附属病院 とちぎ子ども医療センター

門田 行史

モンデン ユキフミ  (monden yukifumi)

基本情報

所属
自治医科大学 附属病院 とちぎ子ども医療センター小児科 准教授
学位
医学博士(自治医科大学)

研究者番号
80382951
J-GLOBAL ID
201301052901808261
researchmap会員ID
B000230064

2010年にMonden labを開設しました。研究室ホームページ http://mon-lab.weblike.jp/
研究テーマである神経発達症については、『脳機能研究』と『PCITを中心とした行動療法』を中心に取り組んでおります。


受賞

 15

論文

 104
  • Hirokazu Yamagishi, Hitoshi Osaka, Kazuhiro Muramatsu, Karin Kojima, Yukifumi Monden, Tadahiro Mitani, Yuta Asakura, Keizo Wakae, Kohei Nagai, Toshihiro Tajima
    Scientific reports 14(1) 30051-30051 2024年12月3日  
    Seizures in patients with developmental and epileptic encephalopathies (DEEs) are often highly resistant to various antiseizure medications. Perampanel (PER) is a novel antiseizure medication that non-competitively inhibits the α-amino-3-hydroxy-5-methyl-4-isoxazolepropionic acid receptor and is expected to reduce seizure frequency not only for focal seizures and generalized tonic-clonic seizures (GTCS) but also for other seizure types. This study aimed to clarify the long-term therapeutic efficacy and tolerability of PER in patients with DEEs. We analyzed data regarding patients' background characteristics, medication retention, trends in seizure frequency, and adverse events obtained from 24 patients with DEEs who had been on PER treatment for 60 months. The retention rates were 62.5% and 46.9% at 12 and 60 months, respectively. At 60 months after PER initiation, the rate of patients with > 50% seizure reduction was 33.3%, 33.3%, 38.5%, 54.5%, 54.5%, and 36.4% among patients with atypical absence seizures, tonic seizures, focal seizures, GTCS, myoclonic seizures, and atonic seizures, respectively. The frequency of adverse events was 70.8%. PER showed long-term efficacy in various seizure types. PER is a promising treatment option for patients with DEEs.
  • Koyuru Kurane, Niannian Lin, Ippeita Dan, Hikari Tanaka, Yuki Tsuji, Wakana Ito, Shiho Yanagida, Yukifumi Monden
    Brain & development 2024年10月10日  
    OBJECTIVE: This study undertook neuropharmacological research on the clinical course of controlled medication discontinuation to guide practitioners who are considering stopping medications for youths with attention-deficit hyperactivity disorder (ADHD). METHODS: This study analyzed the data for 14 ADHD children (12 male and 2 female) in two datasets: The children prescribed methylphenidate (MPH) were at an initial mean age of 7.5 years (SD = 1.70, range: 6-11) with a mean ADHD-Rating Score (ADHD-RS) of 26.6 (SD = 8.64, range 15-40). The children who discontinued MPH based on clinical judgment were at a mean age of 12.21 years (SD = 2.12, range: 8-15) with a mean ADHD-RS of 15.9 (SD = 6.86, range 5-27). The go/no-go task was used to assess response inhibition, while functional near-infrared spectroscopy (fNIRS) was used to measure cerebral hemodynamics. Oxygenated hemoglobin (Oxy-Hb) values from fNIRS data were analyzed for each subject, focusing on past and current measurements. Baseline was set at 10 s pre-task, with interval means from 4 to 24 s analyzed. One-sample t-tests were used to evaluate brain activity magnitude. RESULTS: The results of the study demonstrate that the children who had discontinued the medication exhibited activation in specific brain regions including the frontopolar cortex and the right ventrolateral prefrontal cortex. Activation (t = 2.363, p = 0.034, Cohen's d = 0.632) was found especially in the right dorsolateral prefrontal cortex during the performance of the go/no-go task. These activated areas were consistent with those observed in a previous study comparing brain activity during a go/no-go task between children with ADHD and healthy children. CONCLUSION: The present study showed differences in cerebral hemodynamics before and after discontinuation of MPH in ADHD children whose ADHD symptoms did not recur after MPH was discontinued. In the near future, further investigations that include control groups will be conducted to demonstrate the effects of MPH prior to discontinuation based on the changes in cerebral blood flow in the right prefrontal cortex, which is involved in behavioral inhibition, as observed in this study. This and future research will facilitate the development of criteria for discontinuing treatment.
  • 江頭 晟良, 奥村 一輝, 若江 惠三, 月田 貴和子, 三谷 忠宏, 山岸 裕和, 小島 華林, 門田 行史, 村松 一洋, 小川 仁, 田島 敏広
    栃木県医学会々誌 54 12-12 2024年6月  
  • 山岸 裕和, 門田 行史, 小坂 仁, 渡辺 浩史, 関戸 真理恵, 下泉 秀夫
    脳と発達 56(Suppl.) S209-S209 2024年5月  
  • 三谷 忠宏, 志賀 順一, 松本 歩, 門田 行史, 小坂 仁, 柳橋 達彦
    脳と発達 56(Suppl.) S251-S251 2024年5月  

MISC

 139

書籍等出版物

 2

講演・口頭発表等

 18

共同研究・競争的資金等の研究課題

 9

産業財産権

 3

学術貢献活動

 1

社会貢献活動

 15

その他

 5