基本情報
- 所属
- 自治医科大学 医学部 解剖学講座組織学部門 講師
- 学位
- 博士(薬学)(東京薬科大学)
- 研究者番号
- 00870718
- J-GLOBAL ID
- 201901010102362684
- researchmap会員ID
- B000348657
経歴
5-
2022年5月 - 現在
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2020年2月 - 2022年4月
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2017年10月 - 2020年1月
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2017年4月 - 2017年10月
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2016年4月 - 2017年3月
学歴
2-
2013年4月 - 2017年3月
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2007年4月 - 2013年3月
委員歴
5-
2023年4月 - 現在
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2020年12月 - 現在
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2023年1月 - 2023年8月
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2021年4月 - 2023年3月
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2014年4月 - 2015年3月
受賞
14-
2024年10月
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2024年2月
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2023年11月
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2023年11月
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2023年9月
論文
21-
Acta histochemica et cytochemica 57(4) 131-135 2024年8月29日Multiple sclerosis, neuromyelitis optica, Guillain-Barré syndrome and chronic inflammatory demyelinating polyradiculoneuropathy are representative demyelinating diseases of the central and peripheral nervous system. Remyelination by myelin forming cells is important for functional recovery from the neurological deficits caused in the demyelinating diseases. Lysophosphatidylcholine-induced demyelination in mice is commonly used to identify and study the molecular pathways of demyelination and remyelination. However, detection of focally demyelinated lesions is difficult and usually requires sectioning of demyelinated lesions in tissues for microscopic analysis. In this review, we describe the development and application of a novel vital staining method for labeling demyelinated lesions using intraperitoneal injection of neutral red (NR) dye. NR labeling reduces the time and effort required to search for demyelinated lesions in tissues, and facilitates electron microscopic analysis of myelin structures. NR labeling also has the potential to contribute to the elucidation of pathologies in the central and peripheral nervous system and assist with identification of drug candidates that promote remyelination.
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Journal of neurochemistry 2024年8月13日Myelin is an insulator that forms around axons that enhance the conduction velocity of nerve fibers. Oligodendrocytes dramatically change cell morphology to produce myelin throughout the central nervous system (CNS). Cytoskeletal alterations are critical for the morphogenesis of oligodendrocytes, and actin is involved in cell differentiation and myelin wrapping via polymerization and depolymerization, respectively. Various protein members of the myosin superfamily are known to be major binding partners of actin filaments and have been intensively researched because of their involvement in various cellular functions, including differentiation, cell movement, membrane trafficking, organelle transport, signal transduction, and morphogenesis. Some members of the myosin superfamily have been found to play important roles in the differentiation of oligodendrocytes and in CNS myelination. Interestingly, each member of the myosin superfamily expressed in oligodendrocyte lineage cells also shows specific spatial and temporal expression patterns and different distributions. In this review, we summarize previous findings related to the myosin superfamily and discuss how these molecules contribute to myelin formation and regeneration by oligodendrocytes.
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Acta histochemica et cytochemica 57(1) 1-5 2024年2月29日 査読有り招待有り筆頭著者責任著者Multiple sclerosis (MS) is an inflammatory demyelinating disease of the central nervous system, characterized by remyelination failure and axonal dysfunction. Remyelination by oligodendrocytes is critical for improvement of neurological deficits associated with demyelination. Rodent models of demyelination are frequently used to develop and evaluate therapies for MS. However, a suitable mouse model for assessing remyelination-associated recovery of motor functions is currently unavailable. In this review, we describe the development of the mouse model of internal capsule (IC) demyelination by focal injection of lysolecithin into brain and its application in the evaluation of drugs for demyelinating diseases. This mouse model exhibits motor deficits and subsequent functional recovery accompanying IC remyelination. Notably, this model shows enhancement of functional recovery as well as tissue regeneration when treated with clemastine, a drug that promotes remyelination. The IC demyelination mouse model should contribute to the development of novel drugs that promote remyelination and ameliorate neurological deficits in demyelinating diseases.
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bioRxiv doi: https://doi.org/10.1101/2023.10.03.560586 2023年10月
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Neurochemistry international 164 105505-105505 2023年2月6日 査読有り筆頭著者責任著者Multiple sclerosis (MS) is an inflammatory demyelinating disease of the central nervous system characterized by remyelination failure, axonal degeneration, and progressive worsening of motor functions. Animal models of demyelination are frequently used to develop and evaluate therapies for MS. We recently reported that focal internal capsule (IC) demyelination in mice with lysophosphatidylcholine injection induced acute motor deficits followed by recovery through remyelination. However, it remains unknown whether the IC demyelination mouse model can be used to evaluate changes in motor functions caused by pharmacological treatments that promote remyelination using behavioral testing and histological analysis. In this study, we examined the effect of clemastine, an anti-muscarinic drug that promotes remyelination, in the mouse IC demyelination model. Clemastine administration improved motor function and changed forepaw preference in the IC demyelinated mice. Moreover, clemastine-treated mice showed increased mature oligodendrocyte density, reduced axonal injury, an increased number of myelinated axons and thicker myelin in the IC lesions compared with control (PBS-treated) mice. These results suggest that the lysophosphatidylcholine-induced IC demyelination model is useful for evaluating changes in motor functions following pharmacological treatments that promote remyelination.
MISC
43-
日本組織細胞化学会総会・学術集会講演プログラム・予稿集 64回 38-38 2023年10月
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The Journal of Physiological Sciences 71(Suppl.1) 89-89 2021年8月
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Journal of Neurochemistry 150(146) MTU11-27 2019年8月
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JOURNAL OF NEUROCHEMISTRY 142 172-173 2017年8月
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Journal of Neurochemistry 142(141) WTH01-23 2017年8月
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JOURNAL OF NEUROCHEMISTRY 134 109-109 2015年8月
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Journal of Neurochemistry 134(109) MTU01-21 2015年8月
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Journal of Neurochemistry 125(217) PTW02-30 2013年4月
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JOURNAL OF NEUROCHEMISTRY 123 58-58 2012年10月
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Journal of Neurochemistry 123(58) P01-36 2012年10月 筆頭著者
講演・口頭発表等
51-
第66回日本顕微鏡学会シンポジウム 2023年11月12日
担当経験のある科目(授業)
6共同研究・競争的資金等の研究課題
17-
日本医療研究開発機構 脳神経科学統合プログラム(個別重点研究課題) 2024年9月 - 2027年3月
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小林財団 研究助成 2023年3月 - 2026年9月
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日本学術振興会 科学研究費助成事業 2023年4月 - 2026年3月
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日本学術振興会 科学研究費助成事業 若手研究 2023年4月 - 2025年3月
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上原記念生命科学財団 研究奨励金 2024年3月 - 2025年3月
学術貢献活動
2-
企画立案・運営等, パネル司会・セッションチェア等日本神経化学会、山崎礼二、阿部 欣史 2023年7月8日
メディア報道
2-
MEDICINE INNOVATES https://medicineinnovates.com/advancing-multiple-sclerosis-research-ic-demyelination-mouse-model/ 2023年9月 インターネットメディア