Mingjuan Sun scite author profile

Saxitoxin (STX), a member of the family of paralytic shellfish poisoning toxins, poses toxicological and ecotoxicological risks. To develop an analytical recognition element for STX, a DNA aptamer (APT(STX1)) was previously discovered via an iterative process known as Systematic Evolution of Ligands by Exponential Enrichment (SELEX) by Handy et al. Our study focused on generating an improved aptamer based on APT(STX1) through rational site-directed mutation and truncation. In this study, we generated the aptamer, M-30f, with a 30-fold higher affinity for STX compared with APT(STX1). The Kd value for M-30f was 133 nM, which was calculated by Bio-Layer Interferometry. After optimization, we detected and compared the interaction of STX with aptamers (APT(STX1) or M-30f) through several techniques (ELISA, cell bioassay, and mouse bioassay). Both aptamers' STX-binding ability was demonstrated in all three methods. Moreover, M-30f performs better than its parent sequence with higher suppressive activity against STX. As a molecular recognition element, M-30f has good prospects for practical application.

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Study of the binding mechanism between aptamer GO18-T-d and gonyautoxin 1/4 by molecular simulation

Gao

Zheng

et al. 2016

Phys. Chem. Chem. Phys.

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Mingjuan Sun

Gonyautoxin 1/4 aptamers with high-affinity and high-specificity: From efficient selection to aptasensor application

Enzyme-linked, aptamer-based, competitive biolayer interferometry biosensor for palytoxin

A saxitoxin-binding aptamer with higher affinity and inhibitory activity optimized by rational site-directed mutagenesis and truncation

Study of the binding mechanism between aptamer GO18-T-d and gonyautoxin 1/4 by molecular simulation

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