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101. Syndecan-4 Deficiency Leads to High Mortality of Lipopolysaccharide-injected Mice

Author

Kazuhiro Ishiguro, Mitsunori Iwase, Kenji Kadomatsu, Tetsuhito Kojima, Tadashi Matsushita, Yasunobu Yoshikai, Masamitsu Yanada, Kazuo Kusugami, Hisako Muramatsu, Masahiko Nishimura, Takashi Muramatsu, Koji Yamamoto, and Hidehiko Saito

Subjects
Lipopolysaccharides, medicine.medical_specialty, Time Factors, animal structures, Lipopolysaccharide, Recombinant Fusion Proteins, medicine.medical_treatment, Intraperitoneal injection, Blood Pressure, Stimulation, Biology, Inhibitory postsynaptic potential, Biochemistry, Monocytes, Ventricular Function, Left, Syndecan 1, Mice, chemistry.chemical_compound, Transforming Growth Factor beta, Internal medicine, medicine, Animals, Endothelium, Molecular Biology, Glutathione Transferase, Membrane Glycoproteins, Macrophages, Interleukin, Shock, Cell Biology, Flow Cytometry, Immunohistochemistry, Transmembrane protein, Interleukin-10, Mice, Inbred C57BL, carbohydrates (lipids), Endocrinology, Blood pressure, Liver, chemistry, embryonic structures, Immunology, Cytokines, Proteoglycans, Syndecan-4, Injections, Intraperitoneal, Interleukin-1, Protein Binding
Abstract

Syndecan-4 is a transmembrane heparan sulfate proteoglycan belonging to the syndecan family. Following intraperitoneal injection of lipopolysaccharide (LPS), syndecan-4-deficient mice exhibited high mortality compared with wild-type controls. Severe endotoxin shock was observed in the deficient mice: systolic blood pressure and left ventricular fractional shortening were lower in the deficient mice than in the wild-type controls 9 h after LPS injection. Although histological examinations revealed no apparent differences between two groups, the plasma level of interleukin (IL)-1beta was higher in the deficient mice than in the wild-type controls 9 h after LPS injection. Consistent with the regulatory roles of syndecan-4, its expression in monocytes and endothelial cells of microvasculature increased in the wild-type mice after LPS administration. Although IL-1beta was produced to the same extent by macrophages from syndecan-4-deficient and wild-type mice after LPS stimulation, inhibition of its production by transforming growth factor-beta1 was impaired in the syndecan-4-deficient macrophages. These results indicate that syndecan-4 could be involved in prevention of endotoxin shock, at least partly through the inhibitory action of transforming growth factor-beta1 on IL-1beta production.

Published
2001

102. Clinical Trial to Investigate the Pharmacokinetics, Pharmacodynamics, Safety, and Efficacy of Recombinant Factor VIIa in Japanese Patients With Hemophilia With Inhibitors

Author

Yoko Minamoto, Tetsuhito Kojima, Midori Shima, Shigeru Fujita, Hideji Hanabusa, Katsuyuki Fukutake, Morio Arai, Akira Shirahata, Hiroyuki Naka, Hidehiko Saito, Junki Takamatsu, H. Tagami, Tadashi Kamiya, Akira Yoshioka, and Junji Kamizono

Subjects
Adult, Adolescent, Factor VIIa, Hemophilia A, Japan, Pharmacokinetics, Isoantibodies, medicine, Coagulopathy, Humans, Adverse effect, Prothrombin time, medicine.diagnostic_test, biology, business.industry, Hematology, Middle Aged, medicine.disease, Recombinant Proteins, Therapeutic Equivalency, Consumer Product Safety, Recombinant factor VIIa, Anesthesia, Pharmacodynamics, Hemostasis, biology.protein, business, Partial thromboplastin time
Abstract

A multicenter and open-labeled clinical trial of human recombinant factor VIIa (rFVIIa) was conducted in Japanese patients with severe hemophilia A or B with inhibitors. The trial consisted of 2 parts. In study 1, the pharmacokinetics, pharmacodynamics, and safety of a single dose of 120 microg/kg of rFVIIa were investigated in 8 patients. In the subsequent study 2, the hemostatic effect and safety of rFVIIa were evaluated during a 24-week period in 10 patients. In study 1, the mean maximum FVII-coagulant activity (FVII:C) was found to occur after 10 minutes; activity then decreased rapidly and returned to the baseline within 24 hours after a single intravenous infusion of rFVIIa. The mean half-life of FVII:C was 3.5 hours. The activated partial thromboplastin time and prothrombin time in the patients were immediately shortened but returned to the baseline within 24 hours after dosing. In study 2, 86 microg/kg to 120 microg/kg of rFVIIa (mean, 97 microg/kg) was administered 1 to 85 times to 10 patients. A total of 58.0% (91/157) of bleeding episodes were treated excellently or effectively, with 5 (3.2%) ineffective episodes. There was no apparent trend in the relationship of the hemostatic effect with bleeding sites, mean dose, or number of injections. The efficacy rate, however, was significantly higher (90.0%) in bleeding episodes treated within 3 hours than in those treated at longer intervals (31.0%). No treatment-related adverse events were observed, and there was no evidence of antibody formation to rFVIIa. In conclusion. rFVIIa is an effective and well-tolerated option for treatment of bleeding episodes in hemophilia patients with inhibitors.

Published
2001

103. Asymptomatic Dysprothrombinemia (Prothtombin Himi) with p.M380T and p.R431H Shows Severely Reduced Clotting Activity, Moderate Antithrombin Resistance and Severe Thrombomodulin Binding Defect

Author

Masashi Akiyama, Akira Takagi, Eriko Morishita, Toshiyuki Miyata, Fumina Taniguchi, Mao Takata, Tetsuhito Kojima, and Akiko Sekiya

Subjects
biology, Chemistry, Immunology, Antithrombin, Cell Biology, Hematology, Fibrinogen, medicine.disease, Thrombomodulin, Biochemistry, Molecular biology, Fibrin, Thrombin, medicine, biology.protein, Hypoprothrombinemia, Protein C, medicine.drug, Blood coagulation test
Abstract

Background and purpose:Congenital prothrombin (PT) deficiency is categorized into two phenotypes, true hypoprothrombinemia and dysprothrombinemia. A strong discrepancy between observed values from coagulation tests and bleeding severity can be found in some forms of dysprothrombinemia. Some dysprothrombinemias, such as the PT Himi that we reported previously (Morishita E, et al: Blood 1992), are asymptomatic despite low PT activity. PT Yukuhashi disturbs the interaction between thrombin and antithrombin (AT), causing a paradoxical thrombotic phenotype, called "AT resistance (ATR)". To investigate the mechanisms by which patient with PT Himi is asymptomatic, mutant PTs reflecting each of the two different gene sites identified in gene analysis were prepared, and functional analyses of fibrinogen (Fbg) degradation, ATR, and thrombomodulin (TM)-binding capacity were conducted. This study was approved by the ethics committee at Kanazawa University School of Medicine. Case report: The proband was a 26-year-old Japanese woman who had been diagnosed with congenital dysprothrombinemia at the time of first pregnancy, based on PT activity and PT antigen levels of 10% and 88%, respectively. Although cesarean section was performed for the second delivery, abnormal bleeding did not develop. Genomic DNA analysis revealed compound heterozygosity for two missense mutations in the F2gene (c.1139T>C, p.M380T and c.1292G>A, p.R431H). Methods: We established stable transformants of Chinese hamster ovary cells that expressed wild-type and two mutant recombinant PTs (rPTs), M380T PT and R431H PT. Conditioned media of stable transformants expressing rPTs in serum-free medium were collected, concentrated, and stored at -80°C until use. 1) Fbg clotting assays: We performed a one-stage clotting assay and a chromogenic assay. 2) Kinetic analysis of thrombin inactivation using AT and formation of thrombin-AT complex (TAT): After incubation with PT activator components, samples were treated with excess AT in the absence of heparin for various durations and changes in absorbance per minute were measured. Formed TAT was measured using an enzyme-linked immunosorbent assay (ELISA) kit. 3) TM-binding assay: To evaluate the ability of wild-type and mutant rPTs to bind to TM, after activating PT, we detected TM-binding thrombin using a TM ELISA method. Results:1) M380T PT activity in the one-stage assay was below the threshold of sensitivity (clot not detected), whereas R431H PT activity was decreased to 10% of that of wild-type rPT (100%). On the other hand, both mutant PT activities in the chromogenic assay were slightly decreased compared to wild-type rPT. 2) After 30 min without heparin, relative residual thrombin activity of M380T PT (74%) was higher than that of wild-type (10%), indicating severe ATR, whereas that of R431H PT was slightly increased (21%), indicating mild ATR. TAT formation by wild-type PT increased over time. TAT formation by R431H PT was about 40% of that of wild-type PT, but that by M380T PT was almost negligible after 120 min. 3) TM-binding thrombins of both mutant rPTs were barely detected. Discussion: M380T PT has high ATR and fails to bind with TM, so a large amount of thrombin with greater clotting activity than normal is thought to be present. With this abnormal thrombin, however, fibrin-forming ability is greatly decreased and almost no clotting ability is thought to exist in the body. Hence, R431H PT, which made up about half of the PT protein in the proband, was considered responsible for hemostasis in the body. The mutant thrombin activated from the R431H PT shows decreased clotting activity, but is resistant to inactivity from AT and thus maintains activity longer than ordinary thrombin. At the same time, the activation of protein C is also decreased due to failure to bind with TM, so ultimately the clotting ability necessary for hemostasis was conjectured to have been maintained, resulting in the proband being asymptomatic. Conclusion:Although neither PT position M380 nor R431 are AT binding sites, M380T PT and R431H PT showed ATR. These mutants are the first AT-resistant PTs seen from mutations other than at the Arg596 site. In recent years, TM resistance has been newly proposed as a mechanism producing thrombotic tendencies, and may also apply to the present patient. The reason the proband did not show a bleeding tendency may have been the combined contributions of AT and TM resistance. Disclosures No relevant conflicts of interest to declare.

Published
2016

104. Expression of Protein S in the Murine Heart and Cultured Mouse Cardiomyocytes Is Down-regulated by Cytokines

Author

Tetsuhito Kojima, Koji Yamamoto, Takayoshi Shimokawa, Hidehiko Saito, and Eriko Yamafuji

Subjects
Lipopolysaccharides, Male, Pathology, medicine.medical_specialty, Lipopolysaccharide, medicine.medical_treatment, Down-Regulation, Protein S, Mice, chemistry.chemical_compound, Adrenal Glands, Gene expression, medicine, Animals, Myocyte, Tissue Distribution, RNA, Messenger, Lung, Cells, Cultured, Messenger RNA, biology, Tumor Necrosis Factor-alpha, business.industry, Myocardium, Hematology, Molecular biology, Mice, Inbred C57BL, Kinetics, Cytokine, chemistry, Organ Specificity, Cell culture, biology.protein, Cytokines, Tumor necrosis factor alpha, business, Interleukin-1
Abstract

SummaryProtein S (PS), a co-factor of activated protein C, is a vitamin K-dependent anticoagulant protein and is known to be produced extrahepatically. In the present study, the concentration of PS mRNA was determined tissue by tissue in the mouse, and it was high in lung, adrenal and heart as well as in liver. We further investigated the effects of lipopolysaccharide (LPS), tumor necrosis factor-α (TNF-α), and interleukin-1 (IL-1) on the PS mRNA expression in murine tissues in vivo. Although LPS and TNF-α significantly decreased the expression level of PS mRNA in all tissues examined (e.g., lung, liver, heart, and kidney) and the PS antigen level in plasma, the suppressive effect of IL-1 on PS gene expression was limited to heart. More specifically, considerable amounts of PS mRNA and antigen were expressed in a cultured mouse cardiomyocyte cell line, and again, treatment with IL-1 decreased the PS expression in these cells. These observations raise a possibility that the expression of cardiac PS may contribute to the regional anticoagulant potential in heart, and suggest that the decreased PS expression by cytokines may result in an increase in the systemic and/or regional prothrombotic potential under inflammatory conditions.

Published
2001

105. Plasma Levels of Syndecan-4 (Ryudocan) Are Elevated in Patients with Acute Myocardial Infarction

Author

Hidehiko Saito, Akira Takagi, Atsuya Shimizu, Tadashi Matsushita, Tetsuhito Kojima, Tatsuya Segawa, Masahiro Maeda, and Koji Yamamoto

Subjects
Adult, Male, Vascular Endothelial Growth Factor A, medicine.medical_specialty, Pathology, RNA Stability, medicine.medical_treatment, Myocardial Infarction, Infarction, Endothelial Growth Factors, Cell Line, Syndecan 1, Mice, Japan, Internal medicine, medicine, Animals, Humans, RNA, Messenger, Myocardial infarction, Hypoxia, Aged, Aged, 80 and over, Lymphokines, Membrane Glycoproteins, Vascular Endothelial Growth Factors, Cell growth, business.industry, Myocardium, Growth factor, Hematology, Middle Aged, Hypoxia (medical), medicine.disease, Immunohistochemistry, Thrombosis, Rats, Up-Regulation, carbohydrates (lipids), Kinetics, Endocrinology, Case-Control Studies, Female, Proteoglycans, Syndecan-4, medicine.symptom, business
Abstract

SummarySyndecan-4 (ryudocan) is a cell-surface heparan sulfate proteoglycan, which plays an important role in a variety of biological functions including regulation of blood coagulation, cell adhesion, and cell growth. In this study, we measured plasma levels of syndecan-4 in patients with acute myocardial infarction using an enzyme-immunoassay, and found that they were extremely high, with a peak of average (10.5 ± 5.6 ng/ml, 2 weeks after onset), as compared with those in normal subjects (0.078 ± 0.030 ng/ml) (p < 0.001). We also observed a distinct expression of syndecan-4 in the repair region of the damaged cardiac tissues with infarction, but not in intact region, by immunohistochemical analysis. To clarify the mechanism of syndecan-4 induction, we investigated the hypoxia effect on its expression, and found that hypoxia treatment up-regulated the gene expression of syndecan-4 in various types of cells. Taken together, it is suggested that syndecan-4 is induced by hypoxia stimuli in ischemic heart tissues, and may function as a tissue-repair molecule via biological mediators such as heparin-binding growth factors.

Published
2001

106. Protein S Deficiency

Author

Tetsuhito Kojima and Takayuki Nakayama

Subjects
medicine.medical_specialty, Endocrinology, Chemistry, Internal medicine, medicine, Protein S deficiency, medicine.disease
Published
2001

107. [Untitled]

Author

Takayuki YAMADA, Akira TAKAGI, Yusuke NAKADE, Takashi MURATE, Masamitsu YANADA, Takayuki NAKAYAMA, Koji YAMAMOTO, Tadashi MATSUSHITA, Hidehiko SAITO, and Tetsuhito KOJIMA

Published
2001

108. DNA Sequence Analysis of Protein S Deficiency-Identification of Four Point Mutations in Twelve Japanese Subjects

Author

Naohiro Kanayama, Isamu Sugiura, Kazuo Kagami, Yuka Nomura, Takayuki Iwaki, Junki Takamatsu, Tetsuhito Kojima, Hidehiko Saito, Takayuki Nakayama, Takao Kobayashi, Tadashi Mastushita, and Yukako Yamamoto

Subjects
Genetics, Mutation, Protein S Deficiency, Sequence analysis, Point mutation, Nonsense mutation, Sequence Analysis, DNA, Hematology, Biology, medicine.disease_cause, Protein S, law.invention, Japan, law, medicine, biology.protein, Humans, Point Mutation, Missense mutation, Cardiology and Cardiovascular Medicine, Gene, Polymerase chain reaction
Abstract

The molecular basis for the hereditary type I protein S (PS) deficiency was investigated. DNA sequence analysis of 12 patients with PS deficiency in Japan identified four point mutations and three of them were novel. Nonsense mutations found in two unrelated patients resulted in termination of the PS polypeptide chains at Gln 238 and Lys 392, respectively. Two novel missense mutations were also found in two other patients substituting Asp 202 for Asn and Leu 298 for Pro, respectively. Comparison of the PS amino acid sequences from several mammalians indicated that Asp 202 and Leu 298 were preserved and thus appeared to be responsible for the pathogenesis of PS deficiency.

Published
2001

109. Ryudocan expression by luteinized granulosa cells is associated with the process of follicle atresia

Author

Hiroshi Kobayashi, Osamu Mochizuki, Guang W. Sun, Akira Takagi, Mariko Sakata, and Tetsuhito Kojima

Subjects
Adult, endocrine system, medicine.medical_specialty, medicine.drug_class, Follicular Atresia, Biology, Chorionic Gonadotropin, Follicle, Bolus (medicine), Corpus Luteum, Internal medicine, medicine, Humans, Ovarian follicle, Cells, Cultured, Progesterone, Atretic Follicle, Granulosa Cells, Membrane Glycoproteins, Estradiol, Osmolar Concentration, Obstetrics and Gynecology, medicine.disease, Follicular fluid, Coculture Techniques, Follicular Fluid, medicine.anatomical_structure, Endocrinology, Reproductive Medicine, Estrogen, Atresia, Female, Proteoglycans, Syndecan-4, Gonadotropin
Abstract

Objective: To evaluate the presence of ryudocan in follicular fluid (FF) and its possible correlation with FF E 2 and P, and to study the levels of ryudocan in granulosa-lutein cells stimulated with hCG. Design: Controlled clinical study and in vitro experiment. Setting: University teaching hospital. Patient(s): One hundred seven patients undergoing IVF. Intervention(s): The FF and granulosa-lutein cells were aspirated from follicles 34 hours after an ovulatory gonadotropin bolus. Main Outcome Measure(s): FF ryudocan, E 2 , and P levels as well as hCG-mediated induction of ryudocan. Result(s): Ryudocan was abundant in the FF; the concentration of ryudocan in human FF was estimated to be 305.5 ± 200.8 ng/mL (mean ± SD). Atretic follicles had higher concentrations of ryudocan (559.1 ± 156.5 ng/mL). FF ryudocan levels were inversely correlated with FF E 2 ( r = −0.5023) and P concentrations ( r = −0.4459). A detectable amount of ryudocan was found in pooled granulosa-lutein cells. Ryudocan production was augmented by surge levels of hCG. Conclusion(s): Ryudocan is expressed in luteinized granulosa cells in vitro. The higher concentrations of ryudocan in FF of atretic follicles suggest an involvement of ryudocan in the process of atresia.

Published
2000

110. Cloning and Characterization of the Murine Antithrombin Gene

Author

Tetsuhito Kojima, Hidehiko Saito, Akira Takagi, Koji Yamamoto, Yukiko Nakayama, Masamitsu Yanada, and Tadashi Matsushita

Subjects
Pathology, medicine.medical_specialty, Molecular Sequence Data, Biology, Polymerase Chain Reaction, Antithrombins, Mice, Animal model, medicine, Animals, Humans, RNA, Messenger, Cloning, Molecular, Cloning, Base Sequence, Antithrombin, Exons, Sequence Analysis, DNA, Hematology, Virology, Introns, Mice, Inbred C57BL, Genes, Liver, RNA Splice Sites, Venous disease, Sequence Alignment, medicine.drug
Abstract

ORIGINAL ARTICLE Cloning and Characterization of the Murine Antithrombin Gene Yukiko Nakayama1, Tetsuhito Kojima2, Akira Takagi2, Masamitsu Yanada1, Koji Yamamoto1, Tadashi Matsushita1 and Hidehiko Saito1,3 1First Department of Internal Medicine, Nagoya University School of Medicine, 65 Tsurumai-cho, Showa-ku, Nagoya 466-8550; 2Department of Medical Technology, Nagoya University School of Health Sciences, 1-1-20 Daiko-Minami, Higashi-ku, Nagoya 461-8673; and 3Aichi Blood Research Foundation, 13-2 Machikita, Moriyama-ku, Nagoya 463-0074, Japan.

Published
2000

111. Syndecan-4 Deficiency Impairs Focal Adhesion Formation Only under Restricted Conditions

Author

Kenji Kadomatsu, Shinobu Tsuzuki, Takashi Muramatsu, Hisako Muramatsu, Kazuhiro Ishiguro, Kazuo Kusugami, Hidehiko Saito, Eishin Nakamura, and Tetsuhito Kojima

Subjects
Blotting, Western, PTK2, Integrin, Mice, Transgenic, Biochemistry, Heparan Sulfate Proteoglycans, Syndecan 1, Focal adhesion, Mice, Cell Adhesion, Animals, Humans, Molecular Biology, Cells, Cultured, Actin, Membrane Glycoproteins, biology, Heparin, Chemistry, Exons, Cell Biology, Fibroblasts, Actins, Vinculin, Fibronectins, Cell biology, Mice, Inbred C57BL, carbohydrates (lipids), Fibronectin, Mutagenesis, biology.protein, Proteoglycans, Syndecan-4, Focal adhesion formation
Abstract

Two domains of fibronectin deliver two different but cooperative signals required for focal adhesion formation. The signal from the cell-binding domain is mediated by integrins, whereas the signal from the heparin-binding domain is recognized by heparan sulfate proteoglycans, of which syndecan-4 has been hypothesized to be involved in focal adhesion formation. We generated mice deficient in syndecan-4 to study its role directly. Even in fibroblasts from syndecan-4-deficient mice, focal adhesions were formed, and actin fibers terminated normally at focal adhesions when they were cultured on coverslips coated with fibronectin or with a mixture of its cell-binding and heparin-binding fragments. However, when the cells were cultured on the cell-binding fragment and the heparin-binding fragment was added to the medium, focal adhesion formation was impaired in the syndecan-4 null fibroblasts as compared with that in wild-type cells. Therefore, syndecan-4 is essential for promoting focal adhesion formation only when the signal of the heparin-binding domain of fibronectin is delivered as a soluble form, most probably from the apical surface. When the signal is delivered as a substratum-bound form, other molecule(s) also participate(s) in the signal reception.

Published
2000

112. Syndecan-4 deficiency impairs the fetal vessels in the placental labyrinth

Author

Hidehiko Saito, Tetsuro Nagasaka, Kenji Kadomatsu, Hiroshi Kobayashi, Kazuo Kusugami, Masafumi Ito, Tetsuhito Kojima, Takashi Muramatsu, Hisako Muramatsu, Kazuhiro Ishiguro, and Eishin Nakamura

Subjects
Fetus, Pathology, medicine.medical_specialty, animal structures, biology, In situ hybridization, Heparan sulfate, Fibrin, Transmembrane protein, Syndecan 1, carbohydrates (lipids), chemistry.chemical_compound, medicine.anatomical_structure, chemistry, Placenta, embryonic structures, Immunology, biology.protein, medicine, Immunohistochemistry, Developmental Biology
Abstract

Syndecan-4 is a transmembrane protein bearing heparan sulfate chains, involved in anticoagulation and focal adhesion formation. Here, we revealed that syndecan-4 was expressed in the fetal vessels in the placental labyrinth by in situ hybridization and immunohistochemical staining. At 17.5 gestational days, the area of degenerated fetal vessels in the placental labyrinth was more diffuse and larger in Synd4(-/-) embryos than wild-type controls. Calcium and fibrin(ogen) depositions in the degenerated vessels were also more extensive and more severe in the placentas of Synd4(-/-) embryos. These findings suggest that syndecan-4 deficiency impairs the fetal vessels in the placenta, probably due to a deficit in the anticoagulation mechanism. This article is the first report demonstrating that among a large number of core proteins of heparan sulfate proteoglycans, a defect of a single core protein caused impaired anticoagulation in a specific site. © 2000 Wiley-Liss, Inc.

Published
2000

113. Molecular Biology of Ryudocan, an Endothelial Heparan Sulfate Proteoglycan

Author

Tetsuhito Kojima

Subjects
DNA, Complementary, Molecular Sequence Data, Basic fibroblast growth factor, Chromosomes, Human, Pair 20, Nerve Tissue Proteins, Perlecan, Thromboplastin, Syndecan 1, chemistry.chemical_compound, Species Specificity, Extracellular, Animals, Humans, Amino Acid Sequence, Cloning, Molecular, Transcription factor, Polysaccharide-Lyases, Midkine, Membrane Glycoproteins, Sequence Homology, Amino Acid, biology, Hematology, Heparan sulfate, Molecular biology, Transmembrane protein, Rats, Genes, chemistry, Organ Specificity, biology.protein, Cytokines, Fibroblast Growth Factor 2, Proteoglycans, Syndecan-4, Endothelium, Vascular, Carrier Proteins, Cardiology and Cardiovascular Medicine, Sequence Alignment, Heparan Sulfate Proteoglycans, Protein Binding
Abstract

Ryudocan is a type I integral membrane heparan sulfate proteoglycan, which was originally cloned from rat microvascular endothelial cells. We have cloned the cDNA of rat ryudocan. The deduced amino acids of ryudocan has homologous transmembrane and intracellular domains with syndecan but very distinct extracellular regions. We also cloned the human ryudocan cDNA, of which the gene localizes on the chromosome 20q12. To better understand the regulation of ryudocan expression, we have determined the structural organization of the human ryudocan gene. The human ryudocan gene extends approximately 24 kb and is divided into five exons that appear conserved in syndecan family members. The 5'-flanking sequences of the human ryudocan gene contain a variety of potential binding sites for transcription factors and are capable of functioning as a promoter. We purified human ryudocan and evaluated its interactions with several extracellular ligands. It was found that basic fibroblast growth factor (bFGF), midkine, and tissue factor pathway inhibitor exhibited significant ryudocan bindings. Heparitinase, but not chondroitin ABC lyase treatment, destroyed those ryudocan bindings; thus, the heparan sulfate chains of ryudocan appear to be responsible for those bindings. Immunohistochemical analysis revealed that ryudocan is expressed in peripheral nerve tissues, fibrous connective tissues, and placental trophoblasts. These findings suggest that ryudocan may possess multiple biologic functions, such as bFGF modulation, neurite growth promotion, and anticoagulation, via heparan sulfate-binding effectors in the cellular microenvironment.

Published
2000

114. Severe Factor VII Deficiency Caused by a Novel Mutation His348 to Gln in the Catalytic Domain

Author

Hidehiko Saito, Tomio Yamazaki, Tetsuhito Kojima, Isamu Sugiura, Akira Katsumi, and Tadashi Matsushita

Subjects
Male, medicine.medical_specialty, DNA, Complementary, Factor VII Deficiency, Molecular Sequence Data, Mutant, Mutation, Missense, Gene Expression, Hemorrhage, CHO Cells, Biology, Sulfur Radioisotopes, Transfection, medicine.disease_cause, Exon, chemistry.chemical_compound, Japan, Cricetinae, Internal medicine, medicine, Animals, Humans, Missense mutation, Amino Acid Sequence, Transversion, Blood coagulation test, Family Health, Mutation, Binding Sites, Factor VII, Homozygote, Wild type, Hematemesis, Sequence Analysis, DNA, Hematology, Middle Aged, Recombinant Proteins, Endocrinology, Amino Acid Substitution, chemistry, COS Cells, Blood Coagulation Tests, Sequence Alignment
Abstract

SummaryFactor VII is a vitamin K-dependent zymogen that plays a key role in the initiation of the extrinsic pathway. A severe factor VII deficiency was identified in a 45-year old male whose plasma factor VII antigen was less than 60 ng/ml and expressed 5.2% of normal factor VII activity. DNA sequence analysis of the patient’s factor VII gene showed a thymidine to guanine transversion at nucleotide 10968 in exon VIII that results in a novel amino acid substitution of His348 to Gln. The patient was homozygous for this mutation, whereas some of his family members were heterozygous. Both wild type and mutant factor VII were transiently expressed in COS-1 cells. The level of secreted mutant factor VII antigen was only 11.0% of the level of wild type factor VII. In CHO cells stably transfected with the mutant factor VII, only 37.3% of the total labeled FVII was secreted into the conditioned media and the remainder was retained inside the cells. These data suggest this mutation leads to factor VII deficiency due to the impaired secretion of the molecule.

Published
2000

115. Histocompatibility antigens and alleles in Japanese haemophilia A patients with or without factor VIII antibodies

Author

Midori Shima, Akira Yoshioka, I. Takahashi, Tadashi Kamiya, H. Ohta, Tetsuhito Kojima, Hidehiko Saito, and J. Takamatsu

Subjects
congenital, hereditary, and neonatal diseases and abnormalities, biology, business.industry, Immunology, Haemophilia A, General Medicine, Human leukocyte antigen, Major histocompatibility complex, medicine.disease, Biochemistry, Virology, Serology, Histocompatibility, hemic and lymphatic diseases, Genetics, biology.protein, Immunology and Allergy, Medicine, Typing, Risk factor, Antibody, business
Abstract

We carried out human leukocyte antigen (HLA)-A, B, Cw, DR and DQ serological typing and HLA-DQA1, DQB1, DRB1 and DPB1 genetic typing for 46 Japanese haemophilia A patients, including 20 who had developed an antibody to factor VIII. It appears that anti FVIII inhibitor formation is associated with the major histocompatibility complex in Japanese haemophilia A patients. Absence of HLA-A24 is a principal risk factor for inhibitor formation in Japanese haemophilia A patients. As supplemental risk factors, HLA-DR4.1, DQ4 and DQA1*0301=2 are positively associated with patients exhibiting inhibitor compared with normal subjects. This and previous studies show that the association between HLA antigens and the formation of inhibitor depends on race. Data of HLA typing may be useful for the recognition of groups at high risk for the possible formation of inhibitor among Japanese haemophilia A patients.

Published
1999

116. An Sp1 binding site mutation of the PROS1 promoter in a patient with protein S deficiency

Author

Yuta Fujimori, Takashi Murate, Naomi Sanda, Emi Mizutani, Tadashi Matsushita, Tomoki Naoe, Tetsuhito Kojima, Takahiro Kashiwagi, and Akira Takagi

Subjects
Genetics, Mutation (genetic algorithm), medicine, Electrophoretic mobility shift assay, Luciferase, Hematology, Protein S deficiency, Biology, Binding site, medicine.disease, Molecular biology
Published
2007

117. The first case of antithrombin-resistant prothrombin Belgrade mutation in Japanese

Author

Hitoshi Kiyoi, Akira Takagi, Nobuaki Suzuki, Mayuko Kishimoto, Takeshi Kanematsu, Mika Ogawa, Moe Murata, Tadashi Matsushita, and Tetsuhito Kojima

Subjects
medicine.medical_specialty, Hematology, business.industry, Antithrombin, General Medicine, Drug resistance, 030204 cardiovascular system & hematology, Thrombophilia, medicine.disease, Bioinformatics, 03 medical and health sciences, 0302 clinical medicine, 030220 oncology & carcinogenesis, Internal medicine, Mutation (genetic algorithm), medicine, Young adult, business, Antithrombins, medicine.drug
Published
2015

118. Identification of the Five Hydrophilic Residues (Lys-217, Lys-218, Arg-359, His-360, and Arg-513) Essential for the Structure and Activity of Vitamin K-Dependent Carboxylase

Author

Tetsuhito Kojima, Tadashi Matsushita, Hidehiko Saito, Makoto Hirai, Atsuya Shimizu, and Isamu Sugiura

Subjects
Vitamin K, Biophysics, CHO Cells, Biology, Arginine, Biochemistry, Factor IX, Structure-Activity Relationship, Enzyme activator, Cricetinae, Animals, Histidine, Protein Precursors, Molecular Biology, chemistry.chemical_classification, Alanine, Lysine, Chinese hamster ovary cell, Cell Biology, Molecular biology, Recombinant Proteins, Enzyme assay, Pyruvate carboxylase, Enzyme Activation, Cross-Linking Reagents, Enzyme, Carbon-Carbon Ligases, chemistry, Mutation, biology.protein, Epoxy Compounds, Cattle, Vitamin K epoxide reductase, Amino Acids, Essential
Abstract

Vitamin K-dependent carboxylase catalyzes the posttranslational conversion of glutamic acid to gamma-carboxyglutamic acid in vitamin K-dependent proteins. The clustered charged-to-alanine scanning mutagenesis of bovine carboxylase has identified five distinct candidate regions (I. Sugiura et al., J. Biol. Chem. 271, 17837-17844, 1996) with significant loss-of-function phenotype. To further specify the residues essential for the structure and function of the enzyme, Lys-217, Lys-218, Arg-359, His-360, Lys-361, Arg-513, and Lys-515 were analyzed by substituting to alanine individually. All the mutants except for K217A were expressed in Chinese hamster ovary cells. The carboxylase activities of R359A, H360A, and R513A decreased in parallel with the vitamin K epoxidase activities. Both carboxylations by R359A and H360A were stimulated saturatively at 1 microM factor IX propeptide (proFIX18) concentration, but that by R513A was not at a concentration up to 128 microM. K218A completely lost the enzyme activities but it cross-linked to the propeptide, suggesting that Lys-218 is critical for enzyme activity without affecting propeptide binding. We conclude that Lys-218, Arg-359, and His-360 are involved in the catalytic event, and Arg-513 participates in propeptide binding.

Published
1998

119. Two Distinct Novel Splice Site Mutations in a Compound Heterozygous Patient with Protein S Deficiency

Author

Yoshihiro Okamoto, Hidehiko Saito, Tomio Yamazaki, Kazuo Kagami, Tetsuhito Kojima, Shinobu Tsuzuki, Akira Katsumi, Toshio Takafuta, Kingo Fujimura, and Isamu Sugiura

Subjects
Genetics, Mutation, Splice site mutation, Transition (genetics), Mutant protein, medicine, splice, Hematology, Biology, Transversion, Compound heterozygosity, medicine.disease_cause, Frameshift mutation
Abstract

SummaryGenetic analysis revealed two distinct novel splice site mutations in a compound heterozygous patient with protein S deficiency. The paternal mutation was a G-to-T transition at position -1 of the acceptor splice site of intron N (Mutation I), and the maternal mutation was a G-to-C transversion at position -1 of the donor splice site of intron C (Mutation II). Both splice site mutations decreased the mutated mRNA accumulation to the same extent, approximately 40% of the normal mRNA. However, the mutations were associated with different phenotypical expressions: the paternal mutant protein S was not detected in vivo, while the maternal mutant protein S was present in the plasma in reduced quantity. Because Mutation I caused a cryptic splicing in the mutated mRNA, resulting in a reading frameshift and premature termination, the predicted mutant protein S might be highly unstable. In contrast, Mutation II led to the substitution of Val46 by Leu, which might be much less deleterious for the synthesis, secretion and stability of the predicted mutant protein S. It was supposed that the different post-translational metabolisms produced the distinct phenotypical expressions of the mutations.

Published
1997

120. Development of a new laboratory test to evaluate antithrombin resistance in plasma

Author

Tadashi Matsushita, Atsuo Suzuki, Akira Takagi, Eriko Okuyama, Yumi Ando, Moe Murata, Io Kato, Takashi Murate, Yuki Takagi, Tetsuhito Kojima, Hidehiko Saito, and Yuki Nakamura

Subjects
medicine.medical_specialty, Mutant, Antithrombins, law.invention, Thrombin, law, Prothrombinase, hemic and lymphatic diseases, Internal medicine, medicine, Humans, Chemistry, Heparin, Antithrombin, Anticoagulants, Thrombosis, Hematology, medicine.disease, Recombinant Proteins, Endocrinology, Snake venom, Immunology, Mutation, Recombinant DNA, Prothrombin, Blood Coagulation Tests, Warfarin, circulatory and respiratory physiology, medicine.drug
Abstract

Introduction We recently reported a variant prothrombin (p.Arg596Leu: prothrombin Yukuhashi) that confers antithrombin resistance to patients with hereditary thrombosis. To detect antithrombin resistance in plasma, we devised a laboratory test analyzing the kinetics of thrombin inactivation using antithrombin. Materials and Methods After incubation with prothrombin activator components (phospholipids, CaCl 2 , and snake venom), samples were treated with excess antithrombin in the presence or absence of heparin for various time periods. Subsequently, H-D-Phe-Pip-Arg-p-nitoranilide was added and changes in absorbance/min (ΔA/min) were measured at 405nm. Results After 1min inactivation using antithrombin and heparin, the relative residual thrombin activity of recombinant mutant prothrombin (34.3%±2.2%) was higher than that of the wild-type (6.3%±1.2 %). After 30min without heparin, the relative residual thrombin activity of recombinant mutant prothrombin (95.8%±0.4%) was higher than that of the wild-type (10.1%±1.7%), indicating that this assay could detect antithrombin resistance of the variant 596Leu prothrombin. Moreover, warfarinized plasmas from 2 heterozygous patients with prothrombin Yukuhashi mutation clearly showed higher values of the relative residual thrombin activity than those from 5 thrombosis patients lacking the mutation in the presence or absence of heparin. Conclusions We have devised a laboratory test to detect antithrombin resistance in plasma by analyzing the kinetics of thrombin inactivation using antithrombin. This assay may be useful for detecting antithrombin resistance in plasma, even in warfarinized patients.

Published
2013

121. The DC-HIL ligand syndecan-4 is a negative regulator of T-cell allo-reactivity responsible for graft-versus-host disease

Author

Kyoichi Tamura, Kiyoshi Ariizumi, Jin Sung Chung, Tetsuhito Kojima, Ponciano D. Cruz, and Mizuki Tomihari

Subjects
T cell, Immunology, Graft vs Host Disease, Biology, T-Lymphocytes, Regulatory, Interleukin 21, Mice, medicine, Immunology and Allergy, Cytotoxic T cell, Animals, Transplantation, Homologous, IL-2 receptor, Receptors, Immunologic, Eye Proteins, Mice, Knockout, Mice, Inbred BALB C, Membrane Glycoproteins, ZAP70, Hematopoietic Stem Cell Transplantation, Original Articles, medicine.disease, Haematopoiesis, Graft-versus-host disease, medicine.anatomical_structure, Acute Disease, Syndecan-4, Stem cell
Abstract

Summary Acute graft-versus-host disease (GVHD) is the most important cause of mortality after allogeneic haematopoietic stem cell transplantation. Allo-reactive T cells are the major mediators of GVHD and the process is regulated by positive and negative regulators on antigen-presenting cells (APC). Because the significance of negative regulators in GVHD pathogenesis is not fully understood, and having discovered that syndecan-4 (SD-4) on effector T cells mediates the inhibitory function of DC-HIL on APC, we proposed that SD-4 negatively regulates the T-cell response to allo-stimulation in acute GVHD, using SD-4 knockout mice. Although not different from their wild-type counterparts in responsiveness to anti-CD3 stimulation, SD-4−/− T cells lost the capacity to mediate the inhibitory function of DC-HIL and were hyper-reactive to allogeneic APC. Moreover, infusion of SD-4−/− T cells into sub-lethally γ-irradiated allogeneic mice worsened mortality, with hyper-proliferation of infused T cells in recipients. Although there my be little or no involvement of regulatory T cells in this model because SD-4 deletion had no deleterious effect on T-cell-suppressive activity compared with SD-4+/+ regulatory T cells. We conclude that SD-4, as the T-cell ligand of DC-HIL, is a potent inhibitor of allo-reactive T cells responsible for GVHD and a potentially useful target for treating this disease.

Published
2013

122. Molecular basis of a hereditary type I protein S deficiency caused by a substitution of Cys for Arg474

Author

Junki Takamatsu, Yoshihiro Okamoto, Motohiro Hamaguchi, Akira Katsumi, Kazuo Kagami, Tetsuhito Kojima, Hidehiko Saito, Tomio Yamazaki, and Isamu Sugiura

Subjects
Male, Mutant, Biochemistry, Protein S, law.invention, Consanguinity, Protein structure, law, Cricetinae, Chlorocebus aethiops, Missense mutation, Cell Line, Transformed, chemistry.chemical_classification, biology, Hematology, Middle Aged, Amino acid, Recombinant DNA, Female, Rabbits, DNA, Complementary, Protein S Deficiency, Sequence analysis, Recombinant Fusion Proteins, Genetic Vectors, Molecular Sequence Data, Immunology, CHO Cells, Arginine, Androgen-Binding Protein, Animals, Humans, Point Mutation, Genetic Predisposition to Disease, Secretion, Cysteine, Binding Sites, Base Sequence, Sequence Homology, Amino Acid, Thrombosis, Cell Biology, Molecular biology, Rats, chemistry, biology.protein, Cattle, Laminin, Sequence Alignment
Abstract

The molecular basis for a hereditary type I protein S (PS) deficiency was investigated. DNA sequence analysis in the proband showed a novel missense mutation substituting Cys (TGT) for Arg474 (CGT) that is a highly conserved amino acid residue among the related proteins. This missense mutation cosegregated with the type I PS deficiency in this family. Transient expression studies showed that the secretion of the recombinant Cys-mutant PS was markedly decreased compared with that of the recombinant wild-type PS, reproducing the observed phenotype of type I deficiency. Stable expression and pulse-chase experiments demonstrated an intracellular degradation and an impaired secretion of the recombinant Cys-mutant PS. Furthermore, the substitution of Arg474 by Ala or Glu, but not by Lys, markedly reduced the secretion of the recombinant PS mutants in transient expression studies, suggesting that a positively charged basic amino acid might be needed at residue 474 and might play a key role in the protein structure and conformation of the sex hormone binding globulin-homology domain of the PS molecule. We postulate that the loss of the highly conserved Arg474 might be responsible for the type I PS deficiency inherited in this family.

Published
1996

123. Analysis for antithrombin gene polymorphisms in Japanese subjects and cosegregation studies in families with hereditary antithrombin deficiency

Author

Tomio Yamazaki, Shinobu Tsuzuki, Hidehiko Saito, Tetsuhito Kojima, Isamu Sugiura, Junki Takamatsu, and Akira Katsumi

Subjects
Cosegregation, Antithrombin III, Molecular Sequence Data, Hereditary Antithrombin Deficiency, Biology, Asian People, Japan, Polymorphism (computer science), medicine, Coagulopathy, Humans, Gene, Genetics, Antithrombin III Deficiency, Polymorphism, Genetic, Base Sequence, Models, Genetic, Antithrombin, Hematology, medicine.disease, Pedigree, Meiosis, Haplotypes, Genetic marker, Case-Control Studies, Gene polymorphism, medicine.drug
Published
1996

124. Structural Organization and Promoter Activity of the Human Ryuddcan Gene

Author

Tetsuhito Kojima, Shinobu Tsuzuki, Akira Katsumi, Motohiro Hamaguchi, Akira Takagi, Hidehiko Saito, Tomio Yamazaki, and Isamu Sugiura

Subjects
Signal peptide, Molecular Sequence Data, Restriction Mapping, Response element, Biology, Biochemistry, Syndecan 1, Exon, Genes, Reporter, Animals, Humans, Luciferases, Promoter Regions, Genetic, Molecular Biology, Gene, Transcription factor, Genetics, Binding Sites, Membrane Glycoproteins, Base Sequence, Promoter, Exons, General Medicine, Introns, Genes, COS Cells, TAF2, Proteoglycans, Syndecan-4, Transcription Factors
Abstract

To better understand the regulation of ryudocan (syndecan-4) expression, we have determined the structural organization of the human ryudocan gene. The human ryudocan gene extends approximately 24 kilobases and is divided into five exons, which appear to be conserved in syndecan family members. Exon I encodes the signal peptide; exons II-IV, the extracellular domain; and exon V, the transmembrane and cytoplasmic domains, which are highly homologous among syndecan family members. Primer extension analysis showed that human ryudocan gene had a single transcription initiation site, located 3 bases upstream from the described cDNA [Kojima et al. (1993) BBRC 190, 814-822]. The 5'-flanking sequences of human ryudocan gene contain a TATA-like sequence as well as a variety of other potential binding sites for transcription factors, including Sp1, Ap-2, NF-kB, E-alpha H box, H4TF-2, and LBP-1, and were capable of functioning as a promoter. The determination of the human ryudocan gene structure will allow elucidation of constitutive, cell-specific, tissue-specific, and developmentally regulated expression.

Published
1996

125. Carrier Detection and Prenatal Diagnosis of Hemophilia B Using DNA Polymorphisms of the Factor IX Gene in Japanese Subjects

Author

Tomio Yamazaki, Motohiro Hamaguchi, Junki Takamatsu, Akira Yoshioka, Akira Katsumi, Tadashi Matsushita, Tetsuhito Kojima, and Hidehiko Saito

Subjects
Genetics, education.field_of_study, business.industry, Population, Dna polymorphism, Intron, Prenatal diagnosis, law.invention, law, hemic and lymphatic diseases, medicine, Restriction fragment length polymorphism, education, business, Gene, Polymerase chain reaction, Factor IX, medicine.drug
Abstract

Advances in molecular biology have improved the screening for carriers and the prenatal diagnosis of many genetic disorders, including hemophilia B. For instance, based on the eight described dimorphic restriction fragment length polymorphisms within the factor IX gene, a Caucasian female has a 94% chance of being heterozygous (informative) for at least one of these markers. However, ethnic limitations of molecular genetic techniques have been found in diagnosing hemophilia B families in the Japanese and other populations. Previously, we heve demonstrated that three dinucleotide polymorphisms, which locate in the 5' flanking region at nucleotide-793 (FIX-793), in intron A at nucleotide 192 (FIX192), and in the 3' flanking region (FIXHhaI), of the factor IX gene, are present in normal Japanese. Each of these polymorphisms was able to be rapidly ascertained by the polymerase chain reaction technique.In this study, we analyzed 23 Japanese families with hemophilia B, and found that 19 families (82.6%) were heterozygous for at least one of these polymorphisms. Using these polymorphisms together with the extragenic DXS99/Sac I PFLP, which was previously reported as a useful gene marker for Japanese hemophilia B, the informative rate impproved to 87.0%. Carrier detection and the prenatal diagnosis of hemophilia B can be achieved effectively and rapidly in Japanese with these polymorphisms. In fact, we have successfully performed the prenatal diagnosis in two Japanese families with hemophilia B by using FIXHhaI or FIX192 polymorphism analysis. These polymorphisms may also be present and useful for hemophilia B carrier detection in other Oriental population.

Published
1996

126. A Novel Nonsense Mutation Associated with an Exon Skipping in a Patient with Hereditary Protein S Deficiency Type I

Author

Junki Takamatsu, Akira Katsumi, Hidehiko Saito, Tomio Yamazaki, Mikio Nishida, Yoshihiro Okamoto, and Tetsuhito Kojima

Subjects
Genetics, chemistry.chemical_classification, Messenger RNA, biology, Nonsense mutation, Hematology, Molecular biology, Protein S, Exon skipping, Amino acid, Exon, chemistry, biology.protein, Gene, Heteroduplex
Abstract

SummaryThe genetic defect in a patient with hereditary type I protein S (PS) deficiency was investigated. All the exons and intron-exon junctions of the patient’s PS gene were amplified by PCR and subjected to heteroduplex screening. Only the PCR product of exon 4 revealed heteroduplex bands. A novel nonsense mutation, Ser62 (TCA) to Stop (TGA) was found in exon 4. RT-PCR detected the aberrant mRNA in the patient’s platelets, which was markedly reduced in amount and lacked the region of exon 4, suggesting that the nonsense mutation affected the mutated mRNA metabolism and induced exon skipping. The skipping of exon 4 causes an in-frame deletion of 29 amino acids which just construct the thrombin-sensitive region of the PS molecule. The loss of such an important domain as well as the quantitative decrease in the mutated mRNA appear to be responsible for the type I PS deficiency in this patient.

Published
1996

129. Impact of antithrombin deficiency on efficacy of edoxaban and antithrombin-dependent anticoagulants, fondaparinux, enoxaparin, and heparin

Author

Toshiro Shibano, Yuko Honda, Yoshiyuki Morishima, Tadashi Matsushita, Chikako Kamisato, Tetsuhito Kojima, Taketoshi Furugohri, and Toshio Fukuda

Subjects
Male, medicine.drug_mechanism_of_action, medicine.drug_class, Pyridines, Factor Xa Inhibitor, Antithrombin III, Pharmacology, Fondaparinux, Inferior vena cava, chemistry.chemical_compound, Mice, Edoxaban, Polysaccharides, Antithrombotic, medicine, Animals, Enoxaparin, Venous Thrombosis, Hemostasis, business.industry, Anticoagulant, Antithrombin, Anticoagulants, Hematology, Heparin, Mice, Inbred C57BL, Thiazoles, chemistry, medicine.vein, Female, Blood Coagulation Tests, business, Gene Deletion, medicine.drug, Factor Xa Inhibitors
Abstract

Introduction Oral factor Xa (FXa) inhibitors are a novel class of anticoagulants that, unlike heparins, are expected to demonstrate antithrombotic effects independent of plasma antithrombin (AT) concentrations. We utilized heterozygous AT-deficient (AT +/-) mice to determine the impact of AT deficiency on anticoagulant and antithrombotic effects of edoxaban, a direct FXa inhibitor, and compared with heparins (fondaparinux, enoxaparin, and unfractionated heparin [UHF]). Materials and Methods The effects of edoxaban and heparins on in vitro prothrombin time and activated partial thromboplastin time were measured in plasma obtained from wild type (AT +/+) and AT +/- male mice. To assess the antithrombotic effects of these anticoagulants in vivo, venous thrombosis was induced in the inferior vena cava by FeCl3 treatment. Potency ratios of antithrombotic effects in AT +/- compared with AT +/+ mice were analyzed by a parallel line assay. Results In vitro studies demonstrated that the clotting-time prolongation effects of edoxaban were not affected by heterozygous AT deficiency whereas those of AT-dependent anticoagulants were attenuated. In AT +/- mice, the antithrombotic effects of AT-dependent anticoagulants were less potent than those in AT +/+ mice. In contrast, edoxaban was equipotent in preventing thrombus formation in both wild-type and AT-deficient mice. The attenuated antithrombotic effects of fondaparinux, enoxaparin, and UFH in AT-deficient mice were restored by AT supplementation. Edoxaban exerts a comparable antithrombotic effect even in mice with low plasma AT antigen and activity to that in wild-type mice. Conclusion Edoxaban may potentially be prioritized over AT-dependent anticoagulants in patients with lower plasma AT concentration.

Published
2012

130. A Quantitative Protein S Deficiency Associated with a Novel Nonsense Mutation and Markedly Reduced Levels of Mutated mRNA

Author

Kazuo Kagami, Tetsuhito Kojima, Akira Katsumi, Motohiro Hamaguchi, Hidehiko Saito, Tomio Yamazaki, and Junki Takamatsu

Subjects
Blood Platelets, Male, Protein S Deficiency, DNA Mutational Analysis, Molecular Sequence Data, Mutant, Nonsense mutation, medicine.disease_cause, Polymerase Chain Reaction, Protein S, Exon, Recurrence, medicine, Humans, Point Mutation, Genetic Predisposition to Disease, Amino Acid Sequence, RNA, Messenger, Protein S deficiency, Gene, Glycoproteins, Complement Inactivator Proteins, Messenger RNA, Mutation, Base Sequence, biology, Hematology, Middle Aged, Thrombophlebitis, medicine.disease, Molecular biology, Pedigree, Receptors, Complement, biology.protein, Female, Warfarin
Abstract

SummaryA 50-year-old Japanese man who had experienced recurrent episodes of venous thrombosis was found to have a hereditary protein S deficiency. The amount of total protein S antigen in plasma was reduced by approximately 50% in the patient and his two sons. DNA sequence analysis revealed a novel nonsense mutation, TAG for Gin 522 (CAG), in exon 14 of the protein S gene. Family studies performed by mutagenic PCR followed by restriction enzyme digestion showed that the proband and his two sons were heterozygous for this mutation. An mRNA-based analysis indicated that transcripts of the mutated allele were markedly reduced in the platelets of the affected individuals. Immunoblot analysis failed to detect the truncated mutant of protein S in the plasma or platelets of affected members. Our results demonstrated that this novel nonsense mutation was responsible for the quantitative deficiency of protein S.

Published
1995

131. Ryudocan, Its Molecular Structure and Function

Author

Robert D. Rosenberg and Tetsuhito Kojima

Subjects
Chemistry, Stereochemistry, Organic Chemistry, Biochemistry
Abstract

リュードカンはI型膜貫通型ヘパラン硫酸プロテオグリカンであり、当初、血流の維持に重要な役割を果たす分子としてラット毛細血管内皮細胞から単離されている。我々がラット・リュードカンとラット・シンデカンをともに単離精製したところ、コアタンパクのSDSゲル電気泳動上での分子量はそれぞれ30kDaと50kDaであった。そして、それぞれのコアタンパクをコードするcDNAのクローンニングに成功した。ラット・リュードカンとラット・シンデカンのそれぞれのcDNAから予想されるアミノ酸配列は、細胞外領域は全く異っていたが、膜貫通領域と細胞内領域において高い相同性が認められた。そして、現在ではリュードカンはシンデカン・ファミリーの一つと考えられている。また、我々はヒトの染色体20q12上に遺伝子座を持つリュードカンのヒト分子cDNAのクローンニングにも成功した。リュードカンの発現実験において、cDNAにより発現させたエピトープ標識リュードカンは、内在性リュードカンと同様に抗凝固活性を持つヘパラン硫酸 (HSact) と活性を持たないヘパラン硫酸(HSinact) を有していた。HSactとHSinactはおよそ25~30kDaの分子量を持ち、全体的な糖組成は同じであるが、HSactではグルクロノシル3-O-硫酸化グルコサミン構造がHSinactよりも多い。エピトープ標識リュードカンが発現されて細胞内濃度が増加すると、おそらくHSact合成を制御する糖鎖生合成酵素の許容量を飽和してしまうことになる。さらに、エピトープ標識リュードカンの発現実験から、HS単独のリュードカンや、様々なHS/CS (コンドロイチン硫酸) 複合型、またはCS単独のリュードカン、といった様々なイソフォームが作られることが示された。これらの多様なリュードカン・イソフォームの産生は、それらが発現する細胞表面での分子の多機能性をもたらし、様々な異なった生物活性への関与を可能にしている。

Published
1995

132. Involvement of KRAS G12A mutation in the IL-2-independent growth of a human T-LGL leukemia cell line, PLT-2

Author

Naoki, Mizutani, Hiromi, Ito, Kazumi, Hagiwara, Misa, Kobayashi, Asuka, Hoshikawa, Yayoi, Nishida, Akira, Takagi, Tetsuhito, Kojima, Motoshi, Suzuki, Yosuke, Osawa, Kazunori, Ohnishi, Masanori, Daibata, and Takashi, Murate

Subjects
Flavonoids, Interleukin-15, Original Paper, IL-2 independent growth, KRAS G12A mutation, Ras activity, MOTN-1 and PLT-2, Leukemia, Large Granular Lymphocytic, Proto-Oncogene Proteins p21(ras), Cell Line, Tumor, Proto-Oncogene Proteins, Calcium-Calmodulin-Dependent Protein Kinases, Mutation, ras Proteins, Humans, Interleukin-2, Human LGL leukemia cell lines, Ras/MAP/ERK pathway, Cell Proliferation
Abstract

Cytokine-dependent cell lines have been used to analyze the cytokine-induced cellular signaling and the mechanism of oncogenesis. In the current study, we analyzed MOTN-1 and PLT-2 cell lines established from different stages of a T-cell large granular lymphocyte leukemia patient (Daibata et al. 2004). MOTN-1 is IL-2-dependent derived from the chronic phase, whereas IL-2-independent PLT-2 is from the aggressive and terminal stage. They shared considerable chromosome abnormalities and the pattern of T-cell receptor rearrangement, presuming that the cytokine independence of PLT-2 was due to the additive genetic abnormality. Besides IL-2, IL-15 supported MOTN-1 cell growth, because these receptors share β- and γ-subunits. IL-2 activated ERK, AKT and STAT pathway of MOTN-1. STAT3 pathway of PLT-2 was also activated by IL-2, suggesting intact IL-2 induces signal transduction of PLT-2. However, ERK1/2 but not AKT, was continuously activated in PLT-2, consistent with the increased Ras-activity of PLT-2. Sequence analysis revealed KRAS G12A mutation but not NRAS and HRAS mutation of PLT-2 but not MOTN-1. Another signaling molecule affecting Ras-signaling pathway, SHP2, which has been frequently mutated in juvenile myelomonocytic leukemia (JMML), did not show mutation. Moreover, MEK inhibitor, PD98059, as well as farnesylation inhibitor inhibited PLT-2 cell growth. Using NIH3T3 and MOTN-1, ERK activation, increased cell proliferation and survival by KRAS G12A were shown, suggesting the important role of KRAS G12A in IL-2-independent growth of PLT-2. Taken together, KRAS G12A is important for IL-2-independent growth of PLT-2 cells and suggests the possibility of involvement of KRAS mutation with disease progression.

Published
2012

133. Ribavirin-induced intracellular GTP depletion activates transcription elongation in coagulation factor VII gene expression

Author

Yuki Takagi, Yumi Ando, Tetsuhito Kojima, Akira Takagi, Yuhri Miyawaki, Atsuo Suzuki, Takashi Murate, Io Kato, Moe Murata, Hidehiko Saito, and Eriko Okuyama

Subjects
Intracellular Fluid, Small interfering RNA, Transcription Elongation, Genetic, Antimetabolites, RNA polymerase II, Biology, Biochemistry, chemistry.chemical_compound, Interferon, Transcription (biology), Gene expression, Ribavirin, medicine, Humans, Molecular Biology, Gene knockdown, Factor VII, Cell Biology, Hep G2 Cells, Molecular biology, Elongation factor, chemistry, Gene Expression Regulation, biology.protein, Guanosine Triphosphate, medicine.drug
Abstract

Coagulation FVII (Factor VII) is a vitamin K-dependent glycoprotein synthesized in hepatocytes. It was reported previously that FVII gene ( F7 ) expression was up-regulated by ribavirin treatment in hepatitis C virus-infected haemophilia patients; however, its precise mechanism is still unknown. In the present study, we investigated the molecular mechanism of ribavirin-induced up-regulation of F7 expression in HepG2 (human hepatoma cell line). We found that intracellular GTP depletion by ribavirin as well as other IMPDH (inosine-5′-monophosphate dehydrogenase) inhibitors, such as mycophenolic acid and 6-mercaptopurine, up-regulated F7 expression. FVII mRNA transcription was mainly enhanced by accelerated transcription elongation, which was mediated by the P-TEFb (positive-transcription elongation factor b) complex, rather than by promoter activation. Ribavirin unregulated ELL (eleven-nineteen lysine-rich leukaemia) 3 mRNA expression before F7 up-regulation. We observed that ribavirin enhanced ELL3 recruitment to F7 , whereas knockdown of ELL3 diminished ribavirin-induced FVII mRNA up-regulation. Ribavirin also enhanced recruitment of CDK9 (cyclin-dependent kinase 9) and AFF4 to F7 . These data suggest that ribavirin-induced intracellular GTP depletion recruits a super elongation complex containing P-TEFb, AFF4 and ELL3, to F7 , and modulates FVII mRNA transcription elongation. Collectively, we have elucidated a basal mechanism for ribavirin-induced FVII mRNA up-regulation by acceleration of transcription elongation, which may be crucial in understanding its pleiotropic functions in vivo . Abbreviations: 6-MP, 6-mercaptopurine; CDK, cyclin-dependent kinase; ChIP, chromatin immunoprecipitation; CTD, C-terminal domain; DMEM, Dulbecco’s modified Eagle’s medium; DRB, 5,6-dichlorobenzimidazole 1-β-D-ribofuranoside; ELL, eleven-nineteen lysine-rich leukaemia; EU, 5-ethynyl uridine; FBS, fetal bovine serum; FVII, Factor VII; HCV, hepatitis C virus; IFN, interferon; IMPDH, inosine-5′-monophosphate dehydrogenase; ISG, IFN-stimulated gene; MPA, mycophenolic acid; NS, non-specific; Pol, II, RNA polymerase II; P-TEFb, positive-transcription elongation factor b; pSer, phosphorylated serine; qRT-PCR, quantitative real-time PCR; rFVIIa, recombinant FVIIa; RMP, ribavirin monophosphate; RNAi, RNA interference; SEC, super elongation complex; siRNA, small interfering RNA; TF, tissue factor

Published
2012

134. Transcriptional regulation of neutral sphingomyelinase 2 in all-trans retinoic acid-treated human breast cancer cell line, MCF-7

Author

Tetsuhito Kojima, Masatoshi Ichihara, Asuka Hoshikawa, Hiromi Ito, Kazumi Hagiwara, Akira Takagi, Naoki Mizutani, Misa Kobayashi, Yoshiko Banno, Takashi Murate, Keiko Tamiya-Koizumi, Yoshinori Nozawa, Kouji Tanaka, Motoshi Suzuki, Sayaka Sobue, and Mitsuhiro Nakamura

Subjects
Transcription, Genetic, Cell Survival, Retinoic acid, Tretinoin, Biochemistry, chemistry.chemical_compound, Structure-Activity Relationship, Transcription (biology), medicine, Transcriptional regulation, Humans, RNA, Messenger, Histone H3 acetylation, neoplasms, Molecular Biology, Chemistry, organic chemicals, Gene Expression Profiling, Promoter, General Medicine, Molecular biology, biological factors, Retinoic acid receptor, Sphingomyelin Phosphodiesterase, MCF-7 Cells, Chromatin immunoprecipitation, medicine.drug
Abstract

Effects of all-trans retinoic acid (ATRA) on sphingomyelinase expression were examined using MCF-7 (ATRA-sensitive) and MDA-MB-231 (ATRA-resistant) breast cancer cells. Increased NSMase activity, NSMase2 mRNA and protein were observed in ATRA-treated MCF-7 but not in ATRA-treated MDA-MB-231. Increased NSMase2 mRNA of ATRA-treated MCF-7 was mostly due to enhanced transcription. Promoter analysis revealed the important 5'-promoter region of NSMase2 between -148 and -42 bp containing three Sp1 sites but no retinoic acid responsive elements. Experiments using mutated Sp1 sites of the NSMase2 promoter, Mithramycin A (a Sp inhibitor) and Sp family over-expression demonstrated the importance of Sp family protein and the three Sp1 sites for ATRA-induced NSMase2 transcription of MCF-7 cells. Although no quantitative change of bound Sp1 on NSMase2 promoter region after ATRA treatment was detected, Sp1 phosphorylation (activation) by ATRA was observed. Interestingly, PKCδ was involved in ATRA-induced increased NSMase2 transcription. ATRA-induced PKCδ phosphorylation and then activated PKCδ phosphorylated Sp1. Chromatin immunoprecipitation (ChIP) assay showed Sp1, RARα and RXRα complex formation in MCF-7 cells regardless of ATRA treatment and ATRA-induced acetylated histone H3 of the 5'-promoter. Thus, NSMase2 mRNA expression enhanced by ATRA was due to increased transcription via phosphorylated Sp1 caused by PKCδ activation, followed by chromatin remodelling with histone H3 acetylation.

Published
2012

135. Role of down-regulated neutral ceramidase during all-trans retinoic acid-induced neuronal differentiation in SH-SY5Y neuroblastoma cells

Author

Kouji Tanaka, Motoshi Suzuki, Mitsuhiro Nakamura, Mamoru Kyogashima, Tetsuhito Kojima, Satoshi Fujii, Yoshiko Banno, Takashi Murate, Keiko Tamiya-Koizumi, Tatsuya Tsurumi, Soichiro Iwaki, Hiromi Ito, Reiji Kannagi, Akira Takagi, and Kazumi Hagiwara

Subjects
Ceramide, Cellular differentiation, Cell, Retinoic acid, Down-Regulation, Tretinoin, Biochemistry, chemistry.chemical_compound, Neuroblastoma, Structure-Activity Relationship, Neutral Ceramidase, medicine, Humans, Phosphatidylinositol, Molecular Biology, Cell Proliferation, Neurons, Sphingosine, Cell growth, Cell Differentiation, General Medicine, Sphingolipid, Cell biology, medicine.anatomical_structure, chemistry, Drug Screening Assays, Antitumor
Abstract

Neutral ceramidase (NCDase) is considered to be a critical enzyme for controlling the turnover of ceramide, an important bioactive lipid, which determines cell's fate. All-trans retinoic acid (ATRA) has been reported to induce neuronal differentiation and cell-cycle arrest [Lopez-Carballo, Moreno, Masia, Perez, and Barettino (Activation of the phosphatidylinositol 3-kinase/Akt signalling pathway by retinoic acid is required for neural differentiation of SH-SY5Y human neuroblastoma cells. J Biol Chem 2002:277:25297-304.)]. In this study, we observed that ATRA-induced cellular ceramide accumulation, cell-growth arrest and differentiation accompanied with down-regulation of NCDase in SH-SY5Y cells, without a decrease in sphingosine or sphingosine 1-phosphate. We examined whether the down-regulation of NCDase was involved in the increase in ceramide and cell differentiation. ATRA was found to down-regulate mRNA, protein and the enzyme activity of NCDase. Interestingly, GATA-2 was also decreased with ATRA treatment, and experiments using its expression vector and siRNA and chromatin immunoprecipitation assay demonstrated GATA-2 acted as transcription-factor of NCDase gene expression. By establishing stable transfectants with decreased NCDase expression and activity, we clarified the significance of NCDase down-regulation for ATRA-induced neuronal differentiation. Those sub-clones showed both increased cellular ceramide and reduced cell growth as well as neuronal differentiation phenotypes. These results demonstrate that down-regulation of NCDase through ATRA-induced GATA-2 decrease plays an important role in induction of ceramide accumulation and neuronal differentiation in SH-SY5Y cells.

Published
2012

136. Impaired human tissue factor-mediated activity in blood clotting factor VIINagoya (Arg304–>Trp). Evidence that a region in the catalytic domain of factor VII is important for the association with tissue factor

Author

Tadashi Matsushita, N. Emi, Hidehiko Saito, Tetsuhito Kojima, and I. Takahashi

Subjects
Mutation, Factor VII, Point mutation, Factor X, Ligand binding assay, Mutant, Cell Biology, Biology, medicine.disease_cause, Biochemistry, Molecular biology, law.invention, chemistry.chemical_compound, Tissue factor, chemistry, law, hemic and lymphatic diseases, medicine, Recombinant DNA, cardiovascular diseases, Molecular Biology
Abstract

A 37-year-old man was found to have an inherited abnormal factor VII (FVII) (designated FVIINagoya) that has a lower FVII procoagulant activity when tested in a one-stage assay using rabbit, simian, or human tissue factor (TF), but surprisingly has a nearly normal activity using bovine TF. DNA sequence analysis of the propositus' FVII gene revealed a C to T mutation that results in a novel amino acid substitution of Arg304 to Trp. Restriction enzyme analysis of the amplified fragment obtained from each family member demonstrated that the patient is homozygous for the point mutation, and the mother and sister of the patient are heterozygous for this mutation. To elucidate the abnormality in FVIINagoya, we compared the recombinant mutant FVII with normal FVII. In the presence of human TF, kinetic analyses demonstrated that the apparent Km values of FVIINagoya for factor Xa-mediated FVII activation and for FVIIa-mediated factor X (FX) activation were 3.6- and 4.5-fold higher than those of normal FVII, respectively. The ligand binding assay to human TF also showed that FVIINagoya had a 5.2-fold larger apparent Kd than normal. In the presence of bovine TF, however, these values showed no difference between normal and mutant FVII. These findings indicate that the major abnormality in FVIINagoya is not a catalytic dysfunction but an impaired complex-formation of human TF.FVII.FX, suggesting the importance of Arg304 in the interaction with human TF.

Published
1994

138. Sphingosine kinase 1/S1P pathway involvement in the GDNF-induced GAP43 transcription

Author

Motoshi Suzuki, Kazumi Hagiwara, Yoshiko Banno, Takashi Murate, Asuka Hoshikawa, Keiko Tamiya-Koizumi, Masatoshi Ichihara, Sayaka Sobue, Tetsuhito Kojima, Hiromi Ito, Akira Takagi, Misa Kobayashi, Masashi Murakami, and Yoshinori Nozawa

Subjects
MAPK/ERK pathway, Chromatin Immunoprecipitation, Transcription, Genetic, animal diseases, Blotting, Western, Biochemistry, Polymerase Chain Reaction, chemistry.chemical_compound, GAP-43 Protein, Sphingosine, Cell Line, Tumor, Glial cell line-derived neurotrophic factor, Humans, LY294002, Glial Cell Line-Derived Neurotrophic Factor, Cloning, Molecular, Promoter Regions, Genetic, Molecular Biology, Transcription factor, PI3K/AKT/mTOR pathway, DNA Primers, biology, Base Sequence, urogenital system, MEK inhibitor, Cell Biology, Molecular biology, Cell biology, Phosphotransferases (Alcohol Group Acceptor), nervous system, chemistry, Sphingosine kinase 1, biology.protein, Lysophospholipids, Signal Transduction
Abstract

Glial cell line-derived neurotrophic factor (GDNF) is important for the development and maintenance of dopamine neurons (Lin et al. [1993] Science 260: 1130–1132). GDNF is neuroprotective in animal models of Parkinson disease, where dopamine neurons show selective degeneration. We previously reported GDNF-induced SPHK1 gene expression in a neuroblastoma cell line, TGW (Murakami et al. [2007] J Neurochem 102: 1585–1594). In the present study, we focused on the regulatory mechanism of GAP43 (GDNF-induced neuronal phenotype) transcription to further elucidate physiological roles of GDNF-induced SPHK1 expression and activity. Stable wild-type (SPHK1-WT) but not dominant-negative SPHK1 (SPHK1-DN) overexpression increased both control- and GDNF-induced GAP43 expression. SPHK1-WT cells showed enhanced GDNF-induced sphingosine 1-phosphate (S1P) secretion compared with mock- and SPHK1-DN cells. Exogenous S1P also increased GAP43 expression. In TGW cells, PD98059, a MEK inhibitor, but not SB203580 (a p38 MAPK inhibitor) and LY294002 (a PI3K inhibitor) inhibited GDNF-induced GAP43 expression, suggesting the MEK/ERK pathway has a major role in GDNF-induced GAP43 transcription. A G-protein-coupled receptor inhibitor, pertussis toxin, and S1P1 and S1P3 receptor antagonists (VPC23019 and CAY10444) also inhibited ERK activation. Moreover, both S1P1 and S1P3 were serine-phosphorylated by GDNF, suggesting their activated states. C/EBPβ transcription factor was induced by GDNF, and DNA pull-down and chromatin immunoprecipitation assays revealed the C/EBP binding site between −131 bp and −98 bp from the first exon of GAP43. Taken together, our results showed that in TGW cells, GDNF increased SPHK1 transcription, leading to the production and secretion of S1P. Through MEK/ERK pathway, S1P stimulates GAP43 transcription with increased binding of C/EBPβ to the 5′-promoter. J. Cell. Biochem. 112: 3449–3458, 2011. © 2011 Wiley Periodicals, Inc.

Published
2011

139. A phenotypically neutral dimorphism of protein S: The substitution of Lys155 by Glu in the second EGF domain predicted by an A to G base exchange in the gene

Author

Kazuo Kagami, Junki Takamatsu, Tadashi Matsushita, Hidehiko Saito, Tomio Yamazaki, Tetsuhito Kojima, and Isamu Sugiura

Subjects
Male, Adolescent, DNA Mutational Analysis, Molecular Sequence Data, medicine.disease_cause, Polymerase Chain Reaction, Protein S, law.invention, Exon, Gene Frequency, Japan, Polymorphism (computer science), law, medicine, Humans, Gene, Alleles, Polymerase chain reaction, Genetics, Mutation, Binding Sites, Polymorphism, Genetic, Base Sequence, Epidermal Growth Factor, biology, Structural gene, Heterozygote advantage, Hematology, Molecular biology, Pedigree, Protein Structure, Tertiary, Phenotype, Genes, biology.protein, Pseudogenes
Abstract

During the course of structural gene analysis of a family with type III protein S deficiency, we found a novel DNA polymorphism: an A or G variation at nucleotide 732 in exon 6 of the PS-α gene. This A to G mutation would lead to a substitution of Lys155 by Glu in the second EGF domain. Linkage study with restriction enzyme analysis using mutagenic PCR strategy showed that the same mutation was also present in three other members of the patient's family and two individuals from an unrelated kindred, while they all had normal amounts of both immunological and functional PS levels. Restriction enzyme analysis of 182 normal Japanese genomic samples showed that 1.65% of normal population were heterozygotes for this variant allele. These findings suggest that this substitution in exon 6 is not responsible for the type III protein S deficiency but a phenotypically neutral polymorphism. Hereby we designate this polymorphism as PS-732.

Published
1993

140. Title Page / Table of Contents, Vol. 23, Supplement 1, 1993

Author

Mats Hedberg, Gunilla Bengtsson-Olivecrona, A. Leizorovicz, Lars N. Jorgensen, U. Spannagel, Per Østergaard, Thomas Mätzsch, Tina Au, Ulla Hedner, Graham F. Pineo, Gary E. Raskob, Karl-Gösta Ljungström, Ole Nordfang, Jan Holst, Bengt Lindblad, Jan Frisell, P. Kujath, Qingyu Wu, Robert D. Rosenberg, Per Anders Flordal, P. Østergaard, Ulf Nyman, M.C. Haugh, Peer Wille-Jørgensen, Carlos A. Labarrere, Ulrich Abildgaard, John P. Sheehan, Evan Sadler, Gert Nielsen, Richard D. Kenagy, Page Faulk, Tetsuhito Kojima, Lars C. Borris, Iver Lausen, H. Kristensen, Russell D. Hull, Magnus Hultin, Gwendolyn J. Stewart, Anthony J. Comerota, Joan Dawes, Bertil Friberg, John A. Mclntyre, Alexander W. Clowes, Donald S. Torry, David Bergqvist, Thomas Olivecrona, Trevor W. Barrowcliffe, L.C. Petersen, Olivier Chevreuil, Jens L. Petersen, Jane Wilson, Andrew N. Nicolaides, Monika M. Clowes, Guoqing Liu, Ana Padilla, M.M. Samama, O. Nordfang, Evi Kalodiki, Mira L. Katz, Colin G. Taylor, Dawn R. Wagenknecht, Steven R. Lentz, S. Valentin, V.V. Kakkar, Klas Norrby, Nicholas W. Shworak, Göran Nylander, L. Bara, W. Habscheid, Elaine Gray, Staffan Törngren, Michael R. Lassen, Barry Halliwell, Homayoun Hashemi, and Manuel Tsiang

Subjects
business.industry, Physiology (medical), Medicine, Library science, Table of contents, Hematology, business, Title page
Published
1993

141. FLT3/ ITD regulates leukaemia cell adhesion through α4β1 integrin and Pyk2 signalling

Author

Akira, Katsumi, Hitoshi, Kiyoi, Akihiro, Abe, Ryohei, Tanizaki, Toshihiro, Iwasaki, Miki, Kobayashi, Tadashi, Matsushita, Kozo, Kaibuchi, Takeshi, Senga, Tetsuhito, Kojima, Takayuki, Kohno, Michinari, Hamaguchi, and Tomoki, Naoe

Subjects
Pyridines, Telomere-Binding Proteins, Vascular Cell Adhesion Molecule-1, Integrin alpha4beta1, Coculture Techniques, Shelterin Complex, Leukemia, Myeloid, Acute, Mice, Focal Adhesion Kinase 2, Pyrimidines, fms-Like Tyrosine Kinase 3, Tandem Repeat Sequences, Cell Line, Tumor, Gene Duplication, Multiprotein Complexes, Mutation, Cell Adhesion, Animals, Humans, Phosphorylation, Signal Transduction
Abstract

Internal tandem duplication of FMS-like receptor tyrosine kinase 3 (FLT3/ITD) within its juxtamembrane domain is a frequent mutation in adult acute myeloid leukaemia (AML). This mutation causes constitutive activation of FLT3 and is associated with poor prognosis. The high relapse rate of FLT3/ITD-positive AML might be partly because of insufficient eradication of slow-cycling leukaemic stem cells in the bone marrow microenvironment. β1 integrin mediates haematopoietic stem and progenitor cell homing along with their retention in the bone marrow and also inhibits haematopoietic proliferation and differentiation. Here, we demonstrate that inhibition of FLT3/ITD kinase activity by a FLT3 selective inhibitor named FI-700 decreases affinity of α4β1 integrin to soluble VCAM-1. α4β1 integrin deactivation by FI-700 is independent of Rap1, which is the critical regulator of integrin inside-out signalling. In addition, selective inhibition of FLT3/ITD induces Pyk2 dephosphorylation together with the inhibition of phosphatidylinositol-3-kinase (PI3K)/Akt pathway. Both wild-type and ITD-FLT3 proteins co-immunoprecipitated with β1 integrin and Pyk2 indicating the signal crosstalk between FLT3, β1 integrin and Pyk2. These results collectively indicated that the inhibition of FLT3 kinase might contribute not only to the induction of apoptosis, but also to the leukaemia cell detachment from the bone marrow microenvironment in the treatment of AML.

Published
2010

142. Heterogeneous sphingosine-1-phosphate lyase gene expression and its regulatory mechanism in human lung cancer cell lines

Author

Kazumi Hagiwara, Yoshinori Nozawa, Yoshiko Banno, Akira Takagi, Takashi Murate, Keiko Tamiya-Koizumi, Kayo Yoshida, Mitsuhiro Nakamura, Motoshi Suzuki, Masashi Murakami, Hiromi Ito, Tetsuhito Kojima, Noriko Sasaki, Sayaka Sobue, and Misa Kobayashi

Subjects
Lung Neoplasms, Transcription, Genetic, Sp1 Transcription Factor, Protozoan Proteins, Gene Expression, Biology, Response Elements, Gene Expression Regulation, Enzymologic, chemistry.chemical_compound, Transcription (biology), Cell Line, Tumor, Gene expression, otorhinolaryngologic diseases, Humans, Electrophoretic mobility shift assay, Dictyostelium, Molecular Biology, Aldehyde-Lyases, Regulation of gene expression, Reporter gene, Sphingosine, Promoter, Cell Biology, Molecular biology, GATA4 Transcription Factor, Neoplasm Proteins, Gene Expression Regulation, Neoplastic, chemistry, sense organs, Chromatin immunoprecipitation
Abstract

The role of sphingolipid metabolic pathway has been recognized in determining cellular fate. Although sphingolipid degradation has been extensively studied, gene expression of human sphingosine 1-phosphate lyase (SPL) catalyzing sphingosine 1-phosphate (S1P) remains to be determined. Among 5 human lung cancer cell lines examined, SPL protein levels paralleled the respective mRNA and enzyme activities. Between H1155 and H1299 cells used for further experiments, higher cellular S1P was observed in H1155 with higher SPL activity compared with H1299 with low SPL activity. GATA-4 has been reported to affect SPL transcription in Dictyostelium discoideum. GATA-4 was observed in H1155 but not in other cell lines. Overexpression of GATA-4 in H1299 increased SPL expression. However, promoter analysis of human SPL revealed that the most important region was located between -136bp and -88bp from the first exon, where 2 Sp1 sites exist but no GATA site. DNA pull-down assay of H1155 showed increased DNA binding of Sp1 and GATA-4 within this promoter region compared with H1299. Electrophoresis mobility shift assay (EMSA), chromatin immunoprecipitation (ChIP) assay, reporter assay using mutated binding motif, and mithramycin A, a specific Sp1 inhibitor, suggest the major role of Sp1 in SPL transcription and no direct binding of GATA-4 with this 5' promoter region. The collaborative role of GATA-4 was proved by showing coimmunoprecipitation of Sp1 and GATA-4 using GST-Sp1 and overexpressed GATA-4. Thus, high SPL transcription of H1155 cells was regulated by Sp1 and GATA-4/Sp1 complex formation, both of which bind to Sp1 sites of the 5'-SPL promoter.

Published
2010

143. Down-regulation of PROS1 gene expression by 17beta-estradiol via estrogen receptor alpha (ERalpha)-Sp1 interaction recruiting receptor-interacting protein 140 and the corepressor-HDAC3 complex

Author

Tetsuhito Kojima, Yuta Fujimori, Naomi Sanda, Yuhri Miyawaki, Atsuo Suzuki, Hidehiko Saito, Akira Takagi, Takayuki Yamada, and Takashi Murate

Subjects
Sp1 Transcription Factor, Estrogen receptor, Biology, Biochemistry, Histone Deacetylases, Protein S, Pregnancy, Humans, Nuclear Receptor Co-Repressor 1, Electrophoretic mobility shift assay, Gene Regulation, Promoter Regions, Genetic, Molecular Biology, Nuclear receptor co-repressor 1, Adaptor Proteins, Signal Transducing, Sp1 transcription factor, Estradiol, Pregnancy Complications, Hematologic, Estrogen Receptor alpha, Nuclear Proteins, Estrogens, Thrombosis, Cell Biology, Blood Proteins, Hep G2 Cells, Molecular biology, Chromatin, GC Rich Sequence, Nuclear Receptor Interacting Protein 1, Sp3 Transcription Factor, Gene Expression Regulation, Multiprotein Complexes, Female, Chromatin immunoprecipitation, Estrogen receptor alpha, Corepressor
Abstract

Pregnant women show a low level of protein S (PS) in plasma, which is known to be a risk for deep venous thrombosis. 17Beta-estradiol (E(2)), an estrogen that increases in concentration in the late stages of pregnancy, regulates the expression of various genes via the estrogen receptor (ER). Here, we investigated the molecular mechanisms behind the reduction in PS levels caused by E(2) in HepG2-ERalpha cells, which stably express ERalpha, and also the genomic ER signaling pathway, which modulates the ligand-dependent repression of the PSalpha gene (PROS1). We observed that E(2) repressed the production of mRNA and antigen of PS. A luciferase reporter assay revealed that E(2) down-regulated PROS1 promoter activity and that this E(2)-dependent repression disappeared upon the deletion or mutation of two adjacent GC-rich motifs in the promoter. An electrophoretic mobility shift assay and DNA pulldown assay revealed that the GC-rich motifs were associated with Sp1, Sp3, and ERalpha. In a chromatin immunoprecipitation assay, we found ERalpha-Sp protein-promoter interaction involved in the E(2)-dependent repression of PROS1 transcription. Furthermore, we demonstrated that E(2) treatment recruited RIP140 and the NCoR-SMRT-HDAC3 complex to the PROS1 promoter, which hypoacetylated chromatin. Taken together, this suggested that E(2) might repress PROS1 transcription depending upon ERalpha-Sp1 recruiting transcriptional repressors in HepG2-ERalpha cells and, consequently, that high levels of E(2) leading to reduced levels of plasma PS would be a risk for deep venous thrombosis in pregnant women.

Published
2010

144. Isolation and characterization of heparan sulfate proteoglycans produced by cloned rat microvascular endothelial cells

Author

G A Marchildon, Tetsuhito Kojima, James A. Marcum, Leone Cw, and Robert D. Rosenberg

Subjects
Gel electrophoresis, Protease, biology, medicine.medical_treatment, Size-exclusion chromatography, Cell Biology, Heparan sulfate, Trypsin, Biochemistry, Molecular biology, Protease inhibitor (biology), chemistry.chemical_compound, chemistry, Proteoglycan, Glucosamine, medicine, biology.protein, Molecular Biology, medicine.drug
Abstract

We have isolated heparan sulfate proteoglycans (HSPGs) from cloned rat microvascular endothelial cells using a combination of ion-exchange chromatography, affinity fractionation with antithrombin III (AT III), and gel filtration in denaturing solvents. The anticoagulantly active heparan sulfate proteoglycans (HSPGact) which bind tightly to AT III bear mainly anticoagulantly active heparan sulfate (HSact) whereas the anticoagulantly inactive heparan sulfate proteoglycans (HSPGinact) possess mainly anticoagulantly inactive heparan sulfate (HSinact). HSact and HSinact were also isolated by a combination of ion-exchange chromatography, treatment with protease and chondroitin ABC lyase, and affinity fractionation with AT III. HSact and HSinact have molecular sizes of about 25-30 kDa with the same overall composition of monosaccharides except that HSact exhibits about nine glucuronsyl 3-O-sulfated glucosamines/chain whereas HSinact possesses about three glucuronsyl 3-O-sulfated glucosamines/chain. Direct isolation of the AT III-binding site of HSact by exposing carbohydrate chains to Flavobacterium heparitinase in the presence of protease inhibitor revealed only a single interaction site which contained two to three glucuronsyl 3-O-sulfated glucosamine residues. The core proteins of HSPGact and HSPGinact were isolated by treatment with Flavobacterium heparitinase and purification by ion-exchange chromatography. The molecular sizes of the core proteins were established by sodium dodecyl sulfate-polyacrylamide gel electrophoresis and their primary structures were examined by cleavage with trypsin or endopeptidase Glu-C as well as separation of peptides by reverse-phase high performance liquid chromatography. The results showed that both sets of core proteins exhibited three major components with molecular sizes of 50, 30, and 25 kDa, respectively. The 25-kDa species appears to be a proteolytic degradation product of the 30-kDa species. The peptide mapping revealed that HSPGact and HSPGinact possess extremely similar core proteins.

Published
1992

145. Molecular cloning and expression of two distinct cDNA-encoding heparan sulfate proteoglycan core proteins from a rat endothelial cell line

Author

Nicholas W. Shworak, Tetsuhito Kojima, and Robert D. Rosenberg

Subjects
biology, Cell Biology, Molecular cloning, Cell sorting, Biochemistry, Molecular biology, Transmembrane protein, Syndecan 1, Proteoglycan, Complementary DNA, biology.protein, Extracellular, Molecular Biology, Integral membrane protein
Abstract

The cloned rat fat pad endothelial cell (RFP-EC) line synthesizes anticoagulantly active heparan sulfate proteoglycans (HSPGact) and anticoagulantly inactive heparan sulfate proteoglycans (HSPGinact), both of which exhibit 25-, 30-, and 50-kDa core proteins of extremely similar structure. The primary sequences of internal peptides obtained from HSPGinact core proteins and the NH2-terminal sequence analyses of the 25-kDa component from the HSPGinact core proteins demonstrate that the 30-kDa component is a previously unidentified species, designated as ryudocan, with the 25-kDa component representing a proteolytic degradation product, while the 50-kDa component is the rat homolog of syndecan (Saunders, S. Jalkanen, M., O'Farrell, S., and Bernfield, M. (1989) J. Cell Biol. 108, 1547-1556). Specific oligonucleotide probes were obtained for ryudocan and syndecan by polymerase chain reaction, and the corresponding cDNAs were isolated from a RFP-EC library. The cDNAs encode type I integral membrane proteins of 202 and 313 amino acids, respectively, which have homologous transmembrane and intracellular domains but very distinct extracellular regions. In particular, ryudocan exhibits only three potential glycosaminoglycan attachment sites within the extracellular region while syndecan has five glycosaminoglycan attachment sites within the same domain. Both species are expressed in RFP-EC lines, primary rat aortic smooth muscle cells and primary rat skin fibroblast cells. The levels of ryudocan and syndecan mRNA were measured by quantitative polymerase chain reaction in primary microvascular endothelial cells and closely associated non-endothelial cells isolated by cell sorting. Ryudocan and syndecan mRNAs were abundantly expressed in both populations representing about 0.1-0.5% of mRNA.

Published
1992

146. Mutated ras induced PLD1 gene expression through increased Sp1 transcription factor

Author

Siqiang, Gao, Masashi, Murakami, Hiromi, Ito, Ayako, Furuhata, Kayo, Yoshida, Yoko, Tagawa, Kazumi, Hagiwara, Akira, Takagi, Tetsuhito, Kojima, Motoshi, Suzuki, Yoshiko, Banno, Yoshinori, Nozawa, and Takashi, Murate

Subjects
Mice, Genes, ras, Gene Expression Regulation, Sp1 Transcription Factor, Mutation, Phospholipase D, Animals, Humans, RNA, Messenger, Caco-2 Cells, Promoter Regions, Genetic
Abstract

The underlying mechanisms of oncogene-induced phospholipase D (PLD) activation have not been fully elucidated. The effect of the mutated-ras on PLD mRNA was examined using colon cancer cell lines as well as mock- and mutated ras-transfected NIH3T3 cells. Ras-mutation and activation were correlated, and cells with enhanced ras-activation showed increased PLD1 mRNA and protein. Analysis of the 5' PLD1 promoter using a representative cell line, DLD-1 and also mutated ras-NIH3T3, showed one Sp1-site as the important ras-responsible motif. Spl inhibition with mithramycin A and Spl siRNA inhibited PLD1 protein expression and its promoter activity. Sp1 but not Sp3 protein level and increased Sp1-motif binding activity were correlated with ras activation. Furthermore, overexpression of Sp1 in drosophila SL2 cells lacking Sp family proteins increased PLD1 promoter activity. EMSA and chromatin immunoprecipitation assay confirmed the importance of Sp1 protein binding to the Sp1-motif in ras-induced PLD1 mRNA expression.

Published
2009

147. Activated protein C resistance in the Japanese population due to homozygosity for the factor V R2 haplotype

Author

Akira Takagi, Tomio Yamazaki, Yoshimi Toyoda, Tetsuhito Kojima, Hidehiko Saito, and Hiromi Okada

Subjects
medicine.medical_specialty, Biology, Protein C (activated), Asian People, Japan, Risk Factors, Internal medicine, Coagulopathy, medicine, Humans, Activated Protein C Resistance, Genetics, chemistry.chemical_classification, Hematology, Haplotype, Homozygote, Factor V, Japanese population, medicine.disease, Molecular biology, Enzyme, chemistry, Haplotypes, biology.protein, Activated protein C resistance, Protein C
Published
2009

148. ATRA inhibits ceramide kinase transcription in a human neuroblastoma cell line, SH-SY5Y cells: the role of COUP-TFI

Author

Kazumi Hagiwara, Masatoshi Ichihara, Yoshiko Banno, Takashi Murate, Hiromi Ito, Keiko Tamiya-Koizumi, Kayo Yoshida, Sayaka Sobue, Mamoru Kyogashima, Akira Takagi, Tetsuhito Kojima, Masashi Murakami, Kouji Tanaka, Motoshi Suzuki, and Yoshinori Nozawa

Subjects
Transcriptional Activation, Small interfering RNA, Ceramide, Receptors, Retinoic Acid, Chicken ovalbumin upstream promoter-transcription factor, Molecular Sequence Data, Electrophoretic Mobility Shift Assay, Tretinoin, Retinoid X receptor, Biology, Transfection, Biochemistry, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Neuroblastoma, Ceramide kinase, Gene expression, Neurites, Humans, Immunoprecipitation, Electrophoretic mobility shift assay, RNA, Small Interfering, Promoter Regions, Genetic, neoplasms, Transcription factor, Cell Proliferation, Binding Sites, COUP Transcription Factor I, Cell Death, organic chemicals, Retinoic Acid Receptor alpha, Exons, Cell biology, Phosphotransferases (Alcohol Group Acceptor), Retinoid X Receptors, chemistry
Abstract

Ceramide is the central lipid in the sphingolipid metabolism. Ceramide kinase (CERK) and its product, ceramide 1-phosphate, have been implicated in various cellular functions. However, the regulatory mechanism of CERK gene expression remains to be determined. Here, we examined CERK mRNA level during all-trans retinoic acid (ATRA)-induced differentiation of a human neuroblastoma cell line, SH-SY5Y. ATRA reduced CERK mRNA and protein levels. Over-expression and small interfering RNA (siRNA) of CERK revealed that CERK is inhibitory against ATRA-induced neuronal differentiation and cell growth arrest. ATRA inhibited the transcriptional activity of 5'-promoter of CERK. Truncation and mutation study suggests that ATRA-responsible region was mainly located in the tandem retinoic acid responsive elements (RARE) between -40 bp and the first exon. The electrophoresis mobility shift assay revealed that ATRA produced two retarded bands, which were erased by antibody against chicken ovalbumin upstream promoter transcription factor I (COUP-TFI), RARalpha, and RXRalpha, respectively. DNA pull-down assay confirmed increased binding of these transcription factors to RARE. Transient expression of RAR, RXR, and COUP-TFI and siRNA transfection of these genes revealed that COUP-TFI inhibited CERK mRNA. Furthermore, chromatin immunoprecipitation assay showed the recruitment of co-repressors as well as three transcription factors. These results suggest that COUP-TFI was the ATRA-responsive suppressive transcription factor of CERK gene transcription.

Published
2009

149. Impaired secretion of carboxyl-terminal truncated factor VII due to an F7 nonsense mutation associated with FVII deficiency

Author

Akira Takagi, Daisuke Nakashima, Ryoko Tanaka, Atsuo Suzuki, Tomoki Naoe, Tetsuhito Kojima, Akira Katsumi, Koji Yamamoto, Takashi Murate, Tadashi Matsushita, Yuta Fujimori, Yuhri Miyawaki, and Takayuki Yamada

Subjects
Adult, Factor VII Deficiency, Mutant, Nonsense mutation, Cell Culture Techniques, CHO Cells, Biology, medicine.disease_cause, Culture Media, Serum-Free, chemistry.chemical_compound, Cricetulus, Pregnancy, hemic and lymphatic diseases, Cricetinae, medicine, Animals, Humans, cardiovascular diseases, Fluorescent Antibody Technique, Indirect, Factor IX, Mutation, Factor VII, Wild type, Hematology, Sequence Analysis, DNA, Molecular biology, Recombinant Proteins, Culture Media, Blot, chemistry, Codon, Nonsense, Female, Protein C, Polymorphism, Restriction Fragment Length, medicine.drug
Abstract

Introduction Factor VII (FVII) is a vitamin K-dependent glycoprotein secreted into the blood circulation from hepatic cells. We investigated the molecular basis of the congenital FVII deficiency found in a Japanese patient. Materials and Methods We analyzed the F7 gene of the patient, who was diagnosed with a FVII deficiency at pregnancy. We expressed a carboxyl-terminal truncated FVII (Arg462X FVII) corresponding to the identified mutation in CHO-K1 cells. To study roles of the carboxyl-terminus in the secretion of FVII, we also expressed a series of recombinant FVIIs deleted of limited numbers of carboxyl-terminal amino acids (462Arg-466Pro). Results We identified a nonsense mutation (c.1384C > T: p.Arg462X) in F7 , leading to a lack of five amino acids in the carboxyl-terminus. In expression experiments, Arg462X FVII was undetectable not only by Western blotting, but also by ELISA. A Western blot analysis of the truncated FVIIs revealed that all mutants were expressed in the cells the same as the wild type, but were secreted into the culture medium in lesser amounts than the wild type depending on the length of the deletion, which was confirmed by ELISA. Arg462X FVII did not colocalize with the Golgi on immunofluorescence staining, suggesting that it might be retained in the ER and degraded in the cell. Conclusion The carboxyl-terminal amino acids of FVII play an important role in its secretion, and the p.Arg462X mutation was likely to have caused the FVII deficiency in this patient.

Published
2009

150. Genetic risk factors for thrombophilia in Japanese

Author

Toshiyuki, Miyata, Hiromi, Okada, Tomio, Kawasaki, Hajime, Tsuji, Seiji, Madoiwa, Yoichi, Sakata, Tetsuhito, Kojima, Mitsuru, Murata, and Yasuo, Ikeda

Subjects
Polymorphism, Genetic, Lipoproteins, Thrombomodulin, Blood Proteins, Venous Thromboembolism, Antithrombins, Protein S, Cohort Studies, Asian People, Risk Factors, Mutation, Humans, Thrombophilia, Genetic Predisposition to Disease, Protein C
Published
2009

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