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不带电荷的硫黄素-T衍生物能以高亲和力与β-淀粉样蛋白结合,并能轻易进入大脑。

Uncharged thioflavin-T derivatives bind to amyloid-beta protein with high affinity and readily enter the brain.

作者信息

Klunk W E, Wang Y, Huang G F, Debnath M L, Holt D P, Mathis C A

机构信息

Department of Psychiatry, University of Pittsburgh School of Medicine, PA 15213, USA.

出版信息

Life Sci. 2001 Aug 17;69(13):1471-84. doi: 10.1016/s0024-3205(01)01232-2.

DOI:10.1016/s0024-3205(01)01232-2
PMID:11554609
Abstract

In vivo assessment of the beta-sheet proteins deposited in amyloid plaques (A beta peptide) or neurofibrillary tangles (tau protein) presents a target for the development of biological markers for Alzheimer's disease (AD). In an effort to develop in vivo beta-sheet imaging probes, derivatives of thioflavin-T (ThT) were synthesized and evaluated. These compounds lack the positively charged quaternary heterocyclic nitrogen of ThT and are therefore uncharged at physiological pH. They are 600-fold more lipophilic than ThT. These ThT derivatives bind to A beta(1-40) fibrils with higher affinity (Ki = 20.2 nM) than ThT (Ki = 890 nM). The uncharged ThT derivatives stained both plaques and neurofibrillary tangles in post-mortem AD brain, showing some preference for plaque staining. A carbon-11 labeled compound, [N-methyl-11C]6-Me-BTA-1, was prepared, and its brain entry and clearance were studied in Swiss-Webster mice. This compound entered the brain at levels comparable to commonly used neuroreceptor imaging agents (0.223 %ID-kg/g or 7.61 %ID/g at 2 min post-injection) and showed good clearance of free and non-specifically bound radioactivity in normal rodent brain tissue (brain clearance t(1,2) = 20 min). The combination of relatively high affinity for amyloid, specificity for staining plaques and neurofibrillary tangles in post-mortem AD brain, and good brain entry and clearance makes [N-methyl-11C]6-Me-BTA-1 a promising candidate as an in vivo positron emission tomography (PET) beta-sheet imaging agent.

摘要

对沉积在淀粉样斑块(Aβ肽)或神经原纤维缠结(tau蛋白)中的β-折叠蛋白进行体内评估,是开发阿尔茨海默病(AD)生物标志物的一个目标。为了开发体内β-折叠成像探针,合成并评估了硫黄素-T(ThT)的衍生物。这些化合物缺乏ThT带正电荷的季铵杂环氮,因此在生理pH值下呈电中性。它们的亲脂性比ThT高600倍。这些ThT衍生物与Aβ(1-40)纤维的结合亲和力(Ki = 20.2 nM)高于ThT(Ki = 890 nM)。不带电荷的ThT衍生物对死后AD脑内的斑块和神经原纤维缠结均有染色,对斑块染色表现出一定的偏好。制备了一种碳-11标记的化合物[N-甲基-11C]6-Me-BTA-1,并在瑞士韦伯斯特小鼠中研究了其脑摄取和清除情况。该化合物进入脑内的水平与常用的神经受体显像剂相当(注射后2分钟时为0.223 %ID-kg/g或7.61 %ID/g),并且在正常啮齿动物脑组织中对游离和非特异性结合的放射性表现出良好的清除能力(脑清除半衰期t(1,2) = 20分钟)。对淀粉样蛋白具有相对较高的亲和力、对死后AD脑内的斑块和神经原纤维缠结具有特异性染色、以及良好的脑摄取和清除能力,这些特性的结合使得[N-甲基-11C]6-Me-BTA-1成为一种有前景的体内正电子发射断层扫描(PET)β-折叠成像剂候选物。

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