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  1. 原著論文

Design, synthesis and biological evaluation of small molecule based PET radioligand for 5-HT7 receptor

https://repo.qst.go.jp/records/47064
https://repo.qst.go.jp/records/47064
fcb10d10-8d13-406b-96c3-d56db80bbfc4
Item type 学術雑誌論文 / Journal Article(1)
公開日 2015-03-25
タイトル
タイトル Design, synthesis and biological evaluation of small molecule based PET radioligand for 5-HT7 receptor
言語
言語 eng
資源タイプ
資源タイプ識別子 http://purl.org/coar/resource_type/c_6501
資源タイプ journal article
アクセス権
アクセス権 metadata only access
アクセス権URI http://purl.org/coar/access_right/c_14cb
著者 Tiwari, Anjani

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WEKO 469973

Tiwari, Anjani

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Yui, Joji

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WEKO 469974

Yui, Joji

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Pooja, Singh

× Pooja, Singh

WEKO 469975

Pooja, Singh

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Agrawal, Swati

× Agrawal, Swati

WEKO 469976

Agrawal, Swati

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Yamasaki, Tomoteru

× Yamasaki, Tomoteru

WEKO 469977

Yamasaki, Tomoteru

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Xie, Lin

× Xie, Lin

WEKO 469978

Xie, Lin

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Chadha, Nidhi

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WEKO 469979

Chadha, Nidhi

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Zhang, Yiding

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WEKO 469980

Zhang, Yiding

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Fujinaga, Masayuki

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WEKO 469981

Fujinaga, Masayuki

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Shimoda, Yoko

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WEKO 469982

Shimoda, Yoko

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Kumata, Katsushi

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WEKO 469983

Kumata, Katsushi

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Anil, K Mishra

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WEKO 469984

Anil, K Mishra

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Ogawa, Masanao

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WEKO 469985

Ogawa, Masanao

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Zhang, Ming-Rong

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WEKO 469986

Zhang, Ming-Rong

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ティワリ アンジャニ

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WEKO 469987

en ティワリ アンジャニ

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由井 譲二

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WEKO 469988

en 由井 譲二

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山崎 友照

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WEKO 469989

en 山崎 友照

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謝 琳

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WEKO 469990

en 謝 琳

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張 一鼎

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WEKO 469991

en 張 一鼎

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藤永 雅之

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WEKO 469992

en 藤永 雅之

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下田 陽子

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WEKO 469993

en 下田 陽子

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熊田 勝志

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WEKO 469994

en 熊田 勝志

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小川 政直

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WEKO 469995

en 小川 政直

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張 明栄

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WEKO 469996

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抄録
内容記述タイプ Abstract
内容記述 The 5-HT7 receptor is a recently cloned G-protein-coupled receptor (GPCR) that is important in regulating
sleep, depression, and circadian rhythms. However, the potential pathophysiological roles of 5-HT7 have
not been fully elucidated, and no 5-HT7 positron emission tomography (PET) radioligands are available,
thus limiting imaging studies of this receptor in humans. Here, we present the radiosynthesis and
biological evaluation of 5-(4-([11C]methoxyphenyl)-1-methyl-4-nitro-1H-imidazole ([11C]1) as a new PET
ligand for 5-HT7. Three-dimensional pharmacophore evaluation and docking studies confirmed its high
affinity for 5-HT7, and in vitro binding assays showed that the binding affinity was 16.8 0.9 nM. The
specific activity was found to be 48 29 GBq mmol 1 for [11C]1 in a synthetic time of 26 3 min (n ¼ 8),
having 38 7% radiochemical yield (decay-corrected) based on [11C]CO2. Ligand interactions with
human serum albumin were studied by fluorescence quenching to obtain a Stern–Volmer plot, which
showed a binding constant of 1.15 104 M 1. Whole-body biodistribution patterns were evaluated in
normal mice by 1 h dynamic PET imaging; this analysis showed rapid clearance of radioactivity from the
main peripheral organs, with the exception of the liver. Preliminary PET studies in rat brains showed rapid
accumulation of radioactivity in the brain. The regional radioactivity reached a maximum within 0–2 min
after the radioligand injection and then decreased rapidly, resulting in minimal radiation burden in the
brain during the scan. In summary, this specific biaryl system has shown potential as a 5-HT7 ligand and
further optimization and longitudinal studies may yield the first small molecule-based PET ligand for
5-HT7 in clinical settings.
書誌情報 RSC Advances

巻 5, 号 25, p. 19752-19759, 発行日 2015-02
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