Aβ-binding molecules: Possible application as imaging probes and as anti-aggregation agents 被引量：1

Aβ-binding molecules: Possible application as imaging probes and as anti-aggregation agents

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摘要 As amyloid β (Aβ) is at the centre of pathogenesis of Alzheimer's disease (AD), Aβ aggregate-specific probes for in vivo studies of Aβ are potentially important for the early diagnosis and the assessment of new treatment strategies in the AD brain by noninvasive imaging. Several series of compounds derived from Congo red (CR) and Thioflavin T (ThT) have been evaluated as potential probes for the Aβ imaging. They include a diversity of core structures contributing to their affinities to Aβ. Small-molecule inhibi- tors were known to inhibit the formation of Aβ oligomers and fibrils. This inhibition has to be performed in such a way that these inhibitors bind to Aβ in the binding channel where Aβ-binding probes should sit. Therefore, several of them were used as novel core structures to develop Aβ probes, with their de- rivatives exhibiting good Aβ affinities. This approach will facilitate the design of a variety of candidates for Aβ probe molecules and anti-aggregation-therapeutic drugs. Moreover, the finding of Aβ probes with diverse core structures recognized by binding sites on Aβs will likely provide a promising per- spective for the design of 99mTc-labeled probe-derived molecules. As amyloid β (Aβ) is at the centre of pathogenesis of Alzheimer’s disease (AD), Aβ aggregate-specific probes for in vivo studies of Aβ are potentially important for the early diagnosis and the assessment of new treatment strategies in the AD brain by noninvasive imaging. Several series of compounds derived from Congo red (CR) and Thioflavin T (ThT) have been evaluated as potential probes for the Aβ imaging. They include a diversity of core structures contributing to their affinities to Aβ. Small-molecule inhibitors were known to inhibit the formation of Aβ oligomers and fibrils. This inhibition has to be performed in such a way that these inhibitors bind to Aβ in the binding channel where Aβ-binding probes should sit. Therefore, several of them were used as novel core structures to develop Aβ probes, with their derivatives exhibiting good Aβ affinities. This approach will facilitate the design of a variety of candidates for Aβ probe molecules and anti-aggregation-therapeutic drugs. Moreover, the finding of Aβ probes with diverse core structures recognized by binding sites on Aβs will likely provide a promising perspective for the design of 99mTc-labeled probe-derived molecules.

作者 DUAN XinHong LIU BoLi

机构地区 Key Laboratory of Radiopharmaceuticals College of Science

出处《Science China Chemistry》 SCIE EI CAS 2008年第9期801-807,共7页 中国科学（化学英文版）

基金 the National Natural Science Foundation of China (Grant No. 20471011)

关键词 AΒ binding core structure AΒ inhibitor HYDROPHOBIC and AROMATIC interaction BIFUNCTIONAL candidate Aβ binding core structure Aβ inhibitor hydrophobic and aromatic interaction bifunctional candidate

分类号 R749.16 [医药卫生—神经病学与精神病学]

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Science China Chemistry

2008年第9期

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Aβ-binding molecules: Possible application as imaging probes and as anti-aggregation agents 被引量：1

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