ID | 116497 |
Author |
Kondo, Takayuki
Kyoto University
Banno, Haruhiko
Kyoto University
Okunomiya, Taro
Kyoto University
Amino, Yoko
Kyoto University
Endo, Kayoko
Kyoto University
Nakakura, Akiyoshi
Kyoto University
Uozumi, Ryuji
Kyoto University
Kinoshita, Akemi
Kyoto University
Tada, Harue
Kyoto University
Morita, Satoshi
Kyoto University
Ishikawa, Hidehiro
Mie University
Shindo, Akihiro
Mie University
Yasuda, Ken
Kyoto University
Taruno, Yosuke
Kyoto University
Maki, Takakuni
Kyoto University
Suehiro, Takashi
Osaka University
Mori, Kohji
Osaka University
Ikeda, Manabu
Osaka University
Fujita, Koji
Tokushima University
Tokushima University Educator and Researcher Directory
KAKEN Search Researchers
Izumi, Yuishin
Tokushima University
Tokushima University Educator and Researcher Directory
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Kanemaru, Kazutomi
Tokyo Metropolitan Geriatric Medical Center
Ishii, Kenji
Tokyo Metropolitan Institute of Gerontology
Shigenobu, Kazue
Asakayama Hospital
Kutoku, Yumiko
Kawasaki Medical School
Sunada, Yoshihide
Kawasaki Medical School
Kawakatsu, Shinobu
Fukushima Medical University
Shiota, Shunji
Time Therapeutics
Watanabe, Toshifumi
Time Therapeutics
Uchikawa, Osamu
Towa Pharmaceutical
Takahashi, Ryosuke
Kyoto University
Tomimoto, Hidekazu
Mie University
Inoue, Haruhisa
Kyoto University
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Content Type |
Journal Article
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Description | Introduction
Alzheimer’s disease (AD) is one of the most common causes of dementia. Pathogenic variants in the presenilin 1 (PSEN1) gene are the most frequent cause of early-onset AD. Medications for patients with AD bearing PSEN1 mutation (PSEN1-AD) are limited to symptomatic therapies and no established radical treatments are available. Induced pluripotent stem cell (iPSC)-based drug repurposing identified bromocriptine as a therapeutic candidate for PSEN1-AD. In this study, we used an enrichment strategy with iPSCs to select the study population, and we will investigate the safety and efficacy of an orally administered dose of bromocriptine in patients with PSEN1-AD. Methods and analysis This is a multicentre, randomised, placebo-controlled trial. AD patients with PSEN1 mutations and a Mini Mental State Examination-Japanese score of ≤25 will be randomly assigned, at a 2:1 ratio, to the trial drug or placebo group (≥4 patients in TW-012R and ≥2 patients in placebo). This clinical trial consists of a screening period, double-blind phase (9 months) and extension phase (3 months). The double-blind phase for evaluating the efficacy and safety is composed of the low-dose maintenance period (10 mg/day), high-dose maintenance period (22.5 mg/day) and tapering period of the trial drug. Additionally, there is an open-labelled active drug extension period for evaluating long-term safety. Primary outcomes are safety and efficacy in cognitive and psychological function. Also, exploratory investigations for the efficacy of bromocriptine by neurological scores and biomarkers will be conducted. Ethics and dissemination The proposed trial is conducted according to the Declaration of Helsinki, and was approved by the Institutional Review Board (K070). The study results are expected to be disseminated at international or national conferences and published in international journals following the peer-review process. |
Journal Title |
BMJ Open
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ISSN | 20446055
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Publisher | BMJ Publishing Group
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Volume | 11
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Issue | 6
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Start Page | e051343
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Published Date | 2021-06-30
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Rights | This is an open access article distributed in accordance with the Creative Commons Attribution Non Commercial (CC BY-NC 4.0) license, which permits others to distribute, remix, adapt, build upon this work non-commercially, and license their derivative works on different terms, provided the original work is properly cited, appropriate credit is given, any changes made indicated, and the use is non-commercial. See: http://creativecommons.org/licenses/by-nc/4.0/.
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language |
eng
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Publisher
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departments |
University Hospital
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