Arid
DOI10.1016/j.nucmedbio.2012.05.002
Imaging of VMAT2 binding sites in the brain by F-18-AV-133: The effect of a pseudo-carrier
Zhu, Lin2; Qiao, Hongwen2; Lieberman, Brian P.; Wu, Jingxiao2; Liu, Yajing2,3; Pan, Zhongyun2,3; Ploessl, Karl; Choi, Seok Rye5; Chan, Piu3,4; Kung, Hank F.1,2
通讯作者Kung, Hank F.
来源期刊NUCLEAR MEDICINE AND BIOLOGY
ISSN0969-8051
出版年2012
卷号39期号:7页码:897-904
英文摘要

Objectives: Recently, 9-[F-18]fluoropropyl-(+)-dihydrotetrabenazine (F-18-AV-133) was reported as a new vesicular monoamine transporter (VMAT2) imaging agent for diagnosis of Parkinson’s disease (PD). To shorten the preparation of F-18-AV-133 and to make it more widely available, we evaluated a simple, rapid purification with a solid-phase extraction method (SPE) using an Oasis HLB cartridge instead of high pressure liquid chromatography (HPLC). The SPE method produced doses containing a pseudo-carrier, 9-hydroxypropyl-(+)-dihydrotetrabenazine (AV-149).


Methods: To test the possible side effects of this pseudo-carrier, comparative dynamic PET scans of the brains of normal monkeys (2 each) and uni-laterally 6-OH-dopamine-lesioned PD monkeys (2 each) were performed using F-18-AV-133 doses prepared by either SPE (containing pseudo-carrier) or HPLC (containing no pseudo-carrier). Autoradiographs of post mortem monkey brain sections were evaluated to confirm the relative F-18-AV-133 uptake in the PD monkey brains and the effects of the pseudo-carrier on VMAT2 binding.


Results: The radiochemical purity of the F-18-AV-133, whether prepared by SPE or by HPLC, was excellent (>99%). PET scans of normal and PD monkey brains showed an expected reduction of VMAT2 in the lesioned areas of the striatum. It was not affected by the presence of the pseudo-carrier, AV-149 (maximally 250 mu g/dose). The reduced uptake in the striatum of the lesioned monkey brains was confirmed by autoradiography. Ex vivo inhibition studies of F-18-AV-133 binding in rat brains, conducted with increasing amounts of AV-149, suggested that at the highest concentration (3.5 mg/kg) the VMAT2 binding in the striatum was only moderately blocked (20% reduction).


Conclusions: The pseudo-carrier, AV-149, did not affect the F-18-AV-133/PET imaging of VMAT2 binding sites in normal or uni-laterally lesioned monkey brains. The new streamlined SPE purification method will enable F-18-AV-133 to be widely available for routine clinical application in determining changes in monoamine neurons for patient with movement disorders or other psychiatric illnesses. (c) 2012 Elsevier Inc. All rights reserved.


英文关键词PET imaging Parkinson’s disease Vesicular monoamine transporter 2 Brain imaging and pseudo-carrier effect
类型Article
语种英语
国家USA ; Peoples R China
收录类别SCI-E
WOS记录号WOS:000309033800002
WOS关键词POSITRON-EMISSION-TOMOGRAPHY ; VESICULAR MONOAMINE TRANSPORTERS ; PARKINSONS-DISEASE ; DOPAMINE TRANSPORTER ; UV DETECTION ; PET LIGAND ; DIHYDROTETRABENAZINE ; 2-DEOXY-2-FLUORO-D-GLUCOSE ; F-18-FP-(+)-DTBZ ; TETRABENAZINE
WOS类目Radiology, Nuclear Medicine & Medical Imaging
WOS研究方向Radiology, Nuclear Medicine & Medical Imaging
来源机构北京师范大学
资源类型期刊论文
条目标识符http://119.78.100.177/qdio/handle/2XILL650/174196
作者单位1.Univ Penn, Sch Med, Dept Radiol, Philadelphia, PA 19104 USA;
2.Beijing Normal Univ, Key Lab Radiopharmaceut, Minist Educ, Beijing 100875, Peoples R China;
3.Capital Med Univ, Dept Neurol, Beijing Xuanwu Hosp, Beijing, Peoples R China;
4.Wincon Theracells Biotechnol Co Ltd, Nanning, Peoples R China;
5.Avid Radiopharmaceut Inc, Philadelphia, PA USA
推荐引用方式
GB/T 7714
Zhu, Lin,Qiao, Hongwen,Lieberman, Brian P.,et al. Imaging of VMAT2 binding sites in the brain by F-18-AV-133: The effect of a pseudo-carrier[J]. 北京师范大学,2012,39(7):897-904.
APA Zhu, Lin.,Qiao, Hongwen.,Lieberman, Brian P..,Wu, Jingxiao.,Liu, Yajing.,...&Kung, Hank F..(2012).Imaging of VMAT2 binding sites in the brain by F-18-AV-133: The effect of a pseudo-carrier.NUCLEAR MEDICINE AND BIOLOGY,39(7),897-904.
MLA Zhu, Lin,et al."Imaging of VMAT2 binding sites in the brain by F-18-AV-133: The effect of a pseudo-carrier".NUCLEAR MEDICINE AND BIOLOGY 39.7(2012):897-904.
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