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A carbon based drug delivery system derived from a one-dimensional coordination polymer,doxorubicin loading and redox-responsive release

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摘要 Since the controlled release of drug molecules under external stimuli is an essential strategy for effective tumor therapy,herein a redox-responsive drug delivery system(Ag-SS-MC)has been fabricated successfully through the modification of disulfide bonds on coordination polymer derived mesoporous carbon nanoparticles(MC)with nanoscale Ag as the“cap”.In this drug delivery system,the Ag“caps”are fastened on a disulfide linker tightly,which blocks the pores of MC and impedes unexpected leakage of loaded doxorubicin(DOX).This drug delivery system exhibits a striking DOX loading property,with loading ratio as high as 20.6%.Ag-SS-MC remains stable under normal physiological conditions,but the loaded DOX begins to be released in the presence of a reducing agent,glutathione(GSH),which is caused by reductive breaking of disulfide bonds.MTT assays show that,after incubation with the human cervical cancer cell line(HeLa)for 24 h,the cytotoxicity of blank Ag-SS-MC carriers can almost be ignored.In contrast,under the same conditions,the DOX loaded drug carrier system possesses high antitumor activity.Ag-SS-MC exhibits superior drug loading,high extracellular stability,redox-responsive intracellular drug release and excellent biocompatibility;all these characteristics make it a promising drug delivery system for tumor therapy.
出处 《Inorganic Chemistry Frontiers》 2017年第8期1344-1351,共8页 无机化学前沿(英文)
基金 supported by the National Natural Science Foundation of China(21303010,21673035,and 21571132) the Opening Project of the Key Laboratory of Polyoxometalate Science of the Ministry of Education.

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