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16 results on '"Junko Koiwa"'

1. Lansoprazole Ameliorates Isoniazid-Induced Liver Injury

Author

Eri Wakai, Takashi Shiromizu, Shota Otaki, Junko Koiwa, Satoshi Tamaru, and Yuhei Nishimura

Subjects
drug-induced liver injury, drug repositioning, gene expression signature, connectivity map, FDA adverse event reporting system, zebrafish, Medicine, Pharmacy and materia medica, RS1-441
Abstract

Isoniazid is a first-line drug in antitubercular therapy. Isoniazid is one of the most commonly used drugs that can cause liver injury or acute liver failure, leading to death or emergency liver transplantation. Therapeutic approaches for the prevention of isoniazid-induced liver injury are yet to be established. In this study, we identified the gene expression signature for isoniazid-induced liver injury using a public transcriptome dataset, focusing on the differences in susceptibility to isoniazid in various mouse strains. We predicted that lansoprazole is a potentially protective drug against isoniazid-induced liver injury using connectivity mapping and an adverse event reporting system. We confirmed the protective effects of lansoprazole against isoniazid-induced liver injury using zebrafish and patients’ electronic health records. These results suggest that lansoprazole can ameliorate isoniazid-induced liver injury. The integrative approach used in this study may be applied to identify novel functions of clinical drugs, leading to drug repositioning.

Published
2024
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2. Generation of a Transgenic Zebrafish Line for In Vivo Assessment of Hepatic Apoptosis

Author

Aina Higuchi, Eri Wakai, Tomoko Tada, Junko Koiwa, Yuka Adachi, Takashi Shiromizu, Hidemasa Goto, Toshio Tanaka, and Yuhei Nishimura

Subjects
liver, apoptosis, caspase, Förster resonance energy transfer, zebrafish, in vivo fluorescence imaging, Medicine, Pharmacy and materia medica, RS1-441
Abstract

Hepatic apoptosis is involved in a variety of pathophysiologic conditions in the liver, including hepatitis, steatosis, and drug-induced liver injury. The development of easy-to-perform and reliable in vivo assays would thus greatly enhance the efforts to understand liver diseases and identify associated genes and potential drugs. In this study, we developed a transgenic zebrafish line that was suitable for the assessment of caspase 3 activity in the liver by using in vivo fluorescence imaging. The larvae of transgenic zebrafish dominantly expressed Casper3GR in the liver under control of the promoter of the phosphoenolpyruvate carboxykinase 1 gene. Casper3GR is composed of two fluorescent proteins, tagGFP and tagRFP, which are connected via a peptide linker that can be cleaved by activated caspase 3. Under tagGFP excitation conditions in zebrafish that were exposed to the well-characterized hepatotoxicant isoniazid, we detected increased and decreased fluorescence associated with tagGFP and tagRFP, respectively. This result suggests that isoniazid activates caspase 3 in the zebrafish liver, which digests the linker between tagGFP and tagRFP, resulting in a reduction in the Förster resonance energy transfer to tagRFP upon tagGFP excitation. We also detected isoniazid-induced inhibition of caspase 3 activity in zebrafish that were treated with the hepatoprotectants ursodeoxycholic acid and obeticholic acid. The transgenic zebrafish that were developed in this study could be a powerful tool for identifying both hepatotoxic and hepatoprotective drugs, as well as for analyzing the effects of the genes of interest to hepatic apoptosis.

Published
2021
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3. Generation of a Triple-Transgenic Zebrafish Line for Assessment of Developmental Neurotoxicity during Neuronal Differentiation

Author

Junko Koiwa, Takashi Shiromizu, Yuka Adachi, Makoto Ikejiri, Kaname Nakatani, Toshio Tanaka, and Yuhei Nishimura

Subjects
developmental neurotoxicity, neuronal differentiation, zebrafish, in vivo fluorescence imaging, Medicine, Pharmacy and materia medica, RS1-441
Abstract

The developing brain is extremely sensitive to many chemicals. Exposure to neurotoxicants during development has been implicated in various neuropsychiatric and neurological disorders, including autism spectrum disorders and schizophrenia. Various screening methods have been used to assess the developmental neurotoxicity (DNT) of chemicals, with most assays focusing on cell viability, apoptosis, proliferation, migration, neuronal differentiation, and neuronal network formation. However, assessment of toxicity during progenitor cell differentiation into neurons, astrocytes, and oligodendrocytes often requires immunohistochemistry, which is a reliable but labor-intensive and time-consuming assay. Here, we report the development of a triple-transgenic zebrafish line that expresses distinct fluorescent proteins in neurons (Cerulean), astrocytes (mCherry), and oligodendrocytes (mCitrine), which can be used to detect DNT during neuronal differentiation. Using in vivo fluorescence microscopy, we could detect DNT by 6 of the 10 neurotoxicants tested after exposure to zebrafish from 12 h to 5 days’ post-fertilization. Moreover, the chemicals could be clustered into three main DNT groups based on the fluorescence pattern: (i) inhibition of neuron and oligodendrocyte differentiation and stimulation of astrocyte differentiation; (ii) inhibition of neuron and oligodendrocyte differentiation; and (iii) inhibition of neuron and astrocyte differentiation, which suggests that reporter expression reflects the toxicodynamics of the chemicals. Thus, the triple-transgenic zebrafish line developed here may be a useful tool to assess DNT during neuronal differentiation.

Published
2019
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4. Involvement of homeobox transcription factor Mohawk in palatogenesis

Author

Junko Koiwa, Eri Wakai, Yuka Adachi, Aina Higuchi, Yuhei Nishimura, and Takashi Shiromizu

Subjects
Embryology, animal structures, Cyclopamine, Mice, chemistry.chemical_compound, Cranial neural crest, GLI1, Animals, Hedgehog Proteins, Sonic hedgehog, Zebrafish, Transcription factor, Homeodomain Proteins, biology, Palate, Genes, Homeobox, Gene Expression Regulation, Developmental, General Medicine, biology.organism_classification, Cell biology, Cleft Palate, chemistry, Neural Crest, embryonic structures, Pediatrics, Perinatology and Child Health, biology.protein, Homeobox, Transcription Factors, Developmental Biology, Transforming growth factor
Abstract

Palatogenesis is affected by many factors, including gene polymorphisms and exposure to toxic chemicals during sensitive developmental periods. Cleft palate is one of the most common congenital anomalies, and ongoing efforts to elucidate the molecular mechanisms underlying palatogenesis are providing useful insights to reduce the risk of this disorder. To identify novel potential regulators of palatogenesis, we analyzed public transcriptome datasets from a mouse model of cleft palate caused by selective deletion of transforming growth factor-β (TGFβ) receptor type 2 in cranial neural crest cells. We identified the homeobox transcription factor Mohawk (Mkx) as a gene downregulated in the maxilla of TGFβ knockout mice compared with wild-type mice. To examine the role of mkx in palatogenesis, we used CRISPR/Cas9 editing to generate zebrafish with impaired expression of mkxa and mkxb, the zebrafish homologs of Mkx. We found that mkx crispants expressed reduced levels of gli1, a critical transcription factor in the Sonic hedgehog (SHH) signaling pathway that plays an important role in the regulation of palatogenesis. Furthermore, we found that mkxa-/- zebrafish were more susceptible than mkxa+/+ zebrafish to the deleterious effects of cyclopamine, an inhibitor of SHH signaling, on upper jaw development. These results suggest that Mkx may be involved in palatogenesis regulated by TGFβ and SHH signaling, and that impairment in Mkx function may be related to the etiology of cleft palate.

Published
2021

5. Generation of a Transgenic Zebrafish Line for In Vivo Assessment of Hepatic Apoptosis

Author

Eri Wakai, Toshio Tanaka, Yuka Adachi, Aina Higuchi, Junko Koiwa, Tomoko Tada, Takashi Shiromizu, Hidemasa Goto, and Yuhei Nishimura

Subjects
in vivo fluorescence imaging, caspase, Pharmaceutical Science, Caspase 3, liver, Article, chemistry.chemical_compound, Pharmacy and materia medica, In vivo, Drug Discovery, medicine, Zebrafish, Caspase, Liver injury, biology, apoptosis, Obeticholic acid, medicine.disease, biology.organism_classification, zebrafish, Cell biology, RS1-441, chemistry, Apoptosis, Förster resonance energy transfer, biology.protein, Medicine, Molecular Medicine, hepatoprotectant, Steatosis, drug-induced liver injury
Abstract

Hepatic apoptosis is involved in a variety of pathophysiologic conditions in the liver, including hepatitis, steatosis, and drug-induced liver injury. The development of easy-to-perform and reliable in vivo assays would thus greatly enhance the efforts to understand liver diseases and identify associated genes and potential drugs. In this study, we developed a transgenic zebrafish line that was suitable for the assessment of caspase 3 activity in the liver by using in vivo fluorescence imaging. The larvae of transgenic zebrafish dominantly expressed Casper3GR in the liver under control of the promoter of the phosphoenolpyruvate carboxykinase 1 gene. Casper3GR is composed of two fluorescent proteins, tagGFP and tagRFP, which are connected via a peptide linker that can be cleaved by activated caspase 3. Under tagGFP excitation conditions in zebrafish that were exposed to the well-characterized hepatotoxicant isoniazid, we detected increased and decreased fluorescence associated with tagGFP and tagRFP, respectively. This result suggests that isoniazid activates caspase 3 in the zebrafish liver, which digests the linker between tagGFP and tagRFP, resulting in a reduction in the Förster resonance energy transfer to tagRFP upon tagGFP excitation. We also detected isoniazid-induced inhibition of caspase 3 activity in zebrafish that were treated with the hepatoprotectants ursodeoxycholic acid and obeticholic acid. The transgenic zebrafish that were developed in this study could be a powerful tool for identifying both hepatotoxic and hepatoprotective drugs, as well as for analyzing the effects of the genes of interest to hepatic apoptosis.

Published
2021
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7. Zebrafish-Based Drug Discovery and Precision Medicine

Author

Mayuko Okuno, Junko Koiwa, Naohisa Kuriyama, Ikuko Mikami, Shota Sasagawa, Erina Kitahara, Aiko Sugimura, Yuka Takahashi, Toshio Tanaka, and Shuji Isaji

Subjects
biology, Drug discovery, business.industry, Applied Mathematics, General Mathematics, Medicine, Computational biology, Precision medicine, biology.organism_classification, business, Zebrafish
Published
2018

8. Generation of a Triple-Transgenic Zebrafish Line for Assessment of Developmental Neurotoxicity during Neuronal Differentiation

Author

Kaname Nakatani, Takashi Shiromizu, Toshio Tanaka, Makoto Ikejiri, Yuhei Nishimura, Yuka Adachi, and Junko Koiwa

Subjects
in vivo fluorescence imaging, Pharmaceutical Science, lcsh:Medicine, lcsh:RS1-441, Article, lcsh:Pharmacy and materia medica, Astrocyte differentiation, Drug Discovery, medicine, Biological neural network, Viability assay, Progenitor cell, Zebrafish, neuronal differentiation, biology, lcsh:R, Oligodendrocyte differentiation, biology.organism_classification, zebrafish, Cell biology, medicine.anatomical_structure, nervous system, Molecular Medicine, developmental neurotoxicity, Neuron, mCherry
Abstract

The developing brain is extremely sensitive to many chemicals. Exposure to neurotoxicants during development has been implicated in various neuropsychiatric and neurological disorders, including autism spectrum disorders and schizophrenia. Various screening methods have been used to assess the developmental neurotoxicity (DNT) of chemicals, with most assays focusing on cell viability, apoptosis, proliferation, migration, neuronal differentiation, and neuronal network formation. However, assessment of toxicity during progenitor cell differentiation into neurons, astrocytes, and oligodendrocytes often requires immunohistochemistry, which is a reliable but labor-intensive and time-consuming assay. Here, we report the development of a triple-transgenic zebrafish line that expresses distinct fluorescent proteins in neurons (Cerulean), astrocytes (mCherry), and oligodendrocytes (mCitrine), which can be used to detect DNT during neuronal differentiation. Using in vivo fluorescence microscopy, we could detect DNT by 6 of the 10 neurotoxicants tested after exposure to zebrafish from 12 h to 5 days&rsquo, post-fertilization. Moreover, the chemicals could be clustered into three main DNT groups based on the fluorescence pattern: (i) inhibition of neuron and oligodendrocyte differentiation and stimulation of astrocyte differentiation, (ii) inhibition of neuron and oligodendrocyte differentiation, and (iii) inhibition of neuron and astrocyte differentiation, which suggests that reporter expression reflects the toxicodynamics of the chemicals. Thus, the triple-transgenic zebrafish line developed here may be a useful tool to assess DNT during neuronal differentiation.

Published
2019

9. [Next generation zebrafish-based drug discovery and precision medicine]

Author

Toshio Tanaka and Junko Koiwa

Subjects
0301 basic medicine, Drug, Phenotypic screening, media_common.quotation_subject, Bioinformatics, 03 medical and health sciences, Mice, 0302 clinical medicine, Phenomics, In vivo, Neoplasms, Drug Discovery, Medicine, Animals, Humans, Precision Medicine, Zebrafish, media_common, Pharmacology, biology, business.industry, Drug discovery, Genomics, Precision medicine, biology.organism_classification, Xenograft Model Antitumor Assays, United States, 030104 developmental biology, Personalized medicine, business, 030217 neurology & neurosurgery
Abstract

Even after entering the era of genomic drug discovery in the 21st century, development of a breakthrough therapeutic drug (first-in-class) for intractable diseases (unmet medical needs) has been extremely difficult, but to the US FDA 62% of the approved first-in-class drugs are found by phenotypic screening. The next-generation zebrafish drug discovery enables high-throughput quantitative live in vivo phenotypic screening, and has been impacting global drug discovery strategies now. Compared to severe immunodeficient mice, zebrafish is expected to become a true individualized medical tool as a clinical ex vivo diagnostic system because of the high efficiency and speed of engraftment of patient-derived cancer xenotransplantation. Phenomics-based personalized medicine with the patient-derived cancer xenograft zebrafish in addition to conventional omics platform of individualized medicine is a true next-generation precision medicine to utilize for selection of therapeutic drugs and decision of their doses for the patient, and emerging paradigm shift is realizing in this century.

Published
2019

11. Using zebrafish in systems toxicology for developmental toxicity testing

Author

Reiko Kawase, Atsuto Inoue, Yuhei Nishimura, Shota Sasagawa, Koki Kawaguchi, Toru Maruyama, Soonih Kim, Toshio Tanaka, and Junko Koiwa

Subjects
0301 basic medicine, Embryology, animal structures, Systems toxicology, Research groups, ved/biology, ved/biology.organism_classification_rank.species, Developmental toxicity, General Medicine, Biology, Bioinformatics, biology.organism_classification, Chemical exposure, 03 medical and health sciences, Human health, 030104 developmental biology, Pediatrics, Perinatology and Child Health, Model organism, Zebrafish, Developmental Biology
Abstract

With the high cost and the long-term assessment of developmental toxicity testing in mammals, the vertebrate zebrafish has become a useful alternative model organism for high-throughput developmental toxicity testing. Zebrafish is also very favorable for the 3R perspective in toxicology; however, the methodologies used by research groups vary greatly, posing considerable challenges to integrative analysis. In this review, we discuss zebrafish developmental toxicity testing, focusing on the methods of chemical exposure, the assessment of morphological abnormalities, housing conditions and their effects on the production of healthy embryos, and future directions. Zebrafish as a systems toxicology model has the potential to elucidate developmental toxicity pathways, and to provide a sound basis for human health risk assessments.

Published
2016

13. Zebrafish yolk sac microinjection of thalidomide for assessment of developmental toxicology

Author

Yuka Takahashi, Mina Okamura, Ikuko Mikami, Toshio Tanaka, and Junko Koiwa

Subjects
Embryology, Animal Welfare (journal), biology, General Medicine, biology.organism_classification, Bioinformatics, Fecundity, Thalidomide, medicine.anatomical_structure, Developmental toxicology, Pediatrics, Perinatology and Child Health, medicine, Yolk sac, Zebrafish, Microinjection, Developmental Biology, medicine.drug
Abstract

Zebrafish offer advantages over traditional rodent models in developmental toxicology studies, including low maintenance costs, high fecundity, genetic diversity, and reduced animal welfare concerns (1,2).

Published
2019

14. in vivo Phenomic Screening System for Antiepileptic Drugs using Dravet Syndrome Zebrafish Model

Author

Yuhei Nishimura, Toshio Tanaka, Mayuko Okuno, Junko Koiwa, Erina Kitahara, Shota Sasagawa, Yuka Takahashi, Mina Okamura, and Ikuko Mikami

Subjects
Thesaurus (information retrieval), Dravet syndrome, biology, In vivo, business.industry, Applied Mathematics, General Mathematics, medicine, Computational biology, medicine.disease, biology.organism_classification, business, Zebrafish
Published
2019

15. In Vivo Detection of Mitochondrial Dysfunction Induced by Clinical Drugs and Disease-Associated Genes Using a Novel Dye ZMJ214 in Zebrafish

Author

Takeshi Miyazaki, Junko Koiwa, Shota Sasagawa, Yuhei Nishimura, Taichi Shintou, Reiko Kawase, Koki Kawaguchi, Mizuki Yuge, Tsuyoshi Nomoto, Toshio Tanaka, and Soichiro Murakami

Subjects
0301 basic medicine, Oligomycin, Mitochondrion, Biology, Biochemistry, Nitrophenols, 03 medical and health sciences, chemistry.chemical_compound, Benzophenones, Troglitazone, In vivo, Live cell imaging, Toxicity Tests, medicine, Animals, Hypoglycemic Agents, Chromans, Zebrafish, Fluorescent Dyes, Membrane Potential, Mitochondrial, Pioglitazone, fungi, Optical Imaging, General Medicine, Carbocyanines, Zebrafish Proteins, Mitochondrial carrier, biology.organism_classification, medicine.disease, Molecular biology, Cell biology, Anti-Bacterial Agents, Mitochondria, Mitochondrial toxicity, Disease Models, Animal, 030104 developmental biology, chemistry, Molecular Medicine, Anticonvulsants, Oligomycins, Thiazolidinediones, Tolcapone, medicine.drug
Abstract

Mitochondrial dysfunction has been implicated in various drug-induced toxicities and genetic disorders. Recently, the zebrafish has emerged as a versatile animal model for both chemical and genetic screenings. Taking advantage of its transparency, various in vivo fluorescent imaging methods have been developed to identify novel functions of chemicals and genes in zebrafish. However, there have not been fluorescent probes that can detect mitochondrial membrane potential in living zebrafish. In this study, we identified a novel cyanine dye called ZMJ214 that detects mitochondrial membrane potential in living zebrafish from 4 to 8 days post fertilization and is administered by simple immersion. The fluorescence intensity of ZMJ214 in zebrafish was increased and decreased by oligomycin and FCCP, respectively, suggesting a positive correlation between ZMJ214 fluorescence and mitochondrial membrane potential. In vivo imaging of zebrafish stained with ZMJ214 allowed for the detection of altered mitochondrial membrane potential induced by the antidiabetic drug troglitazone and the antiepileptic drug tolcapone, both of which have been withdrawn from the market due to mitochondrial toxicity. In contrast, pioglitazone and entacapone, which are similar to troglitazone and tolcapone, respectively, and have been used commercially, did not cause a change in mitochondrial membrane potential in zebrafish stained with ZMJ214. Live imaging of zebrafish stained with ZMJ214 also revealed that knock-down of slc25a12, a mitochondrial carrier protein associated with autism, dysregulated the mitochondrial membrane potential. These results suggest that ZMJ214 can be a useful tool to identify chemicals and genes that cause mitochondrial dysfunction in vivo.

Published
2015

16. Using zebrafish in systems toxicology for developmental toxicity testing

Author

Yuhei, Nishimura, Atsuto, Inoue, Shota, Sasagawa, Junko, Koiwa, Koki, Kawaguchi, Reiko, Kawase, Toru, Maruyama, Soonih, Kim, and Toshio, Tanaka

Subjects
Embryo, Nonmammalian, Teratogens, Toxicity Tests, Animals, Embryonic Development, Humans, Zebrafish
Abstract

With the high cost and the long-term assessment of developmental toxicity testing in mammals, the vertebrate zebrafish has become a useful alternative model organism for high-throughput developmental toxicity testing. Zebrafish is also very favorable for the 3R perspective in toxicology; however, the methodologies used by research groups vary greatly, posing considerable challenges to integrative analysis. In this review, we discuss zebrafish developmental toxicity testing, focusing on the methods of chemical exposure, the assessment of morphological abnormalities, housing conditions and their effects on the production of healthy embryos, and future directions. Zebrafish as a systems toxicology model has the potential to elucidate developmental toxicity pathways, and to provide a sound basis for human health risk assessments.

Published
2015

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