Saitoh Sei

(齊藤成)

Profile Information

Affiliation: Fujita Health University

Degree: 医学博士(山梨大学)
医師免許
死体解剖資格認定

J-GLOBAL ID: 200901046035768325
researchmap Member ID: 6000017924

External link: https://www.fujita-hu.ac.jp/faculty/medicine/department/anatomyii.html

Research Areas

Research History

Apr, 2024 - Present

Fujita Health University
Oct, 2018 - Mar, 2024

藤田医科大学
Apr, 2018 - Oct, 2018

講師, 医学部解剖学講座II, 藤田保健衛生大学
Sep, 2016 - Mar, 2018

National Institutes of Natural Sciences
Apr, 2016 - Aug, 2016

助教, 解剖学講座構造生物学教室, 国立大学法人山梨大学大学院総合研究部医学域

Education

Apr, 2003 - Mar, 2008

Department of Education Interdisciplinary Graduate School of Medicine and Engineering, University of Yamanashi
Apr, 1994 - Mar, 2000

医学科, 医学部, 山梨医科大学
Apr, 1991 - Mar, 1994

ラ･サール高等学校

Committee Memberships

Oct, 2020 - Present

Frontiers in Neuroanatomy, Guest Associate Editor
May, 2014 - Present

評議委員, 日本臨床分子形態学会
Aug, 2021 - Aug, 2022

第32回電顕サマースクール実行委員, 日本顕微鏡学会
Jun, 2018 - Jun, 2019

第75回学術集会プログラム委員, 日本顕微鏡学会
Aug, 2018 - Aug, 2018

第29回電顕サマースクール in 信州松本実行委員, 日本顕微鏡学会

Awards

Papers

Kynureninase deficiency ameliorated monocytic recruitment and severity in a mouse model of multiple sclerosis.

Koyo Yoshidomi, Kazuo Kunisawa, Masaya Hasegawa, Yuki Kon, Aika Kosuge, Moeka Tanabe, Haruto Ojika, Yasuko Yamamoto, Hidetsugu Fujigaki, Suwako Fujigaki, Hiroyuki Tezuka, Sei Saitoh, Kanako Kumamoto, Masanori Kugita, Shizuko Nagao, Kuniaki Saito, Toshitaka Nabeshima, Akihiro Mouri

Neurochemistry international, 195 106141-106141, Mar 5, 2026 Peer-reviewed

Multiple 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.
Altered ciliary morphology reduces mechanosensation in a cystic kidney model as indicated by a mathematical model.

Kanako Kumamoto, Hiroyuki Kagami, Sei Saitoh, Shiori Yamada, Mami Matsumoto, Nobuhiko Ohno

Scientific reports, Mar 1, 2026 Peer-reviewed
Complement proteins associated with circulatory and glomerular IgA-containing immune complexes in patients with IgA nephropathy

Scientific Reports, Nov, 2025 Peer-reviewed
A zebrafish model of diabetic nephropathy shows hyperglycemia, proteinuria and activation of the PI3K/Akt pathway.

Liqing Zang, Sei Saitoh, Kan Katayama, Weibin Zhou, Norihiro Nishimura, Yasuhito Shimada

Disease models & mechanisms, 17(5), May 1, 2024 Peer-reviewed

Diabetic nephropathy (DN), as a complication of diabetes, is a substantial healthcare challenge owing to the high risk of morbidity and mortality involved. Although significant progress has been made in understanding the pathogenesis of DN, more efficient models are required to develop new therapeutics. Here, we created a DN model in zebrafish by crossing diabetic Tg(acta1:dnIGF1R-EGFP) and proteinuria-tracing Tg(l-fabp::VDBP-GFP) lines, named zMIR/VDBP. Overfed adult zMIR/VDBP fish developed severe hyperglycemia and proteinuria, which were not observed in wild-type zebrafish. Renal histopathology revealed human DN-like characteristics, such as glomerular basement membrane thickening, foot process effacement and glomerular sclerosis. Glomerular dysfunction was restored upon calorie restriction. RNA sequencing analysis demonstrated that DN zebrafish kidneys exhibited transcriptional patterns similar to those seen in human DN pathogenesis. Notably, the phosphatidylinositol 3-kinase (PI3K)/protein kinase B (Akt) signaling pathway was activated, a phenomenon observed in the early phase of human DN. In addition, metformin improved hyperglycemia and proteinuria in DN zebrafish by modulating Akt phosphorylation. Our results indicate that zMIR/VDBP fish are suitable for elucidating the mechanisms underlying human DN and could be a powerful tool for therapeutic discovery.
Ido2 deficiency exacerbates motor impairment and reduces aryl hydrocarbon receptor activity through decreased kynurenine in a chronic demyelinating mouse model.

Kunisawa K, Hara M, Yoshidomi K, Kon Y, Yamamoto Y, Fujigaki S, Wulaer B, Kosuge A, Tanabe M, Saitoh S, Takahashi K, Saito K, Nabeshima T, Mouri A

Molecular Neurobiology., May, 2024 Peer-reviewed

Misc.

IgA腎症における糸球体とIgA免疫複合体のプロテオミクス

辻雄大, 大山友香子, 齊藤成, 平山将也, 坪井直毅, 高橋和男

日本腎臓学会誌(Web), 67(4), 2025
レーザーマイクロダイセクション法を用いたIgA腎症のヒト糸球体プロテオミクス

齊藤成, 辻雄大, 大山友香子, 大山友香子, 平山将也, 平山将也, 坪井直毅, 高橋和男, 高橋和男

日本解剖学会総会・全国学術集会抄録集(CD-ROM), 129th, 2024
レーザーマイクロダイセクション法を用いたIgA腎症の糸球体プロテオーム解析

齊藤成, 辻雄大, 大山友香子, 平山将也, 坪井直毅, 高橋和男, 大山友香子, 平山将也, 高橋和男

日本臨床分子形態学会総会・学術集会講演プログラム・要旨集, 55th, 2023
RNAヘリカーゼDdx20はオリゴデンドロサイト最終分化に必須である

竹林浩秀, SIMANKOVA Anna, 備前典久, 齊藤成, 芝田晋介, 大野伸彦, 阿部学, 崎村建司

日本解剖学会総会・全国学術集会抄録集(CD-ROM), 127th, 2022
Depression-like behaviors induced by chronic social defeat stress in association with myelin abnormalities in the corpus callosum through microglial activation.

Yumika Sugawara, Kunisawa Kazuo, Iida Tsubasa, Saitoh Sei, Kosuge Aika, Bolati Wulaer, Yamamoto Yasuko, Saito Kuniaki, Mouri Akihiro, Nabeshima Toshitaka

Proceedings for Annual Meeting of The Japanese Pharmacological Society, 94 3-O-E2-2, 2021

White matter abnormalities have been implicated in psychiatric diseases such as major depressive disorder (MDD) ; however, the underlying mechanisms remain poorly understood. The structure and function of the corpus callosum are particularly vulnerable to stress, which may lead to MDD. In the present study, we investigated whether chronic social defeat stress (CSDS) induces myelin abnormalities of the corpus callosum through inflammation that contributes to the pathogenesis of MDD. To produce CSDS, the adult C57BL/6J mouse was exposed to an aggressor ICR mouse for 10 consecutive days. CSDS decreased mature oligodendrocytes in the corpus callosum, and persistently developed depression-like behaviors such as increased immobility in the forced swimming test and impaired social interaction. On transmission electron microscopy, myelin abnormalities and axonal degeneration were observed with necrosis-like cell death of oligodendrocytes in the corpus callosum. Interestingly, CSDS significantly increased the Gasdermin D (Gsdmd), a marker of pyroptosis, concomitantly with enhanced IL-1β production in the corpus callosum. Administration of IL-1β inhibitor prevented the decrease of oligodendrocytes and CSDS-induced depression-like behaviors. These findings suggest that IL-1β acts as a crucial mediator of oligodendroglial pyroptosis induced by the CSDS, which may be responsible for the development of MDD.

Books and Other Publications

Correlative Light-Electron Microscopy (CLEM) and 3D Volume Imaging of Serial Block-Face Scanning Electron Microscopy (SBF-SEM) of Langerhans Islets Electron Microscopy - Novel Microscopy Trends

Saitoh Sei (Role: Contributor)

IntechOpen: Electron Microscopy - Novel Microscopy Trends, Sep, 2018
Immunolocalization of phospho-Arg- directed protein kinase-substrate in hypoxic kidneys.

Saitoh S, Terada N, Ohno N, Saitoh Y, Ohno S (Role: Contributor, pp 135-140.)

In Vivo Cryotechnique in Biomedical Research and Application for Bioimaging of Living Animal Organs, 2016
Distribution of immunoglobulin-producing cells in immunized mouse spleens.

Saitoh S, Terada N, Ohno N, Ohno S (Role: Contributor, pp 51-56.)

In Vivo Cryotechnique in Biomedical Research and Application for Bioimaging of Living Animal Organs, 2016
「免疫組織化学と光イメージングへの凍結技法の応用」

大野伸彦, 齊藤百合花, 寺田信生, 齊藤成, 志茂聡, 藤井靖, 大野伸一

JSHC出版 (日本組織細胞化学学会編), 2015
「電顕用試料作製法の基礎と応用:動物生体内臓器の“真の機能形態像"を探る」

大野伸一, 大野伸彦, 齊藤成, 齊藤百合花, 藤井靖久 (Role: Joint author, P131-147)

JSHC出版 (日本組織細胞化学学会編), 2015
「免疫染色のための固定試料作製法:凍結技法の意義」

大野伸一, 寺田信生, 大野伸彦, 齊藤百合花, 齊藤成, 藤井靖久 (Role: Joint author, P1-10)

JSHC出版 (日本組織細胞化学学会編), 2012
Cryotechniques for Preparation of Animal Tissues for Immunoelectron Microscopy.

Ohno S, Ohno N, Terada N, Ssitoh S, Saitoh Y, Fujii Y (Role: Joint author, p167-179.)

Immunoelectron Microscopy: Methods and Protocols ( Humana Press ), 2010
「種々の凍結技法の免疫組織化学的応用」

寺田信生, 齊藤成, 齊藤百合花, 大野伸彦, 藤井靖久, 大野伸一 (Role: Joint author, P29-38)

JSHC出版 (日本組織細胞化学学会編), 2010
種々の凍結技法と凍結置換固定法の基礎と応用

大野伸一, 寺田信生, 大野伸彦, 齊藤成, 齊藤百合花, 藤井靖久 (Role: Joint author, P179-186)

JSHC出版 (日本組織細胞化学学会編), 2009
免疫組織化学法の基礎と新展開

大野伸一, 寺田信生, 大野伸彦, 齊藤成, 藤井靖久 (Role: Joint author)

JSHC出版 (日本組織細胞化学会編), 2007

Teaching Experience

統合講義 (臨床解剖学, 人体発生学) (山梨大学医学部)
肉眼解剖学 (帝京科学大学)
人体発生学 (藤田医科大学医学部)
組織学 (山梨大学医学部, 藤田医科大学医学部, 帝京科学大学)
神経解剖学 (山梨大学医学部)

Professional Memberships

Research Projects

網羅的プロテオミクスが解明するIgA腎症の糸球体メサンギウム細胞死

2023 - 2025

齊藤成
前向き研究に向けたIgA腎症の組織学的重症度分類の解析プラットフォームの構築

科学研究費助成事業基盤研究(C), 日本学術振興会, Apr, 2020 - Mar, 2023

齊藤成
２型糖尿病性腎症モデルゼブラフィッシュの構築および治療標的遺伝子の探索

基盤(C) （分担), 科研費, Apr, 2018 - Mar, 2020

臧黎清, Zang, Liqing
上皮間葉転換に着目した新規バイオマーカー探索による脳、腎糖尿病疾患の治療法開発

基盤(C), 科研費, Apr, 2016 - Mar, 2020

齊藤成
腎尿細管障害における細胞内Na+制御とミトコンドリア分裂・融合の役割の解明

若手研究(B), 科研費, Apr, 2013 - Mar, 2014

齊藤成

Industrial Property Rights

特開2017-166898 染色方法および観察方法

齊藤成, 高木孝士

Social Activities

愛知県消防学校解剖学講師

Lecturer

2018 - Present
山梨県教育職員免許法認定講習解剖学講師

Lecturer

山梨県, Jul, 2015

To the list screen