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Investigation of ractopamine-imprinted polymer for dispersive solid-phase extraction of trace β-agonists in pig tissues

✍ Scribed by Yuling Hu; Ruijin Liu; Yuanwen Li; Gongke Li


Publisher
John Wiley and Sons
Year
2010
Tongue
English
Weight
277 KB
Volume
33
Category
Article
ISSN
1615-9306

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✦ Synopsis


Abstract

Ractopamine, as an alternative β‐agonist to clenbuterol, is more and more used as leanness‐enhancing agent in the swine industry. This work presents a new molecularly imprinted polymer (MIP) using ractopamine as template for dispersive solid‐phase extraction of trace ractopamine and the structural related β‐agonists in animal tissues. The binding properties and selectivity of MIP were investigated. High selectivity in polar environment was found, since the extraction capacity of ractopamine with the MIP was 4.5‐fold as much as that with the non‐imprinted polymer in acetonitrile. Cross‐selectivity investigation indicates that the MIP preferentially binds the template and then the structural analogues according to their molecular similarity. Thermodynamic and kinetic investigation was performed to interpret the specific adsorption and molecular recognition of the MIP for ractopamine. Standard free energy, standard enthalpy, and standard entropy were determined. Related information suggested that adsorption of ractopamine onto MIP was an exothermic, spontaneous process. The MIP can be applied as dispersive solid‐phase extraction material for enrichment of ractopamine, isoxsuprine, fenoterol and clenbuterol in complex samples before HPLC analysis. The method revealed detection limits of 0.20–0.90 μg/L, recoveries of 83.8–115.2 and 85.2–110.2% for the spiked pig muscle and pig liver, respectively, with the RSD from 2.5 to 8.8%.


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## Abstract A method was developed for the determination of ractopamine in pig urine using molecularly imprinted solid‐phase extraction (MISPE) as the sample clean‐up technique combined with high‐performance liquid chromatography. The molecularly imprinted polymer (MIP) was synthesized in acetonitr