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手性二苯氧基衍生物作为β-淀粉样斑块更具柔性的探针。

Optically Pure Diphenoxy Derivatives as More Flexible Probes for β-Amyloid Plaques.

机构信息

Key Laboratory of Radiopharmaceuticals, Ministry of Education, College of Chemistry, Beijing Normal University , Beijing 100875, P. R. China.

Wuhan Institute for Neuroscience and Neuroengineering, South-Central University for Nationalities , Wuhan 430074, P. R. China.

出版信息

ACS Chem Neurosci. 2016 Sep 21;7(9):1275-82. doi: 10.1021/acschemneuro.6b00155. Epub 2016 Jul 11.

DOI:10.1021/acschemneuro.6b00155
PMID:27337293
Abstract

The highly rigid and planar scaffold with π-conjugated systems has been widely considered to be indispensable for Aβ binding probes. However, the flexible benzyloxybenzene derivative [(125)I]BOB-4 represents an excellent lead candidate for targeting Aβ in AD brains. Based on that, we designed two pairs of more flexible and optically pure diphenoxy derivatives with a chiral center as novel Aβ probes. These compounds possessed high affinity (Ki = 15.8-45.0 nM) for Aβ1-42 aggregates, and (R)-enantiomers showed slightly better binding ability than (S)-enantiomers. In addition, the competition binding assay implied that the optically pure diphenoxy derivatives with more flexible geometry shared the same binding site as IMPY, a classical rigid and planar Aβ probe. For (125)I-radiolabeled enantiomers, (S)-[(125)I]5 and (R)-[(125)I]5, specific plaque labeling on brain sections of Tg mice and AD patients were observed in in vitro autoradiography, persuasively proving the excellent affinity of the probes. In biodistribution, (S)-[(125)I]5 and (R)-[(125)I]5 with relatively low lipophilicity exhibited moderate initial brain uptake (4.37% and 3.72% ID/g at 2 min, respectively) and extremely fast washout from normal mice brain (brain2min/brain60min = 19.0 and 17.7, respectively). In summary, the separate enantiomers displayed similar properties in vitro and in vivo, and (S/R)-[(123)I]5 may be potential SPECT probes for recognizing Aβ plaques in AD brains.

摘要

具有π共轭体系的高度刚性和平面支架被广泛认为是 Aβ结合探针所必需的。然而,柔性苄氧基苯衍生物[(125)I]BOB-4 是靶向 AD 大脑中 Aβ的优秀先导候选物。基于此,我们设计了两对更具柔性和光学纯的手性中心二苯氧基衍生物作为新型 Aβ探针。这些化合物对 Aβ1-42 聚集物具有高亲和力(Ki = 15.8-45.0 nM),并且(R)-对映体的结合能力略优于(S)-对映体。此外,竞争结合测定表明,具有更柔性几何形状的光学纯二苯氧基衍生物与 IMPY 共享相同的结合位点,IMPY 是一种经典的刚性和平面 Aβ探针。对于(125)I 标记的对映体,(S)-[(125)I]5 和(R)-[(125)I]5,在体外放射自显影中观察到 Tg 小鼠和 AD 患者脑切片上的特异性斑块标记,有力地证明了探针的优异亲和力。在生物分布中,具有相对低脂溶性的(S)-[(125)I]5 和(R)-[(125)I]5 表现出适度的初始脑摄取(分别在 2 分钟时为 4.37%和 3.72% ID/g),并从正常小鼠脑中迅速清除(脑 2 分钟/脑 60 分钟 = 19.0 和 17.7,分别)。总之,分离的对映体在体外和体内表现出相似的性质,并且(S/R)-[(123)I]5 可能是用于识别 AD 大脑中 Aβ斑块的潜在 SPECT 探针。

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