Curriculum Vitaes
Profile Information
- Affiliation
- School of Health Sciences Faculty of Clinical Engineering, Fujita Health University
- Degree
- 博士(医学)(藤田医科大学)
- J-GLOBAL ID
- 200901033786050786
- researchmap Member ID
- 1000205082
Research Areas
1Papers
121-
Journal of Medical Virology, 98(2), Feb 16, 2026ABSTRACT Mesial temporal lobe epilepsy with hippocampal sclerosis (MTLE‐HS) is an intractable form of epilepsy involving the hippocampus, and temporal lobectomy remains an effective treatment. Human herpesvirus 6B (HHV‐6B) establishes latency in the hippocampus and may contribute to MTLE‐HS pathogenesis by altering host gene expression; however, transcriptomic data from healthy controls remain limited. This study investigated the role of HHV‐6B to MTLE‐HS pathogenesis by analyzing gene expression in resected hippocampal tissues. Samples were collected from 12 to 43 HHV‐6 DNA‐positive and ‐negative patients, respectively, and three controls. RNA sequencing was performed on eight representative samples, followed by RT‐qPCR validation of nine selected genes in 58 samples. RNA sequencing identified 600 differentially expressed genes (210 upregulated, 390 downregulated) between HHV‐6B‐positive MTLE‐HS and controls. Pathway enrichment analysis revealed involvement of synaptic signaling and inflammatory responses, with prostaglandin biosynthesis specifically upregulated in HHV‐6B‐positive tissues. Two genes were significantly upregulated in HHV‐6B‐positive compared with HHV‐6B‐negative samples. RT‐qPCR confirmed elevated cholesterol 25‐hydroxylase and interleukin 1 beta expression in HHV‐6 DNA‐positive samples (both p = 0.031). These findings suggest that HHV‐6B may contribute to MTLE‐HS pathogenesis by modulating the expression of host inflammatory genes, supporting a role for neuroinflammation and the potential benefits of anti‐inflammatory therapies.
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Journal of medical virology, 98(2) e70834, Feb, 2026BACKGROUND: Biliary atresia (BA) is a severe infantile hepatobiliary disorder of unknown etiology. Perinatal rotavirus (RV) infection has been implicated in animal models of BA; however, supporting human data remains limited. The study investigated the serological evidence of recent RV infection in infants with BA using RV-specific immunoglobulin (Ig)-A, a marker of primary infection unaffected by maternal antibodies. METHODS: Serum samples from 17 infants with BA and 30 age-matched controls without gastrointestinal symptoms or prior RV vaccination were retrospectively analyzed. Anti-RV-IgA titers were measured by enzyme-linked immunosorbent assay using purified WA-strain virions. Cytomegalovirus (CMV)-IgM and Epstein-Barr virus (EBV)-viral capsid antigen (VCA)-IgM levels were assessed using commercial enzyme immunoassays. RESULTS: RV-IgA was detected in 70.6% (12/17) of the patients with BA versus 3.4% (1/29) of the controls (p < 0.001). RV-IgA titers were significantly higher in the BA group (median: interquartile range 28.0:26.0-210.0) than in the control group (23.5:22.0-24.8) (p = 0.004). Among patients diagnosed with BA after 14 days of age, 84.6% (11/13) were RV-IgA-positive. CMV-IgM was detected in three patients in the BA group and one individual in the control group, while EBV-VCA-IgM was negative in BA patients and positive in two controls; neither difference was statistically significant. CONCLUSIONS: The study findings support the potential association between RV infection and BA pathogenesis. However, the lack of an epidemiological reduction in BA following the introduction of the RV vaccine warrants caution in other studies. Further prospective multicenter studies are required to elucidate the causal role of RV infection in BA development.
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Journal of medical virology, 97(12) e70750, Dec, 2025Varicella-zoster virus (VZV) causes varicella in children, establishes lifelong latency and reactivates to cause herpes zoster later in life. Implementation of routine varicella vaccination in Japan since 2014 has reduced varicella cases, however, breakthrough varicella still occurs. This study aimed to clarify the current distribution of VZV clade among pediatric varicella patients and adults with VZV-associated central nervous system (CNS) infections in Japan. Skin swabs were collected from varicella patients (< 15 years) in Aichi Prefecture (September 2015-August 2017). Cerebrospinal fluid (CSF) samples were obtained from adult patients (> 15 years) with VZV-associated CNS infections (November 2014-June 2023). VZV DNA was detected by PCR, and its clade was determined by sequencing open reading frame (ORF) 22 and ORF37 regions. Wild-type and Oka vaccine strains were distinguished by loop-mediated isothermal amplification (LAMP) method. Of 124 pediatric swab samples and 62 adult CSF samples 94.4% belonged to clade 2 and 4.8% clade 1. No clade 1 samples were detected in CSF samples. No vaccine strain was detected. Clinical characteristics did not differ significantly among clades. Clade 2 VZV predominates in both pediatric varicella and adult VZV-related CNS infections in Japan with sporadic clade 1 varicella cases.
Misc.
131-
日本ウイルス学会学術集会プログラム・予稿集(Web), 71st, 2024
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日本ウイルス学会学術集会プログラム・予稿集(Web), 71st, 2024
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日本ウイルス学会学術集会プログラム・予稿集(Web), 71st, 2024
Presentations
38-
8th International Conference on Human Herpesviruses 6 and 7, Apr, 2013
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8th International Conference on Human Herpesviruses 6 and 7, Apr, 2013
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8th International Conference on Human Herpesviruses 6 and 7, Apr, 2013
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8th International Conference on Human Herpesviruses 6 and 7, Apr, 2013
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US-Japan cooperative medical science program ;ubaculosis and leprosy panel Meeting, Mar, 2013
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Project Implementation Meeting on TB and Tryps Research Project (SATREPS), Feb, 2013
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2nd Scientific meeting for HIV/AIDS, Influenza and TB Diagnosis, Oct, 2011
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IUMS & International Union of Microbiological Societies, Sep, 2011
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36th Annual International Hepesvirus Workshop, Jul, 2011
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35th Annual International Hepesvirus Workshop, Jul, 2010
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35th Annual International Hepesvirus Workshop, Jul, 2010
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The development of LAMP assay for quantification of HSV (herpes simplex virus) using quenching probe35th Annual International Hepesvirus Workshop, Jul, 2010
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14th International Conference on Immunobiology and Prophylaxis of Human Herpesvirus Infections kobe, Oct, 2009
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34th Annual International Hepesvirus Workshop, Jul, 2009
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34th Annual International Hepesvirus Workshop, Jul, 2009
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34th Annual International Hepesvirus Workshop, Jul, 2009
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34th Annual International Hepesvirus Workshop, Jul, 2009
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6th International Conference on HHV-6&7 Boltimor, 2008
Research Projects
16-
Grants-in-Aid for Scientific Research, Japan Society for the Promotion of Science, Apr, 2024 - Mar, 2027
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科学研究費助成事業, 日本学術振興会, Apr, 2024 - Mar, 2027
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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, 2021 - Mar, 2024
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Grants-in-Aid for Scientific Research, Japan Society for the Promotion of Science, Apr, 2019 - Mar, 2022
教育内容・方法の工夫(授業評価等を含む)
1-
件名(英語)生体計測装置学講義ノート、画像診断装置学Ⅱ講義ノート終了年月日(英語)2012/04/01概要(英語)担当講義科目について内容を補助する講義ノートを作成した。
作成した教科書、教材、参考書
1-
件名(英語)臨床工学講座 生体計測装置学(医歯薬出版 2010 第1版 第3刷)終了年月日(英語)2013/01/10概要(英語)日本臨床工学技士教育施設協議会監修として発刊された生体計測装置学の第2章生体電気磁気計測(P32-64)、第3章血圧・血流計測(p131-142)を分担執筆
教育方法・教育実践に関する発表、講演等
1-
件名(英語)第5回医療科学部相互研修FD 「留年となる学生の問題点と対応策」
終了年月日(英語)2012/08/07概要(英語)臨床工学科からのテーマとしてFD研修会にて「留年となる学生の問題点と対応策」として本学科における現況と対応策を発表
その他教育活動上特記すべき事項
1-
件名(英語)第4-6回医療科学部相互研修FD 「学習の質をどう評価するか-医療人教育におけるパフォーマンス評価を中心に」終了年月日(英語)2015/08/06概要(英語)医療科学部相互研修FDに参加