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Molecularly Imprinting Polymers (MIP) Based on Nitrogen Doped Carbon Dots and MIL-101(Fe) for Doxorubicin Hydrochloride Delivery

机译:基于氮掺杂的碳点和MIL-101(Fe)的分子印迹聚合物(MIP)用于多柔比星盐酸盐递送

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摘要

MIL-based molecularly imprinted polymer (MIP) nanocomposites were successfully synthesized through a simple and versatile stirring auxiliary encapsulation method. MIP as a carrier has been applied to the highly efficient selective recognition and sustained release of doxorubicin hydrochloride (DOX). The adsorption mechanism and release behavior of MIP@DOX in vitro were also discussed. Adsorption studies showed that MIP using DOX as template had specific selectivity to DOX, and its optimal drug loading efficiency reached 97.99%. The adsorption isotherm accorded with Freundlich models. The cumulative release curve showed that at the conditions of pH 5.5 and 7.4, the nanomaterials have a slow-release effect on the release of DOX. In addition, the cytotoxicity and bioactivity of MIP nanoparticles on HepG2 and HL-7702 cell lines measured by MTT assay also proved their low toxicity and biological activity. The cell activity of HepG2 and HL-7702 incubated with MIP for 24 h was 69.9% and 76.07%, respectively. These results collectively illustrated that the MIP nano-materials synthesized in this study can be efficiently employed to the drug delivery systems.
机译:通过简单且通用的搅拌辅助包封方法成功地合成了基于MIL的分子印迹聚合物(MIP)纳米复合材料。 MIP作为载体已应用于高效的选择性识别和持续释放的多柔比星盐酸盐(DOX)。还讨论了MIP @ Dox体外的吸附机制和释放行为。吸附研究表明,使用DOX作为模板的MIP对DOX具有特异性选择性,其最佳药物负载效率达到97.99%。吸附等温线符合Freundlich模型。累积释放曲线显示,在pH 5.5和7.4的条件下,纳米材料对DOX的释放具有缓释作用。此外,MTT测定测量的HepG2和HL-7702细胞系上的MIP纳米粒子的细胞毒性和生物活性也证明了它们的低毒性和生物活性。将HepG2和HL-7702的细胞活性分别温育24小时,分别为69.9%和76.07%。这些结果集体示出了在该研究中合成的MIP纳米材料可以有效地用于药物递送系统。

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