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42 results on '"Yuki Miyasaka"'

1. Muscle-specific lack of Gfpt1 triggers ER stress to alleviate misfolded protein accumulation

Author

Ruchen Zhang, Paniz Farshadyeganeh, Bisei Ohkawara, Kazuki Nakajima, Jun-ichi Takeda, Mikako Ito, Shaochuan Zhang, Yuki Miyasaka, Tamio Ohno, Madoka Mori-Yoshimura, Akio Masuda, and Kinji Ohno

Subjects
glutamine fructose-6-phosphate transaminase 1 (gfpt1), congenital myasthenic syndrome (cms), neuromuscular junction (nmj), hexosamine biosynthesis pathway (hbp), endoplasmic reticulum (er) stress, unfolded protein response (upr), Medicine, Pathology, RB1-214
Published
2024
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2. C3H/HeNSlc mouse with low phospholipid transfer protein expression showed dyslipidemia

Author

Misato Kobayashi, Fumi Kanbe, Reika Ishii, Hiroki Tsubouchi, Kana Hirai, Yuki Miyasaka, Tamio Ohno, Hiroaki Oda, Saiko Ikeda, Hirokazu Katoh, Kenji Ichiyanagi, Akira Ishikawa, Atsushi Murai, and Fumihiko Horio

Subjects
Medicine, Science
Abstract

Abstract High serum levels of triglycerides (TG) and low levels of high-density lipoprotein cholesterol (HDL-C) increase the risk of coronary heart disease in humans. Herein, we first reported that the C3H/HeNSlc (C3H-S) mouse, a C3H/HeN-derived substrain, is a novel model for dyslipidemia. C3H-S showed hypertriglyceridemia and low total cholesterol (TC), HDL-C, and phospholipid (PL) concentrations. To identify the gene locus causing dyslipidemia in C3H-S, we performed genetic analysis. In F2 intercrosses between C3H-S mice and strains with normal serum lipids, the locus associated with serum lipids was identified as 163–168 Mb on chromosome 2. The phospholipid transfer protein (Pltp) gene was a candidate gene within this locus. Pltp expression and serum PLTP activity were markedly lower in C3H-S mice. Pltp expression was negatively correlated with serum TG and positively correlated with serum TC and HDL-C in F2 mice. Genome sequencing analysis revealed that an endogenous retrovirus (ERV) sequence called intracisternal A particle was inserted into intron 12 of Pltp in C3H-S. These results suggest that ERV insertion within Pltp causes aberrant splicing, leading to reduced Pltp expression in C3H-S. This study demonstrated the contribution of C3H-S to our understanding of the relationship between TG, TC, and PL metabolism via PLTP.

Published
2023
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3. Splicing regulation of GFPT1 muscle-specific isoform and its roles in glucose metabolisms and neuromuscular junction

Author

Paniz Farshadyeganeh, Mohammad Nazim, Ruchen Zhang, Bisei Ohkawara, Kazuki Nakajima, Mohammad Alinoor Rahman, Farhana Nasrin, Mikako Ito, Jun-ichi Takeda, Kenji Ohe, Yuki Miyasaka, Tamio Ohno, Akio Masuda, and Kinji Ohno

Subjects
Biological sciences, Biochemistry, Physiology, Science
Abstract

Summary: Glutamine:fructose-6-phosphate transaminase 1 (GFPT1) is the rate-limiting enzyme of the hexosamine biosynthetic pathway (HBP). A 54-bp exon 9 of GFPT1 is specifically included in skeletal and cardiac muscles to generate a long isoform of GFPT1 (GFPT1-L). We showed that SRSF1 and Rbfox1/2 cooperatively enhance, and hnRNP H/F suppresses, the inclusion of human GFPT1 exon 9 by modulating recruitment of U1 snRNP. Knockout (KO) of GFPT1-L in skeletal muscle markedly increased the amounts of GFPT1 and UDP-HexNAc, which subsequently suppressed the glycolytic pathway. Aged KO mice showed impaired insulin-mediated glucose uptake, as well as muscle weakness and fatigue likely due to abnormal formation and maintenance of the neuromuscular junction. Taken together, GFPT1-L is likely to be acquired in evolution in mammalian striated muscles to attenuate the HBP for efficient glycolytic energy production, insulin-mediated glucose uptake, and the formation and maintenance of the neuromuscular junction.

Published
2023
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4. UVB-Induced Skin Autoinflammation Due to Nlrp1b Mutation and Its Inhibition by Anti-IL-1β Antibody

Author

Yuya Murase, Takuya Takeichi, Jun Koseki, Yuki Miyasaka, Yoshinao Muro, Tamio Ohno, Teppei Shimamura, and Masashi Akiyama

Subjects
NLRP1, NLRP1B, inflammasome, UVB, IL-1β, IL-18, Immunologic diseases. Allergy, RC581-607
Abstract

NLRP1 (NACHT and leucine-rich repeat-containing protein family, pyrin domain-containing protein 1) is an innate immune sensor that is involved in the formation of inflammasome complexes. NLRP1 hyperactivity has been reported to cause inherited autoinflammatory diseases including familial keratosis lichenoides chronica and NLRP1-associated autoinflammation with arthritis and dyskeratosis. We generated Nlrp1b (the mouse homologue of human NLRP1) gain-of-function knock-in (Nlrp1b KI) mice with UVB irradiation-induced autoinflammatory skin lesions. We demonstrated that UVB irradiation induces IL-1β upregulation and IL-1β-dependent inflammation via caspase-1 activation in these Nlrp1b KI mice. RNA sequencing revealed the upregulation of inflammasome pathway-related genes, keratinocyte stress marker genes, and keratinocyte differentiation marker genes in the Nlrp1b KI mice after UVB irradiation. The skin inflammation and hyperkeratosis from UVB irradiation in the Nlrp1b KI mice were inhibited by both intraperitoneal and subcutaneous administration of anti-IL-1β antibodies before UVB irradiation. UVB irradiation and the IL-1β pathway are important in the pathogenesis of NLRP1-associated autoinflammatory skin lesions.

Published
2022
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5. Autoinflammatory Keratinization Disease With Hepatitis and Autism Reveals Roles for JAK1 Kinase Hyperactivity in Autoinflammation

Author

Takuya Takeichi, John Y. W. Lee, Yusuke Okuno, Yuki Miyasaka, Yuya Murase, Takenori Yoshikawa, Kana Tanahashi, Emi Nishida, Tatsuya Okamoto, Komei Ito, Yoshinao Muro, Kazumitsu Sugiura, Tamio Ohno, John A. McGrath, and Masashi Akiyama

Subjects
inflammation, brain, liver, skin, STAT, Immunologic diseases. Allergy, RC581-607
Abstract

Heterozygous mutations in JAK1 which result in JAK-STAT hyperactivity have been implicated in an autosomal dominant disorder that features multi-organ immune dysregulation. This study identifies another previously unreported heterozygous missense JAK1 mutation, H596D, in an individual with a unique autoinflammatory keratinization disease associated with early-onset liver dysfunction and autism. Using CRISPR-Cas9 gene targeting, we generated mice with an identical Jak1 knock-in missense mutation (Jak1H595D/+;I596I/+;Y597Y/+ mice) that recapitulated key aspects of the human phenotype. RNA sequencing of samples isolated from the Jak1H595D/+;I596I/+;Y597Y/+ mice revealed the upregulation of genes associated with the hyperactivation of tyrosine kinases and NF-κB signaling. Interestingly, there was a strong correlation between genes downregulated in Jak1H595D/+;I596I/+;Y597Y/+ mice and those downregulated in the brain of model mice with 22q11.2 deletion syndrome that showed cognitive and behavioral deficits, such as autism spectrum disorders. Our findings expand the phenotypic spectrum of JAK1-associated disease and underscore how JAK1 dysfunction contributes to this autoinflammatory disorder.

Published
2022
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6. Two Loci Contribute to Age-Related Hearing Loss Resistance in the Japanese Wild-Derived Inbred MSM/Ms Mice

Author

Shumpei P. Yasuda, Yuki Miyasaka, Xuehan Hou, Yo Obara, Hiroshi Shitara, Yuta Seki, Kunie Matsuoka, Ai Takahashi, Eri Wakai, Hiroshi Hibino, Toyoyuki Takada, Toshihiko Shiroishi, Ryo Kominami, and Yoshiaki Kikkawa

Subjects
age-related hearing loss, C57BL/6J strain, MSM/Ms strain, consomic strain, congenic strain, ahl loci, Biology (General), QH301-705.5
Abstract

An MSM/Ms strain was established using Japanese wild mice, which exhibit resistance to several phenotypes associated with aging, such as obesity, inflammation, and tumorigenesis, compared to common inbred mouse strains. MSM/Ms strain is resistant to age-related hearing loss, and their auditory abilities are sustained for long durations. The age-related hearing loss 3 (ahl3) locus contributes to age-related hearing in MSM/Ms strain. We generated ahl3 congenic strains by transferring a genomic region on chromosome 17 from MSM/Ms mice into C57BL/6J mice. Although C57BL/6J mice develop age-related hearing loss because of the ahl allele of the cadherin 23 gene, the development of middle- to high-frequency hearing loss was significantly delayed in an ahl3 congenic strain. Moreover, the novel age-related hearing loss 10 (ahl10) locus associated with age-related hearing resistance in MSM/Ms strain was mapped to chromosome 12. Although the resistance effects in ahl10 congenic strain were slightly weaker than those in ahl3 congenic strain, slow progression of age-related hearing loss was confirmed in ahl10 congenic strain despite harboring the ahl allele of cadherin 23. These results suggest that causative genes and polymorphisms of the ahl3 and ahl10 loci are important targets for the prevention and treatment of age-related hearing loss.

Published
2022
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7. Ablation of Iah1, a candidate gene for diet-induced fatty liver, does not affect liver lipid accumulation in mice.

Author

Tomomi Masuya, Miyako Suzuki, Junko Tsujimura, Shinsaku Kanamori, Yuki Miyasaka, Tamio Ohno, Atsushi Murai, Fumihiko Horio, and Misato Kobayashi

Subjects
Medicine, Science
Abstract

Nonalcoholic fatty liver disease (NAFLD) is a pathological condition caused by excess triglyceride deposition in the liver. The SMXA-5 severe fatty liver mouse model has been established from the SM/J and A/J strains. To explore the genetic factors involved in fatty liver development in SMXA-5 mice, we had previously performed quantitative trait locus (QTL) analysis, using (SM/J×SMXA-5)F2 intercross mice, and identified Fl1sa on chromosome 12 (centromere-53.06 Mb) as a significant QTL for fatty liver. Furthermore, isoamyl acetate-hydrolyzing esterase 1 homolog (Iah1) was selected as the most likely candidate gene for Fl1sa. Iah1 gene expression in fatty liver-resistant A/J-12SM mice was significantly higher than in fatty liver-susceptible A/J mice. These data indicated that the Iah1 gene might be associated with fatty liver development. However, the function of murine Iah1 remains unknown. Therefore, in this study, we created Iah1 knockout (KO) mice with two different backgrounds [C57BL/6N (B6) and A/J-12SM (A12)] to investigate the relationship between Iah1 and liver lipid accumulation. Liver triglyceride accumulation in Iah1-KO mice of B6 or A12 background did not differ from their respective Iah1-wild type mice under a high-fat diet. These results indicated that loss of Iah1 did not contribute to fatty liver. On the other hands, adipose tissue dysfunction causes lipid accumulation in ectopic tissues (liver, skeletal muscle, and pancreas). To investigate the effect of Iah1 deficiency on white adipose tissue, we performed DNA microarray analysis of epididymal fat in Iah1-KO mice of A12 background. This result showed that Iah1 deficiency might decrease adipokines Sfrp4 and Metrnl gene expression in epididymal fat. This study demonstrated that Iah1 deficiency did not cause liver lipid accumulation and that Iah1 was not a suitable candidate gene for Fl1sa.

Published
2020
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8. A novel splice site mutation of myosin VI in mice leads to stereociliary fusion caused by disruption of actin networks in the apical region of inner ear hair cells.

Author

Yuta Seki, Yuki Miyasaka, Sari Suzuki, Kenta Wada, Shumpei P Yasuda, Kunie Matsuoka, Yasuhiro Ohshiba, Kentaro Endo, Rie Ishii, Hiroshi Shitara, Shin-Ichiro Kitajiri, Naomi Nakagata, Hirohide Takebayashi, and Yoshiaki Kikkawa

Subjects
Medicine, Science
Abstract

An unconventional myosin encoded by the myosin VI gene (MYO6) contributes to hearing loss in humans. Homozygous mutations of MYO6 result in nonsyndromic profound congenital hearing loss, DFNB37. Kumamoto shaker/waltzer (ksv) mice harbor spontaneous mutations, and homozygous mutants exhibit congenital defects in balance and hearing caused by fusion of the stereocilia. We identified a Myo6c.1381G>A mutation that was found to be a p.E461K mutation leading to alternative splicing errors in Myo6 mRNA in ksv mutants. An analysis of the mRNA and protein expression in animals harboring this mutation suggested that most of the abnormal alternatively spliced isoforms of MYO6 are degraded in ksv mice. In the hair cells of ksv/ksv homozygotes, the MYO6 protein levels were significantly decreased in the cytoplasm, including in the cuticular plates. MYO6 and stereociliary taper-specific proteins were mislocalized along the entire length of the stereocilia of ksv/ksv mice, thus suggesting that MYO6 attached to taper-specific proteins at the stereociliary base. Histological analysis of the cochlear hair cells showed that the stereociliary fusion in the ksv/ksv mutants, developed through fusion between stereociliary bundles, raised cuticular plate membranes in the cochlear hair cells and resulted in incorporation of the bundles into the sheaths of the cuticular plates. Interestingly, the expression of the stereociliary rootlet-specific TRIO and F-actin binding protein (TRIOBP) was altered in ksv/ksv mice. The abnormal expression of TRIOBP suggested that the rootlets in the hair cells of ksv/ksv mice had excessive growth. Hence, these data indicated that decreased MYO6 levels in ksv/ksv mutants disrupt actin networks in the apical region of hair cells, thereby maintaining the normal structure of the cuticular plates and rootlets, and additionally provided a cellular basis for stereociliary fusion in Myo6 mutants.

Published
2017
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11. Characterization and alteration of product specificity of Beijerinckia indica subsp. indica β-fructosyltransferase.

Author

Ding Li, Yuki Miyasaka, Arisa Kubota, Takuma Kozono, Yoshikazu Kitano, Nobumitsu Sasaki, Tadashi Fujii, Takumi Tochio, Yoshihiro Kadota, Atsushi Nishikawa, and Takashi Tonozuka

Subjects
*NUCLEAR magnetic resonance spectroscopy, *HIGH performance liquid chromatography, *SUCROSE
Abstract

The trisaccharide 1-kestose, a major constituent of fructooligosaccharide, has strong prebiotic effects. We used high-performance liquid chromatography and 1H nuclear magnetic resonance spectroscopy to show that BiBftA, a β-fructosyltransferase belonging to glycoside hydrolase family 68, from Beijerinckia indica subsp. indica catalyzes transfructosylation of sucrose to produce mostly 1-kestose and levan polysaccharides. We substituted His395 and Phe473 in BiBftA with Arg and Tyr, respectively, and analyzed the reactions of the mutant enzymes with 180 g/L sucrose. The ratio of the molar concentrations of glucose and 1-kestose in the reaction mixture with wild-type BiBftA was 100:8.1, whereas that in the reaction mixture with the variant H395R/F473Y was 100:45.5, indicating that H395R/F473Y predominantly accumulated 1-kestose from sucrose. The X-ray crystal structure of H395R/F473Y suggests that its catalytic pocket is unfavorable for binding of sucrose while favorable for transfructosylation. BiBftA catalyzed transfructosylation of sucrose to produce 1-kestose, and H395R/F473Y variant predominantly accumulated 1-kestose. [ABSTRACT FROM AUTHOR]

Published
2023
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12. A novel model mouse for type 2 diabetes mellitus with early onset and persistent hyperglycemia

Author

Tamio, Ohno, Yuki, Miyasaka, Kanta, Yoshida, Misato, Kobayashi, Fumihiko, Horio, Norihide, Yokoi, Masashi, Mizuno, and Hiroshi, Ikegami

Subjects
Male, Blood Glucose, General Veterinary, General Medicine, General Biochemistry, Genetics and Molecular Biology, Mice, Diabetes Mellitus, Type 2, Hyperglycemia, Glucose Intolerance, Diabetes Mellitus, Animals, Insulin, Female, Animal Science and Zoology, Obesity
Abstract

Various mouse models of type 2 diabetes have been established, but few of these show early onset and persistent hyperglycemia. We have established a congenic mouse strain (NSY.B6-Tyr

Published
2022

14. IL-17 axis is a significant driver of skin inflammation in Card14 mutant pityriasis rubra pilaris model mice

Author

Takenori Yoshikawa, Takuya Takeichi, Tetsuya Hirabayashi, Yoshinao Muro, Yuki Miyasaka, Tamio Ohno, and Masashi Akiyama

Abstract

Pityriasis rubra pilaris (PRP) is a rare inflammatory keratinization disorder with perifollicular erythema, and most autosomal dominant familial cases of atypical juvenile (type V) PRP are caused by gain-of-function mutations in CARD14, which encodes caspase recruitment domain-containing protein 14 (CARD14). We report the first mouse model of PRP to carry a homozygous knock-in mutation, c.380G>C (p.Cys127Ser) corresponding to a PRP-causative human mutation, in CARD14. The Card14C127S/C127S knock-in mice recapitulate key aspects of human PRP, including hair follicle dilatation, follicular plugs, and palmoplantar hyperkeratosis, and show skin barrier dysfunction, the hyperactivation of innate immunity via the IL-36 signaling and inflammasome pathways, and the excessive activation of the IL-17 axis in the outer root sheath and interfollicular epidermis. Administering anti-IL-17A neutralizing antibody significantly attenuates the skin symptoms in mutant mice. Thus, this knock-in mouse is a valid model for further evaluating early events in the PRP pathogenesis and for developing PRP therapies.

Published
2023

15. Role of an Atypical Cadherin Gene, Cdh23 in Prepulse Inhibition, and Implication of CDH23 in Schizophrenia

Author

Yoshiaki Kikkawa, Chie Shimamoto-Mitsuyama, Motoko Maekawa, Shabeesh Balan, Tetsuro Ohmori, Hisako Ohba, Akiko Watanabe, Tomomi Shimogori, Tetsuo Ohnishi, Takeo Yoshikawa, Shusuke Numata, Yoshimi Iwayama, Tomoko Toyota, Manabu Toyoshima, Yasuko Hisano, Takeshi Hayashi, Yuki Miyasaka, and Tomonori Hara

Subjects
Candidate gene, AcademicSubjects/MED00810, Quantitative Trait Loci, Cadherin Related Proteins, Biology, Quantitative trait locus, 03 medical and health sciences, Mice, 0302 clinical medicine, CDH23, quantitative trait locus, Inbred strain, otorhinolaryngologic diseases, Animals, Humans, Allele, Prepulse inhibition, Alleles, 030304 developmental biology, hearing loss, Genetics, 0303 health sciences, prepulse inhibition, FABP7, Cdh23 (CDH23), Cadherins, schizophrenia, Psychiatry and Mental health, Endophenotype, 030217 neurology & neurosurgery, Regular Articles
Abstract

We previously identified quantitative trait loci (QTL) for prepulse inhibition (PPI), an endophenotype of schizophrenia, on mouse chromosome 10 and reported Fabp7 as a candidate gene from an analysis of F2 mice from inbred strains with high (C57BL/6N; B6) and low (C3H/HeN; C3H) PPI levels. Here, we reanalyzed the previously reported QTLs with increased marker density. The highest logarithm of odds score (26.66) peaked at a synonymous coding and splice-site variant, c.753G>A (rs257098870), in the Cdh23 gene on chromosome 10; the c.753G (C3H) allele showed a PPI-lowering effect. Bayesian multiple QTL mapping also supported the same variant with a posterior probability of 1. Thus, we engineered the c.753G (C3H) allele into the B6 genetic background, which led to dampened PPI. We also revealed an e-QTL (expression QTL) effect imparted by the c.753G>A variant for the Cdh23 expression in the brain. In a human study, a homologous variant (c.753G>A; rs769896655) in CDH23 showed a nominally significant enrichment in individuals with schizophrenia. We also identified multiple potentially deleterious CDH23 variants in individuals with schizophrenia. Collectively, the present study reveals a PPI-regulating Cdh23 variant and a possible contribution of CDH23 to schizophrenia susceptibility.

Published
2021

17. Structural basis for proteolytic processing of Aspergillus sojae α-glucosidase L with strong transglucosylation activity

Author

Yifu Ding, Ayako Oyagi, Yuki Miyasaka, Takuma Kozono, Nobumitsu Sasaki, Yuka Kojima, Makoto Yoshida, Yuji Matsumoto, Nozomu Yasutake, Atsushi Nishikawa, and Takashi Tonozuka

Subjects
Aspergillus, Structural Biology, Catalytic Domain, alpha-Glucosidases, Substrate Specificity
Abstract

An α-glucosidase from Aspergillus sojae, AsojAgdL, exhibits strong transglucosylation activity to produce α-1,6-glucosidic linkages. The most remarkable structural feature of AsojAgdL is that residues 457-560 of AsojAgdL (designated the NC sequence) is not conserved in other glycoside hydrolase family 31 enzymes, and part of this NC sequence is proteolytically cleaved during its maturation. In this study, the enzyme was expressed in Pichia pastoris, and electrophoretic analysis indicated that the recombinant enzyme, rAsojAgdL, consisted of two polypeptide chains, as observed in the case of the enzyme produced in an Aspergillus strain. The crystal structure of rAsojAgdL was determined in complex with the substrate analog trehalose. Electron density corresponding to residues 496-515 of the NC sequence was not seen, and there were no α-helices or β-strands except for a short α-helix in the structures of residues 457-495 and residues 516-560, both of which belong to the NC sequence. The residues 457-495 and the residues 516-560 both formed extra components of the catalytic domain. The residues 457-495 constituted the entrance of the catalytic pocket of rAsojAgdL, and Gly467, Asp468, Pro469, and Pro470 in the NC sequence were located within 4 Å of Trp400, a key residue involved in binding of the substrate. The results suggest that the proteolytic processing of the NC sequence is related to the formation of the catalytic pocket of AsojAgdL.

Published
2022

18. SDR9C7 catalyzes critical dehydrogenation of acylceramides for skin barrier formation

Author

Kana Tanahashi, Akane Kawamoto, Yusuke Okuno, William E. Boeglin, Yoshinao Muro, Chiaki Murase, Alan R. Brash, S. Taguchi, Junko Ishikawa, Tamio Ohno, Hiroyuki Takama, Michihiro Kono, Masashi Akiyama, Calcutt Mw, Yuki Miyasaka, Takuya Takeichi, Daisuke Watanabe, K. Tanaka, and Tetsuya Hirabayashi

Subjects
0301 basic medicine, Ceramide, Plasma protein binding, Reductase, Ceramides, Catalysis, Mice, 03 medical and health sciences, Lipoxygenase, chemistry.chemical_compound, 0302 clinical medicine, Stratum corneum, medicine, Animals, Humans, Mice, Knockout, Corneocyte, biology, Chemistry, Ichthyosis, Genetic Diseases, Inborn, General Medicine, medicine.disease, Disease Models, Animal, 030104 developmental biology, medicine.anatomical_structure, Biochemistry, 030220 oncology & carcinogenesis, biology.protein, NAD+ kinase, Epidermis, Oxidoreductases, Research Article
Abstract

The corneocyte lipid envelope, composed of covalently bound ceramides and fatty acids, is important to the integrity of the permeability barrier in the stratum corneum, and its absence is a prime structural defect in various skin diseases associated with defective skin barrier function. SDR9C7 encodes a short-chain dehydrogenase/reductase family 9C member 7 (SDR9C7) recently found mutated in ichthyosis. In a patient with SDR9C7 mutation and a mouse Sdr9c7-KO model, we show loss of covalent binding of epidermal ceramides to protein, a structural fault in the barrier. For reasons unresolved, protein binding requires lipoxygenase-catalyzed transformations of linoleic acid (18:2) esterified in ω-O-acylceramides. In Sdr9c7(–/–) epidermis, quantitative liquid chromatography–mass spectometry (LC-MS) assays revealed almost complete loss of a species of ω-O-acylceramide esterified with linoleate-9,10-trans-epoxy-11E-13-ketone; other acylceramides related to the lipoxygenase pathway were in higher abundance. Recombinant SDR9C7 catalyzed NAD(+)-dependent dehydrogenation of linoleate 9,10-trans-epoxy-11E-13-alcohol to the corresponding 13-ketone, while ichthyosis mutants were inactive. We propose, therefore, that the critical requirement for lipoxygenases and SDR9C7 is in producing acylceramide containing the 9,10-epoxy-11E-13-ketone, a reactive moiety known for its nonenzymatic coupling to protein. This suggests a mechanism for coupling of ceramide to protein and provides important insights into skin barrier formation and pathogenesis.

Published
2020

19. A case of tracheal pleomorphic adenoma misdiagnosed as asthma

Author

Yuki Miyasaka, Satsuki Miyajima, Kentaro Kodama, Hiroki Takahashi, Tetsuya Taya, Kimiyuki Ikeda, Hirofumi Chiba, Mamoru Takahashi, Yuki Mori, Takahumi Yorozuya, and Takumi Yoshikawa

Subjects
medicine.medical_specialty, Stridor, Case Report, Microbiology, Pulmonary function testing, flow–volume curve, Pleomorphic adenoma, 03 medical and health sciences, 0302 clinical medicine, medicine, Subglottis, Suspected asthma, Asthma, business.industry, asthma, Airway obstruction, medicine.disease, stridor, Infectious Diseases, Tracheal tumor, 030228 respiratory system, tracheal pleomorphic adenoma, 030220 oncology & carcinogenesis, Parasitology, Radiology, medicine.symptom, business
Abstract

A 51-year-old woman had an incidental finding of a tracheal tumor during oesophagogastroduodenoscopy following the diagnosis of asthma for 2 months. A computed tomography scan revealed a 15-mm tumor in the subglottis. Endoscopic resection was performed safely, and pleomorphic adenoma was diagnosed histologically. The patient’s condition was satisfactory 30 months after the procedure. Tracheal pleomorphic adenoma is rare and may be misdiagnosed as asthma. If the tumor is large, surgery may be required; however, endoscopic polypectomy may be effective if the tumor is small. Therefore, early diagnosis of tracheal pleomorphic adenoma is important. At the first visit, the flow–volume curve suggested upper airway obstruction, which should have raised the suspicion of an upper airway obstruction. In patients with suspected asthma, early pulmonary function testing is needed to substantiate asthma diagnosis and prevent an alternative diagnosis being missed.

Published
2019

20. OHC-TRECK: A Novel System Using a Mouse Model for Investigation of the Molecular Mechanisms Associated with Outer Hair Cell Death in the Inner Ear

Author

Hiroshi Shitara, Yuki Miyasaka, Yasumasa Nishito, Shumpei P. Yasuda, Kunie Matsuoka, Kenta Wada, Choji Taya, Yuta Seki, Yoshiaki Kikkawa, and Hiromichi Yonekawa

Subjects
0301 basic medicine, lcsh:Medicine, Biology, Article, 03 medical and health sciences, 0302 clinical medicine, Immune system, Downregulation and upregulation, medicine, otorhinolaryngologic diseases, Animals, Diphtheria Toxin, Inner ear, Hearing Loss, Receptor, Prestin, lcsh:Science, Cochlea, Vestibular system, Multidisciplinary, Molecular Motor Proteins, lcsh:R, Immunohistochemistry, Cell biology, Mice, Inbred C57BL, Disease Models, Animal, Hair Cells, Auditory, Outer, 030104 developmental biology, medicine.anatomical_structure, biology.protein, lcsh:Q, Hair cell, sense organs, 030217 neurology & neurosurgery
Abstract

Outer hair cells (OHCs) are responsible for the amplification of sound, and the death of these cells leads to hearing loss. Although the mechanisms for sound amplification and OHC death have been well investigated, the effects on the cochlea after OHC death are poorly understood. To study the consequences of OHC death, we established an OHC knockout system using a novel mouse model, Prestin-hDTR, which uses the prestin promoter to express the human diphtheria toxin (DT) receptor gene (hDTR). Administration of DT to adult Prestin-hDTR mice results in the depletion of almost all OHCs without significant damage to other cochlear and vestibular cells, suggesting that this system is an effective tool for the analysis of how other cells in the cochlea and vestibula are affected after OHC death. To evaluate the changes in the cochlea after OHC death, we performed differential gene expression analysis between the untreated and DT-treated groups of wild-type and Prestin-hDTR mice. This analysis revealed that genes associated with inflammatory/immune responses were significantly upregulated. Moreover, we found that several genes linked to hearing loss were strongly downregulated by OHC death. Together, these results suggest that this OHC knockout system is a useful tool to identify biomarkers associated with OHC death.

Published
2019

21. Role of an Atypical Cadherin Gene, Cdh23 in Prepulse Inhibition and Implication of CDH23 in Schizophrenia

Author

Takeshi Hayashi, Tetsuro Ohmori, Yoshiaki Kikkawa, Tetsuo Ohnishi, Shusuke Numata, Yasuko Hisano, Takeo Yoshikawa, Shabeesh Balan, Tomomi Shimogori, Akiko Watanabe, Manabu Toyoshima, Yoshimi Iwayama, Yuki Miyasaka, Tomonori Hara, Tomoko Toyota, Hisako Ohba, Chie Shimamoto-Mitsuyama, and Motoko Maekawa

Subjects
Genetics, Candidate gene, CDH23, Inbred strain, Endophenotype, FABP7, Quantitative trait locus, Allele, Biology, Prepulse inhibition
Abstract

We previously identified quantitative trait loci (QTL) for prepulse inhibition (PPI), an endophenotype of schizophrenia, on mouse chromosome 10 and reported Fabp7 as a candidate gene from an analysis of F2 mice from inbred strains with high (C57BL/6N; B6) and low (C3H/HeN; C3H) PPI levels. Here, we reanalyzed the previously reported QTLs with increased marker density. The highest LOD score (26.66) peaked at a synonymous coding and splice-site variant, c.753G>A (rs257098870), in the Cdh23 gene on chromosome 10; the c.753G (C3H) allele showed a PPI-lowering effect. Bayesian multiple QTL mapping also supported the same variant with a posterior probability of 1. Thus, we engineered the c.753G (C3H) allele into the B6 genetic background, which led to dampened PPI. We also revealed an e-QTL (expression-QTL) effect imparted by the c.753G>A variant for the Cdh23 expression in the brain. In a human study, a homologous variant (c.753G>A; rs769896655) in CDH23 showed a nominally significant enrichment in individuals with schizophrenia. We also identified multiple potentially deleterious CDH23 variants in individuals with schizophrenia. Collectively, the present study reveals a PPI-regulating Cdh23 variant and a possible contribution of CDH23 to schizophrenia susceptibility.

Published
2020

22. Ablation of Iah1, a candidate gene for diet-induced fatty liver, does not affect liver lipid accumulation in mice

Author

Fumihiko Horio, Tamio Ohno, Atsushi Murai, Junko Tsujimura, Misato Kobayashi, Shinsaku Kanamori, Miyako Suzuki, Yuki Miyasaka, and Tomomi Masuya

Subjects
0301 basic medicine, Male, Candidate gene, Adipose tissue, Gene Expression, White adipose tissue, Biochemistry, Fats, chemistry.chemical_compound, 0302 clinical medicine, Non-alcoholic Fatty Liver Disease, Nonalcoholic fatty liver disease, Medicine and Health Sciences, Adiposity, Regulation of gene expression, Epididymis, Mice, Knockout, Multidisciplinary, Liver Diseases, Fatty liver, Animal Models, Lipids, Cholesterol, Adipose Tissue, Experimental Organism Systems, 030220 oncology & carcinogenesis, Medicine, Anatomy, Research Article, medicine.medical_specialty, Science, Mouse Models, Gastroenterology and Hepatology, Biology, Diet, High-Fat, Research and Analysis Methods, Gene Expression Regulation, Enzymologic, 03 medical and health sciences, Model Organisms, Internal medicine, medicine, Genetics, Animals, RNA, Messenger, Triglycerides, Nutrition, Triglyceride, Body Weight, Biology and Life Sciences, Lipid metabolism, medicine.disease, Lipid Metabolism, Diet, Mice, Inbred C57BL, Fatty Liver, 030104 developmental biology, Endocrinology, Biological Tissue, Metabolism, chemistry, Animal Studies, Carboxylic Ester Hydrolases, Gene Deletion
Abstract

Nonalcoholic fatty liver disease (NAFLD) is a pathological condition caused by excess triglyceride deposition in the liver. The SMXA-5 severe fatty liver mouse model has been established from the SM/J and A/J strains. To explore the genetic factors involved in fatty liver development in SMXA-5 mice, we had previously performed quantitative trait locus (QTL) analysis, using (SM/J×SMXA-5)F2 intercross mice, and identified Fl1sa on chromosome 12 (centromere-53.06 Mb) as a significant QTL for fatty liver. Furthermore, isoamyl acetate-hydrolyzing esterase 1 homolog (Iah1) was selected as the most likely candidate gene for Fl1sa. Iah1 gene expression in fatty liver-resistant A/J-12SM mice was significantly higher than in fatty liver-susceptible A/J mice. These data indicated that the Iah1 gene might be associated with fatty liver development. However, the function of murine Iah1 remains unknown. Therefore, in this study, we created Iah1 knockout (KO) mice with two different backgrounds [C57BL/6N (B6) and A/J-12SM (A12)] to investigate the relationship between Iah1 and liver lipid accumulation. Liver triglyceride accumulation in Iah1-KO mice of B6 or A12 background did not differ from their respective Iah1-wild type mice under a high-fat diet. These results indicated that loss of Iah1 did not contribute to fatty liver. On the other hands, adipose tissue dysfunction causes lipid accumulation in ectopic tissues (liver, skeletal muscle, and pancreas). To investigate the effect of Iah1 deficiency on white adipose tissue, we performed DNA microarray analysis of epididymal fat in Iah1-KO mice of A12 background. This result showed that Iah1 deficiency might decrease adipokines Sfrp4 and Metrnl gene expression in epididymal fat. This study demonstrated that Iah1 deficiency did not cause liver lipid accumulation and that Iah1 was not a suitable candidate gene for Fl1sa.

Published
2020

23. Intestinal immunity suppresses carrying capacity of rats for the model tapeworm, Hymenolepis diminuta

Author

Tamio Ohno, Akira Ishih, Hideto Kino, Takuya Kai, Yuki Miyasaka, and Haruhiko Maruyama

Subjects
0301 basic medicine, Hymenolepiasis, T-Lymphocytes, T cell, Intestinal immunity, Carrying capacity, X-Linked Combined Immunodeficiency Diseases, Rat Small Intestine, Host-Parasite Interactions, Microbiology, Rats, Nude, 03 medical and health sciences, Immune system, Intestine, Small, parasitic diseases, medicine, Animals, Biomass, Mast Cells, Severe combined immunodeficiency, biology, Mast cell deficient rat, Hymenolepis diminuta, biology.organism_classification, medicine.disease, Mast cell, T cell deficiency, Rats, Inbred F344, Rats, Worm biomass, 030104 developmental biology, Infectious Diseases, medicine.anatomical_structure, Parasitology, Immune-deficient rat
Abstract

Hymenolepis diminuta is a parasitic tapeworm of the rat small intestine and is recognized as a useful model for the analysis of cestode-host interactions. In this study, we analyzed factors affecting the biomass of the tapeworm through use of rat strains carrying genetic mutations, namely X-linked severe combined immunodeficiency (xscid; T, B and NK cells deficiency), nude (rnu; T cell deficiency), and mast cell deficient rats. The worm biomass of F344-xscid rats after infection with 5 cysticercoids was much larger than control F344 rats from 3 to 8 weeks. The biomass of F344-rnu rats was also larger than the controls, but was intermediate between F344-xscid and control rats. These observations demonstrated that host immunity can control the maximal tapeworm biomass, i.e., carrying capacity, of the rat small intestine. Both T cell and other immune cells (B and NK cells) have roles in determining the carrying capacity of tapeworms. Total worm biomass and worm numbers in mast cell deficient rats (WsRC-Ws/Ws) were not significantly different from control WsRC-+/+ rats after 3 and 6 weeks of primary infection. Mast cell deficient rats displayed reinfection resistance for worm biomass but not worm expulsion. These findings suggest that the mast cell has a role for controlling the biomass of this tapeworm in reinfection alone, but does not affect the rate of worm expulsion. Overall, our findings indicate that the mast cell is not a major effector cell for the control of the carrying capacity of tapeworms. The identity of the major effector cell remains unknown., ファイル公開:2019-08-01

Published
2018

24. A new missense mutation in the paired domain of the mouse Pax3 gene

Author

Tamio Ohno, Tomoki Maegawa, Hiroto Katoh, Fumihiko Horio, Yuki Miyasaka, Miyako Suzuki, and Misato Kobayashi

Subjects
0301 basic medicine, Genetics, General Veterinary, Point mutation, Mutant, PAX3, Locus (genetics), General Medicine, Biology, musculoskeletal system, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Exon, 030104 developmental biology, Dominant white, embryonic structures, Missense mutation, Animal Science and Zoology, Gene
Abstract

Mice with dominant white spotting occurred spontaneously in the C3.NSY-(D11Mit74-D11Mit229) strain. Linkage analysis indicated that the locus for white spotting was located in the vicinity of the Pax3 gene on chromosome 1. Crosses of white-spotted mice showed that homozygosity for the mutation caused tail and limb abnormalities and embryonic lethality as a result of exencephaly; these phenotypes were analogous to those found in other Pax3 mutants. Sequence analysis identified a missense point mutation (c.101G>A) in exon 2 of Pax3 that resulted in a methionine to isoleucine conversion at amino acid 62 of the PAX3 protein. This mutation site was located in the N-terminal HTH (helix-turn-helix) motif of the paired domain of Pax3, which is necessary for binding to DNA and is highly conserved in vertebrate species. Alteration of DNA binding affinity was responsible for embryonic lethality in homozygotes and white spotting in heterozygotes. We named the mutant allele as Pax3Sp-Nag. The C3H/HeN-Pax3Sp-Nag strain may be useful for analyzing the function of Pax3 as a new model of the human disease, Waardenburg Syndrome.

Published
2017

25. Mouse NC/Jic strain provides novel insights into host genetic factors for malaria research

Author

Miyoko Matsushima, Yoshiaki Kikkawa, Yuki Miyasaka, Masahide Takahashi, Masashi Mizuno, Tsutomu Kawabe, Masako Kuga, Tamio Ohno, and Kaori Ushida

Subjects
0301 basic medicine, Parasitemia, Review, Lung injury, Plasmodium, General Biochemistry, Genetics and Molecular Biology, Host-Parasite Interactions, Pathogenesis, Rodent Diseases, 03 medical and health sciences, Mice, 0302 clinical medicine, Immune system, parasitic diseases, medicine, Animals, rodent Plasmodium parasite, General Veterinary, biology, mouse NC/Jic strain, business.industry, General Medicine, malaria complications, medicine.disease, biology.organism_classification, 3. Good health, Malaria, host susceptibility, Disease Models, Animal, 030104 developmental biology, Cerebral Malaria, Immunology, Animal Science and Zoology, cerebral malaria, business, Nephrotic syndrome, 030217 neurology & neurosurgery
Abstract

Malaria is caused by Plasmodium parasites and is one of the most life-threatening infectious diseases in humans. Infection can result in severe complications such as cerebral malaria, acute lung injury/acute respiratory distress syndrome, and acute renal injury. These complications are mainly caused by P. falciparum infection and are major causes of death associated with malaria. There are a few species of rodent-infective malaria parasites, and mice infected with such parasites are now widely used for screening candidate drugs and vaccines and for studying host immune responses and pathogenesis associated with disease-related complications. We found that mice of the NC/Jic strain infected with rodent malarial parasites exhibit distinctive disease-related complications such as cerebral malaria and nephrotic syndrome, in addition to a rapid increase in parasitemia. Here, we focus on the analysis of host genetic factors that affect malarial pathogenesis and describe the characteristic features, utility, and future prospects for exploitation of the NC/Jic strain as a novel mouse model for malaria research.

Published
2019

26. 116 SDR9C7 catalyzes the critical dehydrogenation of acylceramides for skin barrier formation

Author

K. Tanaka, Alan R. Brash, S. Taguchi, Tamio Ohno, Tetsuya Hirabayashi, Daisuke Watanabe, Yusuke Okuno, Calcutt Mw, Junko Ishikawa, Chiaki Murase, Yoshinao Muro, William E. Boeglin, Hiromichi Takama, Masaharu Akiyama, Takuya Takeichi, Akane Kawamoto, Kana Tanahashi, Yuki Miyasaka, and Michihiro Kono

Subjects
Skin barrier, Chemistry, Dehydrogenation, Cell Biology, Dermatology, Photochemistry, Molecular Biology, Biochemistry
Published
2021

27. c.753A>G genome editing of a Cdh23 allele delays age-related hearing loss and degeneration of cochlear hair cells in C57BL/6J mice

Author

Shumpei P. Yasuda, Kunie Matsuoka, Hiroshi Shitara, Xuehan Hou, Kenta Wada, Yoshiaki Kikkawa, Yuki Miyasaka, Yuta Seki, Sari Suzuki, and Yasuhiro Ohshiba

Subjects
0301 basic medicine, medicine.medical_specialty, Cadherin, Hearing loss, Stereocilia (inner ear), Degeneration (medical), Biology, Phenotype, Sensory Systems, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Endocrinology, CDH23, Internal medicine, otorhinolaryngologic diseases, medicine, Allele, medicine.symptom, Gene, 030217 neurology & neurosurgery
Abstract

C57BL/6J mice have long been studied as a model of age-related hearing loss (ARHL). In C57BL/6J mice, ARHL begins in the high-frequency range at 3 months of age and spreads toward low frequencies by 10 months of age. We previously confirmed that c.753A>G genome editing of an ahl allele (c.753A) in the cadherin 23 gene (Cdh23) suppressed the onset of ARHL until 12 months of age. We further investigated the hearing phenotypes of the original and genome-edited C57BL/6J-Cdh23+/+ (c.753G/G) mice until 24 months of age. The hearing tests revealed that most of the C57BL/6J mice maintained good hearing levels until 14 months of age following genome editing of a Cdh23ahl allele. However, the hearing levels of the C57BL/6J-Cdh23+/+ mice gradually declined, and severe ARHL developed with increasing age. ARHL in the C57BL/6J mice was correlated with degeneration of the stereocilia in cochlear hair cells. The stereocilia degeneration was rescued in the C57BL/6J-Cdh23+/+ mice at 12 months of age, but the stereocilia bundles exhibited abnormal phenotypes similar to those of the original C57BL/6J mice at more advanced ages. Therefore, genome editing of Cdh23ahl did not completely suppress ARHL in C57BL/6J mice. We also compared the hearing levels of C57BL/6J-Cdh23+/+ mice with those of C3H/HeN and MSM/Ms mice, which carry the Cdh23+ allele. The severity and onset patterns of ARHL in the C57BL/6J-Cdh23+/+ mice differed from those observed in other Cdh23+/+ mice. Therefore, we hypothesize that other susceptible and/or resistant alleles of ARHL exist in the genetic backgrounds of these mice.

Published
2020

28. c.753AG genome editing of a Cdh23

Author

Shumpei P, Yasuda, Yuta, Seki, Sari, Suzuki, Yasuhiro, Ohshiba, Xuehan, Hou, Kunie, Matsuoka, Kenta, Wada, Hiroshi, Shitara, Yuki, Miyasaka, and Yoshiaki, Kikkawa

Subjects
Gene Editing, Mice, Inbred C3H, Otoacoustic Emissions, Spontaneous, Age Factors, Auditory Threshold, Mice, Transgenic, Genetic Therapy, Presbycusis, Cadherins, Mice, Inbred C57BL, Disease Models, Animal, Phenotype, Hearing, Hair Cells, Auditory, Mutation, Evoked Potentials, Auditory, Brain Stem, Animals, Genetic Predisposition to Disease
Abstract

C57BL/6J mice have long been studied as a model of age-related hearing loss (ARHL). In C57BL/6J mice, ARHL begins in the high-frequency range at 3 months of age and spreads toward low frequencies by 10 months of age. We previously confirmed that c.753AG genome editing of an ahl allele (c.753A) in the cadherin 23 gene (Cdh23) suppressed the onset of ARHL until 12 months of age. We further investigated the hearing phenotypes of the original and genome-edited C57BL/6J-Cdh23

Published
2018

29. Congenic mapping and candidate gene analysis for streptozotocin-induced diabetes susceptibility locus on mouse chromosome 11

Author

Misato Kobayashi, Tomoki Maegawa, Fumihiko Horio, Hiroshi Ikegami, Tamio Ohno, Masahide Takahashi, Naru Babaya, and Yuki Miyasaka

Subjects
0301 basic medicine, Blood Glucose, Male, Time Factors, endocrine system diseases, DNA repair, Congenic, Locus (genetics), Biology, Streptozocin, Diabetes Mellitus, Experimental, 03 medical and health sciences, symbols.namesake, Mice, Congenic, Genetics, Animals, Insulin, Genetic Predisposition to Disease, streptozotocin-induced diabetes susceptibility locus, Gene, Genetic Association Studies, Sanger sequencing, consomic strain, Chromosome, Chromosome Mapping, Molecular biology, Chromosomes, Mammalian, 030104 developmental biology, A/J mice, DNA glycosylase, Genetic Loci, congenic mapping, N-methylpurine DNA glycosylase gene, symbols, Female, Candidate Gene Analysis
Abstract

Streptozotocin (STZ) has been widely used to induce diabetes in rodents. Strain-dependent variation in susceptibility to STZ has been reported; however, the gene(s) responsible for STZ susceptibility has not been identified. Here, we utilized the A/J-11SM consomic strain and a set of chromosome 11 (Chr. 11) congenic strains developed from A/J-11SM to identify a candidate STZ-induced diabetes susceptibility gene. The A/J strain exhibited significantly higher susceptibility to STZ-induced diabetes than the A/J-11SM strain, confirming the existence of a susceptibility locus on Chr. 11. We named this locus Stzds1 (STZ-induced diabetes susceptibility 1). Congenic mapping using the Chr. 11 congenic strains indicated that the Stzds1 locus was located between D11Mit163 (27.72 Mb) and D11Mit51 (36.39 Mb). The Mpg gene, which encodes N-methylpurine DNA glycosylase (MPG), a ubiquitous DNA repair enzyme responsible for the removal of alkylated base lesions in DNA, is located within the Stzds1 region. There is a close relationship between DNA alkylation at an early stage of STZ action and the function of MPG. A Sanger sequence analysis of the Mpg gene revealed five polymorphic sites in the A/J genome. One variant, p.Ala132Ser, was located in a highly conserved region among rodent species and in the minimal region for retained enzyme activity of MPG. It is likely that structural alteration of MPG caused by the p.Ala132Ser mutation elicits increased recognition and excision of alkylated base lesions in DNA by STZ., ファイル公開:2019/04/01

Published
2018

30. Quantitative trait loci on chromosome 5 for susceptibility to frequency-specific effects on hearing in DBA/2J mice

Author

Yasuhiro Ohshiba, Michinari Yokohama, Choji Taya, Takuya Ueda, Kazuhiro Okumura, Kunie Matsuoka, Sari Suzuki, Yuki Miyasaka, Yoshiaki Kikkawa, and Masashi Ishikawa

Subjects
medicine.medical_specialty, Aging, early-onset hearing loss, quantitative trait loci (QTL), Hearing loss, Original, Quantitative Trait Loci, Biology, Quantitative trait locus, Audiology, DBA/2J, General Biochemistry, Genetics and Molecular Biology, Hearing, Genetic linkage, medicine, otorhinolaryngologic diseases, chromosome 5, Animals, Humans, Genetic Predisposition to Disease, Allele, Hearing Loss, ahllocus, Alleles, Genetics, General Veterinary, Microfilament Proteins, Chromosome, General Medicine, Progressive hearing loss, Cadherins, Mice, Inbred C57BL, Profound hearing loss, Sound, Acoustic Stimulation, Mice, Inbred DBA, Chromosomes, Human, Pair 5, Animal Science and Zoology, medicine.symptom, Carrier Proteins, Lod scores
Abstract

The DBA/2J strain is a model for early-onset, progressive hearing loss in humans, as confirmed in the present study. DBA/2J mice showed progression of hearing loss to low-frequency sounds from ultrasonic-frequency sounds and profound hearing loss at all frequencies before 7 months of age. It is known that the early-onset hearing loss of DBA/2J mice is caused by affects in the ahl (Cdh23(ahl)) and ahl8 (Fscn2(ahl8)) alleles of the cadherin 23 and fascin 2 genes, respectively. Although the strong contributions of the Fscn2(ahl8) allele were detected in hearing loss at 8- and 16-kHz stimuli with LOD scores of 5.02 at 8 kHz and 8.84 at 16 kHz, hearing loss effects were also demonstrated for three new quantitative trait loci (QTLs) for the intervals of 50.3-54.5, 64.6-119.9, and 119.9-137.0 Mb, respectively, on chromosome 5, with significant LOD scores of 2.80-3.91 for specific high-frequency hearing loss at 16 kHz by quantitative trait loci linkage mapping using a (DBA/2J × C57BL/6J) F1 × DBA/2J backcross mice. Moreover, we showed that the contribution of Fscn2(ahl8) to early-onset hearing loss with 32-kHz stimuli is extremely low and raised the possibility of effects from the Cdh23(ahl) allele and another dominant quantitative trait locus (loci) for hearing loss at this ultrasonic frequency. Therefore, our results suggested that frequency-specific QTLs control early-onset hearing loss in DBA/2J mice.

Published
2015

31. Compound Heterozygosity of the Functionally Null Cdh23v-ngt and Hypomorphic Cdh23ahl Alleles Leads to Early-onset Progressive Hearing Loss in Mice

Author

Kei Watanabe, Kunie Matsuoka, Shumpei P. Yasuda, Yoshiaki Kikkawa, Yoshihiko Sagara, Ryo Kominami, Hiromichi Yonekawa, Yuki Miyasaka, Sari Suzuki, Hiroshi Shitara, and Yasuhiro Ohshiba

Subjects
Genetics, General Veterinary, Stereocilia (inner ear), Usher syndrome, General Medicine, Biology, Compound heterozygosity, medicine.disease, Molecular biology, Null allele, eye diseases, General Biochemistry, Genetics and Molecular Biology, medicine.anatomical_structure, CDH23, otorhinolaryngologic diseases, medicine, Animal Science and Zoology, sense organs, Hair cell, Tip link, Vestibular Hair Cell
Abstract

The waltzer (v) mouse mutant harbors a mutation in Cadherin 23 (Cdh23) and is a model for Usher syndrome type 1D, which is characterized by congenital deafness, vestibular dysfunction, and prepubertal onset of progressive retinitis pigmentosa. In mice, functionally null Cdh23 mutations affect stereociliary morphogenesis and the polarity of both cochlear and vestibular hair cells. In contrast, the murine Cdh23(ahl) allele, which harbors a hypomorphic mutation, causes an increase in susceptibility to age-related hearing loss in many inbred strains. We produced congenic mice by crossing mice carrying the v niigata (Cdh23(v-ngt)) null allele with mice carrying the hypomorphic Cdh23(ahl) allele on the C57BL/6J background, and we then analyzed the animals' balance and hearing phenotypes. Although the Cdh23(v-ngt/ahl) compound heterozygous mice exhibited normal vestibular function, their hearing ability was abnormal: the mice exhibited higher thresholds of auditory brainstem response (ABR) and rapid age-dependent elevation of ABR thresholds compared with Cdh23(ahl/ahl) homozygous mice. We found that the stereocilia developed normally but were progressively disrupted in Cdh23(v-ngt/ahl) mice. In hair cells, CDH23 localizes to the tip links of stereocilia, which are thought to gate the mechanoelectrical transduction channels in hair cells. We hypothesize that the reduction of Cdh23 gene dosage in Cdh23(v-ngt/ahl) mice leads to the degeneration of stereocilia, which consequently reduces tip link tension. These findings indicate that CDH23 plays an important role in the maintenance of tip links during the aging process.

Published
2013

32. Genetic Modifiers of Hearing Loss in Mice: The Case of Phenotypic Modification in Homozygous Cdh23ahl Age-Related Hearing Loss

Author

Yuki Miyasaka and Yoshiaki Kikkawa

Subjects
Genetics, education.field_of_study, Hearing loss, Strain (biology), Population, Quantitative trait locus, Biology, Congenital hearing loss, Reverse genetics, Inbred strain, Mutation (genetic algorithm), otorhinolaryngologic diseases, medicine, medicine.symptom, education
Abstract

There has been considerable progress in identifying the mutations primarily associated with congenital hearing loss caused by a single gene. The next challenge is the discovery of genes and mutations associated with common acquired hearing loss in the human population such as age-related hearing loss (AHL) and presbyacusis, which occur through the effects of environmental risk factors and several quantitative trait loci, namely, genetic modifiers. One approach to identify novel modifier genes is an unbiased genomic strategy that utilizes mouse models, which are investigated in a controlled environment. Here, we describe the genetic modifiers that contribute to hearing loss susceptibility and resistance in inbred mice and the genetic approaches used to identify the modifiers in the genetic background, with emphasis on the AHL mutation of the cadherin 23 gene Cdh23ahl. Cdh23ahl is the mutation responsible for hearing loss in multiple inbred strains and impacts mice hearing phenotypes as a genetic modifier. We then discuss the AHL-resistance effect in the presence of Cdh23ahl identified using a chromosomal substitution (consomic) strain. Finally, we propose future directions for identifying genetic modifiers using forward and reverse genetics approaches.

Published
2016

33. Independent genetic control of early and late stages of chemically induced skin tumors in a cross of a Japanese wild-derived inbred mouse strain, MSM/Ms

Author

Ryo Kominami, Yuichi Wakabayashi, Ikuo Miura, Megumi Saito, Yuki Miyasaka, Shigeharu Wakana, Jian-Hua Mao, Kazuhiro Okumura, and Miho Sato

Subjects
Male, Cancer Research, Skin Neoplasms, Genetic Linkage, 9,10-Dimethyl-1,2-benzanthracene, Mice, Inbred Strains, Locus (genetics), Biology, Mice, Japan, Inbred strain, Genetic linkage, CDKN2A, Animals, Gene, Crosses, Genetic, Mice, Knockout, Genetics, Chromosome 7 (human), Papilloma, Chromosome, General Medicine, Mice, Inbred C57BL, Chromosome 4, Carcinogens, Tetradecanoylphorbol Acetate, Female, Tumor Suppressor Protein p53
Abstract

MSM/Ms is an inbred mouse strain derived from a Japanese wild mouse, Mus musculus molossinus. In this study, we showed that MSM/Ms mice exhibit dominant resistance when crossed with susceptible FVB/N mice and subjected to the two-stage skin carcinogenesis protocol using 7,12-dimethylbenz(a)anthracene (DMBA)/ 12-O-tetradecanoylphorbol-13-acetate (TPA). A series of F1 backcross mice were generated by crossing p53(+/+) or p53(+/-) F1 (FVB/N × MSM/Ms) males with FVB/N female mice. These generated 228 backcross animals, approximately half of which were p53(+/-), enabling us to search for p53-dependent skin tumor modifier genes. Highly significant linkage for papilloma multiplicity was found on chromosomes 6 and 7 and suggestive linkage was found on chromosomes 3, 5 and 12. Furthermore, in order to identify stage-dependent linkage loci we classified tumors into three categories (2mm, 2-6mm and6mm), and did linkage analysis. The same locus on chromosome 7 showed strong linkage in groups with2mm or 2-6mm papillomas. No linkage was detected on chromosome 7 to papillomas6mm, but a different locus on chromosome 4 showed strong linkage both to papillomas6mm and to carcinomas. This locus, which maps near the Cdkn2a/p19(Arf) gene, was entirely p53-dependent, and was not seen in p53 (+/-) backcross animals. Suggestive linkage conferring susceptibility to carcinoma was also found on chromosome 5. These results clearly suggest distinct loci regulate each stage of tumorigenesis, some of which are p53-dependent.

Published
2012

34. Advantages of a Mouse Model for Human Hearing Impairment

Author

Sari Suzuki, Yuki Miyasaka, Yoshihiro Noguchi, Kazuhiro Okumura, Kunie Matsuoka, Mao Ozaki, Yasuhiro Ohshiba, Yuta Seki, Hiromichi Yonekawa, and Yoshiaki Kikkawa

Subjects
medicine.medical_specialty, Hearing loss, Stereocilia (inner ear), Audiology, Biology, General Biochemistry, Genetics and Molecular Biology, Stereocilia, Mice, Hearing, Species Specificity, Hair Cells, Auditory, otorhinolaryngologic diseases, medicine, Animals, Humans, Inner ear, Hearing Loss, Mice, Knockout, General Veterinary, Laboratory mouse, General Medicine, Disease Models, Animal, medicine.anatomical_structure, Animal Science and Zoology, sense organs, medicine.symptom, Auditory Physiology, Neuroscience
Abstract

Hearing is a major factor in human quality of life. Mouse models are important tools for discovering the genes that are responsible for genetic hearing loss, and these models often allow the processes that regulate the onset of deafness in humans to be analyzed. Thus far, in the study of hearing and deafness, at least 400 mutants with hearing impairments have been identified in laboratory mouse populations. Analysis of through a combination of genetic, morphological, and physiological studies is revealing valuable insights into the ontogenesis, morphogenesis, and function of the mammalian ear. This review discusses the advantages of the mouse models of human hearing impairment and highlights the identification of the molecules required for stereocilia development in the inner ear hair cells by analysis of various mouse mutants.

Published
2012

35. Heterozygous mutation of Ush1g/Sans in mice causes early-onset progressive hearing loss, which is recovered by reconstituting the strain-specific mutation in Cdh23

Author

Yasuhiro Ohshiba, Kazuhiro Okumura, Sari Suzuki, Yuta Seki, Toyoyuki Takada, Ken Kitamura, Sachi Yoshimoto, Yoshiaki Kikkawa, Hisashi Tokano, Ryo Kominami, Hiroshi Hibino, Hiromichi Yonekawa, Hiroshi Shitara, Choji Taya, Toshihiko Shiroishi, and Yuki Miyasaka

Subjects
0301 basic medicine, Heterozygote, Hearing loss, Mutant, Nerve Tissue Proteins, Biology, medicine.disease_cause, Stereocilia, 03 medical and health sciences, Mice, CDH23, otorhinolaryngologic diseases, Genetics, medicine, Animals, Humans, Amino Acid Sequence, Allele, Hearing Loss, Molecular Biology, Gene, Genetics (clinical), Alleles, Mutation, Chromosomes, Human, Pair 10, Homozygote, Chromosome, General Medicine, Cadherins, Molecular biology, Disease Models, Animal, Hair Cells, Auditory, Outer, 030104 developmental biology, medicine.symptom
Abstract

Most clinical reports have suggested that patients with congenital profound hearing loss have recessive mutations in deafness genes, whereas dominant alleles are associated with progressive hearing loss (PHL). Jackson shaker (Ush1gjs) is a mouse model of recessive deafness that exhibits congenital profound deafness caused by the homozygous mutation of Ush1g/Sans on chromosome 11. We found that C57BL/6J-Ush1gjs/+ heterozygous mice exhibited early-onset PHL (ePHL) accompanied by progressive degeneration of stereocilia in the cochlear outer hair cells. Interestingly, ePHL did not develop in mutant mice with the C3H/HeN background, thus suggesting that other genetic factors are required for ePHL development. Therefore, we performed classical genetic analyses and found that the occurrence of ePHL in Ush1gjs/+ mice was associated with an interval in chromosome 10 that contains the cadherin 23 gene (Cdh23), which is also responsible for human deafness. To confirm this mutation effect, we generated C57BL/6J-Ush1gjs/+, Cdh23c.753A/G double-heterozygous mice by using the CRISPR/Cas9-mediated Cdh23c.753A>G knock-in method. The Cdh23c.753A/G mice harbored a one-base substitution (A for G), and the homozygous A allele caused moderate hearing loss with aging. Analyses revealed the complete recovery of ePHL and stereocilia degeneration in C57BL/6J-Ush1gjs/+ mice. These results clearly show that the development of ePHL requires at least two mutant alleles of the Ush1g and Cdh23 genes. Our results also suggest that because the SANS and CDH23 proteins form a complex in the stereocilia, the interaction between these proteins may play key roles in the maintenance of stereocilia and the prevention of ePHL.

Published
2015

36. A novel splice site mutation of myosin VI in mice leads to stereociliary fusion caused by disruption of actin networks in the apical region of inner ear hair cells

Author

Naomi Nakagata, Hirohide Takebayashi, Kunie Matsuoka, Shumpei P. Yasuda, Yoshiaki Kikkawa, Rie Ishii, Kentaro Endo, Yuki Miyasaka, Kenta Wada, Sari Suzuki, Yasuhiro Ohshiba, Yuta Seki, Hiroshi Shitara, and Shin-ichiro Kitajiri

Subjects
0301 basic medicine, Stereocilia (inner ear), Mutant, lcsh:Medicine, Cuticular plate, medicine.disease_cause, Cell Fusion, Mice, 0302 clinical medicine, Animal Cells, Myosin, Medicine and Health Sciences, Electron Microscopy, lcsh:Science, Mammals, Neurons, Mutation, Microscopy, Multidisciplinary, Reverse Transcriptase Polymerase Chain Reaction, Cochlea, Phenotypes, medicine.anatomical_structure, Vestibular Hair Cells, Vertebrates, Inner Ear, Scanning Electron Microscopy, Anatomy, Integumentary System, Cellular Types, Research Article, Cell Physiology, Mice, Transgenic, Biology, Research and Analysis Methods, Rodents, 03 medical and health sciences, medicine, Genetics, otorhinolaryngologic diseases, Animals, Inner ear, Immunohistochemistry Techniques, Actin, Hair Cells, Auditory, Inner, Myosin Heavy Chains, lcsh:R, Organisms, Biology and Life Sciences, Afferent Neurons, Cell Biology, Molecular biology, Actins, Histochemistry and Cytochemistry Techniques, Mice, Inbred C57BL, Alternative Splicing, 030104 developmental biology, Ears, Cellular Neuroscience, Amniotes, Immunologic Techniques, lcsh:Q, Head, 030217 neurology & neurosurgery, Hair, Neuroscience
Abstract

An unconventional myosin encoded by the myosin VI gene (MYO6) contributes to hearing loss in humans. Homozygous mutations of MYO6 result in nonsyndromic profound congenital hearing loss, DFNB37. Kumamoto shaker/waltzer (ksv) mice harbor spontaneous mutations, and homozygous mutants exhibit congenital defects in balance and hearing caused by fusion of the stereocilia. We identified a Myo6(c.1381G>A) mutation that was found to be a p.E461K mutation leading to alternative splicing errors in Myo6 mRNA in ksv mutants. An analysis of the mRNA and protein expression in animals harboring this mutation suggested that most of the abnormal alternatively spliced isoforms of MYO6 are degraded in ksv mice. In the hair cells of ksv/ksv homozygotes, the MYO6 protein levels were significantly decreased in the cytoplasm, including in the cuticular plates. MYO6 and stereociliary taper-specific proteins were mislocalized along the entire length of the stereocilia of ksv/ksv mice, thus suggesting that MYO6 attached to taper-specific proteins at the stereociliary base. Histological analysis of the cochlear hair cells showed that the stereociliary fusion in the ksv/ksv mutants, developed through fusion between stereociliary bundles, raised cuticular plate membranes in the cochlear hair cells and resulted in incorporation of the bundles into the sheaths of the cuticular plates. Interestingly, the expression of the stereociliary rootlet-specific TRIO and F-actin binding protein (TRIOBP) was altered in ksv/ksv mice. The abnormal expression of TRIOBP suggested that the rootlets in the hair cells of ksv/ksv mice had excessive growth. Hence, these data indicated that decreased MYO6 levels in ksv/ksv mutants disrupt actin networks in the apical region of hair cells, thereby maintaining the normal structure of the cuticular plates and rootlets, and additionally provided a cellular basis for stereociliary fusion in Myo6 mutants., Article, PLOS ONE.12(8):e0183477(2017)

Published
2017

37. Compound heterozygosity of the functionally null Cdh23(v-ngt) and hypomorphic Cdh23(ahl) alleles leads to early-onset progressive hearing loss in mice

Author

Yuki, Miyasaka, Sari, Suzuki, Yasuhiro, Ohshiba, Kei, Watanabe, Yoshihiko, Sagara, Shumpei P, Yasuda, Kunie, Matsuoka, Hiroshi, Shitara, Hiromichi, Yonekawa, Ryo, Kominami, and Yoshiaki, Kikkawa

Subjects
Aging, Heterozygote, Original, Gene Dosage, Cadherins, cadherin 23, mouse mutant, hair cell, Mice, Mutant Strains, Mice, Inbred C57BL, Stereocilia, Mice, age-related hearing loss, Mutation, Nerve Degeneration, otorhinolaryngologic diseases, Disease Progression, Animals, sense organs, Hearing Loss, Alleles
Abstract

The waltzer (v) mouse mutant harbors a mutation in Cadherin 23 (Cdh23) and is a model for Usher syndrome type 1D, which is characterized by congenital deafness, vestibular dysfunction, and prepubertal onset of progressive retinitis pigmentosa. In mice, functionally null Cdh23 mutations affect stereociliary morphogenesis and the polarity of both cochlear and vestibular hair cells. In contrast, the murine Cdh23(ahl) allele, which harbors a hypomorphic mutation, causes an increase in susceptibility to age-related hearing loss in many inbred strains. We produced congenic mice by crossing mice carrying the v niigata (Cdh23(v-ngt)) null allele with mice carrying the hypomorphic Cdh23(ahl) allele on the C57BL/6J background, and we then analyzed the animals' balance and hearing phenotypes. Although the Cdh23(v-ngt/ahl) compound heterozygous mice exhibited normal vestibular function, their hearing ability was abnormal: the mice exhibited higher thresholds of auditory brainstem response (ABR) and rapid age-dependent elevation of ABR thresholds compared with Cdh23(ahl/ahl) homozygous mice. We found that the stereocilia developed normally but were progressively disrupted in Cdh23(v-ngt/ahl) mice. In hair cells, CDH23 localizes to the tip links of stereocilia, which are thought to gate the mechanoelectrical transduction channels in hair cells. We hypothesize that the reduction of Cdh23 gene dosage in Cdh23(v-ngt/ahl) mice leads to the degeneration of stereocilia, which consequently reduces tip link tension. These findings indicate that CDH23 plays an important role in the maintenance of tip links during the aging process.

Published
2013

38. Bcl11b heterozygosity leads to age-related hearing loss and degeneration of outer hair cells of the mouse cochlea

Author

Hitoshi Okumura, Yukio Mishima, Yuki Miyasaka, Sugata Takahashi, Yuka Morita, Tomoyuki Nomura, and Ryo Kominami

Subjects
medicine.medical_specialty, Pathology, Hearing loss, BCL11B, Presbycusis, Biology, General Biochemistry, Genetics and Molecular Biology, Loss of heterozygosity, Mice, Internal medicine, Hair Cells, Auditory, otorhinolaryngologic diseases, medicine, Evoked Potentials, Auditory, Brain Stem, Animals, Cell Nucleus, Mice, Inbred BALB C, Polymorphism, Genetic, General Veterinary, Tumor Suppressor Proteins, General Medicine, medicine.disease, Repressor Proteins, Cell nucleus, Disease Models, Animal, medicine.anatomical_structure, Endocrinology, Animal Science and Zoology, Brainstem, Hair cell, medicine.symptom, Nucleus
Abstract

BCL11B/CTIP2 zinc-finger transcription factor is expressed in various types of cells in many different tissues. This study showed that BCL11B is expressed in the nucleus of the outer hair cells of the mouse cochlea, degeneration of which is known to cause deafness and presbycusis or age-related hearing loss (AHL). We tested whether or not Bcl11b heterozygosity would affect AHL in mice. Analysis of auditory brainstem responses revealed AHL in Bcl11b (+/-) heterozygous, but not wild-type, mice, which was evident as early as 3 months after birth. Histological abnormalities were observed in the outer hair cells of the Bcl11b (+/-) mice at 6 months of age with hearing loss. These results suggest that the AHL observed in Bcl11b (+/-) mice is the result of impairment of the outer hair cells and that BCL11B activity is required for the maintenance of outer hair cells and normal hearing.

Published
2011

42. SDR9C7 catalyzes critical dehydrogenation of acylceramides for skin barrier formation.

Author

Takuya Takeichi, Tetsuya Hirabayashi, Yuki Miyasaka, Akane Kawamoto, Yusuke Okuno, Shijima Taguchi, Kana Tanahashi, Chiaki Murase, Hiroyuki Takama, Kosei Tanaka, Boeglin, William E., Calcutt, M. Wade, Daisuke Watanabe, Michihiro Kono, Yoshinao Muro, Junko Ishikawa, Tamio Ohno, Brash, Alan R., Masashi Akiyama, and Takeichi, Takuya

Subjects
*DEHYDROGENATION, *BIOLOGICAL extinction, *SKIN, *CARRIER proteins, *ICHTHYOSIS, *LINOLEIC acid, *LIPID metabolism, *BIOLOGICAL models, *RESEARCH, *ANIMAL experimentation, *RESEARCH methodology, *GENETIC disorders, *EVALUATION research, *MEDICAL cooperation, *COMPARATIVE studies, *CHEMISTRY, *OXIDOREDUCTASES, *EPIDERMIS, *MICE, *LIPIDS
Abstract

The corneocyte lipid envelope, composed of covalently bound ceramides and fatty acids, is important to the integrity of the permeability barrier in the stratum corneum, and its absence is a prime structural defect in various skin diseases associated with defective skin barrier function. SDR9C7 encodes a short-chain dehydrogenase/reductase family 9C member 7 (SDR9C7) recently found mutated in ichthyosis. In a patient with SDR9C7 mutation and a mouse Sdr9c7-KO model, we show loss of covalent binding of epidermal ceramides to protein, a structural fault in the barrier. For reasons unresolved, protein binding requires lipoxygenase-catalyzed transformations of linoleic acid (18:2) esterified in ω-O-acylceramides. In Sdr9c7-/- epidermis, quantitative liquid chromatography-mass spectometry (LC-MS) assays revealed almost complete loss of a species of ω-O-acylceramide esterified with linoleate-9,10-trans-epoxy-11E-13-ketone; other acylceramides related to the lipoxygenase pathway were in higher abundance. Recombinant SDR9C7 catalyzed NAD+-dependent dehydrogenation of linoleate 9,10-trans-epoxy-11E-13-alcohol to the corresponding 13-ketone, while ichthyosis mutants were inactive. We propose, therefore, that the critical requirement for lipoxygenases and SDR9C7 is in producing acylceramide containing the 9,10-epoxy-11E-13-ketone, a reactive moiety known for its nonenzymatic coupling to protein. This suggests a mechanism for coupling of ceramide to protein and provides important insights into skin barrier formation and pathogenesis. [ABSTRACT FROM AUTHOR]

Published
2020
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