Suitable carrier systems for sustained release of curcumin were studied by using the selfassembled polymeric micelles. Poly(ethylene glycol) methyl ether and poly(aromatic anhydride) were used as the hydrophilic and hydrophobic blocks, respectively, in forming amphiphilic diblock copolymers. Four different types of polymers methoxy poly(ethylene glycolb-1,3-bis(p-carboxyphenoxy)propane) (mPEG 5000 CPP, mPEG 2000 CPP ), methoxy poly(ethylene glycol-b-1,6-bis(pcarboxyphenoxy)hexane) (mPEG 5000 CPH, mPEG 2000 CPH) were synthesized via melt condensation approach. Micelles were formed at very low polymer concentration with stable hydrophobic cores. The particle sizes of micelles remained stable during degradation period. All four different polymeric micelles showed low cytotoxicity toward human fibroblasts cells and can kill cancer cells in very low concentrations. High loading efficiency and drug content were observed in curcumin-loaded micelles. Curcumin showed mild initial burst (30% of drug loading in the first 24 h) when released from the micelles and its release was sustained for at least 18 days. These micelles, especially those of mPEG 5000 CPP, show potential to serve as the delivery vehicles for sustained release of curcumin.
Poly(methyl methacrylate) (PMMA) is the most frequently used bone void filler in orthopedic surgery. However, the interface between the PMMA-based cement and adjacent bone tissue is typically weak as PMMA bone cement is inherently bioinert and not ideal for bone ingrowth. The present study aims to improve the affinity between the polymer and ceramic interphases. By surface modifying nano-sized hydroxyapatite (nHAP) with ethylene glycol and poly(ɛ-caprolactone) (PCL) sequentially via a two-step ring opening reaction, affinity was improved between the polymer and ceramic interphases of PCL-grafted ethylene glycol-HAP (gHAP) in PMMA. Due to better affinity, the compressive strength of gHAP/PMMA was significantly enhanced compared with nHAP/PMMA. Furthermore, PMMA with 20 wt.% gHAP promoted pre-osteoblast cell proliferation
in vitro
and showed the best osteogenic activity between the composites tested
in vivo
. Taken together, gHAP/PMMA not only improves the interfacial adhesion between the nanoparticles and cement, but also increases the biological activity and affinity between the osteoblast cells and PMMA composite cement. These results show that gHAP and its use in polymer/bioceramic composite has great potential to improve the functionality of PMMA cement.
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