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磁性纳米粒子表面的分子封装器。从 Ferrite/Cyclodextrin-键合聚合物杂化材料中控制药物释放。

Molecular encapsulator on the surface of magnetic nanoparticles. Controlled drug release from calcium Ferrite/Cyclodextrin-tethered polymer hybrid.

机构信息

Chemistry Research Lab, Karunya University, Coimbatore, 641114, Tamil Nadu, India.

Nanotoxicology Research Lab, Department of Science & Humanities, Karunya University, Coimbatore, 641114, Tamil Nadu, India.

出版信息

Colloids Surf B Biointerfaces. 2018 Jan 1;161:347-355. doi: 10.1016/j.colsurfb.2017.10.048. Epub 2017 Oct 18.

Abstract

Magnetic nanoparticles (MNPs) are intriguing due to their potency to deliver anti-cancer drugs. This paper presents the inference from our experimental attempts to add merit to the concept of magnetic drug carrier, by designing calcium ferrite nanoparticles and coating them with a biocompatible dextran tethered with a hydrophobic cavity-containing molecule, β-cyclodextrin (β-CD). The size, crystal system, and the morphology of the MNPs are studied. The magnetic properties are explored using vibrating sample magnetometry, SQUID and Mössbauer spectroscopy. The roughly 75nm MNPs, encapsulated with the β-CD-dextran conjugate allows a slow and sustained in vitro release of the loaded anti-cancer drug, Camptothecin, from the polymer shell. The study of cytotoxicity reveals that the loaded Camptothecin retains its potency as efficient as an effective carrier of the anti-cancer drug. Further, the toxicity of the nanomaterial is tested on an organism which is highly sensitive to toxicity i.e., brine shrimp (Artemia salina). The polymer coating brings down the toxicity of the MNPs.

摘要

磁性纳米粒子(MNPs)因其能够输送抗癌药物而备受关注。本文通过设计并包覆具有生物相容性的葡聚糖纳米载体的四氧化三铁纳米粒子,来进一步提升磁性药物载体的概念,该葡聚糖纳米载体上连接有一个疏水性空腔分子β-环糊精(β-CD)。我们对 MNPs 的尺寸、晶体系统和形态进行了研究。通过振动样品磁强计、超导量子干涉仪和穆斯堡尔光谱对 MNPs 的磁性进行了探索。被β-CD-葡聚糖包裹的大约 75nm 的 MNPs 可以从聚合物壳中缓慢且持续地释放负载的抗癌药物喜树碱。细胞毒性研究表明,负载的喜树碱保留了其作为有效抗癌药物载体的效力。此外,我们还在对毒性非常敏感的生物体内(卤虫)测试了纳米材料的毒性。聚合物涂层降低了 MNPs 的毒性。

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