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适体对多种小分子功能化底物的识别。

Aptamer Recognition of Multiplexed Small-Molecule-Functionalized Substrates.

出版信息

ACS Appl Mater Interfaces. 2018 Jul 18;10(28):23490-23500. doi: 10.1021/acsami.8b02837. Epub 2018 Jul 6.

Abstract

Aptamers are chemically synthesized oligonucleotides or peptides with molecular recognition capabilities. We investigated recognition of substrate-tethered small-molecule targets, using neurotransmitters as examples, and fluorescently labeled DNA aptamers. Substrate regions patterned via microfluidic channels with dopamine or   l-tryptophan were selectively recognized by previously identified dopamine or l-tryptophan aptamers, respectively. The on-substrate dissociation constant determined for the dopamine aptamer was comparable to, though, slightly greater than the previously determined solution dissociation constant. Using prefunctionalized neurotransmitter-conjugated oligo(ethylene glycol) alkanethiols and microfluidics patterning, we produced multiplexed substrates to capture and to sort aptamers. Substrates patterned with l-3,4-dihydroxyphenylalanine, l- threo-dihydroxyphenylserine, and l-5-hydroxytryptophan enabled comparison of the selectivity of the dopamine aptamer for different targets via simultaneous determination of in situ binding constants. Thus, beyond our previous demonstrations of recognition by protein binding partners (i.e., antibodies and G-protein-coupled receptors), strategically optimized small-molecule-functionalized substrates show selective recognition of nucleic acid binding partners. These substrates are useful for side-by-side target comparisons and future identification and characterization of novel aptamers targeting neurotransmitters or other important small molecules.

摘要

适体是具有分子识别能力的化学合成寡核苷酸或肽。我们研究了通过微流控通道图案化的含有多巴胺或 l-色氨酸的底物区域对荧光标记的 DNA 适体的识别,这些适体分别对先前鉴定的多巴胺或 l-色氨酸适体具有选择性。对于多巴胺适体,在底物上的解离常数与先前在溶液中测定的解离常数相当,但略高。使用预官能化的神经递质缀合的寡聚(乙二醇)烷硫醇和微流控图案化,我们制备了用于捕获和分拣适体的多重化底物。用 l-3,4-二羟基苯丙氨酸、l- threo-二羟基苯丝氨酸和 l-5-羟色氨酸图案化的底物,通过同时确定原位结合常数,比较了多巴胺适体对不同靶标的选择性。因此,除了我们之前对蛋白质结合伙伴(即抗体和 G 蛋白偶联受体)识别的演示之外,通过策略优化的小分子功能化底物对核酸结合伙伴具有选择性识别。这些底物可用于并排进行目标比较,并可用于未来鉴定和表征针对神经递质或其他重要小分子的新型适体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/db0f/6087467/feff3ef4a00c/nihms-982891-f0005.jpg

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