关键词:  , 甲基苯丙胺；适配子；SELEX；SPR

Abstract: Objective To screen and identify high-affinity aptamers to methamphetamine by SELEX (System Evolution of Ligands by Exponential Enrichment) method. Methods Methamphetamine-BSA was conjugated to cyanogen bromide-activated-sepharose as the solid phase target, and a synthetic random DNA library with the total length of 76 bp was subjected to selection by SELEX technology. Positive aptamers from the selection were analyzed for their specific association with methamphetamine-BSA by SPR (Surface Plasmon Resonance) sensor. The secondary structures of aptamers and their corresponding binding sites were predicted and analyzed by MFOLD software. Results After 10 rounds of SELEX screening, the binding affinity between the aptamers and methamphetamine increased from 88.3RU to 113.7RU, indicating that specific aptamers were enriched progressively. Ten aptamers have an absolute identical sequence after cloning and sequencing. It was revealed that their secondary structures were stem-loop, which might be the possible binding sites between the aptamers and the target. Conclusion The study obtained the sequence of specific aptamers to methamphetamine, and revealed the basic structure of the binding sites, which paves the way for the future application of these aptamers in a fast and cost-efficient detection of methamphetamine.

Key words: font-size: 10.5pt, mso-bidi-font-size: 10.0pt, mso-font-kerning: 1.0pt, mso-ansi-language: EN-US, mso-fareast-language: ZH-CN, mso-bidi-language: AR-SA, mso-fareast-font-family: 宋体" lang="EN-US">methamphetamine, aptamer, SELEX, SPR