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Universal polyethylene glycol linkers for attaching receptor ligands to quantum dots.

机译:通用聚乙二醇接头,用于将受体配体连接到量子点上。

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摘要

Biologically active small molecule derivatives that can be conjugated to quantum dots have the promise of revolutionizing fluorescent imaging in biology. In order to achieve this several technical hurdles have to be surmounted, one of which is non-specific adsorption of quantum dots to cell membranes. Pegylating quantum dots has been shown to eliminate non-specific binding. Consequently it is necessary to develop a universal synthetic methodology to attach small molecule ligands to polyethylene glycol. These pegylated small molecules may then be conjugated to the surfaces of quantum dots. Ideally this universal strategy should be adaptable and be applicable to PEG chains of varying lengths. This paper describes the development of one such methodology and the synthesis of a pegylated derivative of the known 5HT(2) agonist 1-(2-aminopropyl)-2,5-dimethoxy benzene. This compound was tested and found to be an agonist for the 5HT(2A) and 5HT(2C) receptor having EC(50) values of 250 and 50 nM, respectively.
机译:可与量子点结合的具有生物活性的小分子衍生物有望彻底改变生物学中的荧光成像。为了实现这一点,必须克服几个技术障碍,其中之一是量子点对细胞膜的非特异性吸附。已经证明聚乙二醇化量子点消除了非特异性结合。因此,有必要开发一种通用的合成方法,将小分子配体连接到聚乙二醇上。然后可以将这些聚乙二醇化的小分子缀合到量子点的表面。理想情况下,这种通用策略应该适应并适用于不同长度的PEG链。本文介绍了一种此类方法的开发,以及已知5HT(2)激动剂1-(2-氨基丙基)-2,5-二甲氧基苯的聚乙二醇化衍生物的合成。测试了该化合物,发现该化合物是5HT(2A)和5HT(2C)受体的激动剂,其EC(50)值分别为250和50 nM。

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