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[(11)C]N-甲基兰索拉唑作为用于tau神经原纤维缠结PET成像的放射性药物的评估。

Evaluation of [(11)C]N-Methyl Lansoprazole as a Radiopharmaceutical for PET Imaging of Tau Neurofibrillary Tangles.

作者信息

Shao Xia, Carpenter Garrett M, Desmond Timothy J, Sherman Phillip, Quesada Carole A, Fawaz Maria, Brooks Allen F, Kilbourn Michael R, Albin Roger L, Frey Kirk A, Scott Peter J H

机构信息

Division of Nuclear Medicine, Department of Radiology, The University of Michigan Medical School , Ann Arbor, Michigan 48109, United States.

Geriatrics Research, Education, and Clinical Center, VAAAHS , Ann Arbor, Michigan 48105, United States ; Department of Neurology, The University of Michigan Medical School , Ann Arbor, Michigan 48109, United States.

出版信息

ACS Med Chem Lett. 2012 Sep 25;3(11):936-41. doi: 10.1021/ml300216t. eCollection 2012 Nov 8.

Abstract

[(11)C]N-Methyl lansoprazole ([(11)C]NML, 3) was synthesized and evaluated as a radiopharmaceutical for quantifying tau neurofibrillary tangle (NFT) burden using positron emission tomography (PET) imaging. [(11)C]NML was synthesized from commercially available lansoprazole in 4.6% radiochemical yield (noncorrected RCY, based upon [(11)C]MeI), 99% radiochemical purity, and 16095 Ci/mmol specific activity (n = 5). Log P was determined to be 2.18. A lack of brain uptake in rodent microPET imaging revealed [(11)C]NML to be a substrate for the rodent permeability-glycoprotein 1 (PGP) transporter, but this could be overcome by pretreating with cyclosporin A to block the PGP. Contrastingly, [(11)C]NML was not found to be a substrate for the primate PGP, and microPET imaging in rhesus revealed [(11)C]NML uptake in the healthy primate brain of ∼1600 nCi/cc maximum at 3 min followed by rapid egress to 500 nCi/cc. Comparative autoradiography between wild-type rats and transgenic rats expressing human tau (hTau +/+) revealed 12% higher uptake of [(11)C]NML in the cortex of brains expressing human tau. Further autoradiography with tau positive brain samples from progressive supranuclear palsy (PSP) patients revealed colocalization of [(11)C]NML with tau NFTs identified using modified Bielschowsky staining. Finally, saturation binding experiments with heparin-induced tau confirmed K d and Bmax values of [(11)C]NML as 700 pM and 0.214 fmol/μg, respectively.

摘要

合成了[(11)C]N-甲基兰索拉唑([(11)C]NML, 3),并将其作为一种放射性药物进行评估,用于通过正电子发射断层扫描(PET)成像定量tau神经原纤维缠结(NFT)负荷。[(11)C]NML由市售兰索拉唑合成,放射化学产率为4.6%(未校正RCY,基于[(11)C]MeI),放射化学纯度为99%,比活度为16095 Ci/mmol(n = 5)。Log P测定为2.18。啮齿动物微型PET成像显示缺乏脑摄取,表明[(11)C]NML是啮齿动物通透性糖蛋白1 (PGP)转运蛋白的底物,但这可以通过用环孢菌素A预处理来阻断PGP来克服。相反,[(11)C]NML未被发现是灵长类PGP的底物,恒河猴的微型PET成像显示[(11)C]NML在健康灵长类大脑中的摄取在3分钟时最高约为1600 nCi/cc,随后迅速下降至500 nCi/cc。野生型大鼠和表达人tau的转基因大鼠(hTau +/+)之间的比较放射自显影显示,表达人tau的大脑皮层中[(11)C]NML的摄取高12%。对进行性核上性麻痹(PSP)患者的tau阳性脑样本进行进一步放射自显影,发现[(11)C]NML与使用改良 Bielschowsky染色鉴定的tau NFT共定位。最后,用肝素诱导的tau进行饱和结合实验,确定[(11)C]NML的K d和Bmax值分别为700 pM和0.214 fmol/μg。

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