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Synthesis of polymer-functionalized nanoscale graphene oxide with different surface charge and its cellular uptake, biosafety and immune responses in Raw264.7 macrophages

机译:不同表面电荷的聚合物官能化纳米级氧化物的合成及其在Raw264.7巨噬细胞中的细胞吸收,生物安全和免疫应答

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摘要

Polymer-functionalized graphene oxide (GO) has superior properties such as large surface area, extraordinary mechanical strength, high carrier mobility, good stability in physiological media and low cytotoxicity, making it an attractive material for drug and gene delivery. Herein, we successfully synthesized GO with an average size of 168.3 nm by a modified Hummers' method. Branched polyethylenimine (PEI) and 6-armed polyethylene glycol (PEG) functionalized GO complexes (GO-PEI and GO-PEG) with different zeta potentials of 47.2 mV and -43.0 mV, respectively, were successfully synthesized through amide linkages between the COOH groups of GO and the NH2 groups of PEI and PEG. Then, the interactions between GO-PEI and GO-PEG complexes and Raw264.7 mouse monocyte-macrophage cells were investigated. The GO-PEI and GO-PEG complexes could both be internalized by Raw264.7 cells. However, compared with the GO-PEG complex, the GO-PEI complex showed higher intracellular delivery efficiency in Raw264.7 cells. Moreover, it was found that the GO-PEI complex not only gathered in endosomes but also in the cytoplasm, whereas GO-PEG gathered in endosomes only. The MTT tests showed that both GO-PEI and GO-PEG complexes exhibited very low cytotoxicity towards Raw264.7 cells when at a low concentration. The cellular immune response test demonstrated the GO-PEG complex enhanced the secretion of IL-6, illustrating it was more stimulus towards macrophage cells. The above results indicated that the GO-PEI complex, with a positive surface charge, demonstrated better potential to be used in effective drug and gene delivery.
机译:聚合物官能化的石墨烯氧化物(GO)具有优异的性质,如大型表面积,非机械强度,高载体迁移率,生理介质和低细胞毒性的良好稳定性,使其成为药物和基因递送的有吸引力的材料。在此,我们通过修改的悍马方法成功地合成了平均大小为168.3nm。分别具有47.2mV和-43.0mV的不同Zeta电位的支化聚乙烯胺(PEI)和6臂聚乙二醇(PEG)官能化GO络合物(GO-PEI和GO-PEG)通过COOH基团之间的酰胺键成功地合成了47.2mV和-43.0mV的Zeta电位Go和NH2群体的PEI和PEG。然后,研究了Go-PEI和GO-PEG络合物与RAW264.7小鼠单核细胞 - 巨噬细胞之间的相互作用。 GO-PEI和GO-PEG复合物既可以由Raw264.7细胞内化。然而,与Go-PEG综合物相比,Go-Pei综合体在Raw264.7细胞中显示出更高的细胞内输送效率。此外,发现Go-Pei复合物不仅聚集在内体,而且在细胞质中,而Go-Peg仅聚集在内体中。 MTT测试表明,当以低浓度时,Go-PEI和Go-PEG复合物朝向Raw264.7细胞表现出非常低的细胞毒性。细胞免疫应答试验证明了Go-PEG综合体增强了IL-6的分泌,说明它更加刺激巨噬细胞。上述结果表明,具有阳性表面电荷的Go-Pei复合物证明了有效药物和基因递送的更好潜力。

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