研究者業績

野村 隆士

Ryuji Nomura

基本情報

所属
藤田医科大学 医学部・解剖生理学 教授
学位
博士(医学)(群馬大学)

J-GLOBAL ID
200901032142302206
researchmap会員ID
5000043884

研究キーワード

 2

論文

 29
  • 酒井 一由, 西井 一宏, 安倍 雅人, 加藤 好光, 尾之内 高慶, 会津 直樹, 刑部 恵介, 日比谷 信, 山田 晃司, 秋山 秀彦, 市野 直浩, 野村 隆士, 秦 龍二
    臨床検査学教育 12(2) 151-157 2020年9月  
    本学では、臨床検査技師教育課程において人体解剖実習を導入し、その有効かつ有益な教育方法を考察した。その結果、「心臓の構造を理解できた」と回答した学生は96%であり、他臓器においても80%以上と高率であった。また、医療職として必須の倫理的教育効果についても「ご遺体の尊厳についての理解」に関して96%の学生から肯定的な回答が得られた。一方で、教員の不足等による不満もあったが、今後は大学院生や勉学の意識の強い卒業生の実習参加などを通して、より広くかつ意義深い実習にしていきたいと考えている。(著者抄録)
  • Atsushi Shimomura, Akiko Iizuka-Kogo, Naoki Yamamoto, Ryuji Nomura
    MEDICAL MOLECULAR MORPHOLOGY 49(2) 119-126 2016年6月  査読有り
    Mesenchymal stem cells (MSCs) represent a promising cell source for stem cell therapy to replace neurons damaged by neurodegenerative diseases. A system designed for in vitro neuronal differentiation of MSCs is an indispensable technique, which provides MSC-derived functional neurons for cell-replacement therapies and valuable information in pre-clinical research. This study investigated the effects of reducing the volume of neural induction medium on cell viability and neural differentiation of MSCs. When MSCs were differentiated in low volumes of neural induction medium, rather than using the conventional method, the cell density on culture dishes significantly increased. The % cell death, including apoptosis and necrosis, was significantly lower in the lower volume method than in the conventional method. There were no significant differences between the lower volume and conventional methods in the expression levels of the neuronal marker genes. In an analysis of immunostaining for a mature neuronal marker, no significant difference was detected between the media volumes. These findings demonstrate that neuronal induction of MSCs in low volumes of differentiation medium promoted survival during differentiation and resulted in larger numbers of MSC-derived neurons, compared to the conventional method. This novel lower volume method offers both financial and cell-yield advantages over the conventional method.
  • Akiko Iizuka-Kogo, Takao Senda, Tetsu Akiyama, Atsushi Shimomura, Ryuji Nomura, Yoshimi Hasegawa, Ken-ichi Yamamura, Hiroshi Kogo, Nobuhiko Sawai, Toshiyuki Matsuzaki
    PLOS ONE 10(4) 2015年4月  査読有り
    The Dlg1 gene encodes a member of the MAGUK protein family involved in the polarization of epithelial cells. Null mutant mice for the Dlg1 gene (Dlg1(-/-) mice) exhibit respiratory failure and cyanosis, and die soon after birth. However, the cause of this neonatal lethality has not been determined. In the present study, we further examined Dlg1(-/-) mice and found severe defects in the cardiovascular system, including ventricular septal defect, persistent truncus arteriosus, and double outlet right ventricle, which would cause the neonatal lethality. These cardiovascular phenotypes resemble those of mutant mice lacking planar cell polarity (PCP) genes and support a recent notion that DLG1 is involved in the PCP pathway. We assessed the degree of involvement of DLG1 in the development of other organs, as the cochlea, intestine, and skeleton, in which PCP signaling has been suggested to play a role. In the organ of Corti, tissue elongation was inhibited accompanied by disorganized arrangement of the hair cell rows, while the orientation of the stereocilia bundle was normal. In the sternum, cleft sternum, abnormal calcification pattern of cartilage, and disorganization of chondrocytes were observed. Furthermore, shortening of the intestine, sternum, and long bones of the limbs was observed. These phenotypes of Dlg1(-/-) mice involving cellular disorganization and insufficient tissue elongation strongly suggest a defect in the convergent extension movements in these mice. Thus, our present results provide a possibility that DLG1 is particularly required for convergent extension among PCP signaling-dependent processes.
  • Kazuyoshi Sakai, Ryuji Nomura, Yoshimi Hasegawa, Masanori Sinzato, Kazuhiro Nishii, Yoshimitsu Katoh, Kouji Yamada
    Okajimas Folia Anatomica Japonica 92(2) 43-47 2015年  査読有り
    In order to elucidate the function of anti-aromatic acid decarboxylase (AADC)-only-positive cells in the alimentary canal, 5-hydroxy-L-tryptophan (5-HTP) or L-3,4-dihydroxyphenylalanine (L-DOPA) was intraperitoneally injected into the laboratory shrew, Suncus murinus, and immunohistochemical studies were conducted on continuous sections of the alimentary canal using specific antisera against tyrosine hydroxylase (TH), AADC, dopamine (DA), and serotonin (5-HT). AADC-only-positive cells localized to the epithelial layer of the alimentary canal from the stomach to the large intestine. These AADC-only-positive cells became DA- and AADC-positive cells after L-DOPA injection, and 5-HT- and AADC-positive cells after 5-HTP injection. These results strongly indicate that the AADC-only-positive cells in the alimentary canal of Suncus murinus are capable of synthesizing DA and 5-HT simultaneously upon administration of L-DOPA and 5-HTP.
  • Takanori Onouchi, Katsunori Kobayashi, Kazuyoshi Sakai, Atsushi Shimomura, Ron Smits, Chiho Sumi-Ichinose, Masafumi Kurosumi, Keizo Takao, Ryuji Nomura, Akiko Iizuka-Kogo, Hidenori Suzuki, Kazunao Kondo, Tetsu Akiyama, Tsuyoshi Miyakawa, Riccardo Fodde, Takao Senda
    MOLECULAR BRAIN 7(1) 21 2014年3月  査読有り
    Background: Loss of adenomatous polyposis coli (APC) gene function results in constitutive activation of the canonical Wnt pathway and represents the main initiating and rate-limiting event in colorectal tumorigenesis. APC is likely to participate in a wide spectrum of biological functions via its different functional domains and is abundantly expressed in the brain as well as in peripheral tissues. However, the neuronal function of APC is poorly understood. To investigate the functional role of Apc in the central nervous system, we analyzed the neurological phenotypes of Apc(1638T/1638T) mice, which carry a targeted deletion of the 3' terminal third of Apc that does not affect Wnt signaling. Results: A series of behavioral tests revealed a working memory deficit, increased locomotor activity, reduced anxiety-related behavior, and mildly decreased social interaction in Apc(1638T/1638T) mice. Apc(1638T/1638T) mice showed abnormal morphology of the dendritic spines and impaired long-term potentiation of synaptic transmission in the hippocampal CA1 region. Moreover, Apc(1638T/1638T) mice showed abnormal dopamine and serotonin distribution in the brain. Some of these behavioral and neuronal phenotypes are related to symptoms and endophenotypes of schizophrenia. Conclusions: Our results demonstrate that the C-terminus of the Apc tumor suppressor plays a critical role in cognitive and neuropsychiatric functioning. This finding suggests a potential functional link between the C-terminus of APC and pathologies of the central nervous system.

MISC

 30

書籍等出版物

 5

担当経験のある科目(授業)

 5

共同研究・競争的資金等の研究課題

 19

教育内容・方法の工夫(授業評価等を含む)

 3
  • 件名
    医学部 Best Teacher of the Year 受賞
    開始年月日
    2015/08/25
  • 件名
    人体解剖実習の全実習内容の決定と全実習資料の作製
    開始年月日
    2009
    終了年月日
    2013
    概要
    人体解剖実習(脳を除く)の全実習回分の実習内容の決定と実習資料の作製を行った。
  • 件名
    医学部 Best Teacher of the Year 受賞
    開始年月日
    2014/08/27

作成した教科書、教材、参考書

 1
  • 件名
    Ross組織学
    概要
    核以外の構造/p23-70.分担翻訳

その他教育活動上特記すべき事項

 6
  • 件名
    第4回藤田保健衛生大学医学・医療教育ワークショップ
    開始年月日
    2011/08/24
    終了年月日
    2011/08/24
    概要
    「チーム基盤型学習(TBL)の体験を通して,職種間連携教育(IPE)を考える」に参加した。
  • 件名
    第37回藤田保健衛生大学医学部医学教育ワークショップ
    開始年月日
    2011/04/10
    終了年月日
    2011/04/10
    概要
    「基礎教育の充実 ポートフォーリオの導入」に参加した。
  • 件名
    第18回藤田保健衛生大学医学部医学教育ワークショップ
    開始年月日
    2007/05/19
    終了年月日
    2007/05/19
    概要
    「CBT試験問題作成ワークショップ」に参加
  • 件名
    第1回藤田保健衛生大学医学部医学情報教育ワークショップ
    開始年月日
    2014/07/08
    終了年月日
    2014/07/08
    概要
    eラーニングシステムを体験する−Moodleの基礎−」に参加
  • 件名
    第2回藤田保健衛生大学医学部医学情報教育ワークショップ
    開始年月日
    2015/08/01
    終了年月日
    2015/08/01
    概要
    「医学・医療教育におけるインストラクショナルデザインと学習者評価」に参加。
  • 件名
    第3回藤田保健衛生大学医学部医学情報教育ワークショップ
    開始年月日
    2016/09/16
    終了年月日
    2016/09/16
    概要
    「これであなたも教え上手!入門インストラクショナルデザイン」に参加