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DEVELOPMENTS OF NEW PET LIGANDS BASED ON 3-[5-(PYRIDINE-2-YL)-2H-TETRAZOL-2-YL]BENZONITRILE FOR METABOTROPIC GLUTAMATE RECEPTOR 5 (mGluR5) IMAGING

https://repo.qst.go.jp/records/71869
https://repo.qst.go.jp/records/71869
ab91a9a7-abe8-4c9b-b172-e22d07c90ad8
Item type 会議発表用資料 / Presentation(1)
公開日 2015-11-25
タイトル
タイトル DEVELOPMENTS OF NEW PET LIGANDS BASED ON 3-[5-(PYRIDINE-2-YL)-2H-TETRAZOL-2-YL]BENZONITRILE FOR METABOTROPIC GLUTAMATE RECEPTOR 5 (mGluR5) IMAGING
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_c94f
資源タイプ conference object
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 Shimoda, Yoko

× Shimoda, Yoko

WEKO 707705

Shimoda, Yoko

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Yamasaki, Tomoteru

× Yamasaki, Tomoteru

WEKO 707706

Yamasaki, Tomoteru

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Fujinaga, Masayuki

× Fujinaga, Masayuki

WEKO 707707

Fujinaga, Masayuki

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Ogawa, Masanao

× Ogawa, Masanao

WEKO 707708

Ogawa, Masanao

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Yusuke, Kurihara

× Yusuke, Kurihara

WEKO 707709

Yusuke, Kurihara

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Nengaki, Nobuki

× Nengaki, Nobuki

WEKO 707710

Nengaki, Nobuki

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Kumata, Katsushi

× Kumata, Katsushi

WEKO 707711

Kumata, Katsushi

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Yui, Joji

× Yui, Joji

WEKO 707712

Yui, Joji

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Hatori, Akiko

× Hatori, Akiko

WEKO 707713

Hatori, Akiko

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Xie, Lin

× Xie, Lin

WEKO 707714

Xie, Lin

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Zhang, Yiding

× Zhang, Yiding

WEKO 707715

Zhang, Yiding

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Kawamura, Kazunori

× Kawamura, Kazunori

WEKO 707716

Kawamura, Kazunori

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Zhang, Ming-Rong

× Zhang, Ming-Rong

WEKO 707717

Zhang, Ming-Rong

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下田 陽子

× 下田 陽子

WEKO 707718

en 下田 陽子

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山崎 友照

× 山崎 友照

WEKO 707719

en 山崎 友照

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藤永 雅之

× 藤永 雅之

WEKO 707720

en 藤永 雅之

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小川 政直

× 小川 政直

WEKO 707721

en 小川 政直

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栗原 雄祐

× 栗原 雄祐

WEKO 707722

en 栗原 雄祐

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念垣 信樹

× 念垣 信樹

WEKO 707723

en 念垣 信樹

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熊田 勝志

× 熊田 勝志

WEKO 707724

en 熊田 勝志

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由井 譲二

× 由井 譲二

WEKO 707725

en 由井 譲二

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羽鳥 晶子

× 羽鳥 晶子

WEKO 707726

en 羽鳥 晶子

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謝 琳

× 謝 琳

WEKO 707727

en 謝 琳

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張 一鼎

× 張 一鼎

WEKO 707728

en 張 一鼎

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河村 和紀

× 河村 和紀

WEKO 707729

en 河村 和紀

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張 明栄

× 張 明栄

WEKO 707730

en 張 明栄

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抄録
内容記述タイプ Abstract
内容記述 Objectives: Metabotropic glutamate receptor 5 (mGluR5) is characterized as a G protein coupled receptor and is known as one of regulators for excitatory neurotransmission, which is involved in central nervous system (CNS) disorders, such as fragile X syndrome, Parkinson’s disease, and depression. Therefore, mGluR5 is an important target for development of new pharmaceuticals against these CNS disorders. Recently, 3-[5-(pyridine-2-yl)2H-tetrazol-2-yl]benzonitrile (1) has been reported as a potential compound for mGluR5 (Ki = 190 nM). In this study, we attempt to develop novel a PET ligand for mGluR5 using 1 as a lead compound.
\nResults and Discussions:
1. In vitro binding assay: Five new analogs of 1 were designed and synthesized (Figure 1). Their affinity for mGluR5 was estimated using a binding assay with the mGluR5-seletive radioligand (E)-[11C]ABP688 in rat brain homogenate. Of these analogs, compounds 2a and 2b showed relatively high affinity (2a: Ki = 10.8 nM; 2b: Ki = 9.4 nM) for mGluR5.
2. Radiochemistry: [11C]2a and [11C]2b were synthesized by reacting desmethyl or arylstannyl precursor with [11C]CH3I. Starting from 14.8–22.2 GBq [11C]CO2, 0.58–0.91 GBq [11C]2a was produced with 14 ± 4% (n = 3) radiochemical yield at 32 min after the end of bombardment (EOB). Starting from 22.2–28.1 GBq [11C]CO2, 0.86–2.99 GBq [11C]2b was acquired with 25 ± 14% (n = 11) radiochemical yield at 32 min after EOB. In the final product solution, the specific activity of [11C]2a and [11C]2b was 57–71 and 52–190 GBq/µmol, respectively. Radiochemical purity of both ligands was higher than 98% at the end of synthesis.
3. In vitro Autoradiography: In vitro autoradiography with [11C]2a or [11C]2b was performed using rat brain sections. In the control sections, distribution pattern of both radioligands was heterogeneously exhibited, which corresponded with the biological localization of mGluR5. In blocking study, co-incubation with mGluR5-selective MPEP (1.0 μM) dramatically diminished the accumulations of radioactivity. The specific binding of [11C]2b was slightly higher than that of [11C]2a. Therefore, we decided to perform further evaluation of [11C]2b using PET assessment.
4. Small-animal PET study: In control rats, the uptake of [11C]2b immediately reached maximum levels in the brain regions after injection and quickly decreased after that. The uptake ratio of each region against cerebellum, a reference region for mGluR5, under the equilibrium state was 3.0 ± 0.1 in the striatum, 2.4 ± 0.1 in the hippocampus, 2.3 ± 0.1 in the frontal cortex, and 2.0 ± 0.1 in the thalamus, respectively. By treatment with MPEP, these ratio reduced by 1.3–1.6 in each brain region. As shown in Figure 2, the parametric PET images could identify regional differences in specific binding to mGluR5, demonstrating that PET with [11C]2b could provide significant signal for mGluR5 in brain regions.
Conclusions: We have found out compound  2b as a promising PET ligand candidate for mGluR5 by in vitro binding assay and subsequently synthesized [11C]2b. PET study with [11C]2b in rat brain was possible to visualize regional distribution of mGluR5. [11C]2b is a potential PET ligand for imaging of mGluR5 in brain.
会議概要(会議名, 開催地, 会期, 主催者等)
内容記述タイプ Other
内容記述 Ninth Japan-China Joint Seminar on Radiopharmaceutical Chemistry
発表年月日
日付 2015-11-09
日付タイプ Issued
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