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基于双功能 MOFs 的杂化微凝胶提升水基润滑和抗炎性能。

Dual-functional MOFs-based hybrid microgel advances aqueous lubrication and anti-inflammation.

机构信息

State Key Laboratory of Solidification Processing, Center of Advanced Lubrication and Seal Materials, School of Materials Science and Engineering, Northwestern Polytechnical University, Xi'an 710072, PR China.

State Key Laboratory of Solidification Processing, Center of Advanced Lubrication and Seal Materials, School of Materials Science and Engineering, Northwestern Polytechnical University, Xi'an 710072, PR China.

出版信息

J Colloid Interface Sci. 2023 Aug 15;644:200-210. doi: 10.1016/j.jcis.2023.04.071. Epub 2023 Apr 23.

Abstract

This paper demonstrates the hybridization of copolymer microgel with drug-loaded metal-organic frameworks nanoparticles that can achieve excellent aqueous lubricating performance and anti-inflammatory effect for synergistic treatment of osteoarthritis (OA). Poly(ethylene glycol)-graft-poly(N-isopropylacrylamide) (PEG-g-PNIPAm) microgel layer is grown on the MIL-101(Cr) surface via one-pot soap-free emulsion polymerization method. The lower critical solution temperature of the MIL-101(Cr)@PEG-g-PNIPAm hybrid is raised significantly by incorporating PEG chains into the PNIPAm microgel matrix, which greatly enhances the high-temperature aqueous dispersion stability. The hybrid microgel demonstrated reversibly thermo-sensitive swelling-collapsing behavior to modulate the optical properties and hydrodynamic size. Using as aqueous lubricating additives, the hybrid reduces over 64% and 97% in friction coefficient and wear volume. Also, the hybrid supports desirable temperature-controlled lubrication modulation due to their reversible thermo-responsive behavior, which is benefit to joint lubrication of OA. After encapsulating anti-inflammatory diclofenac sodium (DS), the DS-MIL-101(Cr)@PEG-g-PNIPAm shows thermo-responsive drug release in aqueous media, which can improve the drug-delivery efficiency. By co-culturing the DS-loaded hybrid with human normal chondrocytes, we demonstrate good biocompatibility and anti-inflammatory effect on the chondrocytes with inflammation by regulating the expression of OA-related genes and proteins. Our work establishes multifunctional MOFs-based hybrid microgel systems for advanced colloids modulation and biomedical application.

摘要

本文展示了共聚物微凝胶与载药金属有机骨架纳米粒子的杂交,可实现优异的水润滑性能和抗炎效果,协同治疗骨关节炎(OA)。通过一锅无皂乳液聚合方法在 MIL-101(Cr) 表面生长聚(乙二醇)接枝聚(N-异丙基丙烯酰胺)(PEG-g-PNIPAm)微凝胶层。将 PEG 链引入到 PNIPAm 微凝胶基质中,大大提高了 MIL-101(Cr)@PEG-g-PNIPAm 杂化的低临界溶液温度,从而显著提高了其在高温下的水相分散稳定性。该杂化微凝胶表现出可逆的温敏溶胀-收缩行为,可调节其光学性质和流体力学尺寸。作为水基润滑添加剂,该杂化可将摩擦系数和磨损体积降低 64%和 97%以上。此外,由于其可逆的温度响应行为,该杂化还支持理想的温度控制润滑调节,这有利于 OA 的关节润滑。封装抗炎药双氯芬酸钠(DS)后,DS-MIL-101(Cr)@PEG-g-PNIPAm 在水介质中表现出温敏药物释放,可提高药物递送效率。通过将负载 DS 的杂化与人正常软骨细胞共培养,我们证明了该杂化对具有炎症的软骨细胞具有良好的生物相容性和抗炎作用,通过调节 OA 相关基因和蛋白的表达来实现。我们的工作建立了多功能 MOF 基杂化微凝胶系统,用于先进的胶体调节和生物医学应用。

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