Updated on 2024/10/04

Information

 

写真a

 
FUJII SHINSUKE
 
Organization
Faculty of Dental Science Department of Dental Science Associate Professor
School of Dentistry Department of Dentistry(Joint Appointment)
Graduate School of Dental Science (Joint Appointment)
Graduate School of Dental Science Department of Dental Science(Joint Appointment)
Title
Associate Professor
Contact information
メールアドレス
Profile
研究:歯の発生およびがん形成のメカニズムの解析を行っている。 教育:大学院生に研究指導を行っている。
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Degree

  • Ph.D.

Research History

  • 九州大学 大学院歯学研究院口腔病理学研究分野 准教授

    2024.7 - Present

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  • Kyushu University Lecturer

    2020.4 - 2024.6

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  • 平成23年4月〜平成24年3月 特任研究員・大阪大学大学院医学系研究科・分子病態生化学 平成24年4月〜平成26年9月 特任助教(常勤)・大阪大学・未来戦略機構第二部門 平成24年4月〜平成28年3月 招へい教員・大阪大学大学院医学系研究科・分子病態生化学 平成26年10月〜平成28年3月 特任助教(常勤)・大阪大学医学部・医学科教育センター

Education

  • Kyushu University   Graduate School of Dental Science

    - 2007.3

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  • Kyushu University   School of Dentistry

    - 2003.3

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Research Interests・Research Keywords

  • Research theme:Arl4cががん形成に与える影響

    Keyword:Arl4cががん形成に与える影響

    Research period: 2024

  • Research theme:Wntシグナルが唾液腺の発生に与える影響

    Keyword:Wntシグナルが唾液腺の発生に与える影響

    Research period: 2024

  • Research theme:TGF-β1がヒト歯根膜細胞の増殖および分化に与える影響

    Keyword:TGF-β1がヒト歯根膜細胞の増殖および分化に与える影響

    Research period: 2024

  • Research theme:The expression of Arl4c and its function in tumorigenesis.

    Keyword:Arl4c, Tumorigenesis

    Research period: 2012.4

  • Research theme:The effect of Wnt signaling on salivary gland development.

    Keyword:Wnt signaling, salivary gland

    Research period: 2011.4 - 2016.5

  • Research theme:The effects of TGF-β1 on the proliferation and differentiation of human periodontal ligament cells

    Keyword:TGF-β1、periodontal ligament cell

    Research period: 2008.4

  • Research theme:Establishment of human periodontal ligament stem/progenitor cell lines and its characterization

    Keyword:stem/progenitor cell, periodontal ligament cell

    Research period: 2006.4 - 2008.3

  • Research theme:Immortalization of human periodontal ligament cells

    Keyword:Immortalization. Periodontal ligament

    Research period: 2003.4 - 2006.3

Awards

  • 第63回学術奨励賞

    2023.6   公益財団法人 UBE学術奨励賞   唾液腺悪性腫瘍(腺様嚢胞癌)における「癌細胞-神経連関」による腫瘍形成機構の解明

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  • Jeremy Jass Prize for Research Excellence in Pathology in 2021

    2023.1   The Journal of Pathology   YAP signaling induces PIEZO1 to promote oral squamous cell carcinoma cell proliferation

    Kana Hasegawa, Shinsuke Fujii, Corresponding author, Shinji Matsumoto, Yudai Tajiri, Akira Kikuchi, Tamotsu Kiyoshima

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  • 九大歯学優秀研究者賞(IF部門)

    2022.6   九州大学歯学研究院等   「RAF1–MEK/ERK pathway-dependent ARL4C expression promotes ameloblastoma cell proliferation and osteoclast formation」

  • 第67回日本病理学会秋期特別総会 学術研究賞(A演説)

    2021.2   日本病理学会   口腔癌において異常活性化したシグナル伝達とその機能解析

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    口腔がんにおいて異常活性化したシグナル伝達とその機能解析を行なった。2つの異なるアプローチ(組織発生からアプローチした癌研究、および腫瘍実質-間質相互作用による癌のシグナル伝達異常)から、口腔がんにおいてArl4cシグナルの異常活性化は発がんに関与するだけでなく治療標的となること、および口腔がんにおいてCaチャネルを介したシグナル伝達が異常に活性化していることが明らかにした。

  • Dentsply賞

    2009.10   日本歯科保存学会   TGF-beta1がヒト歯根膜細胞および前駆細胞の増殖および分化に及ぼす影響

  • 優秀論文賞

    2007.5   日本歯内療法学会  

  • 藤野賞

    2007.4   九州大学歯学府   ヒト歯根膜前駆細胞株の樹立とキャラクタリゼーション

  • デンツプライ賞

    2006.5   株式会社デンツプライ   ヒト不死化歯根膜クローン細胞におけるEMDおよびbFGFが石灰化誘導に及ぼす影響

  • 日本歯科保存学会奨励賞

    2006.4   日本歯科保存学会   Establishing and characterizing human periodontal ligament fibroblasts immortalized by SV40T-antigen and hTERT gene transfer

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Papers

  • Wnt/β-catenin-YAP axis in the pathogenesis of primary intraosseous carcinoma NOS, deriving from odontogenic keratocyst. Reviewed International journal

    Yusuke Nakako, Kana Hasegawa, Shinsuke Fujii, Yukiko Kami, Taiki Sakamoto, Mizuki Sakamoto, Masafumi Moriyama, Kari J Kurppa, Kristiina Heikinheimo, Kazunori Yoshiura, Shintaro Kawano, Tamotsu Kiyoshima

    Pathology, research and practice   260   155420 - 155420   2024.6   ISSN:03440338

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    Odontogenic tumors (OGTs), which originate from cells of odontogenic apparatus and their remnants, are rare entities. Primary intraosseous carcinoma NOS (PIOC), is one of the OGTs, but it is even rarer and has a worse prognosis. The precise characteristics of PIOC, especially in immunohistochemical features and its pathogenesis, remain unclear. We characterized a case of PIOC arising from the left mandible, in which histopathological findings showed a transition from the odontogenic keratocyst to the carcinoma. Remarkably, the tumor lesion of this PIOC prominently exhibits malignant attributes, including invasive growth of carcinoma cell infiltration into the bone tissue, an elevated Ki-67 index, and lower signal for CK13 and higher signal for CK17 compared with the non-tumor region, histopathologically and immunohistopathologically. Further immunohistochemical analyses demonstrated increased expression of ADP-ribosylation factor (ARF)-like 4c (ARL4C) (accompanying expression of β-catenin in the nucleus) and yes-associated protein (YAP) in the tumor lesion. On the other hand, YAP was expressed and the expression of ARL4C was hardly detected in the non-tumor region. In addition, quantitative RT-PCR analysis using RNAs and dot blot analysis using genomic DNA showed the activation of Wnt/β-catenin signaling and epigenetic alterations, such as an increase of 5mC levels and a decrease of 5hmC levels, in the tumor lesion. A DNA microarray and a gene set enrichment analysis demonstrated that various types of intracellular signaling would be activated and several kinds of cellular functions would be altered in the pathogenesis of PIOC. Experiments with the GSK-3 inhibitor revealed that β-catenin pathway increased not only mRNA levels of ankyrin repeat domain1 (ANKRD1) but also protein levels of YAP and transcriptional co-activator with PDZ-binding motif (TAZ) in oral squamous cell carcinoma cell lines. These results suggested that further activation of YAP signaling by Wnt/β-catenin signaling may be associated with the pathogenesis of PIOC deriving from odontogenic keratocyst in which YAP signaling is activated.

    DOI: 10.1016/j.prp.2024.155420

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  • The IL-1β-p65 axis stimulates quiescent odontogenic epithelial cell rests via TGF-β signalling to promote cell proliferation of the lining epithelia in radicular cysts: A laboratory investigation. Reviewed International journal

    Ryoko Nagano, Yusuke Nakako, Shinsuke Fujii, Shintaro Kawano, Hidefumi Maeda, Tamotsu Kiyoshima

    International endodontic journal   57 ( 3 )   344 - 354   2024.3   ISSN:0143-2885 eISSN:1365-2591

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    AIM: Cyst formation of the jaws is frequently accompanied by the proliferation of odontogenic epithelial cells located in the periodontal ligament (PDL), which consists of heterozygous cells and includes the most fibroblasts. The lining epithelium of radicular cyst, an odontogenic cyst of inflammatory origin, is derived from the proliferation of the remnants of the Hertwig epithelial root sheath (odontogenic epithelial cell rests of Malassez; ERMs) in the PDL. ERMs are maintained at a lower proliferative state under physiological conditions, but the regulatory mechanisms underlying the inflammation-dependent enhanced-proliferative capabilities of ERMs are not fully understood. The aim of this study was to evaluate the effects of cytokine pathway association between TGF-β signalling and IL-1β signalling on the regulation of odontogenic epithelial cell proliferation using radicular cyst pathological specimens and odontogenic epithelial cell lines. METHODOLOGY: Immunofluorescence analyses were performed to clarify the expression levels of Smad2/3 and Ki-67 in ERMs of 8-week-old mouse molar specimens. In radicular cyst (n = 52) and dentigerous cysts (n = 6) specimens from human patients, the expression of p65 (a main subunit of NF-κB), Smad2/3 and Ki-67 were investigated using immunohistochemical analyses. Odontogenic epithelial cells and PDL fibroblastic cells were co-cultured with or without an inhibitor or siRNAs. Odontogenic epithelial cells were cultured with or without TGF-β1 and IL-1β. The proliferative capabilities and Smad2 phosphorylation levels of odontogenic epithelial cells were examined. RESULTS: Immunohistochemically, Smad2/3-positivity was increased, and p65-positivity and Ki-67-positivity were decreased both in ERMs and in the epithelial cells in dentigerous cysts, a non-inflammatory developmental cyst. In contrast, p65-positive cells, along with the expression of Ki-67, were increased and Smad2/3-positive cells were decreased in the lining epithelia of radicular cysts. Co-culture experiments with odontogenic epithelial cells and PDL fibroblastic cells revealed that PDL cells-derived TGF-β1/2 and their downstream signalling suppressed odontogenic epithelial cell proliferation. Moreover, TGF-β1 stimulation induced Smad2 phosphorylation and suppressed odontogenic epithelial cell proliferation, while IL-1β stimulation reversed these phenotypes through p65 transactivation. CONCLUSIONS: These results suggest that IL-1β-p65 signalling promotes odontogenic epithelial cell proliferation through suppressing TGF-β-Smad2 signalling, which would be involved in the pathogenesis of radicular cysts.

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  • Wnt/β-catenin-C-kit axis may play a role in adenoid cystic carcinoma prognostication Reviewed International journal

    Shinsuke Fujii, Kana Hasegawa, Takashi Maehara, Kari J Kurppa, Kristiina Heikinheimo, Kristy A. Warner, Satoshi Maruyama, Yudai Tajiri, Jacques E. Nör, Jun-ichi Tanuma, Shintaro Kawano, Tamotsu Kiyoshima

    Pathology - Research and Practice   254   155148 - 155148   2024.1   ISSN:0344-0338 eISSN:1618-0631

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    DOI: 10.1016/j.prp.2024.155148

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  • Arl4c is involved in tooth germ development through osteoblastic/ameloblastic differentiation. Reviewed International journal

    Thinh Thi Kim Truong, Shinsuke Fujii, Ryoko Nagano, Kana Hasegawa, Megumi Kokura, Yuta Chiba, Keigo Yoshizaki, Satoshi Fukumoto, Tamotsu Kiyoshima

    Biochemical and biophysical research communications   679   167 - 174   2023.9   ISSN:0006-291X eISSN:1090-2104

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    Authorship:Corresponding author   Language:English   Publishing type:Research paper (scientific journal)  

    Murine tooth germ development proceeds in continuous sequential steps with reciprocal interactions between the odontogenic epithelium and the adjacent mesenchyme, and several growth factor signaling pathways and their activation are required for tooth germ development. The expression of ADP-ribosylation factor (Arf)-like 4c (Arl4c) has been shown to induce cell proliferation, and is thereby involved in epithelial morphogenesis and tumorigenesis. In contrast, the other functions of Arl4c (in addition to cellular growth) are largely unknown. Although we recently demonstrated the involvement of the upregulated expression of Arl4c in the proliferation of ameloblastomas, which have the same origin as odontogenic epithelium, its effect on tooth germ development remains unclear. In the present study, single-cell RNA sequencing (scRNA-seq) analysis revealed that the expression of Arl4c, among 17 members of the Arf-family, was specifically detected in odontogenic epithelial cells, such as those of the stratum intermedium, stellate reticulum and outer enamel epithelium, of postnatal day 1 (P1) mouse molars. scRNA-seq analysis also demonstrated the higher expression of Arl4c in non-ameloblast and inner enamel epithelium, which include immature cells, of P7 mouse incisors. In the mouse tooth germ rudiment culture, treatment with SecinH3 (an inhibitor of the ARNO/Arf6 pathway) reduced the size, width and cusp height of the tooth germ and the thickness of the eosinophilic layer, which would involve the synthesis of dentin and enamel matrix organization. In addition, loss-of-function experiments using siRNAs and shRNA revealed that the expression of Arl4c was involved in cell proliferation and osteoblastic cytodifferentiation in odontogenic epithelial cells. Finally, RNA-seq analysis with a gene set enrichment analysis (GSEA) and Gene Ontology (GO) analysis showed that osteoblastic differentiation-related gene sets and/or GO terms were downregulated in shArl4c-expressing odontogenic epithelial cells. These results suggest that the Arl4c-ARNO/Arf6 pathway axis contributes to tooth germ development through osteoblastic/ameloblastic differentiation.

    DOI: 10.1016/j.bbrc.2023.09.014

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  • The role of Wnt, ARL4C, and Sema3A in developmental process and disease pathogenesis. Invited Reviewed International journal

    Shinsuke Fujii, Tamotsu Kiyoshima

    Pathology international   73 ( 6 )   217 - 233   2023.6   ISSN:1320-5463 eISSN:1440-1827

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    Various types of tumors, including malignant and benign ones, occur in the oral cavity. These arise from the mucosal epithelium, odontogenic epithelium, and salivary gland. To date, few major driver events in oral tumors have been identified. Accordingly, molecular targets in anti-tumor therapy for oral tumors are lacking. We focused on elucidating the function of aberrantly activated signal transduction related to oral tumor formation, especially in oral squamous cell carcinoma, ameloblastoma, and adenoid cystic carcinoma, which are raised as common oral tumors. Wnt/β-catenin-dependent pathway is involved in the developmental process, organ homeostasis and disease pathogenesis through regulating various cellular functions by enhancing transcriptional activity. Recently, we identified ADP-ribosylation factor (ARF)-like 4c (ARL4C) and Semaphorin 3A (Sema3A), the expression of which is regulated by Wnt/β-catenin-dependent pathway, and characterized their functions in the developmental process and tumor formation. This review highlights the recent advances in understanding the roles of Wnt/β-catenin-dependent pathway, ARL4C and Sema3A, as determined by pathological and experimental studies.

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  • Stepwise activation of p63 and the MEK/ERK pathway induces the expression of ARL4C to promote oral squamous cell carcinoma cell proliferation. Reviewed International journal

    Dania Zuhier Ragheb Alkhatib, Thinh Thi Kim Truong, Shinsuke Fujii, Kana Hasegawa, Ryoko Nagano, Yudai Tajiri, Tamotsu Kiyoshima

    Pathology, research and practice   246   154493 - 154493   2023.6   ISSN:0344-0338 eISSN:1618-0631

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    Carcinogenesis is a multistep process wherein cells accumulate multiple genetic alterations and progress to a more malignant phenotype. It has been proposed that sequential accumulation of gene abnormalities in specific genes drives the transition from non-tumorous epithelia through a preneoplastic lesion/benign tumor to cancer. Histologically, oral squamous cell carcinoma (OSCC) progresses in multiple ordered steps that begin with mucosal epithelial cell hyperplasia, which is followed by dysplasia, carcinoma in situ and invasive carcinoma. It is therefore hypothesized that genetic alteration-mediated multistep carcinogenesis would be involved in the development of OSCC; however, the detailed molecular mechanisms are unknown. We clarified the comprehensive gene expression patterns and carried out an enrichment analysis using DNA microarray data from a pathological specimen of OSCC (including a non-tumor region, carcinoma in situ lesion and invasive carcinoma lesion). The expression of numerous genes and signal activation were altered in the development of OSCC. Among these, the p63 expression was increased and the MEK/ERK-MAPK pathway was activated in carcinoma in situ lesion and in invasive carcinoma lesion. Immunohistochemical analyses revealed that p63 was initially upregulated in carcinoma in situ and ERK was sequentially activated in invasive carcinoma lesions in OSCC specimens. ADP-ribosylation factor (ARF)-like 4c (ARL4C), the expression of which is reportedly induced by p63 and/or the MEK/ERK-MAPK pathway in OSCC cells, has been shown to promote tumorigenesis. Immunohistochemically, in OSCC specimens, ARL4C was more frequently detected in tumor lesions, especially in invasive carcinoma lesions, than in carcinoma in situ lesions. Additionally, ARL4C and phosphorylated ERK were frequently merged in invasive carcinoma lesions. Loss-of-function experiments using inhibitors and siRNAs revealed that p63 and MEK/ERK-MAPK cooperatively induce the expression of ARL4C and cell growth in OSCC cells. These results suggest that the stepwise activation of p63 and MEK/ERK-MAPK contributes to OSCC tumor cell growth through regulation of ARL4C expression.

    DOI: 10.1016/j.prp.2023.154493

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  • Wnt signaling promotes tooth germ development through YAP1-TGF-β signaling. Invited Reviewed International journal

    Nagano, Ryoko; Fujii, Shinsuke; Hasegawa, Kana; Maeda, Hidefumi; Kiyoshima, Tamotsu

    BIOCHEMICAL AND BIOPHYSICAL RESEARCH COMMUNICATIONS   630   64 - 70   2022.11   ISSN:0006-291X eISSN:1090-2104

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    Tooth germ development involves continuous and sequential steps with reciprocal interactions between odontogenic epithelium and the adjacent mesenchyme. Several growth factors, including Wnt, are essential for tooth germ development. Molecular mechanisms underlying Wnt/β-catenin-regulated tooth germ development are poorly understood. In tooth germ rudiments culture, we recently demonstrated that Semaphorin 3A (Sema3A), an axonal guidance factor, stimulation reversed Wnt/β-catenin signaling-dependent decreased cell proliferation but did not completely rescue the morphological anomalies of tooth germ, suggesting that an uncharacterized signaling pathway may be essential in Wnt/β-catenin signaling-dependent tooth germ development. Herein, an enrichment analysis using DNA microarray data, which was obtained in our previous research, revealed that Wnt/β-catenin signaling negatively regulates YAP1 and/or TGF-β signalings. In odontogenic epithelial cells and tooth germ rudiments, Wnt/β-catenin signaling activation reduced YAP1 expression, thereby suppressing YAP1 and TGF-β signalings sequentially. Additionally, YAP1 signaling induced TGF-β2 expression to promote TGF-β signaling in the cells. Finally, Wnt/β-catenin signaling-dependent disorganized tooth germ development, in which YAP1 signaling was suppressed, was reversed by TGF-β stimulation. These results suggest that Wnt/β-catenin signaling contributes to the tooth germ development through YAP1-TGF-β signaling.

    DOI: 10.1016/j.bbrc.2022.09.012

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  • The Semaphorin 3A-AKT axis-mediated cell proliferation in salivary gland morphogenesis and adenoid cystic carcinoma pathogenesis Invited Reviewed International journal

    Shinsuke Fujii, Tatsufumi Fujimoto, Kana Hasegawa, Ryoko Nagano, Takuma Ishibashi, Kari J.Kurppa, Yurie Mikami, Megumi Kokura, Yudai Tajiri, Toshiro Kibe, Hiroko Wada, Naohisa Wada, Shosei Kishida, Yoshinori Higuchi, Tamotsu Kiyoshima.

    Pathology - Research and Practice   236   153991   2022.6   ISSN:0344-0338 eISSN:1618-0631

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    We recently demonstrated that Semaphorin 3 A (Sema3A), the expression of which is negatively regulated by Wnt/β-catenin signaling, promotes odontogenic epithelial cell proliferation, suggesting the involvement of Sema3A in tooth germ development. Salivary glands have a similar developmental process to tooth germ development, in which reciprocal interactions between the oral epithelium and adjacent mesenchyme proceeds via stimulation with several growth factors; however, the role of Sema3A in the development of salivary glands is unknown. There may thus be a common mechanism between epithelial morphogenesis and pathogenesis; however, the role of Sema3A in salivary gland tumors is also unclear. The current study investigated the involvement of Sema3A in submandibular gland (SMG) development and its expression in adenoid cystic carcinoma (ACC) specimens. Quantitative RT-PCR and immunohistochemical analyses revealed that Sema3A was expressed both in epithelium and in mesenchyme in the initial developmental stages of SMG and their expressions were decreased during the developmental processes. Loss-of-function experiments using an inhibitor revealed that Sema3A was required for AKT activation-mediated cellular growth and formation of cleft and bud in SMG rudiment culture. In addition, Wnt/β-catenin signaling decreased the Sema3A expression in the rudiment culture. ACC arising from salivary glands frequently exhibits malignant potential. Immunohistochemical analyses of tissue specimens obtained from 10 ACC patients showed that Sema3A was hardly observed in non-tumor regions but was strongly expressed in tumor lesions, especially in myoepithelial neoplastic cells, at high frequencies where phosphorylated AKT expression was frequently detected. These results suggest that the Sema3A-AKT axis promotes cell growth, thereby contributing to morphogenesis and pathogenesis, at least in ACC, of salivary glands.

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  • Clear cell squamous cell carcinoma of the tongue exhibits characteristics as an undifferentiated squamous cell carcinoma Reviewed International journal

    Kana Hasegawa, Shinsuke Fujii, Kari J Kurppa, Takashi Maehara, Kazunari Oobu, Seiji Nakamura, Tamotsu Kiyoshima

    Pathology - Research and Practice   235   153909 - 153909   2022.4   ISSN:03440338

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    Clear cell squamous cell carcinoma (CCSCC), where cells show abundant clear cytoplasm, -is a variant of squamous cell carcinoma (SCC) and a rare entity in the oral cavity. The characteristics of CCSCC, especially in immunohistochemical features, remain unclear. We characterized a case of CCSCC arising from the oral mucosal epithelium of tongue, where the clear cell lesion accounted for a predominant portion of the tumor. This CCSCC, which was partially surrounded by conventional SCC, exhibited cellular atypia immunohistopathologically and histopathologically with a high Ki-67 index, increased number of mitotic figures and enlarged nuclei. Intravascular invasion of the carcinoma cells was also observed. Furthermore, the CCSCC recurred and metastasized to the cervical lymph nodes and both lungs three months after resection. Immunohistochemical analyses demonstrated decreased expression of p40 (an isoform of SCC marker p63), ADP-ribosylation factor (ARF)-like 4c (ARL4C), yes-associated protein (YAP) and 5-methylcytosine (5mC) in the CCSCC lesion compared with the surrounding SCC lesion, where the expression of ARL4C was upregulated compared with non-tumor region and YAP showed nuclear translocation. In addition, siRNA loss-of-function experiments revealed that p63 expression was required for ARL4C expression and DNA methylation was induced by p63 and YAP/transcriptional co-activator with PDZ-binding motif (TAZ) signaling in oral SCC cell lines. These results suggest that CCSCC, in which several markers of SCC-associated intracellular signaling pathways are downregulated, together with evidence of altered epigenetic regulation, is characterized as an undifferentiated SCC variant.

    DOI: 10.1016/j.prp.2022.153909

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  • RAF1-MEK/ERK pathway-dependent ARL4C expression promotes ameloblastoma cell proliferation and osteoclast formation Invited Reviewed International journal

    Fujii, Shinsuke; Ishibashi, Takuma; Kokura, Megumi; Fujimoto, Tatsufumi; Matsumoto, Shinji; Shidara, Satsuki; Kurppa, Kari J.; Pape, Judith; Caton, Javier; Morgan, Peter R.; Heikinheimo, Kristiina; Kikuchi, Akira; Jimi, Eijiro; Kiyoshima, Tamotsu

    JOURNAL OF PATHOLOGY   256 ( 1 )   119 - 133   2022.1   ISSN:0022-3417 eISSN:1096-9896

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    Ameloblastoma is an odontogenic neoplasm characterized by slow intraosseous growth with progressive jaw resorption. Recent reports have revealed that ameloblastoma harbours an oncogenic BRAF V600E mutation with mitogen-activated protein kinase (MAPK) pathway activation and described cases of ameloblastoma harbouring a BRAF V600E mutation in which patients were successfully treated with a BRAF inhibitor. Therefore, the MAPK pathway may be involved in the development of ameloblastoma; however, the precise mechanism by which it induces ameloblastoma is unclear. The expression of ADP-ribosylation factor (ARF)-like 4c (ARL4C), induced by a combination of the EGF-MAPK pathway and Wnt/β-catenin signalling, has been shown to induce epithelial morphogenesis. It was also reported that the overexpression of ARL4C, due to alterations in the EGF/RAS-MAPK pathway and Wnt/β-catenin signalling, promotes tumorigenesis. However, the roles of ARL4C in ameloblastoma are unknown. We investigated the involvement of ARL4C in the development of ameloblastoma. In immunohistochemical analyses of tissue specimens obtained from 38 ameloblastoma patients, ARL4C was hardly detected in non-tumour regions but tumours frequently showed strong expression of ARL4C, along with the expression of both BRAF V600E and RAF1 (also known as C-RAF). Loss-of-function experiments using inhibitors or siRNAs revealed that ARL4C elevation depended on the RAF1-MEK/ERK pathway in ameloblastoma cells. It was also shown that the RAF1-ARL4C and BRAF V600E-MEK/ERK pathways promoted cell proliferation independently. ARL4C-depleted tumour cells (generated by knockdown or knockout) exhibited decreased proliferation and migration capabilities. Finally, when ameloblastoma cells were co-cultured with mouse bone marrow cells and primary osteoblasts, ameloblastoma cells induced osteoclast formation. ARL4C elevation in ameloblastoma further promoted its formation capabilities through the increased RANKL expression of mouse bone marrow cells and/or primary osteoblasts. These results suggest that the RAF1-MEK/ERK-ARL4C axis, which may function in cooperation with the BRAF V600E-MEK/ERK pathway, promotes ameloblastoma development. This article is protected by copyright. All rights reserved.

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  • YAP signaling induces PIEZO1 to promote oral squamous cell carcinoma cell proliferation Reviewed International journal

    Kana Hasegawa, Shinsuke Fujii, Shinji Matsumoto, Yudai Tajiri, Akira Kikuchi and Tamotsu Kiyoshima

    JOURNAL OF PATHOLOGY   253 ( 1 )   80 - 93   2021.1

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    DOI: 10.1002/path.5553

    Repository Public URL: http://hdl.handle.net/2324/4481560

  • The TRPV4-AKT axis promotes oral squamous cell carcinoma cell proliferation via CaMKII activation. Reviewed International journal

    Fujii S, Tajiri Y, Hasegawa K, Matsumoto S, Yoshimoto RU, Wada H, Kishida S, Kido MA, Yoshikawa H, Ozeki S, Kiyoshima T

    Lab Invest   2019.12

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    Repository Public URL: http://hdl.handle.net/2324/4123614

  • Wnt/beta-catenin signaling, which is activated in odontomas, reduces Sema3A expression to regulate odontogenic epithelial cell proliferation and tooth germ development Invited Reviewed International journal

    Fujii, Shinsuke; Nagata, Kengo; Matsumoto, Shinji; Kohashi, Ken-ichi; Kikuchi, Akira; Oda, Yoshinao; Kiyoshima, Tamotsu; Wada, Naohisa

    SCIENTIFIC REPORTS   9   2019.3

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    DOI: 10.1038/s41598-019-39686-1

  • Chemically Modified Antisense Oligonucleotide Against ARL4C Inhibits Primary and Metastatic Liver Tumor Growth Reviewed International journal

    Harada, Takeshi; Matsumoto, Shinji; Hirota, Suguru; Kimura, Hirokazu; Fujii, Shinsuke; Kasahara, Yuuya; Gon, Hidetoshi; Yoshida, Toshihiko; Itoh, Tomoo; Haraguchi, Naotsugu; Mizushima, Tsunekazu; Noda, Takehiro; Eguchi, Hidetoshi; Nojima, Satoshi; Morii, Eiichi; Fukumotol, Takumi; Obika, Satoshi; Kikuchi, Akira

    MOLECULAR CANCER THERAPEUTICS   18 ( 3 )   602 - 612   2019.3

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    DOI: 10.1158/1535-7163.MCT-18-0824

  • Low grade myofibroblastic sarcoma arising in the tip of the tongue with intravascular invasion A case report Reviewed

    Yurie Mikami, Shinsuke Fujii, Kenichi Kouhashi, Yuichi Yamada, Masafumi Moriyama, Shintarou Kawano, Seiji Nakamura, Yoshinao Oda, Tamotsu Kiyoshima

    Oncology Letters   16 ( 3 )   3889 - 3894   2018.9

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    DOI: 10.3892/ol.2018.9115

  • GLI-mediated Keratin 17 expression promotes tumor cell growth through the anti-apoptotic function in oral squamous cell carcinomas. Reviewed International journal

    Mikami Yurie, Fujii Shinsuke, Kengo Nagata, Hiroko Wada, Kana Hasegawa, Misaki Abe, Reiko U. Yoshimoto, Shintaro Kawano, Seiji Nakamura, Tamotsu Kiyoshima

    J Cancer Res Clin Oncol   143 ( 8 )   1381 - 1393   2017.3

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    DOI: 10.1007/s00432-017-2398-2

  • Epigenetic upregulation of ARL4C, due to DNA hypomethylation in the 3’-untranslated region, promotes tumorigenesis of lung squamous cell carcinoma Reviewed International journal

    Fujii S, Shinjo K, Matsumoto S, Harada T, Nojima S, Sato S, Usami Y, Toyosawa S, Morii E, Kondo Y, Kikuchi A

    6 ( 49 )   81571 - 81587   2016.10

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    DOI: doi: 10.18632/oncotarget.13147.

  • The Wnt-Myb pathway suppresses KIT expression to control the timing of salivary proacinar differentiation and duct formation. Reviewed International journal

    Matsumoto S, Kurimoto T, Taketo M, Fujii S, Kikuchi A

    Development.   2016.4

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  • Arl4c expression in colorectal and lung cancers promotes tumorigenesis and may represent a novel therapeutic target. Invited Reviewed International journal

    Fujii S, Matsumoto S, Nojima S, Morii E, Kikuchi A

    Oncogene   34   4834 - 4844   2015.9

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  • The P2Y2 receptor promotes Wnt3a- and EGF-induced epithelial tubular formation by IEC6 cells by binding to integrins. Reviewed International journal

    Ibuka S, Matsumoto S, Fujii S, Kikuchi A

    J Cell Sci.   128 ( 11 )   2156 - 2158   2015.6

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    DOI: 10.1242/jcs.169060.

  • A combination of Wnt and growth factor signaling induces Arl4c expression to form epithelial tubular structures. Reviewed International journal

    Matsumoto S, Fujii S, Sato A, Ibuka S, Kagawa Y, Ishii M, Kikuchi A

    EMBO J   33   702 - 718   2014.4

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  • The effects of TGF-β1 on the proliferation and differentiation of human periodontal ligament cells and a human periodontal ligament stem/progenitor cell line. Reviewed International journal

    2011.11

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  • Investigating a clonal human periodontal ligament progenitor/stem cell line in vitro and in vivo. Reviewed International journal

    Fujii S, Maeda H, Wada N, Tomokiyo A, Saito M, Akamine A

    J Cell Physiol   2008.3

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  • Establishing and characterizing human periodontal ligament fibroblasts immortalized by SV40T-antigen and hTERT gene transfer. International journal

    Shinsuke Fujii., Hidefumi Maeda., Naohisa Wada., Yoshio Kano., Akifumi Akamine.

    Cell and tissue research   2006.1

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  • A Case of Myxoid Pleomorphic Liposarcoma with Rhabdoid Cells: A Diagnostic Pitfall

    Arai, T; Kato, I; Kawabata, Y; Tsujimoto, S; Ishikawa, Y; Kato, S; Takeyama, M; Yamanaka, S; Kohashi, K; Oda, Y; Fujii, S

    INTERNATIONAL JOURNAL OF SURGICAL PATHOLOGY   10668969241226695   2024.2   ISSN:1066-8969 eISSN:1940-2465

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  • Expansion of CD4+ cytotoxic T lymphocytes with specific gene expression patterns may contribute to suppression of tumor immunity in oral squamous cell carcinoma: single-cell analysis and in vitro experiments. Reviewed International journal

    Hu Chen, Junsei Sameshima, Shiho Yokomizo, Tomoki Sueyoshi, Haruki Nagano, Yuka Miyahara, Taiki Sakamoto, Shinsuke Fujii, Tamotsu Kiyoshima, Thomas Guy, Seiji Nakamura, Masafumi Moriyama, Naoki Kaneko, Shintaro Kawano

    Frontiers in immunology   14   1305783 - 1305783   2023.11   ISSN:1664-3224

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    BACKGROUND: Cancer immunotherapy targeting CD8+ T cells has made remarkable progress, even for oral squamous cell carcinoma (OSCC), a heterogeneous epithelial tumor without a substantial increase in the overall survival rate over the past decade. However, the therapeutic effects remain limited due to therapy resistance. Thus, a more comprehensive understanding of the roles of CD4+ T cells and B cells is crucial for more robust development of cancer immunotherapy. METHODS: In this study, we examined immune responses and effector functions of CD4+ T cells, CD8+ T cells and B cells infiltrating in OSCC lesions using single-cell RNA sequencing analysis, T cell receptor (TCR) and B cell receptor (BCR) repertoire sequencing analysis, and multi-color immunofluorescence staining. Finally, two Kaplan-Meier curves and several Cox proportional hazards models were constructed for the survival analysis. RESULTS: We observed expansion of CD4+ cytotoxic T lymphocytes (CTLs) expressing granzymes, which are reported to induce cell apoptosis, with a unique gene expression patterns. CD4+ CTLs also expressed CXCL13, which is a B cell chemoattractant. Cell-cell communication analysis and multi-color immunofluorescence staining demonstrated potential interactions between CD4+ CTLs and B cells, particularly IgD- CD27- double negative (DN) B cells. Expansion of CD4+ CTLs, DN B cells, and their contacts has been reported in T and B cell-activated diseases, including IgG4-related disease and COVID-19. Notably, we observed upregulation of several inhibitory receptor genes including CTLA-4 in CD4+ CTLs, which possibly dampened T and B cell activity. We next demonstrated comprehensive delineation of the potential for CD8+ T cell differentiation towards dysfunctional states. Furthermore, prognostic analysis revealed unfavorable outcomes of patients with a high proportion of CD4+ CTLs in OSCC lesions. CONCLUSION: Our study provides a dynamic landscape of lymphocytes and demonstrates a systemic investigation of CD4+ CTL effects infiltrating into OSCC lesions, which may share some pathogenesis reported in severe T and B cell-activated diseases such as autoimmune and infectious diseases.

    DOI: 10.3389/fimmu.2023.1305783

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  • Dopamine is involved in reparative dentin formation through odontoblastic differentiation of dental pulp stem cells. Reviewed International journal

    Shoko Fujino, Sayuri Hamano, Atsushi Tomokiyo, Risa Sugiura, Daiki Yamashita, Daigaku Hasegawa, Hideki Sugii, Shinsuke Fujii, Tomohiro Itoyama, Hirofumi Miyaji, Hidefumi Maeda

    Scientific reports   13 ( 1 )   5668 - 5668   2023.4   ISSN:2045-2322

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    Conventional direct pulp-capping materials induce pulp cells to secrete various biomolecules in pulp tissues that promote reparative dentin formation through induction of odontoblastic differentiation of dental pulp stem cells (DPSCs). However, these biomolecules sometimes induce bone-like dentin with poor sealing properties. Therefore, exploration of biomolecules that allow tight sealing by tubular reparative dentin is required. We recently reported that dopamine (DA) is involved in dentinogenesis. Hence, we investigated the effect of DA on odontoblastic differentiation of DPSCs and reparative dentin formation. Both tyrosine hydroxylase (TH), a DA synthetase, and DA were expressed in odontoblast-like cells in vivo. In vitro, their expression was increased during odontoblastic differentiation of DPSCs. Furthermore, TH-overexpressing DPSCs had promoted odontoblastic differentiation and DA production. Moreover, DA stimulation promoted their differentiation and induced tubular reparative dentin. These results suggest that DA produced by TH is involved in odontoblastic differentiation of DPSCs and has an inductive capacity for reparative dentin formation similar to primary dentin. This study may lead to the development of therapy to preserve vital pulp tissues.

    DOI: 10.1038/s41598-023-32126-1

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  • p130Cas is required for androgen-dependent postnatal development regulation of submandibular glands. Reviewed International journal

    Jing Gao, Aonan Li, Shinsuke Fujii, Fei Huang, Chihiro Nakatomi, Ichiro Nakamura, Hiroaki Honda, Tamotsu Kiyoshima, Eijiro Jimi

    Scientific reports   13 ( 1 )   5144 - 5144   2023.3   ISSN:2045-2322 eISSN:20452322

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    Salivary glands develop through epithelial-mesenchymal interactions and are formed through repeated branching. The Crk-associated substrate protein (p130Cas) serves as an adapter that forms a complex with various proteins via integrin and growth factor signaling, with important regulatory roles in several essential cellular processes. We found that p130Cas is expressed in ductal epithelial cells of the submandibular gland (SMG). We generated epithelial tissue-specific p130Cas-deficient (p130Cas^<Δepi–>) mice and aimed to investigate the physiological role of p130Cas in the postnatal development of salivary glands. Histological analysis showed immature development of granular convoluted tubules (GCT) of the SMG in male p130Cas^<Δepi–> mice. Immunofluorescence staining showed that nuclear-localized androgen receptors (AR) were specifically decreased in GCT cells in p130Cas^<Δepi–> mice. Furthermore, epidermal growth factor-positive secretory granules contained in GCT cells were significantly reduced in p130Cas^<Δepi–> mice with downregulated AR signaling. GCTs lacking p130Cas showed reduced numbers and size of secretory granules, disrupted subcellular localization of the cis-Golgi matrix protein GM130, and sparse endoplasmic reticulum membranes in GCT cells. These results suggest that p130Cas plays a crucial role in androgen-dependent GCT development accompanied with ER-Golgi network formation in SMG by regulating the AR signaling.

    DOI: 10.1038/s41598-023-32390-1

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  • Lipomatous mixed tumor of the skin with cystic formation affecting the upper lip: A case report Invited Reviewed International journal

    Nagano, Ryoko; Fujii, Shinsuke; Wada, Hiroko; Matsumura-Kawashima, Mayu; Mikami, Yurie; Moriyama, Masafumi; Chikui, Toru; Yoshiura, Kazunori; Nakamura, Seiji; Kiyoshima, Tamotsu

    EXPERIMENTAL AND THERAPEUTIC MEDICINE   24 ( 5 )   664 - 664   2022.11   ISSN:17920981 eISSN:17921015

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    Mixed tumor of the skin (MTS) is a rare neoplasm derived from the sweat glands with a reported frequency of 0.01‑0.098% among all primary skin tumors. MTS often occurs in the head and neck region and is characterized by a mixture of epithelial, myoepithelial and stromal components. MTS also shows various morphological patterns, thus the presence of variants with rare components and its rarity make the clinical diagnosis even more difficult. A 47‑year‑old man was referred due to a painless, slowly growing, exophytic swelling intracutaneous mass of the upper lip. Magnetic resonance imaging revealed that the mass was a solid tumor with a fatty component in the proximal portion, while the distal portion was cystic and possibly contained highly viscous fluid. The mass was located between the skin and the orbicularis oris muscle in the upper lip. Excisional biopsy was performed and the lesion showed two intriguing features: A tumor with extensive lipomatous stroma and some large cysts. It was histopathologically diagnosed as lipomatous MTS with cystic formation in the upper lip. No evident signs of recurrence were observed during follow‑up. The present report describes this case and includes a brief literature review of reported cases in the lip, since MTS can be confused with various skin lesions in clinical settings due to this rarity. Recognition by clinicians of different variants of MTSs, including the present case, is important for preventing erroneous diagnosis and treatment.

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  • 大阪大学医学部「MD研究者育成プログラム」10年間の成果とその課題 Reviewed

    河盛 段, 佐田 遼太, 木村 公一, 藤井 慎介, 高橋 剛, 和佐 勝史, 渡部 健二

    医学教育   53 ( Suppl. )   167 - 167   2022.7

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  • Usefulness of reconstructed images of Gd-enhanced 3D gradient echo sequences with compressed sensing for mandibular cancer diagnosis: comparison with CT images and histopathological findings Invited Reviewed International journal

    Kami, Yukiko; Chikui, Toru; Togao, Osamu; Kawano, Shintaro; Fujii, Shinsuke; Ooga, Masahiro; Kiyoshima, Tamotsu; Yoshiura, Kazunori

    EUROPEAN RADIOLOGY   33 ( 2 )   845 - 853   2022.6   ISSN:0938-7994 eISSN:1432-1084

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    OBJECTIVES: To compare the delineation of mandibular cancer by 3D T1 turbo field echo with compressed SENSE (CS-3D-T1TFE) images and MDCT images, and to compare both sets of images with histopathological findings, as the gold standard, to validate the accuracy and clinical usefulness of CS-3D-T1TFE reconstruction. METHODS: Twenty-four patients with mandibular squamous cell carcinoma (SCC) who underwent MRI including CS-3D-T1TFE and MDCT examinations before surgery were retrospectively included. For both examinations, 0.5-mm-thick coronal plane images and 0.5-mm-thick plane images perpendicular and parallel to the dentition were constructed. Two radiologists rated bone invasion in three categories indexed by cortical bone, cancellous bone, and mandibular canal (MC), and inter-rater agreement was assessed by weighted kappa statistics. In 20 of the 24 patients who underwent surgery, the correlation of bone invasion with the histopathological evaluation by pathologists was assessed using Pearson's correlation coefficient. Soft-tissue invasion was assessed by diagnosing the presence of invasion into the mylohyoid muscle, gingivobuccal fold, and masticator space, and inter-rater agreement was assessed by kappa statistics. RESULTS: The interobserver agreement for bone invasion assessment was almost perfect with CS-3D-T1TFE and substantial with MDCT. The image evaluations by both observers agreed with the pathological evaluations in 15 of the 20 cases, showing high correlation (r > 0.8). CS-3D-T1TFE also showed higher inter-rater agreement than MDCT for all measures of soft-tissue invasion. CONCLUSIONS: CS-3D-T1TFE reconstructed images were clinically useful in accurately depicting the extent of mandibular cancer invasion and potentially solving the problem of lesion overestimation associated with conventional MRI. KEY POINTS: • Reconstructed CS-3D-T1TFE images were useful for the diagnosis of mandibular cancer. • CS-3D-T1TFE images showed higher inter-rater agreement than MDCT and high correlation with pathological findings. • CS-3D-T1TFE images may solve the problem of overestimation of the tumor extent, which has been associated with MRI in the past.

    DOI: 10.1007/s00330-022-09075-w

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  • Bone morphogenetic protein induces bone invasion of melanoma by epithelial-mesenchymal transition via the Smad1/5 signaling pathway Invited Reviewed International journal

    Gao, Jing; Muroya, Ryusuke; Huang, Fei; Nagata, Kengo; Shin, Masashi; Nagano, Ryoko; Tajiri, Yudai; Fujii, Shinsuke; Yamaza, Takayoshi; Aoki, Kazuhiro; Tamura, Yukihiko; Inoue, Mayuko; Chishaki, Sakura; Kukita, Toshio; Okabe, Koji; Matsuda, Miho; Mori, Yoshihide; Kiyoshima, Tamotsu; Jimi, Eijiro

    LABORATORY INVESTIGATION   101 ( 11 )   1475 - 1483   2021.11

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    DOI: 10.1038/s41374-021-00661-y

  • Effect of CTGF/CCN2 on osteo/cementoblastic and fibroblastic differentiation of a human periodontal ligament stem/progenitor cell line. Reviewed International journal

    Yuda A, Maeda H, Fujii S, Monnouchi S, Yamamoto N, Wada N, Koori K, Tomokiyo A, Hamano S, Hasegawa D, Akamine A

    J. Cell. Physiol.   2015.1

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  • The roles of calcium-sensing receptor and calcium channel in osteogenic differentiation of undifferentiated periodontal ligament cells. Reviewed International journal

    Koori K, Maeda H, Fujii S, Tomokiyo A, Kawachi G, Hasegawa D, Hamano S, Sugi H, Wada N, Akamine A

    Cell Tissue Res.   2014.9

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  • Semaphorin 3A induces mesenchymal stem-like properties in human periodontal ligament cells Reviewed International journal

    Wada N, Maeda H, Gronthos S, Bartold PM, Menicanin D, Fujii S, Yoshida S, Tomokiyo A, Monnouchi S, Akamine A

    Stem Cells Dev.   2014.9

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  • The potential role of transient receptor potential typeA2 as a mechanoreceptor in human periodontal ligament. Reviewed International journal

    Tsutsumi T, Kajiya H, Fukawa T, Sasaki M, Nemoto T, Tsuzuki T, Takahashi Y, Fujii S, Maeda H, Okabe K

    Eur J Oral Sci.   2013.12

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  • Exposure to transforming growth factor-β1 after basic fibroblast growth factor promotes the fibroblastic differentiation of human periodontal ligament stem/progenitor cell lines. Reviewed International journal

    2013.6

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  • Alternation of extracellular matrix remodeling and apoptosis by activation of the aryl hydrocarbon receptor pathway in human periodontal ligament cells. Invited Reviewed International journal

    Tomokiyo A, Maeda H, Fujii S, Monnouchi S, Wada N, Hori K, Koori K, Yamamoto N, Teramatsu Y, Akamine A

    J. Cell. Biochem.   2012.10

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  • Expression and effects of glial cell line-derived neurotrophic factor on periodontal ligament cells. Reviewed International journal

    Yamamoto N, Maeda H, Tomokiyo A, Fujii S, Wada N, Monnouchi S, Kono K, Koori K, Teramatsu Y, Akamine A

    J Clin Periodontol.   2012.6

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  • A multipotent clonal human periodontal ligament cell line with neural crest cell phenotypes promotes neurocytic differentiation, migration, and survival. Reviewed International journal

    Tomokiyo A, Maeda H, Fujii S, Monnouchi S, Wada N, Kono K, Yamamoto N, Koori K, Teramatsu Y, Akamine A

    J. Cell. Physiol.   2012.5

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  • Transforming Growth Factor β1 Promotes Migration of Human Periodontal Ligament Cells through Heat Shock Protein 27 Phosphorylation. Reviewed International journal

    2011.5

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  • The roles of angiotensin II in stretched periodontal ligament cells. Reviewed International journal

    Monnouchi S, Maeda H, Fujii S, Tomokiyo A, Kono K, Akamine A

    J. Dent. Res.   2011.5

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  • An in vitro evaluation of two resin-based sealers on proliferation and differentiation of human periodontal ligament cells. Reviewed International journal

    Maeda H, Tomokiyo A, Koori K, Monnouchi S, Fujii S, Wada N, Kono K, Yamamoto N, Saito T, Akamine A

    Int. Endod. J.   2011.1

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  • Mineral Trioxide Aggregate Induces Bone Morphogenetic Protein-2 Expression and Calcification in Human Periodontal Ligament Cells. Reviewed International journal

    Maeda H, Nakano T, Tomokiyo A, Fujii S, Wada N, Monnouchi S, Hori K, Akamine A

    J Endod   36 ( 4 )   2010.4

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  • MTAがヒト歯根膜線維芽細胞に及ぼす影響に関する研究 Reviewed

    前田英史,友清淳,藤井慎介,島一也,和田尚久,門野内聡,堀清美,中野嗣久,吉嶺嘉人,赤峰昭文

    日本歯科保存学会誌   52 ( 4 )   2009.8

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  • Development of a multipotent clonal human periodontal ligament cell line. Reviewed International journal

    Tomokiyo A, Maeda H, Fujii S, Wada N, Shima K, Akamine A.

    Differentiation   2008.4

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  • EDTAならびにNaOClによる根管洗浄後のSEM観察 -超音波洗浄との比較- Reviewed

    島一也、前田英史、後藤康治、畦森雅子、安田善之、和田尚久、藤井慎介、友清淳、吉嶺嘉人、齋藤隆史、赤峰昭文

    日本歯内療法学会誌   2008.1

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  • 油症患者における歯周疾患ならびに口腔内色素沈着の疫学調査(第六報) Reviewed

    橋口勇、吉嶺嘉人、前田英史、後藤康治、石河真幸、藤井慎介、友清淳、福山宏、奥村英彦、赤峰昭文

    福岡医学雑誌   2007.5

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  • MTA及びSuper-Bondのヒト歯根膜細胞の骨芽細胞様分化に及ぼす影響に関する研究 Reviewed

    野田亮、前田英史、藤井慎介、和田尚久、友清淳、吉嶺嘉人、赤峰昭文

    日本歯内療法学会誌   2006.9

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Books

  • Periodontal ligament stem cells.

    Maeda H, Wada N, Fujii S, Tomokiyo A, Akamine A

    InTech  2011.7 

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    Responsible for pages:Rijeka, Croatia, Chapter 25, 619-636   Language:Japanese  

Presentations

  • Abnormality of Signal Network in Oral Tumor Invited International conference

    Shinsuke Fujii

    IAOP 2023, 21st International Congress of Oral Pathology and Medicine  2023.8 

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    Event date: 2023.9

    Language:English   Presentation type:Oral presentation (general)  

    Country:Japan  

  • 口腔扁平上皮癌におけるp63とMAPKシグナルによる低分子量Gタンパク質ARL4Cの発現制御機構解明

    藤井 慎介、Dania Zuhier Ragheb Alkhatib、Thinh Thi-Kim Truong、長谷川 佳那、長野 良子、清島 保

    第112回日本病理学会総会  2023.4 

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    Event date: 2023.4

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:海峡メッセ下関   Country:Japan  

  • 口腔腫瘍において異常活性化したシグナル伝達とその機能解析 Invited

    藤井慎介

    第41回 日本口腔腫瘍学会総会・学術大会  2023.1 

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    Event date: 2023.1 - 2023.2

    Language:Japanese   Presentation type:Symposium, workshop panel (public)  

    Venue:Web開催   Country:Japan  

  • 低分子量Gタンパク質ARL4Cの発現はエナメル上皮腫における腫瘍細胞増殖と破骨細胞形成を促進する

    藤井 慎介、自見 英治郎、清島 保

    第64回歯科基礎医学会学術大会  2022.9 

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    Event date: 2022.9

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    Venue:徳島大学   Country:Japan  

  • エナメル上皮腫における低分子量Gタンパク質ARL4Cの発現は腫瘍細胞増殖と破骨細胞形成を促進する

    藤井 慎介、自見 英治郎、清島 保

    第111回日本病理学会総会  2022.4 

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    Event date: 2022.4

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    Venue:神戸コンベンションセンター   Country:Japan  

  • 口腔扁平上皮癌における「腫瘍実質-間質連関」による細胞増殖制御機構の解明 Invited

    藤井 慎介、清島 保

    第63回歯科基礎医学会学術大会  2021.10 

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    Event date: 2021.10

    Language:Japanese   Presentation type:Symposium, workshop panel (public)  

    Venue:Web開催   Country:Japan  

  • エナメル上皮腫におけるRAF1-MAPK依存性の低分子量Gタンパク質ARL4Cの高発現は腫瘍細胞増殖と破骨細胞形成を促進する

    小倉 萌、藤井 慎介、自見 英治郎、清島 保

    第63回歯科基礎医学会学術大会  2021.10 

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    Event date: 2021.10

    Language:Japanese  

    Venue:Web開催   Country:Japan  

  • 口腔がんにおいて異常活性化したシグナル伝達とその機能解析 Invited

    藤井慎介

    第67回日本病理学会秋期特別総会 学術研究賞演説(A演説)  2021.11 

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    Event date: 2021.6 - 2022.6

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:岡山   Country:Japan  

  • YAP-PIEZO1シグナルは口腔扁平上皮癌の細胞増殖を制御する

    藤井 慎介、長谷川 佳那、清島 保

    第110回日本病理学会総会  2021.4 

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    Event date: 2021.4

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:京王プラザホテル、Web開催   Country:Japan  

  • Sema3A-AKT Axis In Salivary Gland And Adenoid Cystic Carcinoma Developments International conference

    2020.11 

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    Event date: 2020.11

    Language:English  

    Country:Japan  

  • 口腔扁平上皮癌における増殖および分化転換の新規分子基盤の解明 Invited

    藤井 慎介、清島 保

    第62回歯科基礎医学会学術大会  2020.9 

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    Event date: 2020.9

    Language:Japanese   Presentation type:Symposium, workshop panel (public)  

    Venue:オンライン   Country:Japan  

  • ヒト口腔扁平上皮癌に高発現した機械受容器TRPV4はCaMK II/AKTシグナル伝達を介して癌細胞の増殖を制御する

    田尻 祐大、藤井 慎介、清島 保

    第62回歯科基礎医学会学術大会  2020.9 

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    Event date: 2020.9

    Language:Japanese  

    Country:Japan  

  • 歯原性腫瘍におけるWntシグナルネットワークの破綻 Invited

    藤井 慎介、清島 保

    第109回日本病理学会  2020.7 

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    Event date: 2020.6

    Language:Japanese   Presentation type:Symposium, workshop panel (public)  

    Venue:オンライン   Country:Japan  

  • 新規癌関連遺伝子のエナメル上皮腫における発現とその機能解析-課外授業での研究活動報告-

    #設楽 沙月、#小倉 萌、@藤井 慎介、@清島 保

    第38回日本歯科医学教育学会総会および学術大会  2019.7 

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    Event date: 2019.7

    Language:Japanese  

    Venue:パピヨン24   Country:Japan  

  • Wnt/β-カテニン−Sema3aシグナルは唾液腺の発生を制御する-課外授業での研究活動報告-

    #藤本 龍史、@藤井 慎介、@和田 尚久、@清島 保

    第38回日本歯科医学教育学会総会および学術大会  2019.7 

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    Event date: 2019.7

    Language:Japanese  

    Venue:パピヨン24   Country:Japan  

  • 機械受容器TRPV4はヒト口腔癌細胞の増殖を制御する

    藤井 慎介、田尻 祐大、大関 悟、清島 保

    第108回日本病理学会  2019.5 

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    Event date: 2019.5

    Language:Japanese  

    Venue:東京国際フォーラム   Country:Japan  

  • 歯牙腫におけるWnt シグナル依存的Sema3A の発現を介する増殖制御機構の解明 Invited

    藤井慎介

    第60回歯科基礎医学会学術大会  2018.9 

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    Event date: 2018.9

    Language:Japanese   Presentation type:Symposium, workshop panel (public)  

    Venue:九州大学病院キャンパス 百年講堂   Country:Japan  

  • 歯牙腫におけるWnt/β-cateninシグナルの活性化は軸索伸張制御因子(Sema3A)を介して増殖を制御する

    藤井 慎介、 永田 健吾、清島 保、和田 尚久

    第107回日本病理学会総会  2018.6 

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    Event date: 2018.6

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:ロイトン札幌   Country:Japan  

  • 歯牙腫におけるWnt/β-cateninシグナルの活性化は軸索伸張制御因子を介して増殖を制御する

    藤井慎介, 永田 健吾, 清島 保, 和田 尚久

    第63回日本病理学会秋期特別総会  2017.11 

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    Event date: 2017.11

    Language:Japanese  

    Venue:日本教育会館   Country:Japan  

  • ヒト肺癌(腺癌および肺扁平上皮癌)におけるArl4cの発現は癌形成を促進する

    藤井慎介, 清島保, 松本真司

    第59回歯科基礎医学会大会  2017.9 

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    Event date: 2017.11

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:松本歯科大学   Country:Japan  

  • ヒト肺腺癌および肺扁平上皮癌におけるArl4cの発現はがん形成を促進する

    藤井慎介, 松本真司, 清島 保, 菊池章

    第106回日本病理学会総会  2017.4 

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    Event date: 2017.4 - 2017.6

    Language:Japanese  

    Venue:京王プラザホテル   Country:Japan  

  • 低分子量Gタンパク質Arl4cはヒト大腸癌および肺癌における癌形成を促進する

    藤井慎介

    第2回口腔医科学フロンティア研究会  2017.3 

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    Event date: 2017.3

    Language:Japanese  

    Country:Japan  

  • ヒト大腸癌、肺腺癌および肺扁平上皮癌におけるArl4cの発現はがん形成を促進する

    藤井慎介, 松本真司, 清島 保, 菊池 章

    第62回日本病理学会秋期特別総会  2016.11 

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    Event date: 2016.11

    Language:Japanese  

    Venue:金沢市文化ホール   Country:Japan  

  • Arl4c expression is involved in tumorigenesis of colorectal cancer, lung adenocarcinoma and squamous cell carcinoma.

    2016.10 

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    Event date: 2016.10

    Language:Japanese   Presentation type:Oral presentation (general)  

    Country:Japan  

  • WntとKITシグナルの活性化バランスによる唾液腺の形づくりと機能獲得過程の制御 Invited

    松本真司, 栗本聖之, 藤井慎介, 菊池章

    第58回歯科基礎医学会学術大会  2016.8 

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    Event date: 2016.8

    Language:Japanese   Presentation type:Symposium, workshop panel (public)  

    Venue:札幌コンベンションセンター   Country:Japan  

  • ヒト大腸癌、肺腺癌および扁平上皮癌におけるArl4cの発現とその機能解析

    藤井慎介, 松本真司

    第58回歯科基礎医学会学術大会  2016.8 

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    Event date: 2016.8

    Language:Japanese  

    Venue:札幌コンベンションセンター   Country:Japan  

  • ヒト大腸がんおよび肺がんにおけるArl4cの高発現はがん形成を促進する

    藤井慎介, 松本 真司, 菊池 章

    第13回日本病理学会カンファレンス  2016.7 

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    Event date: 2016.7

    Language:Japanese   Presentation type:Symposium, workshop panel (public)  

    Venue:六甲ホテル   Country:Japan  

  • Arl4c expression is involved in tumorigenesis of colorectal cancer, lung adenocarcinoma and lung squamous cell carcinoma.

    Shinsuke Fujii, Shinji Matsumoto, Akira Kikuchi

    2015.10 

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    Event date: 2016.5

    Language:Japanese   Presentation type:Oral presentation (general)  

    Country:Japan  

  • 基底膜蛋白質Nidogen-1はWnt3aと結合しWnt/βカテニン経路の活性化を促進する

    藤井慎介, 松本真司, 佐藤祐哉, 下野知性, 関口清俊, 菊池章

    第85回日本生化学会大会  2012.12 

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    Event date: 2016.5

    Language:Japanese  

    Country:Japan  

  • Wnt/β-catenin シグナル経路は唾液腺上皮の発生を制御する

    藤井慎介, 松本真司, 菊池章

    2013.12 

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    Event date: 2016.5

    Language:Japanese  

    Venue:神戸国際展示場   Country:Japan  

  • Arl4c expression is involved in tumorigenesis of colorectal and lung cancers.

    Shinsuke Fujii, Shinji Matsumoto, Akira Kikuchi

    2014.9 

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    Event date: 2016.5

    Language:Japanese  

    Country:Japan  

  • TGF-beta1がヒト歯根膜細胞および前駆細胞の増殖および分化に及ぼす影響

    藤井慎介、前田英史、友清淳、橋口勇、門野内聡、堀清美、和田尚久、赤峰昭文

    第130回日本歯科保存学会春季学術大会  2009.6 

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    Event date: 2009.6

    Presentation type:Symposium, workshop panel (public)  

    Venue:札幌市   Country:Japan  

  • MTA stimulates BMP2 expression in human PDL cells. International conference

    H. MAEDA, A.TOMOKIYO, S. FUJII, S. MONNOUCHI, N. WADA, K. HORI, and A. AKAMINE

    87th General Session & Exhibition of the IADR/AADR/CADR  2009.4 

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    Event date: 2009.4

    Presentation type:Oral presentation (general)  

    Country:United States  

  • Expression and effects of TGFβ-1 in periodontal ligament tissue. International conference

    2009.4 

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    Event date: 2009.4

    Presentation type:Oral presentation (general)  

    Country:United States  

  • MTAが歯根膜細胞の分化に及ぼす影響に関する研究

    前田英史、友清淳、藤井慎介、中野嗣久、和田尚久、門野内聡、堀清美、赤峰昭文

    第21回日本歯科医学会総会  2008.11 

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    Event date: 2008.11

    Presentation type:Oral presentation (general)  

    Country:Japan  

  • MTAはヒト歯根膜細胞の骨芽細胞様分化を誘導する.

    前田英史、中野嗣久、友清淳、藤井慎介、門野内聡、和田尚久、赤峰昭文,

    第128回日本歯科保存学会  2008.11 

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    Event date: 2008.11

    Presentation type:Oral presentation (general)  

    Venue:新潟   Country:Japan  

  • Investigating a clonal human periodontal ligament progenitor/stem cell line in vitro and in vivo. International conference

    Shinsuke Fujii., Hidefumi Maeda., Naohisa Wada., Atsushi Tomokiyo., Akifumi Akamine

    Dental and Craniofacial Morphogenesis and Tissue Regeneration.  2007.3 

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    Presentation type:Oral presentation (general)  

    Country:Japan  

  • ヒト不死化歯根膜細胞株の樹立とキャラクタリゼーション

    藤井慎介、前田英史、和田尚久、野田亮、赤峰昭文

    日本歯科保存学会  2004.11 

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    Presentation type:Oral presentation (general)  

    Venue:長崎市   Country:Japan  

  • Establishment of Human Periodontal Ligament Cell Lines and Their Characterization. International conference

    S Fujii., H Maeda., N Wada., A Akamine

    2005.3 

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    Presentation type:Symposium, workshop panel (public)  

    Country:United States  

  • Characterizing of clonal human periodontal ligament cell lines. International conference

    S. Fujii., H. Maeda., N. Wada., A. Tomokiyo., A. Akamine

    Dental and Craniofacial Morphogenesis and Tissue Regeneration  2006.3 

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    Presentation type:Symposium, workshop panel (public)  

    Country:Japan  

  • Characterization of clonal human periodontal ligament cell lines Invited International conference

    S. Fujii., H. Maeda., N. Wada., A. Tomokiyo., A. Akamine

    General Session & Exhibition of the IADR  2006.6 

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    Presentation type:Symposium, workshop panel (public)  

    Country:Australia  

  • ヒト不死化歯根膜細胞のクローニングとキャラクタリゼーション

    藤井慎介、前田英史、和田尚久、野田亮、赤峰昭文

    日本歯科保存学会  2006.6 

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    Presentation type:Symposium, workshop panel (public)  

    Venue:札幌市   Country:Japan  

  • ヒト歯根膜前駆細胞株の樹立とキャラクタリゼーション

    藤井慎介

    先端歯学スクール  2006.11 

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    Presentation type:Oral presentation (general)  

    Venue:三浦市   Country:Japan  

  • Investigating a clonal human periodontal ligament progenitor/stem cell line in vitro and in vivo International conference

    Shinsuke Fujii, Hidefumi Maeda, Naohisa Wada, Atsushi Tomokiyo, and Akifumi Akamine

    2nd International symposium on Dental and Craniofacial Morphogenesis and Tissue Regeneration  2007.3 

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    Presentation type:Symposium, workshop panel (public)  

    Country:Japan  

  • CLEAR CELL SQUAMOUS CELL CARCINOMA OF THE TONGUE EXHIBITS CHARACTERISTICS AS AN UNDIFFERENTIATED SQUAMOUS CELL CARCINOMA International conference

    Kana Hasegawa, Shinsuke Fujii, Tamotsu Kiyoshima

    IAOP 2023, 21st International Congress of Oral Pathology and Medicine  2023.8 

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    Event date: 2023.9

    Language:English  

    Country:Japan  

  • WNT-YAP1-TGF-β AXIS PROMOTES TOOTH GERM DEVELOPMENT International conference

    2023.8 

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    Event date: 2023.9

    Language:English  

    Venue:台湾   Country:Japan  

  • 未分化な扁平上皮癌の特徴を有する舌に生じたclear cell squamous cell carcinoma

    長谷川 佳那、藤井 慎介、清島 保

    第33回日本臨床口腔病理学会  2022.9 

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    Event date: 2022.9

    Language:Japanese  

    Venue:札幌市教育文化会館   Country:Japan  

  • p130casはマウス顎下腺の顆粒性導管細胞分化のためのER―ゴルジネットワークの形成に重要な役割を果たす

    第64回歯科基礎医学会学術大会  2022.9 

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    Event date: 2022.9

    Language:Japanese  

    Country:Japan  

  • 口腔扁平上皮癌においてp63シグナルはYAPシグナルと協調的に細胞内シグナルおよびDNAメチル化を制御する

    長谷川 佳那、藤井 慎介、清島 保

    第64回歯科基礎医学会学術大会  2022.9 

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    Event date: 2022.9

    Language:Japanese  

    Venue:徳島大学   Country:Japan  

  • Wnt経路はYAP1-TGF-β経路を介して歯胚の発生を促進する

    長野 良子、藤井 慎介、清島 保

    第64回歯科基礎医学会学術大会  2022.9 

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    Event date: 2022.9

    Language:Japanese  

    Venue:徳島大学   Country:Japan  

  • 液腺発生と腺様嚢胞癌腫瘍形成における軸索誘導因子Semaphorin 3A(Sema3A)の役割の解明 Invited

    藤本 龍史、藤井 慎介、清島 保

    第64回歯科基礎医学会学術大会  2022.9 

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    Event date: 2022.9

    Language:Japanese  

    Venue:徳島大学   Country:Japan  

  • 口腔癌においてYAPシグナルは異型性および上皮間葉転換を誘導する

    長谷川 佳那、藤井 慎介、清島 保

    第111回日本病理学会総会  2022.4 

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    Event date: 2022.4

    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:神戸コンベンションセンター   Country:Japan  

  • 軸索誘導因子Sema3Aによる唾液腺形態形成および腺様嚢胞癌の増殖制御メカニズムの解明

    藤本 龍史、藤井 慎介、清島 保

    第63回歯科基礎医学会学術大会  2021.10 

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    Event date: 2021.10

    Language:Japanese  

    Country:Japan  

  • p130Cas はマウス顎下腺の顆粒性導管の発達に関与する

    第63回歯科基礎医学会学術大会  2021.10 

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    Event date: 2021.10

    Language:Japanese  

    Venue:Web開催   Country:Japan  

  • WntシグナルがYAPを介して歯胚の形態形成を制御する分子基盤の解明

    長野 良子、藤井 慎介、清島 保

    第63回歯科基礎医学会学術大会  2021.10 

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    Event date: 2021.10

    Language:Japanese  

    Venue:Web開催   Country:Japan  

  • YAP-PIEZO1シグナルは口腔扁平上皮癌の細胞増殖を促進する

    長谷川 佳那、藤井 慎介、清島 保

    第63回歯科基礎医学会学術大会  2021.10 

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    Event date: 2021.10

    Language:Japanese  

    Venue:Web開催   Country:Japan  

  • 遠位筋優位の症状を呈したシェーグレン症候群合併免疫介在性壊死性筋症の1例

    山本賢、山嵜奨、平峯智、柏戸佑介、貞島祥子、藤井慎介、松本佑慈、太田梓、髙山耕治、池崎裕昭、豊田一弘、小川栄一、村田昌之、清島保、下野信行

    第23回日本病院総合診療医学会総会  2021.9 

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    Event date: 2021.9

    Language:Japanese  

    Venue:Web開催   Country:Japan  

  • 新規癌関連遺伝子のエナメル上皮腫における高発現とその機能解析

    石橋 拓馬、藤井 慎介、清島 保

    第62回歯科基礎医学会学術大会  2020.9 

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    Event date: 2020.9

    Language:Japanese  

    Country:Japan  

  • 軸索ガイダンス因子Sema3aによる唾液腺発生制御メカニズムの解明

    藤本 龍史、藤井 慎介、清島 保

    第62回歯科基礎医学会学術大会  2020.9 

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    Event date: 2020.9

    Language:Japanese  

    Venue:オンライン   Country:Japan  

  • Wnt-Sema3aシグナルは唾液腺の発生を制御する

    藤本 龍史、藤井 慎介、清島 保

    第109回日本病理学会  2020.7 

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    Event date: 2020.6

    Language:Japanese  

    Venue:オンライン   Country:Japan  

  • 機械受容器TRPV4はヒト口腔扁平上皮癌細胞の増殖を制御する

    田尻 祐大、藤井 慎介、大関 悟、清島 保

    第109回日本病理学会  2020.7 

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    Event date: 2020.6

    Language:Japanese  

    Venue:Web開催   Country:Japan  

  • Hippo-PIEZO1シグナルは口腔扁平上皮癌の細胞増殖を制御する

    長谷川 佳那、 藤井 慎介、 清島 保

    第109回日本病理学会  2020.7 

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    Event date: 2020.6

    Language:Japanese  

    Venue:オンライン   Country:Japan  

  • エナメル上皮腫における新規癌関連遺伝子の発現とその機能解析

    石橋 拓馬、藤井 慎介、設楽 沙月、小倉 萌、清島 保

    第109回日本病理学会  2020.7 

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    Event date: 2020.6

    Language:Japanese  

    Country:Japan  

  • 急激な増悪の経過をたどった心肥大の一例

    今給黎 智美、大谷 規彰、池田翔大、筒井好知、森 涼子、橋本 亨、肥後 太基 、林谷 俊児、藤井 慎介、大石 善丈、小田 義直、筒井 裕之

    第126回日本循環器学会九州地方会  2019.7 

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    Event date: 2019.8

    Language:Japanese  

    Venue:宮崎市民プラザ   Country:Japan  

  • 口腔扁平上皮癌の腺癌組織への転換および悪性化におけるDNAメチル化機構の解明

    三上 友理恵、藤井 慎介、中村 誠司、清島 保

    第108回日本病理学会  2019.5 

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    Event date: 2019.5

    Language:Japanese  

    Venue:東京国際フォーラム   Country:Japan  

  • 唾液腺の発生および機能発現におけるp130Cas の役割

    #室屋龍佑, 高靖, 中富千尋, 藤井慎介, 清島保, 自見英治郎

    第60回歯科基礎医学会学術大会  2018.9 

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    Event date: 2018.9

    Language:Japanese  

    Venue:九州大学病院キャンパス 百年講堂   Country:Japan  

  • ヒト口腔癌におけるTRPV4の発現と機能解析

    田尻祐大, 藤井慎介, 大関悟, 清島保

    第60回歯科基礎医学会  2018.9 

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    Event date: 2018.9

    Language:Japanese  

    Venue:九州大学病院キャンパス 百年講堂   Country:Japan  

  • 唾液腺腫瘍におけるβ-カテニン発現に関する免疫組織化学的研究

    #岡崎裕紀, #稲葉日和吏, 永田健吾, 藤井慎介, 清島保

    第60回歯科基礎医学会学術大会  2018.9 

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    Event date: 2018.9

    Language:Japanese  

    Country:Japan  

  • 腺扁平上皮癌におけるエピジェネティックな変化は扁平上皮組織を腺組織に転換する

    三上友理恵, 藤井慎介, 中村誠司, 清島保

    第60回歯科基礎医学会  2018.9 

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    Language:Japanese  

    Country:Japan  

  • 機械感受性イオンチャネルPiezo1 の発現は口腔扁平上皮癌の細胞増殖を制御する

    長谷川佳那, 藤井慎介, 清島保

    第60回歯科基礎医学会学術大会  2018.9 

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    Language:Japanese  

    Country:Japan  

  • TRPV4遺伝子欠失マウスにおける口腔粘膜創傷治癒の解析

    吉本怜子, 合島怜央奈, 大崎康吉, 藤井慎介, 張旌旗, 曹愛琳, 高イキ, 清島保, 城戸瑞穂

    第60回歯科基礎医学会学術大会  2018.9 

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    Language:Japanese  

    Venue:九州大学病院キャンパス百年講堂   Country:Japan  

  • ヒト口腔癌におけるTRPV4の発現と機能解析

    田尻 祐大, 藤井 慎介, 大関 悟, 清島 保

    Journal of Oral Biosciences Supplement  2018.9  (一社)歯科基礎医学会

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  • 口腔扁平上皮癌においてGLI-KRT17連関は腫瘍における増殖を抗アポトーシス作用を介して促進する

    三上友理恵、藤井慎介、清島保

    第107回日本病理学会総会  2018.6 

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    Language:Japanese   Presentation type:Oral presentation (general)  

    Venue:札幌   Country:Japan  

  • 口腔扁平上皮癌においてGLI-KRT17連関は腫瘍細胞の増殖を促進する

    三上友理恵, 藤井慎介, 永田 健吾, 和田 裕子, 長谷川 佳那, 安部みさき, 吉本怜子, 中村 誠司, 清島保

    第59回歯科基礎医学会学術大会  2017.11 

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    Language:Japanese  

    Venue:松本歯科大学   Country:Japan  

  • Arl4c expression in pancreatic cancer promotes tumorigenesis

    2016.10 

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    Event date: 2016.10

    Language:Japanese   Presentation type:Symposium, workshop panel (public)  

    Country:Japan  

  • ヒト膵癌におけるArl4cの発現および機能解析

    庄嶋 健作, 藤井 慎介, 松本 真司, 江口 英利, 土岐 祐一郎, 菊池 章

    日本癌学会総会記事  2016.10  (一社)日本癌学会

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  • Arfファミリー低分子量Gタンパク質群が介在する多彩な生理機能と関連疾患 低分子量Gタンパク質Arl4cによる上皮の形づくりと発がんの制御

    松本 真司, 藤井 慎介, 原田 武志, 菊池 章

    日本生化学会大会プログラム・講演要旨集  2016.9  (公社)日本生化学会

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  • 機能と形態の統合的アプローチによる血管・唾液腺・骨の共創的研究 WntとKITシグナルの活性化バランスによる唾液腺の形づくりと機能獲得過程の制御

    松本 真司, 栗本 聖之, 藤井 慎介, 菊池 章

    Journal of Oral Biosciences Supplement  2016.9  (一社)歯科基礎医学会

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  • 口腔扁平上皮癌においてGli阻害剤(GANT61)は細胞死を誘導する

    三上友理恵, 永田 健吾, 和田 裕子, 藤井慎介, 安部みさき, 吉本怜子, 清島 保, 中村 誠司

    第58回歯科基礎医学会学術大会  2016.8 

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    Event date: 2016.8

    Language:Japanese   Presentation type:Symposium, workshop panel (public)  

    Venue:札幌コンベンションセンター   Country:Japan  

  • 3次元構築の中のがん細胞 増殖因子シグナルによる上皮形態形成の分子機構とその破綻による腫瘍形成

    菊池 章, 松本 真司, 藤井 慎介

    日本細胞生物学会大会講演要旨集  2016.5  (一社)日本細胞生物学会

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  • 器官形成における多細胞動態の階層を超えた理解に向けて Wntシグナルによる上皮管腔器官の形態形成と分化の調整

    菊池 章, 藤井 慎介, 栗本 聖之, 井深 奏司, 松本 真司

    日本生化学会大会・日本分子生物学会年会合同大会講演要旨集  2015.12  (公社)日本生化学会

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  • 上皮管腔形成研究を基盤にしたがん治療のための新規標的分子の同定

    菊池 章, 藤井 慎介, 木村 公一, 麓 勝巳, 松本 真司

    日本癌学会総会記事  2015.10  日本癌学会

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  • がんのシグナル伝達異常と分子標的治療戦略 増殖因子シグナルの協調的作用による上皮管腔形成と腫瘍形成の制御(Aberrant signal transduction and therapeutic strategy for molecular target Regulation of tubulogenesis and tumorigenesis by a combination of growth factor signaling)

    菊池 章, 松本 真司, 藤井 慎介, 佐藤 朗, 井深 奏司

    日本癌学会総会記事  2013.10  (一社)日本癌学会

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  • CCNファミリー研究のメルティングポット CTGF/CCN2が未分化なヒト歯根膜細胞株の骨芽細胞様分化に及ぼす影響

    祐田 明香, 前田 英史, 藤井 慎介, 門野内 聡, 山本 直秀, 和田 尚久, 友清 淳, 郡 勝明, 濱野 さゆり, 赤峰 昭文

    Journal of Oral Biosciences Supplement  2013.9  (一社)歯科基礎医学会

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  • 分化能の異なるヒト歯根膜細胞クローンの単離及びキャラクタライゼーション

    長谷川 大学, 和田 尚久, 前田 英史, 藤井 慎介, 郡 勝明, 友清 淳, 門野内 聡, 河野 清美, 山本 直秀, 寺松 陽子, 濱野 さゆり, 祐田 明香, 赤峰 昭文

    特定非営利活動法人日本歯科保存学会学術大会プログラムおよび講演抄録集  2012.10  (NPO)日本歯科保存学会

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  • Sema3Aがヒト歯根膜細胞の幹細胞/未分化細胞誘導に及ぼす影響

    和田 尚久, 前田 英史, 長谷川 大学, 藤井 慎介, 山本 直秀, 友清 淳, 門野内 聡, 赤峰 昭文

    特定非営利活動法人日本歯科保存学会学術大会プログラムおよび講演抄録集  2012.5  (NPO)日本歯科保存学会

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  • EGFがヒト歯根膜細胞に及ぼす影響について

    寺松 陽子, 前田 英史, 友清 淳, 門野内 聡, 山本 直秀, 和田 尚久, 藤井 慎介, 河野 清美, 郡 勝明, 赤峰 昭文

    特定非営利活動法人日本歯科保存学会学術大会プログラムおよび講演抄録集  2011.9  (NPO)日本歯科保存学会

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  • Passive Ultrasonic Irrigationによる根管洗浄の効果 SEM観察

    木原 智子, 前田 英史, 郡 勝明, 寺松 陽子, 和田 尚久, 藤井 慎介, 友清 淳, 門野内 聡, 河野 清美, 山本 直秀, 後藤 康治, 赤峰 昭文

    特定非営利活動法人日本歯科保存学会学術大会プログラムおよび講演抄録集  2011.5  (NPO)日本歯科保存学会

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  • ヒト歯根膜細胞への伸展刺激はInterleukin-11の発現を促進する

    門野内 聡, 前田 英史, 山本 直秀, 藤井 慎介, 友清 淳, 和田 尚久, 河野 清美, 郡 勝明, 寺松 陽子, 木原 智子, 赤峰 昭文

    特定非営利活動法人日本歯科保存学会学術大会プログラムおよび講演抄録集  2011.5  (NPO)日本歯科保存学会

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  • 【油症とPCB及びダイオキシン関連化合物に関する研究 報告集 第23集】油症患者における歯周疾患ならびに口腔内色素沈着の疫学的調査(第八報)

    橋口 勇, 吉嶺 嘉人, 前田 英史, 後藤 康治, 和田 尚久, 藤井 慎介, 友清 淳, 齋籐 桐枝, 門野内 聡, 河野 清美, 奥村 英彦, 赤峰 昭文

    福岡医学雑誌  2011.4  福岡医学会

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    油症患者における歯周疾患や口腔内色素沈着の罹患状況と経年的変化を把握するために、平成22年度の福岡県油症一斉検診時に歯科を受診した油症認定患者122名(男性56名、女性66名)を対象に、問診、視診やX線診(パントモグラフ)と同時に歯周ポケット診査を行った。主訴としては歯周組織炎や歯髄炎が多かった。深さ3mm以上の歯周ポケットを1歯でも有している患者は、被験者117名中104名(88.9%)と高い割合を示した。3mm以上の歯周ポケットを有する歯牙は総被検歯551歯中314歯(57.0%)であったが、その殆どは深さ4mm未満であった。口腔内色素沈着を有している患者は63名(51.6%)で、部位としては歯肉の色素沈着が最も多かった。女性より男性の発現率が高く、また70歳未満の患者に多く認められた。

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  • bFGFが未分化なヒト歯根膜細胞株の線維芽細胞様分化に及ぼす影響について

    河野 清美, 前田 英史, 和田 尚久, 藤井 慎介, 友清 淳, 門野内 聡, 山本 直秀, 郡 勝明, 寺松 陽子, 木原 智子, 赤峰 昭文

    特定非営利活動法人日本歯科保存学会学術大会プログラムおよび講演抄録集  2010.10  (NPO)日本歯科保存学会

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  • 未分化なヒト歯根膜細胞株の分化に及ぼすカルシウムの影響について

    郡 勝明, 前田 英史, 藤井 慎介, 友清 淳, 門野内 聡, 和田 尚久, 河野 清美, 山本 直秀, 寺松 陽子, 木原 智子, 赤峰 昭文

    特定非営利活動法人日本歯科保存学会学術大会プログラムおよび講演抄録集  2010.10  (NPO)日本歯科保存学会

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  • ヒト歯根膜および歯髄細胞の免疫抑制特性に関する研究

    和田 尚久, 前田 英史, 藤井 慎介, 友清 淳, 赤峰 昭文

    特定非営利活動法人日本歯科保存学会学術大会プログラムおよび講演抄録集  2010.10  (NPO)日本歯科保存学会

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  • スーパーボンドシーラーの特性について ヒト歯根膜細胞の増殖と分化に与える影響

    前田 英史, 友清 淳, 郡 勝明, 藤井 慎介, 門野内 聡, 安田 善之, 山本 直秀, 堀 清美, 和田 尚久, 斎藤 隆史, 赤峰 昭文

    日本歯内療法学会学術大会プログラム・抄録集  2010.5  日本歯内療法学会

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  • Angiotensin II is involved in the loading signal in stretched human PDL cells.

    Satoshi Monnouchi, Hidefumi Maeda, Shinsuke Fujii, Atsushi Tomokiyo, Kiyomi Hori, Akifumi Akamine

    3rd Hiroshima Conference on Education and Science in Dentistry  2009.11 

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    Presentation type:Oral presentation (general)  

    Country:Japan  

  • AhRシグナルがヒト歯根膜細胞のコラーゲン代謝に及ぼす影響

    友清 淳, 前田 英史, 藤井 慎介, 和田 尚久, 門野内 聡, 堀 清美, 郡 勝明, 山本 直秀, 赤峰 昭文

    特定非営利活動法人日本歯科保存学会学術大会プログラムおよび講演抄録集  2009.10  (NPO)日本歯科保存学会

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  • 伸展力が負荷されたヒト歯根膜細胞のシグナル伝達にはAngiotensin IIが関与している

    門野内聡、前田英史、藤井慎介、友清淳、堀清美、赤峰昭文

    第130回日本歯科保存学会春季学術大会  2009.6 

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    Presentation type:Symposium, workshop panel (public)  

    Venue:札幌市   Country:Japan  

  • TGF-β1がヒト歯根膜細胞および前駆細胞の増殖および分化に及ぼす影響

    藤井 慎介, 前田 英史, 友清 淳, 橋口 勇, 門野内 聡, 堀 清美, 和田 尚久, 赤峰 昭文

    特定非営利活動法人日本歯科保存学会学術大会プログラムおよび講演抄録集  2009.5  (NPO)日本歯科保存学会

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  • Angiotensin II mediates the loading signal in human periodontal ligament cells

    Satoshi Monnouchi, Hidefumi Maeda, Shinsuke Fujii, Atsushi Tomokiyo, Kiyomi Hori, Akifumi Akamine

    The 5th International Symposium on "Dental and Craniofacial Morphogenesis and Tissue Regeneration: A View from Stem Cell Researches  2009.2 

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    Presentation type:Oral presentation (general)  

    Country:Japan  

  • What are the characteristics of PDL stem cells?

    Hidefumi Maeda, Shinsuke Fujii, Atsushi Tomokiyo, Naohisa Wada, Satoshi Monnouchi, Kiyomi Hori, Katsuaki Koori, Naohide Yamamoto, Akifumi Akamine

    The 5th International Symposium on "Dental and Craniofacial Morphogenesis and Tissue Regeneration: A View from Stem Cell Researches  2009.2 

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    Presentation type:Oral presentation (general)  

    Country:Japan  

  • MTAはヒト歯根膜細胞のBMP2発現を誘導する

    前田 英史, 友清 淳, 藤井 慎介, 島 一也, 中野 嗣久, 和田 尚久, 門野内 聡, 堀 清美, 赤峰 昭文

    特定非営利活動法人日本歯科保存学会学術大会プログラムおよび講演抄録集  2008.10  (NPO)日本歯科保存学会

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  • 多分化能を有するヒト歯根膜クローン細胞株が神経細胞分化及び細胞遊走に及ぼす影響

    友清 淳, 前田 英史, 藤井 慎介, 和田 尚久, 門野内 聡, 赤峰 昭文

    日本歯科保存学雑誌  2008.5  (NPO)日本歯科保存学会

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  • 多分化能を持つヒト歯根膜クローン細胞株の樹立とキャラクタリゼーション

    友清 淳, 前田 英史, 藤井 慎介, 和田 尚久, 島 一也, 赤峰 昭文

    日本歯科保存学雑誌  2006.10  (NPO)日本歯科保存学会

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  • ヒト不死化歯根膜クローン細胞におけるEMDおよびbFGFが石灰化誘導に及ぼす影響

    友清 淳, 前田 英史, 藤井 慎介, 和田 尚久, 野田 亮, 島 一也, 赤峰 昭文

    日本歯科保存学雑誌  2005.10  (NPO)日本歯科保存学会

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  • スメアクリーン洗浄後の根管象牙質のSEM観察像-超音波洗浄との比較-

    島一也、前田英史、後藤康治、畦森雅子、和田尚久、藤井慎介、友清淳、赤峰昭文

    第125回日本歯科保存学会  2006.11 

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    Country:Japan  

  • 歯根嚢胞の病態形成に関与する歯原性上皮細胞の増殖機構の解明

    長野 良子, 藤井 慎介, 清島 保

    Journal of Oral Biosciences Supplement  2023.9  (一社)歯科基礎医学会

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  • 唾液腺発生と腺様嚢胞癌腫瘍形成における軸索誘導因子Semaphorin 3A(Sema3A)の役割の解明(Investigation of the role of Semaphorin 3A(Sema3A), an axonal guidance factor, in salivary gland development and adenoid cystic carcinoma tumorigenesis)

    藤本 龍史, 藤井 慎介, 清島 保

    Journal of Oral Biosciences Supplement  2022.9  (一社)歯科基礎医学会

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  • 口腔扁平上皮癌においてp63シグナルはYAPシグナルと協調的に細胞内シグナルおよびDNAメチル化を制御する(p63 signaling and YAP signaling cooperatively regulate intracellular signaling and DNA methylation in oral squamous cell carcinoma)

    長谷川 佳那, 藤井 慎介, 清島 保

    Journal of Oral Biosciences Supplement  2022.9  (一社)歯科基礎医学会

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  • 低分子量Gタンパク質ARL4Cの発現はエナメル上皮腫における腫瘍細胞増殖と破骨細胞形成を促進する(RAF1-MEK/ERK pathway-dependent ARL4C expression promotes ameloblastoma cell proliferation and osteoclast formation)

    藤井 慎介, 自見 英治郎, 清島 保

    Journal of Oral Biosciences Supplement  2022.9  (一社)歯科基礎医学会

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    Language:Japanese  

  • Wnt経路はYAP1-TGF-β経路を介して歯胚の発生を促進する(Wnt signaling promotes tooth germ development through YAP1-TGF-β signaling)

    長野 良子, 藤井 慎介, 清島 保

    Journal of Oral Biosciences Supplement  2022.9  (一社)歯科基礎医学会

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    Language:Japanese  

  • p130casはマウス顎下腺の顆粒性導管細胞分化のためのER-ゴルジネットワークの形成に重要な役割を果たす(p130cas plays a crucial role in ER-Golgi network formation for cell differentiation of granular convoluted tubules in mouse submandibular glands)

    李 傲男, 高 靖, 藤井 慎介, 清島 保, 自見 英治郎

    Journal of Oral Biosciences Supplement  2022.9  (一社)歯科基礎医学会

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MISC

  • Arl4c is a key regulator of tubulogenesis and tumorigenesis as a target gene of Wnt–β-catenin and growth factor–Ras signaling

    2016.10

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    Language:Japanese   Publishing type:Article, review, commentary, editorial, etc. (scientific journal)  

  • 発生過程及び疾患発症におけるWnt、ARL4C及びSema3Aの役割(The role of Wnt, ARL4C, and Sema3A in developmental process and disease pathogenesis)

    Fujii Shinsuke, Kiyoshima Tamotsu

    Pathology International   73 ( 6 )   217 - 233   2023.6   ISSN:1320-5463

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    Language:English   Publisher:John Wiley & Sons Australia, Ltd  

  • Periodontal tissue engineering: defining the triad.

    Maeda H, Fujii S, Tomokiyo A, Wada N, Akamine A

    Int J Oral Maxillofac Implants.   2013.11

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    Language:Japanese   Publishing type:Article, review, commentary, editorial, etc. (scientific journal)  

  • Promise of periodontal ligament stem cells in regeneration of periodontium.

    Maeda H, Tomokiyo A, Fujii S, Wada N, Akamine A

    Stem Cell Res Ther.   2011.7

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    Language:Japanese   Publishing type:Article, review, commentary, editorial, etc. (scientific journal)  

Professional Memberships

  • International Association of Dental Research

  • Japan Asssociation of Dental Research

  • 日本歯内療法学会

  • 日本歯科保存学会

  • 日本病理学会

  • 日本癌学会

  • 歯科基礎医学会

  • 日本臨床細胞学会

  • 日本歯科医学教育学会

  • THE JAPANESE SOCIETY OF ORAL PATHOLOGY

  • JAPANESE ASSOCIATION FOR ORAL BIOLOGY

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  • 日本臨床細胞学会

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  • 日本臨床口腔病理学会

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  • THE JAPANESE SOCIETY OF PATHOLOGY

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Committee Memberships

  • 日本臨床口腔病理学会   研究委員会、企画委員会、将来検討委員会  

    2024.6 - Present   

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  • 日本臨床口腔病理学会   研究委員会、将来検討委員会  

    2022.6 - 2024.5   

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  • 歯科基礎医学会   代議員  

    2022 - Present   

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  • Councilor   Domestic

    2021.6 - 2022.6   

  • 日本病理学会   学術評議員   Domestic

    2021.6 - 2022.6   

  • 日本病理学会   学術評議員  

    2021.4 - Present   

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Academic Activities

  • Screening of academic papers

    Role(s): Peer review

    2024

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    Type:Peer review 

    Number of peer-reviewed articles in foreign language journals:5

  • Screening of academic papers

    Role(s): Peer review

    2023

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    Type:Peer review 

    Number of peer-reviewed articles in foreign language journals:5

  • Screening of academic papers

    Role(s): Peer review

    2022

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    Type:Peer review 

    Number of peer-reviewed articles in foreign language journals:5

  • Screening of academic papers

    Role(s): Peer review

    2021

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    Type:Peer review 

    Number of peer-reviewed articles in foreign language journals:2

  • Screening of academic papers

    Role(s): Peer review

    2019

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    Type:Peer review 

    Number of peer-reviewed articles in foreign language journals:2

  • Screening of academic papers

    Role(s): Peer review

    2017

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    Type:Peer review 

    Number of peer-reviewed articles in foreign language journals:1

  • 科学技術の状況に係る総合的意識調査(NISTEP定点調査)

    Role(s): Review, evaluation

    文部科学省技術・学術政策研究所  2016.4 - 2018.3

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    Type:Scientific advice/Review 

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Other

  • 口腔病理専門医 認定番号 246

    2023.4

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  • 死体解剖資格(10021号)

    2022.11

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  • 細胞診専門歯科医(8071号)

    2019.1

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Research Projects

  • Elucidation of the mechanism of jaw bone destruction caused by oral tumor-stromal interaction.

    Grant number:24K02615  2024 - 2027

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research  Grant-in-Aid for Scientific Research (B)

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    Authorship:Principal investigator  Grant type:Scientific research funding

    CiNii Research

  • 超早期癌発見戦略に向けた変異細胞-隣接正常細胞-間質細胞における不安定性出現解明

    Grant number:23H03102  2023 - 2026

    日本学術振興会  科学研究費助成事業  基盤研究(B)

    清島 保, 自見 英治郎, 川野 真太郎, 藤井 慎介, 和田 裕子, 長谷川 佳那, 田尻 祐大

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    Authorship:Coinvestigator(s)  Grant type:Scientific research funding

    癌に対し早期発見・早期治療は最も重要である。遺伝子異常の蓄積した変異細胞が出現、異常増殖し癌組織が形成され、癌微小環境も影響する。しかし、形態学的変化に乏しい変異細胞を病理診断時に捉えるのは非常に困難である。口腔扁平表皮癌(OSCC)の癌化超初期における変異細胞の検出は必要とされながらも、その追求は十分ではない。
    そこで、遺伝子異常にて形質転換した変異細胞の出現による「隣接正常細胞や間質細胞の反応」や「変異細胞の隣接正常細胞や間質細胞への反応」といった細胞の不安定性を時空間的に解明し、OSCCの超早期癌発見戦略の開拓を目指す。

    CiNii Research

  • 口腔細胞診における遺伝子検査法(GSC)の創出とその臨床応用

    Grant number:23K11897  2023 - 2026

    日本学術振興会  科学研究費助成事業  基盤研究(C)

    山口 知彦, 清島 保, 藤井 慎介, 野上 美和子

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    Authorship:Coinvestigator(s)  Grant type:Scientific research funding

    診療では、臨床診断および細胞診・生検により病理診断される。口腔腫瘍、特に悪性腫瘍では、治療後の定期的な経過観察が重要である。細胞診は非健常部位の細胞を擦りとる検査であり、スクリーニングと推定診断を目的とする。細胞診・生検では、細胞・組織型の分類はなされるが、数値による基準値が設定されていないため、患者にとって診断結果を理解しやすい検査とは言い難い。本研究では、細胞診試料における口腔扁平上皮癌の発癌に関与する過剰発現した遺伝子群の発現量を検討する「細胞診を用いた遺伝子検査法(GSC; Genetic Screening Cytology」を創出する。また、検査値に基づく経過観察への展開を目指す。

    CiNii Research

  • シングルセル解析を用いた口腔腫瘍間質由来破骨細胞形成因子(SODF)の同定

    Grant number:22KK0262  2023 - 2025

    日本学術振興会  科学研究費助成事業  国際共同研究強化(A)

    藤井 慎介

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    Authorship:Principal investigator  Grant type:Scientific research funding

    口腔腫瘍では、顎骨への腫瘍細胞浸潤と広範な顎骨破壊を伴う場合が多い。顎骨破壊は臨床的にも最も重要な因子と考えられ、顎骨破壊に関与する口腔腫瘍による破骨細胞分化誘導の分子基盤の解明が待望されている。研究代表者らは低分子量Gタンパク質ARL4Cの腫瘍形成における増殖等の機能を解析してきた。また、口腔腫瘍におけるARL4Cの発現が腫瘍組織と接する間質細胞の破骨細胞活性化因子(RANKL)の発現を誘導して破骨細胞形成を促進することを見出した。本研究では口腔腫瘍顎骨破壊モデルマウスを作出し、病変部間質細胞におけるRANKLの発現を制御する間質由来破骨細胞形成因子(SODF)の同定を目的とする。

    CiNii Research

  • 唾液腺悪性腫瘍(腺様嚢胞癌)における「癌細胞-神経連関」による腫瘍形成機構の解明

    2023 - 2024

    公益財団法人 UBE 学術振興財団 第63回学術奨励賞

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  • Compressed sensingを用いた正確な口腔癌深達度の三次元的取得

    Grant number:22K10174  2022 - 2024

    日本学術振興会  科学研究費助成事業  基盤研究(C)

    加美 由紀子, 川野 真太郎, 筑井 徹, 吉浦 一紀, 藤井 慎介

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    Authorship:Coinvestigator(s)  Grant type:Scientific research funding

    近年登場したMRI の新しい高速撮像法であるCompressed Sensing (CS) は、高時間分解能および高空間分解能を有する。本研究では、腫瘍の深達度 (depth of invasion:DOI)計測の基準となり得る画像検査法を確立するため、CS の特性に注目し、造影剤の腫瘍と周囲炎症への到達時間の差を利用して、腫瘍実質のみを三次元的に正確に描出する。得られた画像は、拡散強調画像 (Diffusion weighted image:DWI) の新しい手法であるCS併用DWI (CS DWI) や三次元超音波画像、病理組織と比較し検証する。

    CiNii Research

  • シングルセル RNA-seq 解析を用いた口腔腫瘍における間質由来破骨細胞形成因子(SODF)の同定

    2022 - 2024

    公益財団法人新日本先進医療研究財団

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    Authorship:Principal investigator  Grant type:On-campus funds, funds, etc.

  • 口腔腫瘍における腫瘍実質-間質連関による顎骨破壊機構の解明

    2022 - 2023

    公益財団法人 テルモ生命科学振興財団 研究助成

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    Authorship:Principal investigator  Grant type:On-campus funds, funds, etc.

  • シングルセル解析を用いた口腔腫瘍における腫瘍-間質連関による顎骨吸収機構の解明

    2022 - 2023

    公益財団法人 持田記念医学薬学振興財団

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  • 早期癌に認められる異型におけるHippo-YAPシグナルの機能解析

    Grant number:21K09843  2021 - 2023

    日本学術振興会  科学研究費助成事業  基盤研究(C)

    長谷川 佳那, 清島 保, 藤井 慎介, 和田 裕子

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    Authorship:Coinvestigator(s)  Grant type:Scientific research funding

    悪性腫瘍の早期発見・早期治療は予後に大きく影響する。口腔癌では90%以上を口腔扁平上皮癌(Oral squamous cell carcinoma; OSCC)が占める。OSCCでは他の癌腫において治療標的となる遺伝子異常が少ないことが報告されているため、異常活性化した細胞内シグナルが発癌に寄与すると予想される。そのため異常に活性化した細胞内シグナルとその異常を引き起こす責任分子を同定することを目的とする。本研究結果はOSCCの診断に有用な新規マーカーや治療標的分子の発見に繋がると期待される。

    CiNii Research

  • Analysis of the signal pathways between oral squamous cell carcinoma cells and surrounding microenvironment as novel therapeutic target for novel anti-cancer therapy

    Grant number:20K10096  2020.4 - 2024.3

    Grants-in-Aid for Scientific Research  Grant-in-Aid for Scientific Research (C)

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    Grant type:Scientific research funding

    CiNii Research

  • 歯原性間葉系幹細胞誘導因子の同定と歯の再生への応用

    Grant number:20K09920  2020.4 - 2024.3

    科学研究費助成事業  基盤研究(C)

    和田 裕子, 清島 保, 藤井 慎介, 長谷川 佳那

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    「歯の再生医療」の具現化には、上皮間葉相互作用を含む歯の発生メカニズムの解明が重要である。
    我々はこれまでに歯胚上皮由来のエナメル質形成に重要な因子を認めた。
    しかしながら、歯の主体をなす歯胚間葉由来の象牙質の発生に関わる特異的な因子の同定には至っていない。
    そこで本研究では、微量RNA seq解析により歯胚発生過程の上皮間葉相互作用における間葉系幹細胞に重要な特異的因子を同定し、その発現様式と分子機構および機能を解析する。

    CiNii Research

  • Functional analysis and development of novel adenoid cystic carcinoma therapy targeting Wnt signaling

    Grant number:20K10107  2020.4 - 2023.3

    Grants-in-Aid for Scientific Research  Grant-in-Aid for Scientific Research (C)

    Higuchi Yoshinori

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    This study investigated the involvement of Semaphorin 3A (Sema3A) in submandibular gland development and adenoid cystic carcinoma (ACC) pathogenesis. Sema3A expression is negatively regulated by Wnt/β-catenin signaling and Sema3A positively regulates cell proliferation via phosphorylation of AKT in salivary gland development. Immunohistochemical analysis of ACC specimens revealed that Sema3A is strongly expressed in the tumor lesion and frequently co-expressed in phosphorylated AKT-positive areas. These results suggest that the Sema3A-AKT axis promotes cell growth to contribute to morphogenesis and pathogenesis, at least in ACC, of salivary glands.

    CiNii Research

  • Elucidating the mechanisms to induce ameloblastoma and its trial for the clinical setting

    Grant number:20K09906  2020 - 2022

    Japan Society for the Promotion of Science  Grants-in-Aid for Scientific Research  Grant-in-Aid for Scientific Research (C)

    Fujii Shinsuke

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    Ameloblastoma is an odontogenic neoplasm characterized by slow intraosseous growth with progressive jaw resorption. Recent reports revealed that ameloblastoma harbors an oncogenic BRAF V600E mutation with MAPK pathway activation. However, the precise mechanism by which MAPK pathway induces ameloblastoma is unclear. In immunohistochemical analyses of tissue specimens obtained from ameloblastoma patients, ARL4C was frequently expressed with both BRAF V600E and RAF1. ARL4C-depleted tumour cells exhibited decreased proliferation and migration capabilities. Finally, when ameloblastoma cells were co-cultured with mouse bone marrow cells and primary osteoblasts, ameloblastoma cells induced osteoclast formation. ARL4C elevation in ameloblastoma further promoted its formation capabilities. These results suggest that the RAF1-MEK/ERK-ARL4C axis, which may function in cooperation with the BRAF V600E-MEK/ERK pathway, promotes ameloblastoma development.

    CiNii Research

  • 口腔腺扁平上皮癌におけるエピゲノム異常に関する研究:癌の悪性度に関与する扁平上皮-腺上皮分化転換機構の解明

    2020 - 2021

    公益財団法人SGH財団 SGHがん研究助成

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  • The physiological role of p130Cas in salivary gland development

    Grant number:19K10054  2019.4 - 2023.3

    Grants-in-Aid for Scientific Research  Grant-in-Aid for Scientific Research (C)

    Gao Jing

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    We aimed to elucidate the physiological role of p130Cas in salivary glands using epithelium-specific p130Cas-deficient mice. Premature development of granular ducts (GCTs) in the submandibular gland of p130Cas-deficient mice was shown, and nuclear-localized androgen receptors (ARs) were specifically reduced in GCT cells. We found that the expression levels of target genes for AR signaling were markedly reduced in p130Cas-deficient mice, indicating that AR signaling was suppressed. These results suggest that p130Cas plays an important role in the development of androgen-dependent submandibular GCTs by regulating AR signaling.

    CiNii Research

  • オミックス解析を用いた歯根膜発生機構の解明と幹細胞誘導型組織再生技術への応用

    Grant number:19H03832  2019 - 2022

    日本学術振興会  科学研究費助成事業  基盤研究(B)

    和田 尚久, 前田 英史, 友清 淳, 祐田 明香, 藤井 慎介, 御手洗 裕美, 和田 裕子

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    Authorship:Coinvestigator(s)  Grant type:Scientific research funding

    近年、歯周病などによって大きく喪失した歯周組織の新たな再生療法として、幹細胞移植によって歯根膜および歯槽骨の再生を積極的に促す方法が提案されているが実現に至っていない。本研究では、歯胚発生期に着目してオミックス解析により歯根膜発生・形成に重要な特異的因子を同定、機能解析することで歯根膜発生機構の一端を解明する。さらに歯根膜発生・形成に重要な同定因子を幹細胞分化制御候補因子として歯根膜細胞への分化誘導能についてin vitroおよびin vivo両面から機能解析を行い、歯根膜組織再生のための幹細胞分化制御機構を解明する。

    CiNii Research

  • 癌微小環境の機械侵襲と新規癌遺伝子シグナル制御の相互強化による新たな癌治療戦略

    Grant number:19K10302  2019 - 2021

    日本学術振興会  科学研究費助成事業  基盤研究(C)

    大関 悟, 清島 保, 藤井 慎介, 田尻 祐大

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    Authorship:Coinvestigator(s)  Grant type:Scientific research funding

    これまでの癌研究では、腫瘍を構成する実質と間質とが各々個別に検討されてきたが、 一方のみを標的とする試みだけでは十分な抗腫瘍効果をあげられない場合がある。臨床において固形癌の周囲に触れる硬結が癌の進行を促進する可能性について報告されているが、その分子基盤は不明である。本研究では、機械受容器であるTRPV4が腫瘍間質の硬結を感知することによって腫瘍実質の増殖に与える影響を明らかにする。また、研究分担者らは腫瘍実質における新規癌遺伝子を見出している。
    本研究では、腫瘍間質からと腫瘍実質を併せて標的とする、これまでにない抗腫瘍効果を目指した癌治療法の開発を企図している。

    CiNii Research

  • Wntシグナル下流癌抑制遺伝子を分子標的とした新規唾液腺腫瘍治療法の開発

    2019 - 2020

    公益財団法人新日本先進医療研究財団:

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    Authorship:Principal investigator  Grant type:On-campus funds, funds, etc.

  • 新規オルガノイド培養法を用いた歯数を決定する分子基盤の解明

    2019

    武田科学振興財団 医学系研究助成(基礎)

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    Authorship:Principal investigator  Grant type:On-campus funds, funds, etc.

  • 細胞外環境が口腔癌に与える影響の解析

    2017.6 - 2020.6

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  • メカノセンサーを基盤とした歯の発生メカニズムの解明

    Grant number:17K11616  2017 - 2019

    日本学術振興会  科学研究費助成事業  基盤研究(C)

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    Authorship:Coinvestigator(s)  Grant type:Scientific research funding

  • Arl4cを標的とした核酸医薬による口腔がんの新規分子標的治療法の開発

    Grant number:16K11501  2016 - 2019

    日本学術振興会  科学研究費助成事業  基盤研究(C)

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    Authorship:Principal investigator  Grant type:Scientific research funding

  • TRPチャネルを介したがん組織微小環境ストレスによる癌細胞形質への影響の解明

    Grant number:16K11738  2016 - 2018

    日本学術振興会  科学研究費助成事業  基盤研究(C)

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    Authorship:Coinvestigator(s)  Grant type:Scientific research funding

  • エナメル質形成における分子シャペロンGRP78の関与

    Grant number:16K11448  2016 - 2018

    科学研究費助成事業  一般研究(C)

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    Authorship:Coinvestigator(s)  Grant type:Scientific research funding

  • Arl4cを分子標的とする核酸医薬を応用した新規エナメル上皮腫治療法の開発

    2016 - 2018

    公益財団法人福岡県すこやか健康事業団 がん研究助成金

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    Authorship:Principal investigator  Grant type:On-campus funds, funds, etc.

  • 低分子量Gタンパク質を標的とする新規がん治療のための核酸医薬の探索

    2016

    国立研究開発法人日本医療研究開発機構(AMED)創薬支援ネットワーク

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    Authorship:Coinvestigator(s)  Grant type:Contract research

  • 低分子量Gタンパク質を標的とする新規がん治療のための核酸医薬の探索

    2015

    国立研究開発法人日本医療研究開発機構(AMED)創薬支援ネットワーク

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    Authorship:Coinvestigator(s)  Grant type:Contract research

  • Arl4cを標的としたがん治療を目的とする新規医薬品の創出

    2015

    大阪大学橋渡し研究支援推進プログラム

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    Authorship:Coinvestigator(s)  Grant type:On-campus funds, funds, etc.

  • 肺がん治療を目指した新規核酸医薬品の創出

    2015

    大阪大学未来戦略機構・第二部門・生体統御ネットワーク医学教育プログラム・異分野融合教育研究推進プロジェクト

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    Authorship:Principal investigator  Grant type:On-campus funds, funds, etc.

  • 唾液腺上皮組織の発生および再生におけるWntシグナルの役割の解明

    Grant number:26861547  2014 - 2016

    科学研究費助成事業  若手研究(B)

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    Authorship:Principal investigator  Grant type:Scientific research funding

  • Arl4cを標的としたがん治療を目的とする新規医薬品の創出

    2014

    大阪大学橋渡し研究支援推進プログラム

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    Authorship:Coinvestigator(s)  Grant type:On-campus funds, funds, etc.

  • 唾液腺の発生および再生におけるWntシグナルの役割の解明

    2013

    大阪大学未来戦略機構・第二部門・生体統御ネットワーク医学教育プログラム・異分野融合教育研究推進プロジェクト

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    Authorship:Principal investigator  Grant type:On-campus funds, funds, etc.

  • 歯周靭帯の再生を主軸にした新規歯周組織再生療法の開発

    Grant number:22592123  2010 - 2012

    日本学術振興会  科学研究費助成事業  基盤研究(C)

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    Authorship:Principal investigator  Grant type:Scientific research funding

  • 歯根膜を有した次世代型人工歯根の開発

    Grant number:22390359  2010 - 2012

    日本学術振興会  科学研究費助成事業  基盤研究(B)

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    Authorship:Coinvestigator(s)  Grant type:Scientific research funding

  • 歯根膜はその再生に何を必要とするか?

    Grant number:21390510  2009 - 2011

    日本学術振興会  科学研究費助成事業  基盤研究(B)

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    Authorship:Coinvestigator(s)  Grant type:Scientific research funding

  • ヒト歯根膜組織再生に関連した遺伝子の同定

    Grant number:20791387  2009 - 2010

    科学研究費助成事業  若手研究(B)

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    Authorship:Principal investigator  Grant type:Scientific research funding

  • ヒト歯根膜組織再生に関連した遺伝子の同定

    Grant number:20791387  2008 - 2009

    科学研究費助成事業  若手研究(B)

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    Authorship:Principal investigator  Grant type:Scientific research funding

  • ヒト歯根膜前駆細胞クローン株を用いた歯根膜再生機構の解明

    Grant number:19390486  2007 - 2009

    日本学術振興会  科学研究費助成事業  基盤研究(B)

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    Authorship:Coinvestigator(s)  Grant type:Scientific research funding

  • ヒト歯根膜前駆細胞株の分化メカニズム解明

    Grant number:09890159  2007

    科学研究費助成事業  若手研究(スタートアップ)

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    Authorship:Principal investigator  Grant type:Scientific research funding

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Class subject

  • 口腔病理学

    2023.4 - 2023.11   Full year

  • リサーチエクスポージャー

    2022.4 - 2023.3   Full year

  • 口腔病理学

    2022.4 - 2023.3   Full year

  • 課題協学科目

    2021.10 - 2022.3   Second semester

  • 細胞培養の理論と応用

    2021.4 - 2022.3   Full year

  • 口腔病理学

    2021.4 - 2022.3   Full year

  • リサーチエクスポージャー

    2021.4 - 2021.9   First semester

  • リサーチエクスポージャー

    2020.4 - 2021.3   Full year

  • 口腔病理学

    2020.4 - 2021.3   Full year

  • リサーチエクスポージャー

    2019.4 - 2020.3   Full year

  • 細胞生物学

    2019.4 - 2020.3   Full year

  • 口腔病理学

    2019.4 - 2020.3   Full year

  • 細胞培養の理論と応用

    2018.4 - 2019.3   Full year

  • リサーチエクスポージャー

    2018.4 - 2019.3   Full year

  • 口腔病理学

    2018.4 - 2019.3   Full year

  • 細胞生物学

    2018.4 - 2019.3   Full year

  • 口腔組織学Ⅰ

    2018.4 - 2018.9   First semester

  • 細胞培養の理論と応用

    2017.4 - 2018.3   Full year

  • 口腔病理学

    2017.4 - 2018.3   Full year

  • 細胞生物学

    2017.4 - 2018.3   Full year

  • 口腔組織学Ⅰ

    2017.4 - 2017.9   First semester

  • 細胞生物学

    2016.4 - 2017.3   Full year

  • 口腔病理学

    2016.4 - 2017.3   Full year

  • 口腔組織学Ⅰ

    2016.4 - 2016.9   First semester

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FD Participation

  • 2023.9   Role:Participation   Title:ハラスメントにならない指導の仕方 (これまでに発生した事例・最近の傾向を踏まえた内容の予定)

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2023.6   Role:Participation   Title:R6年度科研費獲得セミナー〜科研費制度及び研究計画書の書き方〜

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2022.7   Role:Participation   Title:科研費申請のススメ!〜科学研究費補助金制度と研究計画調書作成時の注意点〜

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2021.5   Role:Participation   Title:課題協学科目FD

    Organizer:University-wide

  • 2020.11   Role:Participation   Title:令和2年度馬出地区4部局合同男女共同参画FD

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2020.6   Role:Participation   Title:電子ジャーナルをめぐる現状と今後に向けた対応について

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2019.9   Role:Participation   Title:科研費申請のススメ!〜科学研究費補助金制度と研究計画調書作成時の注意点〜

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2018.8   Role:Participation   Title:「歯学研究院の研究力分析と研究力強化に向けたScopus/Scival/Pure活用例」 「BIツールを用いた研究力分析の紹介」

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2018.5   Role:Participation   Title:2018年度臨床能力試験トライアル

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2018.3   Role:Participation   Title:東京医歯大における国家試験対策の実践

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2017.11   Role:Participation   Title:平成29年度第1回歯学研究院FD ARO次世代医療センターの活用方法

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2017.10   Role:Participation   Title:「無意識のバイアスからの開放:ダイバーシティのススメ」 東北大学 大学院医学系研究科・教授 大隅 典子 先生

  • 2016.12   Role:Participation   Title:歯学教育の現状と課題・反グローバル化と「国際交流」

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2016.10   Role:Participation   Title:男女共同参画の必要性と九州大学における取組み

    Organizer:University-wide

  • 2016.6   Role:Participation   Title:国立大学改革プランへの対応・東医歯大歯学部改革への取り組み

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2010.3   Role:Participation   Title:歯学研究院次期中期目標・計画について

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2010.1   Role:Participation   Title:化学物質の安全管理対策

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2009.9   Role:Participation   Title:歯学研究院QUEST-MAPの最終案について

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2009.4   Role:Participation   Title:歯学研究院のQUEST-MAP(最終版)について

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2008.10   Role:Participation   Title:患者の肖像権と個人情報保護

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2008.4   Role:Participation   Title:歯学研究院のQUEST-MAP(最終版)について

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2008.3   Role:Participation   Title:歯学研究院の現状と将来構想(QUEST-MAP)

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2008.1   Role:Participation   Title:歯科医療領域の政策・経営シンクタンク

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2007.12   Role:Participation   Title:歯学研究院の理念について

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2007.7   Role:Participation   Title:歯学研究院の課題とその解決策

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2007.5   Role:Participation   Title:歯学を取り巻く現状分析(その1)

    Organizer:[Undergraduate school/graduate school/graduate faculty]

  • 2007.4   Role:Participation   Title:歯学研究院FD

    Organizer:[Undergraduate school/graduate school/graduate faculty]

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Visiting, concurrent, or part-time lecturers at other universities, institutions, etc.

  • 2024  博多メディカル専門学校  

  • 2023  博多メディカル専門学校  Classification:Part-time lecturer  Domestic/International Classification:Japan 

    Semester, Day Time or Duration:通年

  • 2022  博多メディカル専門学校  Classification:Part-time lecturer 

    Semester, Day Time or Duration:通年

  • 2021  博多メディカル専門学校  Classification:Part-time lecturer  Domestic/International Classification:Japan 

    Semester, Day Time or Duration:通年

  • 2020  博多メディカル専門学校  Classification:Part-time lecturer  Domestic/International Classification:Japan 

    Semester, Day Time or Duration:通年

  • 2019  福岡歯科衛生専門学校  Classification:Part-time lecturer  Domestic/International Classification:Japan 

    Semester, Day Time or Duration:前期

  • 2019  博多メディカル専門学校  Classification:Part-time lecturer 

    Semester, Day Time or Duration:前期

  • 2018  博多メディカル専門学校  Classification:Part-time lecturer 

    Semester, Day Time or Duration:前期

  • 2018  福岡歯科衛生専門学校  Classification:Part-time lecturer  Domestic/International Classification:Japan 

    Semester, Day Time or Duration:前期

  • 2017  博多メディカル専門学校  Classification:Part-time lecturer  Domestic/International Classification:Japan 

    Semester, Day Time or Duration:後期

  • 2017  福岡歯科衛生専門学校  Classification:Part-time lecturer  Domestic/International Classification:Japan 

    Semester, Day Time or Duration:前期

  • 2016  福岡歯科衛生専門学校  Classification:Part-time lecturer  Domestic/International Classification:Japan 

    Semester, Day Time or Duration:前期

  • 2016  博多メディカル専門学校  Classification:Part-time lecturer  Domestic/International Classification:Japan 

    Semester, Day Time or Duration:後期

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Other educational activity and Special note

  • 2016  Special Affairs 

  • 2009  Special Affairs 

  • 2008  Special Affairs 

  • 2007  Special Affairs 

Outline of Social Contribution and International Cooperation activities

  • 平成21年9月30日 「治る感染根管治療をめざす! 「根管数の多様性と歯根破折」」  臨床医のための症例検討セミナー (主催:九州大学歯学部同窓会)

Social Activities

  • 口腔癌の細胞診断、組織診断 -口腔腫瘍基礎研究をあわせて-

    第82回細胞検査士教育セミナー 日本臨床細胞学会教育委員会  2022.8

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    Audience: General, Scientific, Company, Civic organization, Governmental agency

    Type:Seminar, workshop

  • 口腔癌の細胞診断、組織診断 -扁平上皮癌を中心に-

    令和3年度 子宮がん検診従事者講習会(福岡地区)  2022.3

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    Audience: General, Scientific, Company, Civic organization, Governmental agency

    Type:Seminar, workshop

  • 地域病院からの依頼により病理解剖および病理診断を行い、臨床病理カンファレンス(CPC)にて報告している。 学外の大学や医療専門学校において病理学の講義・実習を行っている。 九州・沖縄スライドコンファレンスに参加した。

    2018

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    地域病院からの依頼により病理解剖および病理診断を行い、臨床病理カンファレンス(CPC)にて報告している。 学外の大学や医療専門学校において病理学の講義・実習を行っている。
    九州・沖縄スライドコンファレンスに参加した。

  • 地域病院からの依頼により病理解剖および病理診断を行い、臨床病理カンファレンス(CPC)にて報告している。 学外の大学や医療専門学校において病理学の講義・実習を行っている。 九州・沖縄スライドコンファレンスに参加した。

    2017

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    地域病院からの依頼により病理解剖および病理診断を行い、臨床病理カンファレンス(CPC)にて報告している。 学外の大学や医療専門学校において病理学の講義・実習を行っている。
    九州・沖縄スライドコンファレンスに参加した。

  • 地域病院からの依頼により病理解剖および病理診断を行い、臨床病理カンファレンス(CPC)にて報告している。 学外の大学や医療専門学校において病理学の講義・実習を行っている。

    2016

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    地域病院からの依頼により病理解剖および病理診断を行い、臨床病理カンファレンス(CPC)にて報告している。
    学外の大学や医療専門学校において病理学の講義・実習を行っている。

  • 成21年度 同窓会主催 「臨床医のための症例検討セミナー」 治る感染根管治療をめざす.「根管数の多様性と歯根破折」について

    九州大学歯学部同窓会  福岡県歯科医師会館  2009.9

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    Audience: General, Scientific, Company, Civic organization, Governmental agency

    Type:Seminar, workshop

  • カネミ油症歯科検診

    2009

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    カネミ油症歯科検診

  • カネミ油症歯科検診

    2008

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    カネミ油症歯科検診

  • カネミ油症歯科検診

    2007

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    カネミ油症歯科検診

  • カネミ油症歯科検診

    2006

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    カネミ油症歯科検診

  • カネミ油症歯科検診

    2005

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    カネミ油症歯科検診

  • カネミ油症歯科検診

    2004

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    カネミ油症歯科検診

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Acceptance of Foreign Researchers, etc.

  • Faculty of Dentistry, University of Medicine and Pharmacy - Ho Chi Minh City

    Acceptance period: 2019.12 - 2020.3   (Period):1 month or more

    Nationality:Viet Nam

Travel Abroad

  • 2023.11 - 2024.7

    Staying countory name 1:Finland   Staying institution name 1:Institute of Biomedicine and MediCity Research Laboratories, University of Turku, and Turku Bioscience Centre, University of Turku and Åbo Akademi University

Specialized clinical area

  • Biology / Medicine, Dentistry and Pharmacy / Dentistry / Conservative Dentistry

  • Biology / Medicine, Dentistry and Pharmacy / Dentistry / Pathophysiological Dentistry / Dental Radiology

Clinician qualification

  • Specialist

    The Japanese Society of Clinical Cytology

  • Specialist

    The Japanese Society of Pathology

Year of medical license acquisition

  • 2003

Notable Clinical Activities

  • 歯学部学生の臨床実習・研修歯科医の指導を行っている。