Incorporation of carboxymethyl chitosan (CMCS) for the modulation of physio-chemical characteristics and cell proliferation environment of the composite hydrogel microspheres.

Qin Liying, Yang Yining, Sun Yongjian, Han Guojiang, Dong Wenli, Han Baoqin, Su Ting, Jin Liming, Zhou Chao, Yang Yan
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Abstract

Hydrogels have excellent swelling properties and have been widely applied in tissue engineering because of their similarity to the extracellular matrix (ECM). Sodium alginate (SA) and carboxymethyl chitosan (CMCS) were prepared into hydrogel microspheres with Ca2+crosslinking in our study. The morphology, inner structure, mechanical properties, water content, swelling rate and BMP-2 loading and releasing properties were characterized. Our results showed that the composite SA /CMCS hydrogel microspheres were translucent and spherical in shape with uniform particle size. The incorporation of CMCS further increased the diameters of the microspheres, internal pore structure, water content, and mechanical properties of the SA/CMCS hydrogel microspheres. At the same SA concentration, with the increase of CMSC concentration, the diameter of microspheres could be increased by about 0.4 mm, the water content can be increased about 1%-2%. As for the mechanical properties, the compressive strength can be increased by 0.04-0.1 MPa, and the modulus of elasticity can be increased by 0.1-0.15 MPa. BMP-2 was chosen as a model agent and it could be loaded into SA/CMCS microspheres, and the incorporation of CMCS increased BMP-2 loading. The encapsulated BMP-2 was sustainably releasedin vitro. The leaching solutions of the SA/CMCS hydrogel microspheres exhibited good cytocompatibility and could increase ALP activity, ALP expression, and biomineralization on MC3T3-E1 cells. After 7 d of co-culture, ALP activities in S2.5C2 and S2.5C3 groups was increased by 50% and 45% compared with that of the control group. When embedded in the SA/CMCS microspheres, the MC3T3-E1 cells were evenly distributed inside the hydrogel microspheres and remained viable. Transcriptomic studies showed that incorporation of CMCS induced upregulation of 1141 differentially expressed genes (DEGs) and downregulation of 1614 DEGs compared with SA microspheres. The most significantly enriched pathways were the Wnt and MAPK signaling pathways induced by the incorporation of CMCS and BMP-2. In conclusion, our results indicated that the physiochemical characteristics of the SA hydrogel microspheres could be greatly modulated by CMCS to better mimic the ECM microenvironment and induce osteo-inductive activities of MC3T3-E1 cells.

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加入羧甲基壳聚糖(CMCS)以调节复合水凝胶微球的理化特性和细胞增殖环境。
水凝胶具有极佳的溶胀特性,因其与细胞外基质相似而被广泛应用于组织工程中。本研究将海藻酸钠(SA)和羧甲基壳聚糖(CMCS)通过 Ca2+ 交联制备成水凝胶微球。研究人员对其形态、内部结构、机械性能、含水量、膨胀率以及 BMP-2 负载和释放性能进行了表征。结果表明,SA/CMCS 复合水凝胶微球呈半透明球形,粒径均匀。CMCS 的加入进一步增加了 SA/CMCS 水凝胶微球的直径、内部孔隙结构、含水量和机械性能。在相同的 SA 浓度下,随着 CMCS 浓度的增加,微球直径可增加约 0.4 毫米,含水量可增加约 1%-2%。在机械性能方面,抗压强度可增加 0.04-0.1 兆帕,弹性模量可增加 0.1-0.15 兆帕。选择 BMP-2 作为模型剂,将其载入 SA/CMCS 微球,CMCS 的加入增加了 BMP-2 的载量。封装的 BMP-2 可在体外持续释放。SA/CMCS 水凝胶微球的浸出液具有良好的细胞相容性,能提高 MC3T3-E1 细胞的 ALP 活性、ALP 表达和生物矿化。共培养 7 天后,与对照组相比,S2.5C2 组和 S2.5C3 组的 ALP 活性分别提高了 50%和 45%。嵌入 SA/CMCS 微球后,MC3T3-E1 细胞均匀地分布在水凝胶微球中并保持活力。转录组学研究表明,与 SA 微球相比,CMCS 诱导了 1141 个差异表达基因(DEGs)的上调和 1614 个差异表达基因(DEGs)的下调。CMCS和BMP-2诱导的Wnt和MAPK信号通路是最明显的富集通路。总之,我们的研究结果表明,CMCS可以极大地调节SA水凝胶微球的理化特性,从而更好地模拟细胞外基质微环境,诱导MC3T3-E1细胞的骨诱导活性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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