Profile Information
- Affiliation
- Professor, Faculty of Veterinary Science School of Veterinary Medicine, Nippon Veterinary and Life Science University
- Degree
- 博士(農学)(名古屋大学)
- J-GLOBAL ID
- 200901017318751437
- researchmap Member ID
- 5000041338
主にネコの肥満について研究しております。専門は遺伝子工学、内分泌学と発生生物学です。
Research Interests
6Research Areas
1Research History
8-
Apr, 2024 - Present
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Apr, 2014 - Mar, 2022
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Apr, 2011 - Mar, 2014
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Apr, 2008 - Mar, 2011
Education
3-
Apr, 1997 - Mar, 1999
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Apr, 1993 - Mar, 1997
Committee Memberships
1-
Sep, 2014 - Present
Awards
2Papers
93-
Mammalian Genome, Apr 24, 2024 Peer-reviewed
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General and comparative endocrinology, 353 114520-114520, Apr 18, 2024 Peer-reviewedLead authorCorresponding authorG protein-coupled receptor 84 (GPR84) was cloned as an orphan receptor, and medium-chain fatty acids were then revealed as endogenous ligands. GPR84 is expressed in immune cells and is believed to protect liver function from lipotoxicity caused by overeating and high-fat diet intake. This study aimed to present the molecular characterization of GPR84 in domestic cats. The deduced amino acid sequence of the feline GPR84 shows high sequence homology (83-89 %) with the orthologues from other mammalians by cDNA cloning of feline GPR84. Remarkably high mRNA expression was observed in the bone marrow by Q-PCR analysis. The inhibition of intracellular cAMP concentration was observed in cells transfected with feline GPR84 and treated with medium-chain fatty acids. Immunostaining of GPR84 and free fatty acid receptor 2 (FFAR2)/GPR43 in the bone marrow, where high mRNA expression was observed, showed reactions in macrophages and myeloid cells. To clarify whether the receptor formed homo/hetero-merization, GPR84 and FFARs were analyzed using Nano-Luc binary technology and NanoLuc bioluminescence resonance energy transfer technologies, which revealed that GPR84 formed more heteromers with FFAR2 than homomers with each other. In addition, when GPR84 and FFAR2/GPR43 were cotransfected in the cell, their localization on the cell membrane was reduced compared with that when single receptors were transfected. These results indicated that GPR84 is a functional receptor protein that is expressed in cat tissues and may have a protein-protein interaction with FFAR2/GPR43 on the cell membrane.
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Veterinary Medicine and Science, 7(1) 77-85, Jan, 2021 Peer-reviewedLead authorCorresponding authorG protein-coupled receptors 41 and 43 were identified and characterized as free fatty acid receptors (FFAR) 3 and 2, respectively. FFAR2 and FFAR3 mediate short-chain fatty acids (SCFAs) as signalling molecules. The present study aimed to give molecular characterization of FFAR2 and FFAR3 in the domestic cat. High homology with that in other mammals was revealed by cDNA cloning of cat FFAR2 FFAR3. We analyzed the tissue distribution of cat FFAR2 and FFAR3 mRNA using quantitative polymerase chain reaction. The inhibition of intracellular cAMP concentrations was observed in cells transfected with cat FFAR2 or FFAR3 and treated with SCFAs. The activation of nuclear factor of activated T cells-luciferase reporter was only observed in cat FFAR2 transfected cells but not in FFAR3. Split luciferase assay (NanoLuc Binary Technology; NanoBiT) for FFAR2 or FFAR3 and Arrestin-3/β-arrestin-2 revealed acetate-/propionate-induced recruitment to cat FFAR2 or FFAR3 in CHO-K1 cells. Our results indicate that FFAR2 and FFAR3 are functional receptor proteins that are expressed in cat tissues and show differential distribution patterns.
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Veterinary Medicine: Research and Reports, Volume 11 131-137, Nov, 2020 Peer-reviewed
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Frontiers in Nutrition, 5, Sep 7, 2018 Peer-reviewed
Misc.
16-
Clinic note : journal of clinical daily treatment for small animals, 9(9) 102-105, Sep, 2013
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Japanese journal of prophylactic veterinary medicine, 3(1) 11-19[含 英語文要旨], 2011
Presentations
78-
18th International Society for Animal Clinical Pathology (ISACP) Tokyo, Japan
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18th International Society for Animal Clinical Pathology (ISACP) Tokyo, Japan
Teaching Experience
10-
Apr, 2022 - Present
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Apr, 2018 - Present
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Apr, 2008 - Present獣医生化学実習(分担) (日本獣医生命科学大学)
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Apr, 2008 - Present研究用機器論(分担) (日本獣医生命科学大学)
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2008 - Present
Professional Memberships
8-
Apr, 2008 - Present
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2020 - 2020
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Apr, 2009 - Mar, 2014
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Apr, 2008 - Mar, 2011
Research Projects
11-
Apr, 2023 - Mar, 2026
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文部科学省: 科学研究費補助金(基盤(B)), Apr, 2019 - Mar, 2023
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文部科学省: 科学研究費補助金(基盤研究(C)), Apr, 2019 - Mar, 2022
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科学研究費補助金(基盤研究(C)), 文部科学省, Apr, 2016 - Mar, 2019
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Grants-in-Aid for Scientific Research, Japan Society for the Promotion of Science, 2013 - 2015