Tissue engineering aims at fabricating biological substitutes to improve, repair, and regenerate failing human tissues or organs. Designing a nanocomposite scaffolds with tailored properties that enhance the development of functional tissue can be an appropriate approach to achieve this purpose. In this study, the uniform and bead-free nanofibers of poly(ε-caprolactone) composited with different graphene oxide nanosheet contents (ranging from 0.5 to 2 wt%) were successfully fabricated through electrospinning process. A decrease in the average diameter of poly(ε-caprolactone) nanofibers was observed with the addition of graphene oxide nanosheets. Moreover, the nanocomposite scaffolds containing 2 wt% of graphene oxide nanosheets exhibited superior mechanical properties compared to that of pure poly(ε-caprolactone). Compared with pure poly(ε-caprolactone) scaffold, the degradation rate of poly(ε-caprolactone)-graphene oxide nanosheet nanofibers was enhanced, while the integrity of fibers was preserved. The presence of graphene oxide nanosheets in poly(ε-caprolactone) fibers promoted in vitro biomineralization, indicating bioactive features of the nanocomposite scaffolds. Compared to the pure one, nanocomposite fibers also showed better ability in protein adsorption. The in vitro cell culture studies showed that the addition of graphene oxide nanosheets did not diminish the biocompatibility of the electrospun poly(ε-caprolactone) nanofiber. Furthermore, the adhesion and proliferation of MG63 cells were increased. Altogether, the results demonstrated that electrospun poly(ε-caprolactone)-graphene oxide nanosheet nanofiber may be a suitable candidate for tissue engineering scaffold applications.
The ability of inkjet-based 3D printing (3DP) to fabricate biocompatible ceramics has made it one of the most favorable techniques to generate bone tissue engineering (BTE) scaffolds. Calcium sulfates exhibit various beneficial characteristics, and they can be used as a promising biomaterial in BTE. However, low mechanical performance caused by the brittle character of ceramic materials is the main weakness of 3DP calcium sulfate scaffolds. Moreover, the presence of certain organic matters in the starting powder and binder solution causes products to have high toxicity levels. A post-processing treatment is usually employed to improve the physical, chemical, and biological behaviors of the printed scaffolds. In this study, the effects of heat treatment on the structural, mechanical, and physical characteristics of 3DP calcium sulfate prototypes were investigated. Different microscopy and spectroscopy methods were employed to characterize the printed prototypes. The in vitro cytotoxicity of the specimens was also evaluated before and after heat treatment. Results showed that the as-printed scaffolds and specimens heat treated at 300°C exhibited severe toxicity in vitro but had almost adequate strength. By contrast, the specimens heat treated in the 500°C–1000°C temperature range, although non-toxic, had insufficient mechanical strength, which was mainly attributed to the exit of the organic binder before 500°C and the absence of sufficient densification below 1000°C. The sintering process was accelerated at temperatures higher than 1000°C, resulting in higher compressive strength and less cytotoxicity. An anhydrous form of calcium sulfate was the only crystalline phase existing in the samples heated at 500°C–1150°C. The formation of calcium oxide caused by partial decomposition of calcium sulfate was observed in the specimens heat treated at temperatures higher than 1200°C. Although considerable improvements in cell viability of heat-treated scaffolds were observed in this study, the mechanical properties were not significantly improved, requiring further investigations. However, the findings of this study give a better insight into the complex nature of the problem in the fabrication of synthetic bone grafts and scaffolds via post-fabrication treatment of 3DP calcium sulfate prototypes.
In recent years, nanotechnology in merging with biotechnology has been employed in the area of cancer management to overcome the challenges of chemopreventive strategies in order to gain promising results. Since most biological processes occur in nano scale, nanoparticles can act as carriers of certain drugs or agents to deliver it to specific cells or targets. In this study, we intercalated Epigallocatechin-3-Gallate (EGCG), the most abundant polyphenol in green tea, into Ca/Al-NO3 Layered double hydroxide (LDH) nanoparticles, and evaluated its efficacy compared to EGCG alone on PC3 cell line. The EGCG loaded LDH nanohybrids were characterized by X-ray diffraction, Fourier transform infrared spectroscopy, transmission electron microscopy (TEM) and nanosizer analyses. The anticancer activity of the EGCG-loaded LDH was investigated in prostate cancer cell line (PC3) while the release behavior of EGCG from LDH was observed at pH 7.45 and 4.25. Besides enhancing of apoptotic activity of EGCG, the results showed that intercalation of EGCG into LDH can improve the anti- tumor activity of EGCG over 5-fold dose advantages in in-vitro system. Subsequently, the in-vitro release data showed that EGCG-loaded LDH had longer release duration compared to physical mixture, and the mechanism of diffusion through the particle was rate-limiting step. Acidic attack was responsible for faster release of EGCG molecules from LDH at pH of 4.25 compared to pH of 7.4. The results showed that Ca/Al-LDH nanoparticles could be considered as an effective inorganic host matrix for the delivery of EGCG to PC3 cells with controlled release properties.
In this study, Ca-Al-NO 3 layered double hydroxide (LDH) nanoparticles of varying sizes were synthesised by a process involving co-precipitation under hydrothermal condition. This method produces stable homogeneous LDH suspensions under variable hydrothermal treatment conditions with particle size in the range of 7?5-2?5 mm. Layered double hydroxides were characterised by X-ray diffraction, Fourier transform infrared spectroscopy, thermal gravimetric/ differential thermal analysis, scanning electron microscopy and transmission electron microscopy (TEM) and nanosizer analyses. By increasing the hydrothermal treatment time, the crystallinity and the particle size of obtained LDH increased. Scanning electron microscopy and TEM observations showed uniform hexagonal flake-like particles with high aspect ratio. Finally, Ca-Al-NO 3 LDH did not show any acute cytotoxic effect up to 100 mg mL 21 as measured by 3-(4,5dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide assay.
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