine.anatomical_structure, chemistry, Mechanics of Materials, Ceramics and Composites, Fibroblast Growth Factor 2, Rabbits, medicine.symptom, Gels, Biomedical engineering

Abstract

The effect of tetrapod-shaped alpha tricalcium phosphate granules (TB) as a scaffold combined with basic fibroblast growth factor (bFGF)-binding ion complex gel (f-IC gel) on neovascularization and bone regeneration was evaluated in segmental femoral defects of rabbits. The defects were stabilized using a plate with a polypropylene mesh cage (PMC) containing one of the following: PMC alone (PMC group), TB (TB group), TB and bFGF (TB/f group), TB and IC gel (TB/IC group), or TB and f-IC gel (TB/f-IC group). Four rabbits from each group were euthanized at 2 and 4 weeks after surgery. Histomorphometry showed that the number of vessels and the volume of new bone in the TB/f-IC group were significantly higher than those in the other groups at all time points. There were no differences in the extent of neovascularization and new bone formation between the TB and TB/f groups. These findings suggest that the combination of TB and f-IC gel facilitated both neovascularization and new bone formation in segmental femoral defects of rabbits. This combination may be of considerable use for treating segmental long bone defects.

Published

2013

66. Bone healing by sterilizable calcium phosphate tetrapods eluting osteogenic molecules

Author

Yujiro Maeda, Ung-il Chung, Hironori Hojo, Tsuyoshi Takato, Nobuyuki Shimohata, Kenichi Yamamoto, Shinsuke Ohba, and Sungjin Choi

Subjects

Calcium Phosphates, Male, Time Factors, Materials science, Biocompatibility, Biophysics, chemistry.chemical_element, Bioengineering, Bone healing, Calcium, Lignans, Cell Line, Bone remodeling, Mesoderm, Biomaterials, Mice, Implants, Experimental, Osteogenesis, Bone cell, Animals, Femur, Rats, Wistar, Progenitor cell, Bone regeneration, Wound Healing, Sterilization, Rats, Radiography, chemistry, Mechanics of Materials, Ceramics and Composites, Implant, Biomedical engineering

Abstract

Although bone grafts and prosthetic implants have shown some clinical success in the treatment of bone defects, the graft availability, biocompatibility, function, and longevity still remain to be improved. One possible solution to these problems is to develop bone implants acting on host cells to induce rapid bone regeneration. Here, we demonstrate bone healing by means of a sterilizable and osteogenic molecule-eluting implant system in which two small molecules, a smoothened agonist (SAG) and a helioxanthin derivative (TH), are loaded onto tetrapod-shaped calcium phosphate granules (Tetrabone). We succeeded in directing progenitor cells toward mature osteoblasts with the combined application of the two small molecules acting on different stages of osteogenesis. Tetrabone released SAG and TH for prolonged periods when loaded with these molecules. EOG sterilization did not affect the osteogenic activity of the SAG- and TH-loaded Tetrabones. The combinatorial use of SAG- and TH-loaded Tetrabones achieved bone healing without cell transplantation in a rat femur bone defect model within two weeks. This system will allow us to vary the combination rate of implants loaded with different osteogenic factors depending on the types and sizes of defects, potentially allowing full temporal and spatial control of the bone regeneration.

Published

2013

67. Cell-sheet technology combined with a thienoindazole derivative small compound TD-198946 for cartilage regeneration

Author

Taku Saito, Shinsuke Ohba, Hiroshi Kawaguchi, Hironori Hojo, Ung-il Chung, Tsuyoshi Takato, Fumiko Yano, Muneki Honnami, and Manabu Mochizuki

Subjects

Cartilage, Articular, Indazoles, Materials science, Cell Culture Techniques, Biophysics, Bone Marrow Cells, Bioengineering, Chondrocyte hypertrophy, Osteoarthritis, Heterocyclic Compounds, 4 or More Rings, Chondrocyte, Biomaterials, Mice, Chondrocytes, Dogs, Tissue engineering, medicine, Animals, Humans, Regeneration, Endochondral ossification, Cell Proliferation, Stem cell transplantation for articular cartilage repair, Stem Cells, Cartilage, Cell Differentiation, medicine.disease, Chondrogenesis, Cell biology, Mice, Inbred C57BL, medicine.anatomical_structure, Mechanics of Materials, Ceramics and Composites, Biomedical engineering

Abstract

Articular cartilage is a permanent tissue, with poor self-regenerative capacity. Consequently, a tissue engineering approach to cartilage regenerative therapy could greatly advance the current treatment options for patients with cartilage degeneration and/or defects. A successful tissue engineering approach would require not only induction of chondrogenic differentiation, but also suppression of subsequent endochondral ossification and chondrocyte dedifferentiation. We previously reported that direct injection of the thienoindazole derivative, TD-198946, into the knee joints of mice halted the progression of osteoarthritis; the compound induced chondrogenic differentiation without promoting endochondral ossification. In the present study, we applied TD-198946 to a cell-based cartilage reconstruction model, taking advantage of the cell-sheet technology. Cartilaginous cell-sheets were generated by culturing mouse and canine costal chondrocytes and human mesenchymal stem cells with TD-198946 on temperature-responsive dishes. The transplanted cell-sheets were then successfully used to promote the reconstruction of permanent cartilage, with no evidence of chondrocyte hypertrophy in the knee articular cartilage defects created in mice and canines. Thus, TD-198946 is a promising candidate for cell-based cartilage reconstruction therapies, enabling us to avoid any concern surrounding the use of scaffolds or cytokines to stimulate regeneration.

Published

2013

68. Targeted therapy of spontaneous murine pancreatic tumors by polymeric micelles prolongs survival and prevents peritoneal metastasis

Author

Nobuhiro Nishiyama, Mami Murakami, Mitsunobu R. Kano, Hironori Hojo, Ung-il Chung, Kazunori Kataoka, Yasuko Terada, and Horacio Cabral

Subjects

Genetically modified mouse, Pathology, medicine.medical_specialty, Angiogenesis, medicine.medical_treatment, Antineoplastic Agents, Inflammation, Targeted therapy, Metastasis, Mice, Antigen, Pancreatic cancer, medicine, Animals, Micelles, Peritoneal Neoplasms, Drug Carriers, Multidisciplinary, Chemistry, Biological Sciences, medicine.disease, Survival Analysis, Pancreatic Neoplasms, Cancer research, Nanocarriers, medicine.symptom

Abstract

Nanoscaled drug-loaded carriers are of particular interest for efficient tumor therapy as numerous studies have shown improved targeting and efficacy. Nevertheless, most of these studies have been performed against allograft and xenograft tumor models, which have altered microenvironment features affecting the accumulation and penetration of nanocarriers. Conversely, the evaluation of nanocarriers on genetically engineered mice, which can gradually develop clinically relevant tumors, permits the validation of their design under normal processes of immunity, angiogenesis, and inflammation. Therefore, considering the poor prognosis of pancreatic cancer, we used the elastase 1-promoted luciferase and Simian virus 40 T and t antigens transgenic mice, which develop spontaneous bioluminescent pancreatic carcinoma, and showed that long circulating micellar nanocarriers, incorporating the parent complex of oxaliplatin, inhibited the tumor growth as a result of their efficient accumulation and penetration in the tumors. The reduction of the photon flux from the endogenous tumor by the micelles correlated with the decrease of serum carbohydrate-associated antigen 19-9 marker. Micelles also reduced the incidence of metastasis and ascites, extending the survival of the transgenic mice.

Published

2013

69. AP-1 family members act with Sox9 to promote chondrocyte hypertrophy

Author

Xinjun He, Shinsuke Ohba, Andrew P. McMahon, and Hironori Hojo

Subjects

0301 basic medicine, endocrine system, Chromatin Immunoprecipitation, Chondrocyte hypertrophy, SOX9, Biology, Chondrocyte, 03 medical and health sciences, Chondrocytes, stomatognathic system, Transcription (biology), Gene expression, medicine, Animals, Humans, Enhancer, Molecular Biology, Cells, Cultured, Cell Differentiation, SOX9 Transcription Factor, FOSL2, Molecular biology, Transcription Factor AP-1, Enhancer Elements, Genetic, 030104 developmental biology, medicine.anatomical_structure, embryonic structures, Chondrogenesis, Chromatin immunoprecipitation, Transcription Factors, Research Article, Developmental Biology

Abstract

An analysis of Sox9 binding profiles in developing chondrocytes identified marked enrichment of an AP-1-like motif. Here, we have explored the functional interplay between Sox9 and AP-1 in mammalian chondrocyte development. Among AP-1 family members, Jun and Fosl2 were highly expressed within prehypertrophic and early hypertrophic chondrocytes. Chromatin immunoprecipitation followed by DNA sequencing (ChIP-seq) showed a striking overlap in Jun- and Sox9-bound regions throughout the chondrocyte genome. The similar profiles reflect direct binding of each factor to the same enhancers and a potential for protein-protein interactions within AP-1 and Sox9 containing complexes. In vitro reporter analysis indicated that direct co-binding of Sox9 and AP-1 at target motifs promoted gene activity. In contrast, where only one factor can engage its DNA target, the presence of the other factor suppresses target activation consistent with protein-protein interactions attenuating transcription. Analysis of prehypertrophic chondrocyte removal of Sox9 confirmed the requirement of Sox9 for hypertrophic chondrocyte development, while in vitro and ex vivo analyses showed AP-1 promotes chondrocyte hypertrophy. Sox9 and Jun co-bound and co-activated a Col10a1 enhancer in Sox9 and AP-1 motif-dependent manners consistent with their combined action promoting hypertrophic gene expression. Together, the data support a model where AP-1-family members contribute to Sox9-action in the transition of chondrocytes to the hypertrophic program.

Published

2016

70. Gli1 Protein Participates in Hedgehog-mediated Specification of Osteoblast Lineage during Endochondral Ossification

Author

Fumiko Yano, Shinsuke Ohba, Naomi Nakagata, Yuske Komiyama, Ung-il Chung, Taku Saito, Kentaro Suzuki, Hiroshi Kawaguchi, Keiji Nakajima, Toshiyuki Ikeda, Hironori Hojo, and Tsuyoshi Takato

Subjects

musculoskeletal diseases, medicine.medical_specialty, animal structures, Cellular differentiation, Kruppel-Like Transcription Factors, Core Binding Factor Alpha 1 Subunit, Nerve Tissue Proteins, Zinc Finger Protein Gli2, Biology, Zinc Finger Protein GLI1, Biochemistry, Cell Line, Mice, Fetus, Osteogenesis, Zinc Finger Protein Gli3, GLI1, Internal medicine, GLI3, medicine, Animals, Hedgehog Proteins, Molecular Biology, Endochondral ossification, Hedgehog, Mice, Knockout, Osteoblasts, integumentary system, Gene Expression Regulation, Developmental, Cell Differentiation, Osteoblast, Cell Biology, Spine, Hedgehog signaling pathway, Up-Regulation, Cell biology, RUNX2, medicine.anatomical_structure, Endocrinology, embryonic structures, biology.protein, Developmental Biology

Abstract

With regard to Hedgehog signaling in mammalian development, the majority of research has focused on Gli2 and Gli3 rather than Gli1. This is because Gli1(-/-) mice do not show any gross abnormalities in adulthood, and no detailed analyses of fetal Gli1(-/-) mice are available. In this study, we investigated the physiological role of Gli1 in osteogenesis. Histological analyses revealed that bone formation was impaired in Gli1(-/-) fetuses compared with WT fetuses. Gli1(-/-) perichondrial cells expressed neither runt-related transcription factor 2 (Runx2) nor osterix, master regulators of osteogenesis, in contrast to WT cells. In vitro analyses showed that overexpression of Gli1 up-regulated early osteogenesis-related genes in both WT and Runx2(-/-) perichondrial cells, and Gli1 activated transcription of those genes via its association with their 5'-regulatory regions, underlying the function of Gli1 in the perichondrium. Moreover, Gli1(-/-);Gli2(-/-) mice showed more severe phenotypes of impaired bone formation than either Gli1(-/-) or Gli2(-/-) mice, and osteoblast differentiation was impaired in Gli1(-/-);Gli3(-/-) perichondrial cells compared with Gli3(-/-) cells in vitro. These data suggest that Gli1 itself can induce early osteoblast differentiation, at least to some extent, in a Runx2-independent manner. It also plays a redundant role with Gli2 and is involved in the repressor function of Gli3 in osteogenesis. On the basis of these findings, we propose that upon Hedgehog input, Gli1 functions collectively with Gli2 and Gli3 in osteogenesis.

Published

2012

71. Repair of segmental radial defects in dogs using tailor-made titanium mesh cages with plates combined with calcium phosphate granules and basic fibroblast growth factor-binding ion complex gel

Author

Amaya Koichi, Ryohei Nishimura, Ung-il Chung, Nobuyuki Shimohata, Nobuo Sasaki, Yukinori Urushisaki, Manabu Mochizuki, Tetsushi Taguchi, Shinsuke Ohba, Sungjin Choi, I-Li Liu, Hironori Hojo, Hiroyuki Koyama, Wataru Kamimura, Muneki Honnami, and Makoto Ichimura

Subjects

Calcium Phosphates, Bone Regeneration, 0206 medical engineering, Basic fibroblast growth factor, Long bone, Biomedical Engineering, Medicine (miscellaneous), chemistry.chemical_element, 02 engineering and technology, Calcium, medicine.disease_cause, Beagle, Weight-bearing, Biomaterials, Neovascularization, Weight-Bearing, chemistry.chemical_compound, Dogs, medicine, Animals, Bone regeneration, Titanium, Wound Healing, Anatomy, 021001 nanoscience & nanotechnology, 020601 biomedical engineering, Apposition, Radius, medicine.anatomical_structure, chemistry, Fibroblast Growth Factor 2, medicine.symptom, 0210 nano-technology, Cardiology and Cardiovascular Medicine, Bone Plates, Biomedical engineering

Abstract

Repair of large segmental defects of long bones are a tremendous challenge that calls for a novel approach to supporting immediate weight bearing and bone regeneration. This study investigated the functional and biological characteristics of a combination of a tailor-made titanium mesh cage with a plate (tTMCP) with tetrapod-shaped alpha tricalcium phosphate granules (TB) and basic fibroblast growth factor (bFGF)-binding ion complex gel (f-IC gel) to repair 20-mm segmental radial defects in dogs. The defects were created surgically in 18 adult beagle dogs and treated by implantation of tTMCPs with TB with (TB-gel group) or without (TB group) f-IC gel. Each tTMCP fitted the defect well, and all dogs could bear weight on the affected limb immediately after surgery. Dogs were euthanized 4, 8 and 24 weeks after implantation. Histomorphometry showed greater infiltration of new vessels and higher bone union rate in the TB-gel group than in the TB group. The lamellar bone volume and mineral apposition rate did not differ significantly between the groups, indicating that neovascularization may be the primary effect of f-IC gel on bone regeneration. This combination method which is tTMCP combined with TB and f-IC gel, would be useful for the treatment of segmental long bone defects.

Published

2015

72. Harmine promotes osteoblast differentiation through bone morphogenetic protein signaling

Author

Ung-il Chung, Je-Tae Woo, Hironori Hojo, Midori Asai, Ayaka Hibino, Toshiaki Teruya, Kazuo Nagai, Kazumi Yagasaki, Ji-Won Lee, Takayuki Yonezawa, and Byung-Yoon Cha

Subjects

Inhibitor of Differentiation Protein 1, musculoskeletal diseases, medicine.medical_specialty, Cellular differentiation, Biophysics, Gene Expression, Core Binding Factor Alpha 1 Subunit, Mice, Inbred Strains, Biology, Bone morphogenetic protein, Biochemistry, Bone resorption, Cell Line, Mice, Structure-Activity Relationship, chemistry.chemical_compound, Harmine, Osteogenesis, Osteoclast, Internal medicine, medicine, Animals, Humans, Bone regeneration, Molecular Biology, Osteoblasts, Skull, Cell Differentiation, Osteoblast, Cell Biology, Cell biology, RUNX2, medicine.anatomical_structure, Endocrinology, chemistry, Sp7 Transcription Factor, Bone Morphogenetic Proteins, embryonic structures, Carbolines, Signal Transduction, Transcription Factors

Abstract

Bone mass is regulated by osteoblast-mediated bone formation and osteoclast-mediated bone resorption. We previously reported that harmine, a β-carboline alkaloid, inhibits osteoclast differentiation and bone resorption in vitro and in vivo. In this study, we investigated the effects of harmine on osteoblast proliferation, differentiation and mineralization. Harmine promoted alkaline phosphatase (ALP) activity in MC3T3-E1 cells without affecting their proliferation. Harmine also increased the mRNA expressions of the osteoblast marker genes ALP and Osteocalcin. Furthermore, the mineralization of MC3T3-E1 cells was enhanced by treatment with harmine. Harmine also induced osteoblast differentiation in primary calvarial osteoblasts and mesenchymal stem cell line C3H10T1/2 cells. Structure-activity relationship studies using harmine-related β-carboline alkaloids revealed that the C3-C4 double bond and 7-hydroxy or 7-methoxy group of harmine were important for its osteogenic activity. The bone morphogenetic protein (BMP) antagonist noggin and its receptor kinase inhibitors dorsomorphin and LDN-193189 attenuated harmine-promoted ALP activity. In addition, harmine increased the mRNA expressions of Bmp-2, Bmp-4, Bmp-6, Bmp-7 and its target gene Id1. Harmine also enhanced the mRNA expressions of Runx2 and Osterix, which are key transcription factors in osteoblast differentiation. Furthermore, BMP-responsive and Runx2-responsive reporters were activated by harmine treatment. Taken together, these results indicate that harmine enhances osteoblast differentiation probably by inducing the expressions of BMPs and activating BMP and Runx2 pathways. Our findings suggest that harmine has bone anabolic effects and may be useful for the treatment of bone-decreasing diseases and bone regeneration as a lead compound.

Published

2011

73. Coordination of chondrogenesis and osteogenesis by hypertrophic chondrocytes in endochondral bone development

Author

Ung-il Chung, Fumiko Yano, Shinsuke Ohba, and Hironori Hojo

Subjects

Endocrinology, Diabetes and Metabolism, Chondrocyte hypertrophy, Biology, Chondrocyte, Chondrocytes, Endocrinology, Osteogenesis, medicine, Paraxial mesoderm, Animals, Humans, Orthopedics and Sports Medicine, Endochondral ossification, Bone Development, Ossification, Lateral plate mesoderm, Cell Differentiation, Hypertrophy, General Medicine, Anatomy, Chondrogenesis, Cell biology, medicine.anatomical_structure, embryonic structures, Intramembranous ossification, medicine.symptom, Signal Transduction, Transcription Factors

Abstract

Mammalian bones have three distinct origins (paraxial mesoderm, lateral plate mesoderm, and neural crest) and undergo two different modes of formation (intramembranous and endochondral). Bones derived from the paraxial mesoderm and lateral plate mesoderm mainly form through the endochondral process. During this process, hypertrophic chondrocytes play a vital role in inducing osteogenesis. So far, a number of published papers have provided evidence that chondrocyte hypertrophy and osteoblast differentiation are controlled by a variety of signaling pathways and factors; however, little is known about their hierarchy (which are upstream? which are most potent?). In this review, we discuss the signaling pathways and transcriptional factors regulating chondrocyte hypertrophy and osteoblast differentiation based on the evidence that has been reported and confirmed by multiple independent groups. We then discuss which factor would provide the most coherent evidence for its role in endochondral ossification.

Published

2010

74. Enhancement of bone formation ex vivo and in vivo by a helioxanthin-derivative

Author

Keiji, Nakajima, Yusuke, Komiyama, Hironori, Hojo, Shinsuke, Ohba, Fumiko, Yano, Naoko, Nishikawa, Sigeo, Ihara, Hiroyuki, Aburatani, Tsuyoshi, Takato, and Ung-Il, Chung

Subjects

Scaffold, Bone Regeneration, Thienopyridines, Pyridines, Biophysics, Thiophenes, Biochemistry, Lignans, Mice, chemistry.chemical_compound, Organ Culture Techniques, Osteogenesis, In vivo, Animals, Bone formation, Bone regeneration, Molecular Biology, Osteoblasts, Chemistry, Skull, 3T3 Cells, Cell Biology, Anatomy, Bone cement, In vitro, Metatarsus, Cell biology, Ex vivo, Derivative (chemistry)

Abstract

To effectively treat serious bone defects using bone-regenerative medicine, a small chemical compound that potently induces bone formation must be developed. We previously reported on the osteogenic effect of 4-(4-methoxyphenyl)pyrido[40,30:4,5]thieno[2,3-b]pyridine-2-carboxamide (TH), a helioxanthin-derivative, in vitro. Here, we report on TH's osteogenic effects ex vivo and in vivo. TH-induced new bone formation in both calvarial and metatarsal organ cultures. A novel monitoring system of osteoblastic differentiation using MC3T3-E1 cells revealed that TH was released from alpha-TCP bone cement and this release continued for more than one month. Lastly, the implantation of the alpha-TCP carrier containing TH into defects in mouse skull resulted in increased new bone areas within the defects after 4 weeks. A TH-containing scaffold may help establish a more efficient bone regeneration system.

Published

2010

75. Screening of chondrogenic factors with a real-time fluorescence-monitoring cell line ATDC5-C2ER: Identification of sorting nexin 19 as a novel factor

Author

Hiroshi Kawaguchi, Toshiyuki Ikeda, Taku Saito, Atushi Fukai, Toru Ogasawara, Hironori Hojo, Akinori Kan, Kozo Nakamura, Fumiko Yano, Ung-il Chung, and Naoshi Ogata

Subjects

Cartilage, Articular, Immunology, Vesicular Transport Proteins, Bone Morphogenetic Protein 2, In situ hybridization, Biology, Bone morphogenetic protein 2, Cell Line, Mice, Chondrocytes, Rheumatology, Transforming Growth Factor beta, Osteoarthritis, Animals, Humans, Immunology and Allergy, Pharmacology (medical), Enhancer, Collagen Type II, Sorting Nexins, SOX Transcription Factors, Messenger RNA, Stem Cells, Transfection, Cell Dedifferentiation, Chondrogenesis, Molecular biology, Mice, Inbred C57BL, Disease Models, Animal, Cell culture, Expression cloning, Disease Progression, Carrier Proteins

Abstract

Objective To establish a cell culture system for noninvasive and real-time monitoring of chondrogenic differentiation in order to screen for chondrogenic factors. Methods The optimum reporter construct transfected into chondrogenic ATDC5 cells was selected by a luciferase reporter assay and fluorescence analysis during cultures with insulin. The established cell line was validated according to its fluorescence following stimulation with SOX proteins, bone morphogenetic protein 2 (BMP-2), or transforming growth factor beta (TGFbeta) and was compared with the level of messenger RNA for COL2A1 as well as with the degree of Alcian blue staining. Screening of chondrogenic factors was performed by expression cloning using a retroviral expression library prepared from human tracheal cartilage. The expression pattern of the identified molecule was examined by in situ hybridization and immunohistochemistry. Functional analysis was performed by transfection of the identified gene, the small interfering RNA, and the mutated gene. Results We established an ATDC5 cell line with 4 repeats of a highly conserved enhancer ligated to a COL2A1 basal promoter and the DsRed2 reporter (ATDC5-C2ER). Fluorescence was induced under the stimulations with SOX proteins, BMP-2, or TGFbeta, showing good correspondence to the chondrogenic markers. Screening using the ATDC5-C2ER system identified several chondrogenic factors, including sorting nexin 19 (SNX19). SNX19 was expressed in the limb cartilage of mouse embryos and in the degraded cartilage of adult mouse knee joints during osteoarthritis progression. The gain-of-function and loss-of-function analyses revealed a potent chondrogenic activity of SNX19. Conclusion We established the ATDC5-C2ER system for efficient monitoring of chondrogenic differentiation by fluorescence analysis, and we identified a novel chondrogenic factor (SNX19) using this system. This system will be useful for elucidating the molecular network of chondrogenic differentiation.

Published

2009

76. Development of high-throughput screening system for osteogenic drugs using a cell-based sensor

Author

Takayuki Yonezawa, Je-Tae Woo, Kazuyo Igawa, Shinsuke Ohba, Alexander C. Lichtler, Ung-il Chung, Keiji Nakajima, Yuske Komiyama, Toshiyuki Ikeda, Tsuyoshi Takato, Hironori Hojo, and Fumiko Yano

Subjects

Green Fluorescent Proteins, Osteocalcin, Drug Evaluation, Preclinical, Biophysics, Clone (cell biology), Bone Morphogenetic Protein 2, Biosensing Techniques, Biochemistry, Bone morphogenetic protein 2, Collagen Type I, Fluorescence, Cell Line, Green fluorescent protein, Mice, Genes, Reporter, Osteogenesis, Transforming Growth Factor beta, medicine, Animals, Molecular Biology, Osteoblasts, biology, Osteoblast, Cell Biology, Transfection, Alkaline Phosphatase, Isoflavones, Molecular biology, Rats, medicine.anatomical_structure, Bone Morphogenetic Proteins, biology.protein, Osteoporosis, Alkaline phosphatase, Type I collagen

Abstract

To effectively treat osteoporosis and other bone-loss disorders, small compounds that potently induce bone formation are needed. The present study initially attempted to establish a monitoring system that could detect osteogenic differentiation easily, precisely, and noninvasively. For this purpose, we established pre-osteoblastic MC3T3E1 cells stably transfected with the GFP reporter gene driven by a 2.3 kb fragment of rat type I collagen promoter (Col1a1GFP-MC3T3E1). Among these cells, we selected a clone that fluoresced upon osteogenic stimulation by BMP2. The GFP fluorescence intensity corresponded well to the intensity of alkaline phosphatase (ALP) staining and to the level of osteocalcin (Oc) mRNA. Using this system, we screened natural and synthetic compound libraries and thus identified an isoflavone derivative, glabrisoflavone (GI). GI induced ALP staining and Oc mRNA in a dose-dependent manner. The Col1a1GFP-MC3T3E1 system may be useful for identifying novel osteogenic drugs.

Published

2008

77. Up-regulation of per mRNA Expression by Parathyroid Hormone through a Protein Kinase A-CREB-dependent Mechanism in Chondrocytes

Author

Mika Iemata, Eiichi Hinoi, Taichi Ueshima, Takeshi Takarada, Hironori Hojo, and Yukio Yoneda

Subjects

Male, endocrine system, Period (gene), Type II collagen, CLOCK Proteins, Parathyroid hormone, Cell Cycle Proteins, Cyclic AMP-Dependent Protein Kinase Type II, Biology, CREB, Biochemistry, Cell Line, Mice, Chondrocytes, Organ Culture Techniques, Animals, RNA, Messenger, Cyclic AMP Response Element-Binding Protein, Collagen Type II, Molecular Biology, Metatarsal Bones, Tibia, Nuclear Proteins, Period Circadian Proteins, Cell Biology, Chondrogenesis, Cyclic AMP-Dependent Protein Kinases, Molecular biology, Circadian Rhythm, Up-Regulation, Parathyroid Hormone, Trans-Activators, biology.protein, Signal transduction, Transcription Factors, PER1

Abstract

In bone, clock genes are involved in the circadian oscillation of bone formation and extracellular matrix expression. However, to date little attention has been paid to circadian rhythm in association with expression of clock genes during chondrogenesis in cartilage. In this study, we investigated the functional expression of different clock genes by chondrocytes in the course of cartilage development. The mRNA expression of types I, II, and X collagens exhibited a 24-h rhythm with a peak at zeitgeber time 6, in addition to a 24-h rhythmicity of all the clock genes examined in mouse femurs in vivo. Marked expression of different clock genes was seen in both osteoblastic MC3T3-E1 and chondrogenic ATDC5 cells in vitro, whereas parathyroid hormone (PTH) transiently increased period 1 (per1) mRNA expression at 1 h in both cell lines. Similar increases were seen in the mRNA levels for both per1 and per2 in prehypertrophic chondrocytes in metatarsal organotypic cultures within 2 h of exposure to PTH. PTH significantly activated the mouse per1 (mper1) and mper2 promoters but not the mper3 promoter in a manner sensitive to both a protein kinase A inhibitor and deletion of the cAMP-responsive element sequence (CRE) in ATDC5 cells. In HEK293 cells, introduction of brain and muscle aryl hydrocarbon receptor nuclear translocator-like protein 1 (bmal1)/clock enhanced mouse type II collagen first intron reporter activity without affecting promoter activity, with reduction effected by either per1 or per2. These results suggest that PTH directly stimulates mper expression through a protein kinase A-CRE-binding protein signaling pathway for subsequent regulation of bmal1/clock-dependent extracellular matrix expression in cartilage.

Published

2006

78. Nrf2 Negatively Regulates Osteoblast Differentiation via Interfering with Runx2-dependent Transcriptional Activation

Author

Eiichi Hinoi, Hironori Hojo, Liyang Wang, Yukio Yoneda, Kyosuke Uno, and Sayumi Fujimori

Subjects

Transcriptional Activation, musculoskeletal diseases, NF-E2-Related Factor 2, Ovariectomy, Cellular differentiation, Osteocalcin, Core Binding Factor Alpha 1 Subunit, Transfection, digestive system, environment and public health, Biochemistry, Mice, Chlorocebus aethiops, Animals, Outbred Strains, medicine, Animals, RNA, Messenger, Promoter Regions, Genetic, Molecular Biology, Transcription factor, Cell Nucleus, Messenger RNA, Osteoblasts, Expression vector, biology, Cell Differentiation, Osteoblast, 3T3 Cells, Cell Biology, respiratory system, musculoskeletal system, Molecular biology, Up-Regulation, RUNX2, medicine.anatomical_structure, Gene Expression Regulation, COS Cells, biology.protein, Alkaline phosphatase, Female, Cell Division

Abstract

Nrf2 (nuclear factor E2 p45-related factor 2) is believed to be a transcription factor essential for the regulation of many detoxifying and antioxidative genes in different tissues. In the present study, we investigated the role of Nrf2 in the regulation of osteoblastic differentiation. nrf2 mRNA expression was significantly up-regulated in femur isolated from ovariectomized mice, whereas in situ hybridization analysis revealed that up-regulation of nrf2 mRNA was mainly found in osteoblasts attached on cancellous bone in femur of ovariectomized mice. Expression of Nrf2 protein was also seen in osteoblasts in neonatal mouse tibia and calvaria. In osteoblastic MC3T3-E1 cells stably transfected with nrf2 expression vector, significant inhibition was seen in the maturation-dependent increase in alkaline phosphatase activity as well as the mineralized matrix formation. Stable overexpression of nrf2 significantly impaired Runx2 (runt-related transcription factor 2)-dependent stimulation of osteocalcin promoter activity and recruitment of Runx2 on osteocalcin promoter without affecting the expression of runx2 mRNA. Coimmunoprecipitation and mammalian two-hybrid assay revealed a physical interaction between Runx2 and Nrf2, whereas cellular distribution of endogenous Runx2 was not apparently changed by nrf2 overexpression in MC3T3-E1 cells. Alternatively, Nrf2 bound to antioxidant-responsive element-like-2 sequence of osteocalcin promoter. The inhibition by nrf2 on runx2-dependent osteocalcin promoter activity was partially prevented by the introduction of reporter of deletion mutant for ARE-like-2 sequence of osteocalcin promoter. These data suggest that Nrf2 may negatively regulate cellular differentiation through inhibition of the Runx2-dependent transcriptional activity in osteoblasts.

Published

2006

79. Bone regeneration by the combined use of tetrapod-shaped calcium phosphate granules with basic fibroblast growth factor-binding ion complex gel in canine segmental radial defects

Author

Hironori Hojo, Muneki Honnami, Nobuyuki Shimohata, Ryohei Nishimura, Hiroyuki Koyama, Manabu Mochizuki, Nobuo Sasaki, Sungjin Choi, I-Li Liu, Tetsushi Taguchi, Shinsuke Ohba, Ung-il Chung, and Wataru Kamimura

Subjects

Calcium Phosphates, Male, collagen, Pathology, medicine.medical_specialty, Bone Regeneration, Callus formation, Long bone, Basic fibroblast growth factor, chemistry.chemical_element, Calcium, histomorphometry, calcium phosphate, Neovascularization, chemistry.chemical_compound, Dogs, Implants, Experimental, Osteogenesis, fibroblast growth factor, medicine, Animals, Bone regeneration, Wound Healing, General Veterinary, Tissue Scaffolds, Full Paper, Anatomy, Apposition, medicine.anatomical_structure, chemistry, Bone Substitutes, Fibroblast Growth Factor 2, Surgery, medicine.symptom, Wound healing, Gels, Protein Binding

Abstract

The effect of tetrapod-shaped alpha tricalcium phosphate granules (Tetrabones® [TB]) in combination with basic fibroblast growth factor (bFGF)-binding ion complex gel (f-IC gel) on bone defect repair was examined. Bilateral segmental defects 20-mm long were created in the radius of 5 dogs, stabilized with a plate and screws and implanted with 1 of the following: TB (TB group), TB and bFGF solution (TB/f group), and TB and f-IC gel (TB/f-IC group). Dogs were euthanized 4 weeks after surgery. Radiographs showed well-placed TB granules in the defects and equal osseous callus formation in all the groups. Histomorphometry revealed that the number of vessels and volume of new bone in the TB/f-IC group were significantly higher than those in the other groups. However, no significant differences in neovascularization and new bone formation were observed between the TB/f and TB groups. Furthermore, no significant difference in the lamellar bone volume or rate of mineral apposition was observed among groups. These results suggest that increased bone formation might have been because of the promotion of neovascularization by the f-IC gel. Therefore, the combinatorial method may provide a suitable scaffold for bone regeneration in large segmental long bone defects.

Published

2014

80. Tenomodulin Expression in the Periodontal Ligament Enhances Cellular Adhesion

Author

Yuji Hiraki, Tsuyoshi Takato, Nobuyuki Shimohata, Hironori Hojo, Chisa Shukunami, Yuske Komiyama, Fumiko Yano, Denitsa Docheva, Shinsuke Ohba, Keiji Nakajima, and Ung-il Chung

Subjects

Anatomy and Physiology, Mouse, Periodontal Ligament, Science, Biochemistry, Mice, Model Organisms, stomatognathic system, Molecular Cell Biology, Extracellular, Morphogenesis, Cell Adhesion, Periodontal fiber, Animals, Humans, Cell adhesion, Biology, Musculoskeletal System, Musculoskeletal Anatomy, Extracellular Matrix Adhesions, Cell Line, Transformed, Extracellular Matrix Proteins, Multidisciplinary, Proteins, Membrane Proteins, Transfection, Animal Models, Transmembrane protein, In vitro, Extracellular Matrix Composition, Cell biology, Tenomodulin, Extracellular Matrix, Membrane protein, Connective Tissue, Immunology, Cytochemistry, NIH 3T3 Cells, Medicine, Skeletal Development, Research Article, Developmental Biology

Abstract

Tenomodulin (Tnmd) is a type II transmembrane protein characteristically expressed in dense connective tissues such as tendons and ligaments. Its expression in the periodontal ligament (PDL) has also been demonstrated, though the timing and function remain unclear. We investigated the expression of Tnmd during murine tooth eruption and explored its biological functions in vitro. Tnmd expression was related to the time of eruption when occlusal force was transferred to the teeth and surrounding tissues. Tnmd overexpression enhanced cell adhesion in NIH3T3 and human PDL cells. In addition, Tnmd-knockout fibroblasts showed decreased cell adhesion. In the extracellular portions of Tnmd, the BRICHOS domain or CS region was found to be responsible for Tnmd-mediated enhancement of cell adhesion. These results suggest that Tnmd acts on the maturation or maintenance of the PDL by positively regulating cell adhesion via its BRICHOS domain.

Published

2013

81. Generation of Col2a1-EGFP iPS cells for monitoring chondrogenic differentiation

Author

Hiroshi Kawaguchi, Koji Eto, Daisuke Mori, Hiromitsu Nakauchi, Shinsuke Ohba, Taku Saito, Sakae Tanaka, Fumiko Yano, Ung-il Chung, Hironori Hojo, and Makoto Otsu

Subjects

Science, Cellular differentiation, Green Fluorescent Proteins, Induced Pluripotent Stem Cells, Kruppel-Like Transcription Factors, Mice, Transgenic, Biology, Regenerative medicine, Chondrocyte, Kruppel-Like Factor 4, Mice, Proto-Oncogene Proteins c-myb, SOX2, medicine, Animals, Induced pluripotent stem cell, Collagen Type II, Cells, Cultured, Embryonic Stem Cells, Multidisciplinary, SOXB1 Transcription Factors, Cell Differentiation, Chondrogenesis, Embryonic stem cell, Molecular biology, Cell biology, medicine.anatomical_structure, KLF4, Medicine, Octamer Transcription Factor-3, Research Article

Abstract

Induced pluripotent stem cells (iPSC) are a promising cell source for cartilage regenerative medicine; however, the methods for chondrocyte induction from iPSC are currently developing and not yet sufficient for clinical application. Here, we report the establishment of a fluorescent indicator system for monitoring chondrogenic differentiation from iPSC to simplify screening for effective factors that induce chondrocytes from iPSC. We generated iPSC from embryonic fibroblasts of Col2a1-EGFP transgenic mice by retroviral transduction of Oct4, Sox2, Klf4, and c-Myc. Among the 30 clones of Col2a1-EGFP iPSC we established, two clones showed high expression levels of embryonic stem cell (ESC) marker genes, similar to control ESC. A teratoma formation assay showed that the two clones were pluripotent and differentiated into cell types from all three germ layers. The fluorescent signal was observed during chondrogenic differentiation of the two clones concomitant with the increase in chondrocyte marker expression. In conclusion, Col2a1-EGFP iPSC are useful for monitoring chondrogenic differentiation and will contribute to research in cartilage regenerative medicine.

Published

2013

82. Hedgehog-Gli Activators Direct Osteo-chondrogenic Function of Bone Morphogenetic Protein toward Osteogenesis in the Perichondrium*

Author

Shinsuke Ohba, Tomohiro Konno, Hironori Hojo, Yuji Mishina, Hideki Kambara, Keiji Nakajima, Masataka Shirai, Naomi Nakagata, Yuske Komiyama, Ung-il Chung, Kiyomi Taniguchi, Fumiko Yano, Tsuyoshi Takato, Toshiyuki Ikeda, Hiroshi Kawaguchi, Masahisa Yamada, Kentaro Suzuki, and Taku Saito

Subjects

musculoskeletal diseases, Transcriptional Activation, medicine.medical_specialty, animal structures, Cellular differentiation, Kruppel-Like Transcription Factors, Biology, Bone morphogenetic protein, Biochemistry, Osteocytes, Zinc Finger Protein GLI1, Chondrocyte, Mice, Chondrocytes, Osteogenesis, Internal medicine, medicine, Bone collar, Perichondrium, Animals, Cluster Analysis, Cell Lineage, Hedgehog Proteins, Molecular Biology, Endochondral ossification, Mice, Inbred C3H, Osteoblasts, Osteoblast, Cell Differentiation, SOX9 Transcription Factor, Cell Biology, musculoskeletal system, Recombinant Proteins, Cell biology, Mice, Inbred C57BL, Endocrinology, medicine.anatomical_structure, Gene Expression Regulation, embryonic structures, Bone Morphogenetic Proteins, Ectopic expression, SOXD Transcription Factors

Abstract

Specification of progenitors into the osteoblast lineage is an essential event for skeletogenesis. During endochondral ossification, cells in the perichondrium give rise to osteoblast precursors. Hedgehog (Hh) and bone morphogenetic protein (BMP) are suggested to regulate the commitment of these cells. However, properties of perichondrial cells and regulatory mechanisms of the specification process are still poorly understood. Here, we investigated the machineries by combining a novel organ culture system and single-cell expression analysis with mouse genetics and biochemical analyses. In a metatarsal organ culture reproducing bone collar formation, activation of BMP signaling enhanced the bone collar formation cooperatively with Hh input, whereas the signaling induced ectopic chondrocyte formation in the perichondrium without Hh input. Similar phenotypes were also observed in compound mutant mice, where signaling activities of Hh and BMP were genetically manipulated. Single-cell quantitative RT-PCR analyses showed heterogeneity of perichondrial cells in terms of natural characteristics and responsiveness to Hh input. In vitro analyses revealed that Hh signaling suppressed BMP-induced chondrogenic differentiation; Gli1 inhibited the expression of Sox5, Sox6, and Sox9 (SRY box-containing gene 9) as well as transactivation by Sox9. Indeed, ectopic expression of chondrocyte maker genes were observed in the perichondrium of metatarsals in Gli1(-/-) fetuses, and the phenotype was more severe in Gli1(-/-);Gli2(-/-) newborns. These data suggest that Hh-Gli activators alter the function of BMP to specify perichondrial cells into osteoblasts; the timing of Hh input and its target populations are critical for BMP function.

Published

2013

83. A novel disease-modifying osteoarthritis drug candidate targeting Runx1

Author

Ung-il Chung, Makoto Hirata, Tsuyoshi Takato, Yoko Hosaka, Taku Saito, Hiroshi Kawaguchi, Atsushi Fukai, Fumiko Yano, Hirotaka Chikuda, Shinsuke Ohba, Hironori Hojo, and Toshiyuki Ikeda

Subjects

Cartilage, Articular, Male, Pathology, medicine.medical_specialty, Indazoles, Knee Joint, Cellular differentiation, Immunology, Gene Expression, Drug action, Osteoarthritis, Heterocyclic Compounds, 4 or More Rings, General Biochemistry, Genetics and Molecular Biology, Injections, Intra-Articular, Mice, Rheumatology, In vivo, Immunology and Allergy, Medicine, Animals, RNA, Messenger, business.industry, Microarray analysis techniques, Cartilage, Cell Differentiation, Osteoarthritis, Knee, Chondrogenesis, medicine.disease, In vitro, Disease Models, Animal, medicine.anatomical_structure, Antirheumatic Agents, Drug Design, Core Binding Factor Alpha 2 Subunit, Cancer research, business

Abstract

Objectives To identify a new disease-modifying osteoarthritis drug (DMOAD) candidate that can effectively repair cartilage by promoting chondrogenic differentiation and halt osteoarthritis (OA) progression by suppressing aberrant hypertrophy. Methods We screened 2500 natural and synthetic small compounds for chondrogenic agents via four steps using the Col2GFP-ATDC5 system and identified a small thienoindazole derivative compound, TD-198946, as a novel DMOAD candidate. We tested its efficacy as a DMOAD via intra-articular injections directly into the joint space in a surgically-induced mouse model of OA both at the onset (prevention model) and 4 weeks after (repair model) OA induction. The downstream molecules were screened by microarray analysis. We further investigated the mechanism of the drug action and its molecular target using in vitro and in vivo assays. Results TD-198946 strongly induced chondrogenic differentiation without promoting hypertrophy in cell and metatarsal organ cultures. When administered directly into the joint space, TD-198946 successfully prevented and repaired degeneration of the articular cartilage. TD-198946 exerted its effect through the regulation of Runx1 expression, which was downregulated in both mouse and human OA cartilage compared with normal tissue. Conclusions Our data suggest that TD-198946 is a novel class of DMOAD candidate, and that targeting Runx1 will provide a promising new approach in the development of disease-modifying drugs against OA.

Published

2012

84. Famotidine suppresses osteogenic differentiation of tendon cells in vitro and pathological calcification of tendon in vivo

Author

Kenichi, Yamamoto, Hironori, Hojo, Isao, Koshima, Ung-il, Chung, and Shinsuke, Ohba

Subjects

Male, Osteoblasts, Administration, Oral, Calcinosis, Cell Differentiation, 3T3 Cells, In Vitro Techniques, Famotidine, Cell Line, Tendons, Mice, Histamine H2 Antagonists, Osteogenesis, Animals, Receptors, Histamine H2, RNA, Messenger, Signal Transduction

Abstract

Heterotopic ossification or calcification follows any type of musculoskeletal trauma and is known to occur after arthroplasties of hip, knee, shoulder, or elbow; fractures; joint dislocations; or tendon ruptures. Histamine receptor H2 (Hrh2) has been shown to be effective for reducing pain and decreasing calcification in patients with calcifying tendinitis, which suggested that H2 blockers were effective for the treatment of tendon ossification or calcification. However, the detailed mechanisms of its action on tendon remain to be clarified. We investigated the mechanisms underlying H2 blocker-mediated suppression of tendon calcification, with a focus on the direct action of the drug on tendon cells. Famotidine treatment suppressed the mRNA expressions of Col10a1 and osteocalcin, ossification markers, in a tendon-derived cell line TT-D6, as well as a preosteoblastic one MC3T3-E1. Both of the cell lines expressed Hrh2; histamine treatment induced osteocalcin expression in these cells. Famotidine administration suppressed calcification in the Achilles tendon of ttw mice, a mouse model of ectopic ossification. These data suggest that famotidine inhibits osteogenic differentiation of tendon cells in vitro, and this inhibition may underlie the anti-calcification effects of the drug in vivo. This study points to the use of H2 blockers as a promising strategy for treating heterotopic ossification or calcification in tendon, and provides evidence in support of the clinical use of famotidine.

Published

2011

85. [Novel small compound in combination with cell-sheet technology for articular cartilage regeneration]

Author

Fumiko, Yano, Hironori, Hojo, and Ung il, Chung

Subjects

Cartilage, Articular, Tissue Engineering, Green Fluorescent Proteins, Drug Evaluation, Preclinical, Cell Differentiation, Oxytetracycline, SOX9 Transcription Factor, Disease Models, Animal, Mice, Chondrocytes, Dogs, Animals, Regeneration, Collagen Type II, Cells, Cultured

Abstract

Aiming at regeneration of articular cartilage, we have established stable lines of mouse chondrogenic ATDC5 cells expressing green fluorescent protein under the control of type II collagen promoter fused with four repeats of a SOX9 enhancer (COL2A1-GFP) , as a monitoring system for chondrogenic differentiation. A screening of natural and synthetic compound libraries using the system identified some novel compounds. Combined with cell-sheet technology, a novel small compound was applied to the treatment of full-thickness knee cartilage defects in murine and canine models.

Published

2011

86. Identification of oxytetracycline as a chondrogenic compound using a cell-based screening system

Author

Yuske Komiyama, Hironori Hojo, Keiji Nakajima, Je-Tae Woo, Kozo Nakamura, Akinori Kan, Toshiyuki Ikeda, Kazuyo Igawa, Takayuki Yonezawa, Tsuyoshi Takato, Shinsuke Ohba, Ung-il Chung, Fumiko Yano, and Hiroshi Kawaguchi

Subjects

Inhibitor of Differentiation Protein 1, Pathology, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Cellular differentiation, Drug Evaluation, Preclinical, Oxytetracycline, Bone morphogenetic protein, Chondrocyte, Cell Line, Small Molecule Libraries, Tissue Culture Techniques, Mice, Endocrinology, Chondrocytes, Osteogenesis, Osteoarthritis, medicine, Animals, Orthopedics and Sports Medicine, RNA, Messenger, Noggin, Collagen Type II, Cells, Cultured, Metatarsal Bones, Antibacterial agent, Chemistry, Cartilage, Cell Differentiation, General Medicine, Chondrogenesis, Embryo, Mammalian, Antigens, Differentiation, Cell biology, High-Throughput Screening Assays, Mice, Inbred C57BL, medicine.anatomical_structure, Gene Expression Regulation, Cell culture, Bone Morphogenetic Proteins

Abstract

To effectively treat degenerative joint diseases including osteoarthritis (OA), small chemical compounds need to be developed that can potently induce chondrogenic differentiation without promoting terminal differentiation. For this purpose, we screened natural and synthetic compound libraries using a Col2GFP-ATDC5 system and identified oxytetracycline (Oxy) as a chondrogenic compound. Oxy induced cartilaginous matrix synthesis and mRNA expressions of chondrocyte markers in ATDC5 cells. In addition, Oxy suppressed mineralization and mRNA expressions of terminal chondrocyte differentiation markers in ATDC5 cells, primary chondrocytes, and cultured metatarsal bones. Oxy's induction of Col2 mRNA expression was decreased by the addition of Noggin and was increased by the addition of BMP2. Furthermore, Oxy increased mRNA expression of Id1, Bmp2, Bmp4, and Bmp6. These data suggest that Oxy induces chondrogenic differentiation in a BMP-dependent manner and suppresses terminal differentiation. Oxy may be useful for treatment of OA and also for regeneration of cartilage tissue.

Published

2009

87. Interference by adrenaline with chondrogenic differentiation through suppression of gene transactivation mediated by Sox9 family members

Author

Hironori Hojo, Ayumi Kodama, Mika Iemata, Nobuhiro Nakamura, Yukio Yoneda, Eiichi Hinoi, Takeshi Takarada, and Koichi Sahara

Subjects

CAMP Responsive Element Binding Protein, Transcriptional Activation, medicine.medical_specialty, Histology, Epinephrine, Physiology, Endocrinology, Diabetes and Metabolism, Cellular differentiation, Biology, Chondrocyte, Transactivation, Fractures, Bone, Mice, Chondrocytes, Downregulation and upregulation, Adrenergic beta-2 Receptor Antagonists, Receptors, Adrenergic, alpha-2, Internal medicine, medicine, Cyclic AMP, Animals, RNA, Messenger, Protein kinase A, Cells, Cultured, Metatarsal Bones, Tibia, Cell Differentiation, SOX9 Transcription Factor, Chondrogenesis, Embryo, Mammalian, Endocrinology, medicine.anatomical_structure, Animals, Newborn, Receptors, Adrenergic, beta-2, SOXD Transcription Factors, Type I collagen, Signal Transduction

Abstract

In contrast to osteoblasts, little attention has been paid to the functional expression of adrenergic signaling machineries in chondrocytes. Expression of mRNA was for the first time demonstrated for different adrenergic receptor (AdR) subtypes in chondrogenic ATDC5 cells and mouse metatarsals isolated before vascularization in culture, but not for other molecules related to adrenergic signaling. In neonatal mouse tibial sections, beta(2)AdR and alpha(2a)AdR mRNA expression was found in chondrocytes at different developmental stages by in situ hybridization. Exposure to adrenaline significantly suppressed expression of several maturation markers through the cAMP/protein kinase A pathway activated by beta(2)AdR without affecting cellular proliferation in both cultured ATDC5 cells and metatarsals. Adrenaline also significantly inhibited gene transactivation by sry-type HMG box 9 (Sox9) family members essential for chondrogenic differentiation in a manner prevented by the general betaAdR antagonist propranolol, with a concomitant significant decrease in the levels of Sox6 mRNA and corresponding protein, in ATDC5 cells and primary cultured mouse costal chondrocytes. Systemic administration of propranolol significantly promoted the increased expression of mRNA for collagen I and collagen X, but not for collagen II, in callus of fractured femur in mice. These results suggest that adrenaline may interfere with chondrogenic differentiation through downregulation of Sox6 expression for subsequent suppression of gene transactivation mediated by Sox9 family members after activation of beta(2)AdR expressed by chondrocytes.

Published

2009

88. Excitatory amino acid transporters expressed by synovial fibroblasts in rats with collagen-induced arthritis

Author

Takeshi Takarada, Ryosuke Ohashi, Mika Iemata, Eiichi Hinoi, Hironori Hojo, Susumu Miyata, Yasuko Kato, and Yukio Yoneda

Subjects

Male, medicine.medical_specialty, Arthritis, Glutamic Acid, Biochemistry, Internal medicine, medicine, Glutamate aspartate transporter, Synovial fluid, Animals, RNA, Messenger, Receptor, Fibroblast, Cells, Cultured, Pharmacology, biology, Synovial Membrane, Glutamate receptor, Fibroblasts, medicine.disease, Arthritis, Experimental, Rats, Excitatory Amino Acid Transporter 1, medicine.anatomical_structure, Endocrinology, Excitatory Amino Acid Transporter 3, Excitatory Amino Acid Transporter 2, Metabotropic glutamate receptor, Rats, Inbred Lew, Immunology, biology.protein, Cytokines, Synovial membrane, Signal Transduction

Abstract

Although previous studies have demonstrated increased levels of the brain neurotransmitter glutamate (Glu) in the synovial fluid from patients with arthritis, not much attention has been paid to the possible role of Glu in joint synovial tissues to date. Constitutive expression of mRNA was for the first time shown with glutamate aspartate transporter, glutamate transporter-1 and excitatory amino acid carrier-1 (EAAC1), in addition to with particular ionotropic and metabotropic Glu receptors, in cultured synovial fibroblasts prepared from knee joints of male Lewis rats. Immunohistochemical analysis revealed high localization of immunoreactive EAAC1 at synovial tissues. The accumulation of [3H]Glu occurred in a temperature- and sodium-dependent manner in cultured synovial fibroblasts, with a Km of 23.1 ± 1.1 μM and a Vmax of 237.1 ± 31.1 pmol/(mg protein min), respectively. In rats with arthritis induced by immunization to type-II collagen, marked increases were seen in hind paw volume, cytokine mRNA expression and Glu levels in synovial tissues, in addition to histological erosion. In cultured synovial fibroblasts prepared from these arthritic rats, [3H]Glu accumulation was drastically increased with biochemical and pharmacological profiles similar to those seen in normal synovial fibroblasts. The exposure to Glu at 500 μM doubled the incorporation of 5-bromo-2′-deoxyuridine in cultured synovial fibroblasts of arthritic but not normal rats, without significantly affecting mRNA expression of different cytokines in both synovial fibroblasts. These results suggest that Glu may at least in part play a role in mechanisms associated with cellular proliferation through particular transporters functionally expressed by synovium in rheumatoid arthritis.

Published

2005

89. Prevention and repair of cartilage degeneration by a novel small thienoindazole-derivative compound

Author

Yoko Hosaka, Ung-il Chung, Shinsuke Ohba, Atsushi Fukai, Hiroshi Kawaguchi, Hironori Hojo, T. Saito, and Fumiko Yano

Subjects

chemistry.chemical_compound, Rheumatology, Chemistry, Biophysics, Biomedical Engineering, Orthopedics and Sports Medicine, Cartilage degeneration, Derivative (chemistry)

Published

2012

90. Current Progress on Tissue Engineering of Bone and Cartilage

Author

Shinsuke Ohba, Hironori Hojo, and Ung-il Chung

Subjects

Endocrinology, Endocrinology, Diabetes and Metabolism, Library science, Integrative medicine

Abstract

Corresponding author: Ung-il Chung Department of Bioengineering, The University of Tokyo Graduate School of Engineering, 7-3-1 Hongo, Bunkyo-gu, Tokyo 113-0033, Japan Tel: +81-3-5841-1427, Fax: +81-3-5841-1428, E-mail: tei@bioeng.t.u-tokyo.ac.jp Current Progress on Tissue Engineering of Bone and Cartilage Shinsuke Ohba, Hironori Hojo, Ung-il Chung 1,2 Division of Clinical Biotechnology, Center for Disease Biology and Integrative Medicine, The University of Tokyo Graduate School of Medicine, Toyko; Department of Bioengineering, The University of Tokyo Graduate School of Engineering, Tokyo, Japan Endocrinol Metab 27(1):1-11, March 2012 http://dx.doi.org/10.3803/EnM.2012.27.1.1 REVIEW ARTICLE

Published

2012

91. Bioactive factors for tissue regeneration: state of the art.

Author

Ohba, Shinsuke, Hironori Hojo, and Ung-il Chung

Subjects

*TISSUE engineering, *BONE regeneration, *CARTILAGE, *CARTILAGE cells, *MESENCHYMAL stem cells, *OSTEOBLASTS, *BONE metabolism, *PROTEIN metabolism, *GENES, *GROWTH factors, *REGENERATION (Biology), *WOUND healing

Abstract

There are three components for the creation of new tissues: cell sources, scaffolds, and bioactive factors. Unlike conventional medical strategies, regenerative medicine requires not only analytical approaches but also integrative ones. Basic research has identified a number of bioactive factors that are necessary, but not sufficient, for organogenesis. In skeletal development, these factors include bone morphogenetic proteins (BMPs), transforming growth factor β TGF-β , Wnts, hedgehogs (Hh), fibroblast growth factors (FGFs), insulin-like growth factors (IGFs), SRY boxcontaining gene (Sox) 9, Sp7, and runt-related transcription factors (Runx). Clinical and preclinical studies have been extensively performed to apply the knowledge to bone and cartilage regeneration. Given the large number of findings obtained so far, it would be a good time for a multi-disciplinary, collaborative effort to optimize these known factors and develop appropriate drug delivery systems for delivering them. [ABSTRACT FROM AUTHOR]

Published

2012

92. Percolation induced gel-gel phase separation in a dilute polymer network

Author

Shohei Ishikawa, Naoyuki Sakumichi, Takamasa Sakai, Yasuhide Iwanaga, Takashi Uneyama, Xiang Li, Hironori Hojo, Ikuo Fujinaga, Takuya Katashima, Taku Saito, and Ungil Chung

Subjects

Condensed Matter - Materials Science, Soft Condensed Matter (cond-mat.soft), Materials Science (cond-mat.mtrl-sci), FOS: Physical sciences, Condensed Matter - Soft Condensed Matter

Abstract

Cosmic large-scale structures, animal flocks, and living tissues are non-equilibrium organized systems created by dissipative processes. Despite the uniqueness, the realization of dissipative structures is still difficult. Herein, we report that a network formation process in a dilute system is a dissipative process, leading to percolation induced gel-gel phase separation (GGPS) in a prominent miscible polymer-water system. The dilute system, which forms a monophase structure at the percolation threshold, eventually separates into two gel phases in a longer time scale as the network formation progresses. The dilute hydrogel with GGPS exhibits an unexpected mesoscale co-continuous structure and induces adipose growth in subcutaneous. The formation mechanism of GGPS and a cosmic large-scale structure is analogous, in terms of attractive interactions in a diluted system driving phase separation. This unique phenomenon unveils the possibility of dissipative structures enabling advanced functionalities and will stimulate research fields related to dissipative structures., Comment: 23+5 pages, 4+4 figures