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Synthesis of a carbon-11 labeled spiro-quinazolinone based PDE7 ligand for PET neuroimaging

https://repo.qst.go.jp/records/86450
https://repo.qst.go.jp/records/86450
7d938e81-7241-4a91-a64c-6ed2c7d63045
Item type 会議発表論文 / Conference Paper(1)
公開日 2022-06-07
タイトル
タイトル Synthesis of a carbon-11 labeled spiro-quinazolinone based PDE7 ligand for PET neuroimaging
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_5794
資源タイプ conference paper
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 Xiao, Zhiwei

× Xiao, Zhiwei

WEKO 1055135

Xiao, Zhiwei

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Sun, Jiyun

× Sun, Jiyun

WEKO 1055136

Sun, Jiyun

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Masayuki, Fujinaga

× Masayuki, Fujinaga

WEKO 1055137

Masayuki, Fujinaga

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Zhao, Chunyu

× Zhao, Chunyu

WEKO 1055138

Zhao, Chunyu

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Haider Haider, Ahmed

× Haider Haider, Ahmed

WEKO 1055139

Haider Haider, Ahmed

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Rong, Jian

× Rong, Jian

WEKO 1055140

Rong, Jian

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Shao, Yihan

× Shao, Yihan

WEKO 1055141

Shao, Yihan

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Lee Collier, Thomas

× Lee Collier, Thomas

WEKO 1055142

Lee Collier, Thomas

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C Kent Lloyd, K

× C Kent Lloyd, K

WEKO 1055143

C Kent Lloyd, K

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Lu, Wang

× Lu, Wang

WEKO 1055144

Lu, Wang

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Zhang, Ming-Rong

× Zhang, Ming-Rong

WEKO 1055145

Zhang, Ming-Rong

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Liang, Steven

× Liang, Steven

WEKO 1055146

Liang, Steven

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Masayuki, Fujinaga

× Masayuki, Fujinaga

WEKO 1055147

en Masayuki, Fujinaga

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Lu, Wang

× Lu, Wang

WEKO 1055148

en Lu, Wang

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Zhang, Ming-Rong

× Zhang, Ming-Rong

WEKO 1055149

en Zhang, Ming-Rong

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抄録
内容記述タイプ Abstract
内容記述 Background: The intracellular second messengers, cAMP and cGMP, play a substantial role in signal transduction pathways involving a myriad of processes in the central nervous system (CNS), immune system, and cardiovascular system. Cyclic nucleotide phosphodiesterases (PDEs) constitute a superfamily of enzymes that degrade cAMP and cGMP to regulate the functions of these second messengers. Among the PDE subfamilies (PDE1-PDE11), PDE7 is cAMP-specific and found to be primarily expressed in the brain and heart, followed by liver, skeletal muscles, kidneys and pancreas. Due to the broad expression, PDE7 inhibitors recently have gained increasing attention for their potential applications in neurological, inflammatory, and immunological disorders. This study was aimed to develop a novel PDE7 specific radioligand for PET neuroimaging.
Methods: Based on the spiro-quinazolinone structure which has shown PDE7 inhibitory properties, a methoxy analog P7-2104 was designed and synthesized. The target compound was labeled with carbon-11 using [11C]MeI from the respective desmethyl precursor and tested for its utility by cell uptake studies, ex vivo biodistribution and radiometabolite studies.
Results: From commercially available chemicals, target compound and the corresponding precursor were efficiently synthesized with 49.5% and 12.4% overall yields, respectively (Scheme 1A). After the condensation between 2-chloro-5-methoxyaniline and potassium isocyanate, target compound was synthesized by intermolecular spirocyclization, while the respective precursor was then obtained through demethylation of target compound using hydrobromic acid. [11C]P7-2104 was synthesized in high molar activities (170 - 220 GBq/µmol) with radiochemical yields of 34±7% (Scheme 1B). Compared with HEK293 control cells, higher uptake was found in HEK293-PDE7B recombinant cells which revealed PDE7 specific binding, and ex vivo metabolite studies showed the excellent in vivo stability in rat brain (75% of intact parent at 30 min post injection). In whole body ex vivo biodistribution in CD-1 mice, significant radioactivity accumulation was found in the brain and heart that was consistent with the PDE7 expression profile.
Conclusion: Based on the spiro-quinazolinone scaffold, we have successfully developed a PDE7-targeted radioligand [11C]P7-2104 with excellent specificity and stability. Further evaluation by PET imaging in rodents will be reported in due course.
書誌情報 Nuclear Medicine and Biology

発行日 2022-06
出版者
出版者 Elsevier Ltd.
ISSN
収録物識別子タイプ ISSN
収録物識別子 0969-8051
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