Curriculum Vitaes
Profile Information
- Affiliation
- Unit leader, Professor, Deapartment of Regulatory Science, Reasearch Promotion Unit, Graduate School and School of Medical Sciences , Fujita Health University(Concurrent)Division head, Division of Neurochemistry, International Center for Brain Science
- Degree
- 博士(医学)(名古屋大学大学院医学系研究科)
- J-GLOBAL ID
- 201001019721259872
- researchmap Member ID
- 6000026156
- External link
Research Interests
7Research Areas
4Research History
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Apr, 2024 - Present
Education
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Apr, 2003 - Mar, 2007
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Apr, 1997 - Mar, 2001
Awards
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Oct, 2017
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Oct, 2011
Papers
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Neuroscience, 603 239-251, May 25, 2026Animal models are essential for studying aversive states such as fear and pain. Facial expressions may provide non-invasive readouts of aversive states in animals. This study investigated whether changes in facial expressions, which are potentially consistent between humans and mice, can serve as objective indicators of fear responses and distinguish fear from pain. We analyzed changes in the facial expressions of mice associated with conditioned fear stress (CFS) using convolutional neural networks (CNNs). Photographs of CFS and control mice were analyzed using four advanced CNN models: VGG16, ResNet50, DenseNet121, and InceptionV3. The CNNs identified CFS mice from facial images under contrasts: control/non-freezing vs CFS/freezing and control/non-freezing vs CFS/non-freezing, with consistently high performance (Control/non-freezing vs CFS/freezing: sensitivity 0.942, specificity 0.929, accuracy 0.935, precision 0.929, AUC 0.966; Control/non-freezing vs CFS/non-freezing: sensitivity 0.912, specificity 0.900, accuracy 0.906, precision 0.902, AUC 0.950). The ability to detect CFS without freezing decreased as stress intensity weakened, from an AUC of 0.950 to 0.701, suggesting that CNNs can detect facial changes depending on the degree of stress exposure. Facial changes were particularly pronounced in freezing mice, further supporting their association with CFS-related emotional responses. During testing, mice were returned to the conditioning chamber without shock; therefore, this facial expression could reflect fear response rather than pain response. These findings demonstrate the potential of CNNs to serve as non-invasive tools for detecting stress-induced affective changes in mice.
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Neurochemistry international, 197 106184-106184, May 14, 2026High salt (HS) intake is a major risk factor of hypertension and has been implicated in emotional and cognitive decline. On the other hand, dietary supplementation may represent a potential preventive strategy against health risks induced by HS intake. Soybean lecithin is widely used as a phospholipid supplement. Here, we investigated the effects of lysolecithin enriched in lysophosphatidylcholine (>70% of total phospholipids; LPC70) on hypertension and behavioral impairments under high-salt diet (HSD) conditions in mice. To further characterize these effects, we examined changes in prostaglandin (PG)-related pathways by integrating gene expression and lipidomic analyses. Mice were fed an HSD (chow containing 8% NaCl) with or without LPC70 for 10 weeks. HSD elevated systolic blood pressure and impaired social behavior and object recognition memory in mice. Quantitative gene expression analyses revealed that HSD increased renal expression of cyclooxygenase-2 (COX-2) and EP3 (PGE2 receptor), and reduced expression of DP1 (PGD2 receptor) in the prefrontal cortex. LPC70 attenuated these changes in behavior, blood pressure, and PG-related gene expression. Furthermore, lipidomic analyses revealed that HSD reduced circulating arachidonic acid (AA) levels, whereas LPC70 increased AA-derived PG, such as PGE2 and PGD2, in HSD-fed mice. These findings demonstrate that LPC70 may protect against hypertension and behavioral impairments under HSD conditions in mice, potentially in association with modulation of PG signaling. LPC70 may serve as a functional dietary component that reshapes lipid mediator signaling under HSD conditions.
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Neurochemistry international, 195 106141-106141, May, 2026Multiple sclerosis (MS) is a common autoimmune demyelinating disease of the central nervous system (CNS). Although activation of the kynurenine (KYN) pathway has been observed in patients with MS, its pathological significance remains unclear. In this study, we investigated the role of the KYN pathway in MS using an experimental autoimmune encephalomyelitis (EAE) mouse model, a widely recognized animal model of MS. We found an increase in the expression of kynureninase (KYNU), a key enzyme in the KYN pathway that is specifically localized within monocytes in the spinal cord of EAE mice. This was accompanied by a significant accumulation of quinolinic acid (QUIN) in the spinal cord. Importantly, similar increases in KYNU expression and QUIN levels were observed in the spinal cord of proteolipid protein overexpressing mice (PLP-tg mice), another model of demyelination. Notably, KYNU knockout (KO) reduced EAE severity and monocyte recruitment to the spinal cord of EAE model mice. These findings suggest that the increase in KYNU expression and the subsequent accumulation of QUIN may contribute to the exacerbation of MS. Taken together, our results indicate that KYNU could be a novel therapeutic target for MS.
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Trials, 27(1), Mar 13, 2026BACKGROUND: Although the number of frozen-thawed blastocysts transfer is increasing worldwide, the live birth rate following blastocyst transfer using assisted reproductive technology remains at 30-60%. Thus, improving the pregnancy rate per transfer is an urgent issue. In a previous retrospective study, we evaluated the use of granulocyte-macrophage colony-stimulating factor (GM-CSF)-containing medium for recovery culture to improve the outcomes of frozen-thawed blastocyst transfers. The results demonstrated that the live birth rates increased by approximately 10% following recovery culture in the GM-CSF-containing culture medium. This study aims to prospectively evaluate whether GM-CSF-containing blastocyst recovery culture following thawing increases live birth. METHODS: This is a multicenter, randomized, parallel-group, active-controlled, single-blind trial. The recruitment target is 750 participants meeting the criteria. Enrolled patients are randomized 1:1 to the GM-CSF-containing culture medium group (test group) or the non-GM-CSF-containing culture medium group (control group). The blastocyst recovery culture after warming was defined as an intervention in this study; frozen-thawed blastocysts will be cultured for 3-7 h in GM-CSF-containing medium (test group) or medium without GM-CSF (control group) followed by blastocyst transfer. The primary outcome will be live birth. We will also evaluate embryo transfer outcomes as secondary efficacy endpoints and evaluate perinatal and neonatal outcomes as a safety endpoint. DISCUSSION: This is the first large-scale prospective study to investigate the efficacy of a GM-CSF-containing medium for frozen-thawed blastocyst transfer. The study findings will provide evidence regarding the efficiency of GM-CSF-containing medium for blastocyst recovery culture after warming. TRIAL REGISTRATION: Japan Registry of Clinical Trials jRCT1040240159. Registered on January 6, 2025.
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Movement disorders : official journal of the Movement Disorder Society, Feb 2, 2026BACKGROUND: Alterations in tryptophan-kynurenine (TRP-KYN) metabolism, which is associated with neuroinflammation, remain unclear in multiple system atrophy (MSA). OBJECTIVE: The aim was to investigate cerebrospinal fluid (CSF) TRP metabolites in MSA and their associations with other biomarkers. METHODS: A total of 51 patients with MSA and 56 controls were included. CSF TRP metabolites, such as KYN, quinolinic acid (QA), and kynurenic acid (KA), along with neurofilament light chain (NfL), glycoprotein nonmetastatic melanoma protein B (GPNMB), and soluble triggering receptor expressed on myeloid cells 2 (sTREM2), were analyzed. RESULTS: Patients with MSA exhibited higher levels of QA, a neuroinflammatory marker, and lower levels of KA, a neuroprotective marker, yielding an elevated QA-to-KA ratio. Neither QA nor KA correlated with clinical scores. GPNMB, sTREM2, and NfL were increased; however, these markers were independent of KYN pathway metabolites. CONCLUSIONS: MSA exhibited a significant imbalance in KYN metabolism, suggesting a shift toward inflammatory processes distinct from classic neuroinflammatory markers. © 2026 The Author(s). Movement Disorders published by Wiley Periodicals LLC on behalf of International Parkinson and Movement Disorder Society.
Misc.
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乱用薬物による薬物依存の発症メカニズム・予防・診断及び治療法に関する研究 平成23年度 総括研究報告書, 2012
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乱用薬物による薬物依存の発症メカニズム・予防・診断及び治療法に関する研究 平成23年度 総括研究報告書, 2012
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 118 189P-189P, 2012
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 118 189P-189P, 2012
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 118 189P-189P, 2012
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 118 67P-67P, 2012
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 118 99P-99P, 2012
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 118 190P-190P, 2012
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 118 189P-189P, 2012
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アレルギー, 61(9) 1356-1356, 2012
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名城大学総合研究所紀要, (17) 71-74, 2012
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日本医療薬学会年会講演要旨集, 22 294-294, 2012
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日本医療薬学会年会講演要旨集, 22 313-313, 2012
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日本医療薬学会年会講演要旨集, 22 481-481, 2012
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薬学雑誌, 131(11) 1629-1638, Nov, 2011外来喘息教室での薬剤師による吸入指導が患者の喘息治療に有益であるか調査した。解析対象は外来喘息教室で初めて吸入指導を受けた26名であり、喘息の薬物療法に対する患者の理解度(吸入器具やピークフローメーターの操作、治療薬の理解及びコンプライアンス、喘息日記の記入)、自覚症状、ピークフロー値、アドヒアランス、患者満足度などを評価した。その結果、吸入指導後は自覚症状、肺機能や患者の理解度が有意に改善し、喘息コントロール不良と評価された患者の割合は減少した。また、吸入指導前後に吸入ステロイド薬の増量及び長時間型β2刺激薬の追加を要した患者はなく、吸入指導について肯定的であり、外来喘息教室に対する患者満足度は高かった。薬剤師による外来喘息教室での服薬指導は、患者の喘息治療及び喘息の自己管理に有用であることが強く示唆された。
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日本臨床精神神経薬理学会・日本神経精神薬理学会合同年会プログラム・抄録集, 21回・41回 171-171, Oct, 2011
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APJHP: 愛知県病院薬剤師会雑誌, 39(2) 8-12, Sep, 2011過去1年間と最近1年間における肺ガン緩和治療における非ステロイド性抗炎症薬(NSAID)あるいはステロイド薬を処方する場合の胃酸分泌抑制薬(ヒスタミンH2拮抗薬とプロトンポンプ阻害薬)および胃粘膜保護薬の使用状況の変遷をレトロスペクティブに調査した。最近処方におけるNSAID単独群あるいはNSAID+ステロイド薬併用群のプロトンポンプ阻害薬の処方割合は、ヒスタミンH2受容体拮抗薬に比べて有意に高かった。NSAID単独群においてプロトンポンプ阻害薬が予防的に処方されていた割合は、最近処方の方が過去処方に比べて有意に高かった。以前はNSAIDに加え、ステロイド薬が処方された場合には、胃酸分泌抑制薬が予防的に処方されていたが、現在ではNSAIDが単独で処方されていても、特に強力な胃酸分泌抑制作用を持つプロトンポンプ阻害薬が予防的に処方されていた。
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第73回全国大会講演論文集, 2011(1) 779-780, Mar 2, 2011近年、液晶を中心とする表示デバイスやコンピュータによるディジタル信号技術などの進歩により、物体を立体的に見せる三次元(3D)ディスプレイの研究開発が活発化し、パソコン対応の3Dディスプレイや家庭用立体テレビが登場するなど応用も急速に発展している。本研究では、レンチキュラ板を用いて投射型での立体視範囲を確認し、立体映像の範囲の可能性について研究する。
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乱用薬物による薬物依存の発症メカニズム・予防・診断及び治療法に関する研究 平成22年度 総括研究報告書, 2011
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 115 250P-250P, 2011
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 115 248P-248P, 2011
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 115 194P-194P, 2011
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 115 195P-195P, 2011
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Iryo Yakugaku (Japanese Journal of Pharmaceutical Health Care and Sciences), 37(8) 475-480, 2011Falls and fall-related injuries among inpatients are one of the most important concerns in medical safety management and sometimes cause a significant decrease in activities of daily living (ADL). It has been suggested that the adverse reactions of psychotropic drugs related to their sedative-hypnotic, cognitive deficit producing and muscle reaction-related effects are closely associated with falls.<br>In this study, we examined a relationship between the risk of falls and psychotropic drugs based on prescriptions in fall incident reports at Nagoya University Hospital in a 12-month period beginning in April 1, 2005. In July 2006, we conducted an educational intervention involving instructing health care staff on the optimal use of psychotropics. After doing this, we examined prescriptions in fall incident reports over a 12-month period beginning in April 1, 2006. The results showed a decrease in fall incidence due to long-acting drugs in 2006 as compared with 2005 and this indicated that, among psychotropics, sedativehypnotic-anxiolytics were one of the highest risk factors for falls. These results suggest that an educational intervention can be an effective means of reducing the number of falls and fall-related injuries among inpatients.
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日本医療薬学会年会講演要旨集, 21 303-303, 2011
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日本臨床精神神経薬理学会・日本神経精神薬理学会合同年会プログラム・抄録集, 20回・40回 200-200, Sep, 2010
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乱用薬物による神経毒性・依存症に対する診断・予防及び治療法に関する研究 平成21年度 総括研究報告書 平成19-21年度3年間のまとめ・総合研究報告書, 2010
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乱用薬物による神経毒性・依存症に対する診断・予防及び治療法に関する研究 平成21年度 総括研究報告書 平成19-21年度3年間のまとめ・総合研究報告書, 2010
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 112 221P-221P, 2010
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 112 63P-63P, 2010
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 112 229P-229P, 2010
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 112 228P-228P, 2010
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 112 172P-172P, 2010
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JOURNAL OF PHARMACOLOGICAL SCIENCES, 112 97P-97P, 2010
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NEUROSCIENCE RESEARCH, 68 E202-E202, 2010
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日本医療薬学会年会講演要旨集, 20 393-393, 2010
Books and Other Publications
1Research Projects
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Grants-in-Aid for Scientific Research, Japan Society for the Promotion of Science, Apr, 2025 - Mar, 2028
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戦略的な研究開発の推進 創発的研究支援事業, 科学技術振興機構, 2022 - 2028
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Grants-in-Aid for Scientific Research, Japan Society for the Promotion of Science, Apr, 2022 - Mar, 2025
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Grants-in-Aid for Scientific Research, Japan Society for the Promotion of Science, Apr, 2020 - Mar, 2023
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Grants-in-Aid for Scientific Research Grant-in-Aid for Scientific Research (B), Japan Society for the Promotion of Science, Apr, 2017 - Mar, 2022
Industrial Property Rights
16Media Coverage
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https://www.zakzak.co.jp/lif/news/210823/hea2108230001-n1.html, Aug, 2021 Internet
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刑事事件弁護士ナビ, 違法薬物で罰せられる薬物四法とは|依存症回復は可能?, https://keiji-pro.com/magazine/175/, Nov 11, 2020 Internet
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ラジオNIKKEI, 薬学の時間, http://medical.radionikkei.jp/yakugaku/tag/tag_953.html, Mar, 2010 TV or radio program