TAMINATO Tomoya
Kindai University Hospital | Lecturer in Medical School |
Last Updated :2024/11/22
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- Yuzo Fujino; Morio Ueyama; Taro Ishiguro; Daisaku Ozawa; Toshihiko Sugiki; Hayato Ito; Asako Murata; Akira Ishiguro; Tania F. Gendron; Kohji Mori; Eiichi Tokuda; Tomoya Taminato; Takuya Konno; Akihide Koyama; Yuya Kawabe; Toshihide Takeuchi; Yoshiaki Furukawa; Toshimichi Fujiwara; Manabu Ikeda; Toshiki Mizuno; Hideki Mochizuki; Hidehiro Mizusawa; Keiji Wada; Kinya Ishikawa; Osamu Onodera; Kazuhiko Nakatani; Hideki Taguchi; Leonard Petrucelli; Yoshitaka NagaieLife Sciences Publications, Ltd 2023/02Abnormal expansions of GGGGCC repeat sequence in the noncoding region of the C9orf72 gene is the most common cause of familial amyotrophic lateral sclerosis and frontotemporal dementia (C9-ALS/FTD). The expanded repeat sequence is translated into dipeptide repeat proteins (DPRs) by noncanonical repeat-associated non-AUG (RAN) translation. Since DPRs play central roles in the pathogenesis of C9-ALS/FTD, we here investigate the regulatory mechanisms of RAN translation, focusing on the effects of RNA-binding proteins (RBPs) targeting GGGGCC repeat RNAs. Using C9-ALS/FTD model flies, we demonstrated that the ALS/FTD-linked RBP FUS suppresses RAN translation and neurodegeneration in an RNA-binding activity-dependent manner. Moreover, we found that FUS directly binds to and modulates the G-quadruplex structure of GGGGCC repeat RNA as an RNA chaperone, resulting in the suppression of RAN translation in vitro. These results reveal a previously unrecognized regulatory mechanism of RAN translation by G-quadruplex-targeting RBPs, providing therapeutic insights for C9-ALS/FTD and other repeat expansion diseases.
- Tomoya Taminato; Toshihide Takeuchi; Morio Ueyama; Kohji Mori; Manabu Ikeda; Hideki Mochizuki; Yoshitaka NagaiHuman molecular genetics 32 (10) 1673 - 1682 2023/01The abnormal expansion of GGGGCC hexanucleotide repeats within the C9orf72 gene is the most common genetic cause of amyotrophic lateral sclerosis (ALS) and frontotemporal dementia (FTD). The accumulation of GGGGCC repeat-containing RNAs as RNA foci, and the deposition of dipeptide repeat proteins (DPR) produced from these repeat RNAs by unconventional translation are major pathological hallmarks of C9orf72-linked ALS/FTD (C9-ALS/FTD), and are both thought to play a crucial role in the pathogenesis of these diseases. Because GGGGCC repeat RNA is likely to be the most upstream therapeutic target in the pathogenic cascade of C9-ALS/FTD, lowering the cellular level of GGGGCC repeat RNA is expected to mitigate repeat RNA toxicity, and will therefore be a disease-modifying therapeutic strategy for the treatment of C9-ALS/FTD. In this study, we demonstrated using a Drosophila model of C9-ALS/FTD that elevated expression of a subset of human RNA-binding proteins that bind to GGGGCC repeat RNA, including hnRNPA3, IGF2BP1, hnRNPA2B1, hnRNPR, and SF3B3, reduces the level of GGGGCC repeat RNA, resulting in the suppression of neurodegeneration. We further showed that hnRNPA3-mediated reduction of GGGGCC repeat RNA suppresses disease pathology, such as RNA foci and DPR accumulation. These results demonstrate that hnRNPA3 and other RNA-binding proteins negatively regulate the level of GGGGCC repeat RNA, and mitigate repeat RNA toxicity in vivo, indicating the therapeutic potential of the repeat RNA-lowering approach mediated by endogenous RNA-binding proteins for the treatment of C9-ALS/FTD.
- fragile X-associated tremor/ataxia syndrome (FXTAS)Tomoya Taminato; Yoshitaka NagaiGene & Medicine (37) 2021/07
- Elucidation of the pathogenesis of ALS and development of treatment methods using the Drosophila modelTomoya Taminato; Yoshitaka NagaiIgakunoayumi 272 (6) 535 - 540 2020/06
- Tomoya Taminato; Madoka Mori-Yoshimura; Jun Miki; Ryogen Sasaki; Noriko Sato; Yasushi Oya; Ichizo Nishino; Yuji TakahashiJournal of neuromuscular diseases 7 (2) 193 - 201 2020BACKGROUND: Paramyotonia congenita (PC; OMIM 168300) is a non-dystrophic myotonia caused by mutations in the SCN4A gene. Transient muscle stiffness, usually induced by exposure to cold and aggravated by exercise, is the predominant clinical symptom, and interictal persistent weakness is uncommon. CASE REPORT: We report a family with a history of PC accompanied by persistent hand muscle weakness with masticatory muscle involvement. Persistent weakness was exacerbated with age, and MR analysis showed marked atrophy of temporal, masseter, and finger flexor muscles with fatty replacement. The PC causative mutation T1313M in the SCN4A gene was prevalent in the family. Administration of acetazolamide chloride improved clinical symptoms and the results of cold and short exercise tests. Phenotypic variation within the family was remarkable, as the two younger affected patients did not present with persistent weakness or muscle atrophy. CONCLUSIONS: PC associated with the T1313M mutation is a possible cause of persistent distal hand weakness.
- hnRNPA3はC9orf72関連FTDモデルショウジョウバエのリピートRNA毒性を軽減する田港 朝也; 上山 盛夫; 森 康治; 池田 学; 永井 義隆Dementia Japan (一社)日本認知症学会 33 (4) 549 - 549 1342-646X 2019/10
- Tomoya Taminato; Manabu Araki; Noriko Sato; Hiroyuki Ishiura; Jun Mitsui; Jun Yoshimura; Koichiro Doi; Shinichi Morishita; Shoji Tsuji; Yuji TakahashiNeurology and Clinical Neuroscience Wiley 7 (5) 294 - 296 2049-4173 2019/07
- Yuji Takahashi; Masahiro Kanai; Tomoya Taminato; Shoko Watanabe; Chihiro Matsumoto; Toshiyuki Araki; Tomoko Okamoto; Masafumi Ogawa; Miho MurataNeurology. Genetics 3 (1) e123 2376-7839 2016/02Spinocerebellar degeneration (SCD) is a group of disorders characterized by progressive ataxia caused by dysfunction and atrophy of the cerebellum or its projections. Approximately one-third of SCD cases are familial SCD, the majority of which are attributed to CAG triplet repeat expansions including spinocerebellar ataxia (SCA)1, SCA2, Machado-Joseph disease (MJD)/SCA3, SCA6, SCA8, SCA12, SCA17, and dentate-rubro-pallido-luysian atrophy (DRPLA). The triplet repeat number of the alleles representing complete penetrance varies among diseases. Generally, there is a gap between the normal alleles and the complete penetrance alleles. Rarely, intermediate alleles with the repeat numbers between the abnormal and normal ranges are observed, although the implications of these intermediate alleles remain ambiguous.
- Neurodegenerative Mechanisms and Therapeutic OutlookYoshitaka Nagfai; Tomoya TaminatoMonthly Mebio 33 (11) 62 - 70 2016
- Yoshihiko Furusawa; Takashi Hanakawa; Yohei Mukai; Yuki Aihara; Tomoya Taminato; Yasuyuki Iawata; Tomohiko Takei; Takashi Sakamoto; Miho MurataParkinsonism & related disorders 21 (7) 765 - 70 2015/07BACKGROUND: We previously classified camptocormia of Parkinson's disease (PD) into upper and lower types based on the inflection point, and reported improvement of upper camptocormia after lidocaine injection into the external oblique. However, the exact pathophysiology of this phenomenon remains obscure. METHODS: Surface electromyography (sEMG) was recorded in 11 PD patients with upper camptocormia, 11 PD patients with lower camptocormia, and 10 age-matched PD patients without postural deformity. Electrodes were positioned above the external oblique, hip flexors and paraspinal muscles at Th11 level bilaterally. Recording commenced with the patient in supine position on a tilt table, and continued when the table was tilted up to vertical position. Lidocaine was injected into the external oblique in patients with upper camptocormia and the psoas major in patients with lower camptocormia. RESULTS: All patients with upper and lower camptocormia developed the corresponding camptocormic posture during tilt up. The onset of camptocormic posture was preceded by the appearance of sEMG activity in the external oblique in 10 out of 11 patients with upper camptocormia, but less frequently in patients with lower camptocormia and the controls. Hip flexors sEMG activity was recorded in almost all patients. Posture was improved in 8 out of 9 patients with upper camptocormia, and 9 out of 11 patients with lower camptocormia following injections of lidocaine. CONCLUSIONS: The results suggest the external oblique is involved, at least in part, in the development of upper camptocormia. Although EMG findings cannot differentiate pathogenicity, the psoas major is probably involved in lower camptocormia.
- Tomoya Taminato; Naoki Miura; Motoaki Sugiura; Ryuta KawashimaNeuroscience research 89 61 - 8 2014/12Visual object recognition is classically believed to involve two stages: a perception stage in which perceptual information is integrated, and a memory stage in which perceptual information is matched with an object's representation. The transition from the perception to the memory stage can be slowed to allow for neuroanatomical segregation using a degraded visual stimuli (DVS) task in which images are first presented at low spatial resolution and then gradually sharpened. In this functional magnetic resonance imaging study, we characterized these two stages using a DVS task based on the classic model. To separate periods that are assumed to dominate the perception, memory, and post-recognition stages, subjects responded once when they could guess the identity of the object in the image and a second time when they were certain of the identity. Activation of the right medial occipitotemporal region and the posterior part of the rostral medial frontal cortex was found to be characteristic of the perception and memory stages, respectively. Although the known role of the former region in perceptual integration was consistent with the classic model, a likely role of the latter region in monitoring for confirmation of recognition suggests the advantage of recently proposed interactive models.
MISC
- 多系統萎縮症患者(MSA-P)に対するL-ドパ合剤の有効性の評価滝澤 歩武; 水野 由輝郎; 磯部 隆; 小松 奏子; 松本 千尋; 金井 雅裕; 田港 朝也; 川添 僚也; 向井 洋平; 古澤 嘉彦; 村田 美穂 臨床神経学 55- (Suppl.) S221 -S221 2015/12
- パーキンソン症候群の誤嚥と咳嗽反射障害の検討山本 敏之; 若杉 憲孝; 磯部 隆; 小松 奏子; 水野 由輝郎; 滝澤 歩武; 田港 朝也; 金井 雅裕; 松本 千尋; 川添 僚也; 向井 洋平; 古澤 嘉彦; 村田 美穂 嚥下医学 4- (2) 278 -278 2015/09
- 痙攣を発症した多発性硬化症・視神経脊髄炎患者の検討田港 朝也; 岡本 智子; 佐藤 和貴郎; 荒木 学; 林 幼偉; 山村 隆; 村田 美穂 臨床神経学 54- (Suppl.) S204 -S204 2014/12
- パーキンソン病患者のL-ドパ内服後のL-ドパ血中濃度の変動滝澤 歩武; 山本 敏之; 松本 千尋; 田港 朝也; 金井 雅弘; 川添 僚也; 三橋 佳奈; 佐野 輝典; 古澤 嘉彦; 坂本 崇; 村田 美穂 臨床神経学 54- (Suppl.) S88 -S88 2014/12
- パーキンソン病における不安の考察小林 惠; 川端 康尋; 古澤 嘉彦; 佐野 輝典; 三橋 佳奈; 川添 僚也; 金井 雅裕; 田港 朝也; 城戸 秀倫; 滝澤 歩武; 松本 千尋; 村田 美穂 臨床神経学 54- (Suppl.) S187 -S187 2014/12
- レビー小体病における誤嚥と咳嗽反射の検討山本 敏之; 滝澤 歩武; 城戸 秀倫; 田港 朝也; 金井 雅裕; 松本 千尋; 三橋 佳奈; 西川 敦子; 佐野 輝典; 向井 洋平; 古澤 嘉彦; 村田 美穂 臨床神経学 54- (Suppl.) S195 -S195 2014/12
- A 59-year-old woman with neuronal intranuclear inclusion body disease presenting with two TIA-like seizures and mild trunk ataxiaTomoya Taminato; Wakiro Sato; Takashi Sakamoto; Yuji Takahashi; Yuko Saito; Miho Murata Clinical neurology 54- (8) 692 -692 2014/08
- A 68-year-old man with ophthalmopharyngeal muscular dystrophy who was unable to walk unaided and had respiratory dysfunction at 5 years of onsetTomoya Taminato; Yoshihiko Furusawa; Madoka Mori; Tadashi Tsukamoto; Toshiyuki Yamamoto; Yasushi Ohya; Ichizo Nishino; Miho Murata Clinical neurology 54- (3) 260 -260 2014/03
- Wearing offに対する入院での薬剤調整の検討向井 洋平; 田港 朝也; 三橋 佳奈; 川添 僚也; 佐野 輝典; 佐藤 和貴郎; 古澤 嘉彦; 坂本 崇; 村田 美穂 臨床神経学 53- (12) 1490 -1490 2013/12
- 携帯型モーションレコーダーを用いた腰曲がりの定量評価に関する検討田港 朝也; 古澤 嘉彦; 金井 雅裕; 佐野 輝典; 向井 洋平; 佐藤 和貴郎; 坂本 崇; 村田 美穂 臨床神経学 53- (12) 1615 -1615 2013/12
- Vestibular evoked muscle potential testing (VEMP) in Parkinson's disease-related disorders and multiple system atrophyTadashi Tsukamoto; Masahiro Kanai; Tomoya Kawazoe; Wakiro Sato; Terunori Sano; Tomoya Taminato; Atsuko Nishikawa; Kana Mitsuhashi; Hiroshi Mukai; Yoshihiko Furusawa; Masafumi Ogawa; Miho Murata Clinical neurology 53- (12) 1520 -1520 2013/12