基本情報(Profile)
最終更新日(Last Updated)2022/11/21稲垣 舞
MAI INAGAKI
稲垣 舞
徳島大学(Tokushima University)
大学院医歯薬学研究部(薬学域)(Graduate School of Biomedical Sciences)
| 薬剤学、薬物動態学、胎盤関門、胎盤‐脳連関に基づく脳への薬物送達 |
| 医歯薬学(Medicine,dentistry, and pharmacy) | 薬学(Pharmacy) | 医療系薬学(Medical pharmacy)(Medical pharmacy) |
教員(Faculty) - 助教相当(Assistant Prof. Equiv.)
自己アピール(Appealing Points)
愛知県出身。2014年、慶應義塾大学薬学部を卒業。2020年に同大学大学院薬学研究科博士後期課程を修了し、学位を取得。同年4月より徳島大学大学院医歯薬学研究部(薬学域)の助教に着任し、現在に至る。
胎盤研究を通して、女性のヘルスケア向上に貢献していきたい。
研究活動(Research Activities)
- 論文(Published Papers)
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2022 Transport characteristics of placenta-derived extracellular vesicles and its relevance to placenta-to-maternal tissues communication.
Chem Pharm Bull (Tokyo), 70(5), 324-329 , Peer-Reviewed , 10.1248/cpb.c22-0007235491187 2021/09/20 ATF4-mediated transcriptional regulation protects against β-cell loss during endoplasmic reticulum stress in a mouse model.
Molecular metabolism, 54, 101338 , 10.1016/j.molmet.2021.10133834547510 概要はこちら(Description) OBJECTIVE: Activating transcription factor 4 (ATF4) is a transcriptional regulator of the unfolded protein response and integrated stress response (ISR) that promote the restoration of normal endoplasmic reticulum (ER) function. Previous reports demonstrated that dysregulation of the ISR led to development of severe diabetes. However, the contribution of ATF4 to pancreatic β-cells remains poorly understood. In this study, we aimed to analyze the effect of ISR enhancer Sephin1 and ATF4-deficient β-cells to clarify the role of ATF4 in β-cells under ER stress conditions. METHODS: To examine the role of ATF4 in vivo, ISR enhancer Sephin1 (5 mg/kg body weight, p.o.) was administered daily for 21 days to Akita mice. We also established β-cell-specific Atf4 knockout (βAtf4-KO) mice that were further crossed with Akita mice. These mice were analyzed for characteristics of diabetes, β-cell function, and morphology of the islets. To identify the downstream factors of ATF4 in β-cells, the islets of βAtf4-KO mice were subjected to cDNA microarray analyses. To examine the transcriptional regulation by ATF4, we also performed in situ PCR analysis of pancreatic sections from mice and ChIP-qPCR analysis of CT215 β-cells. RESULTS: Administration of the ISR enhancer Sephin1 improved glucose metabolism in Akita mice. Sephin1 also increased the insulin-immunopositive area and ATF4 expression in the pancreatic islets. Akita/βAtf4-KO mice exhibited dramatically exacerbated diabetes, shown by hyperglycemia at an early age, as well as a remarkably short lifespan owing to diabetic ketoacidosis. Moreover, the islets of Akita/βAtf4-KO mice presented increased numbers of cells stained for glucagon, somatostatin, and pancreatic polypeptide and increased expression of aldehyde dehydrogenase 1 family member 3, a marker of dedifferentiation. Using microarray analysis, we identified atonal BHLH transcription factor 8 (ATOH8) as a downstream factor of ATF4. Deletion of ATF4 in β-cells showed reduced Atoh8 expression and increased expression of undifferentiated markers, Nanog and Pou5f1. Atoh8 expression was also abolished in the islets of Akita/βAtf4-KO mice. CONCLUSIONS: We conclude that transcriptional regulation by ATF4 maintains β-cell identity via ISR modulation. This mechanism provides a promising target for the treatment of diabetes.
2020/05 Contribution of Prostaglandin Transporter OATP2A1/SLCO2A1 to Placenta-to-Maternal Hormone Signaling and Labor Induction
iScience, 23(5), 101098 , Peer-Reviewed , 10.1016/j.isci.2020.1010982589-0042 2017/05 Co-localization of microsomal prostaglandin E synthase-1 with cyclooxygenase-1 in layer II of murine placental syncytiotrophoblasts
Placenta, 53, 76-82 , Peer-Reviewed , 10.1016/j.placenta.2017.04.0020143-4004
- 講演・口頭発表等(Lecture/Oral Presentation)
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2021/05/14 胎盤治療の基盤としての胎盤関門・細胞外小胞輸送システム, 稲垣舞,立川正憲, 日本薬剤学会第36年会 , invited 2021/03/29 ヒト胎盤絨毛細胞株BeWo細胞由来エクソソームのヒト脳血管内皮細胞 (hCMEC/D3)への内在化, 稲垣舞,佐野陽乃里,中野瑛介,登美斉俊,立川正憲, 日本薬学会第141年会 2021/10 ヒト血液脳関門モデルhCMEC/D3細胞におけるクレアチンプロドラッグの輸送特性, 稲垣舞、杉山司、佐藤桃子、吉田将人、土井隆行、和田敬仁、新保裕子、露崎悠、後藤知英、寺崎哲也、立川正憲, 第42回生体膜と薬物の相互作用シンポジウム 2021/11 ヒト脳血管内皮細胞における胎盤栄養膜細胞から分泌される細胞外小胞の輸送特性, 稲垣舞、佐野陽乃里、稲井美紅、赤沼伸乙、細谷健一、立川正憲, 第36回日本薬物動態学会
- 競争的資金等の研究課題(External Funds)
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2021/04-2023/03 胎盤-脳連関に立脚した胎盤エクソソームの血液脳関門透過機構と脳細胞送達性の解明, 日本学術振興会 / Japan Society for the Promotion of Science, 科学研究費助成事業 若手研究 / Grants-in-Aid for Scientific Research Grant-in-Aid for Early-Career Scientists (連携研究者)稲垣 舞, 若手研究 / Grant-in-Aid for Early-Career Scientists, 4680000(円), 徳島大学 / The University of Tokushima 2020/09-2022/03 内在性ウイルスエンベロープを介したエクソソーム輸送機構に基づく胎盤への薬物送達, 日本学術振興会 / Japan Society for the Promotion of Science, 科学研究費助成事業 研究活動スタート支援 / Grants-in-Aid for Scientific Research Grant-in-Aid for Research Activity Start-up (連携研究者)稲垣 舞, 研究活動スタート支援 / Grant-in-Aid for Research Activity Start-up, 2860000(円), 徳島大学 / The University of Tokushima 2018/04-2020/03 プロスタグランジン輸送体による胎児発育・分娩の統合調整機構の解明, 日本学術振興会 / Japan Society for the Promotion of Science, 科学研究費助成事業 特別研究員奨励費 / Grants-in-Aid for Scientific Research Grant-in-Aid for JSPS Fellows (連携研究者)稲垣 舞, 特別研究員奨励費 / Grant-in-Aid for JSPS Fellows, 1900000(円), 慶應義塾大学 / Keio University