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首页> 外文期刊>Journal of biomedical materials research. Part B, Applied biomaterials. >Fabrication of crosslinked carboxymethylchitosan microspheres and their incorporation into composite scaffolds for enhanced bone regeneration.
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Fabrication of crosslinked carboxymethylchitosan microspheres and their incorporation into composite scaffolds for enhanced bone regeneration.

机译:交联羧甲基壳聚糖微球的制备及其掺入复合支架中以增强骨再生。

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Carboxymethylchitosan (CMCS) microspheres were prepared by the carboxymethylation of chitosan (CS) beads using monochloroacetic acid. The CMCS microspheres were crosslinked using two different methods: the amine-amine crosslinker genipin and carbodiimide chemistry, yielding Gen-X CMCS and X-CMCS beads, respectively. The Gen-X CMCS beads were found to have poor degradation and drug release profiles. The X-CMCS microspheres displayed good potential for use in tissue engineering applications in which degradation and local drug delivery are desired. The X-CMCS beads displayed enzymatic degradation of 82.7 ± 1.2% in 100 μg/mL lysozyme after 1 month. An extended release of rhBMP-2 for at least 45 days was also observed with the X-CMCS microspheres. Scaffolds were formed by fusing beads together, and the X-CMCS beads were successfully incorporated into composite X-CMCS/CS scaffolds. The composite scaffolds had increased degradation of 14.5 ± 6.6% compared to 0.5 ± 0.4% for CS-only scaffolds, and the X-CMCS/CS scaffolds released more rhBMP-2 at all timepoints. The composite scaffolds also supported the attachment and proliferation of SAOS-2 cells. The addition of X-CMCS beads resulted in fabrication of scaffolds with improved properties for use in bone tissue engineering.
机译:羧甲基壳聚糖(CMCS)微球是通过使用一氯乙酸对壳聚糖(CS)珠进行羧甲基化制备的。使用两种不同的方法将CMCS微球交联:胺-胺交联剂Genipin和碳二亚胺化学法,分别产生Gen-X CMCS和X-CMCS珠。发现Gen-X CMCS珠具有较差的降解和药物释放曲线。 X-CMCS微球在需要降解和局部药物递送的组织工程应用中显示出良好的潜力。 1个月后,X-CMCS珠在100μg/ mL溶菌酶中的酶降解显示为82.7±1.2%。 X-CMCS微球还观察到rhBMP-2的延长释放至少45天。通过将珠子融合在一起形成支架,并将X-CMCS珠子成功地整合到复合X-CMCS / CS支架中。与仅使用CS的支架的0.5±0.4%相比,复合支架的降解增加了14.5±6.6%,并且X-CMCS / CS支架在所有时间点均释放了更多的rhBMP-2。复合支架还支持SAOS-2细胞的附着和增殖。 X-CMCS珠的添加导致了用于骨组织工程的具有改进的性质的支架的制造。

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