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Determine the Anticancer Activity and Mechanism of Overcoming Drug Resistance by Cu(DDC)2 NPs in Prostate Cancers


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dc.contributor.advisorLi, Feng
dc.contributor.authorWang, Junwei
dc.date.accessioned2021-07-14T18:43:59Z
dc.date.available2021-07-14T18:43:59Z
dc.date.issued2021-07-14
dc.identifier.urihttps://etd.auburn.edu//handle/10415/7800
dc.description.abstractCopper diethyldithiocarbamate [Cu(DDC)2] complex formed by disulfiram (DSF) and copper ions is a promising therapeutic agent for cancer treatment. However, the poor aqueous solubility of Cu(DDC)2 limited its clinical application. In our previous studies, we developed a stabilized metal ion ligand complex (SMILE) method to prepare Cu(DDC)2 nanoparticle (NP) as an injectable formulation with high drug concentration and excellent physicochemical properties. Our initial in vitro studies also demonstrated its potent anticancer activities. In the current study, we extensively investigated the in vitro anticancer activities of Cu(DDC)2 NP and demonstrated that it could kill drug-resistant prostate cancer cells by inducing non-apoptotic cell death. Further, Cu(DDC)2 NP effectively inhibited the tumor growth in an in vivo paclitaxel-resistant tumor model. In addition, we also performed studies to explore the mechanism of overcoming drug resistance by Cu(DDC)2 NP. Our results showed that Cu(DDC)2 NP did not affect the P-gp activity or change the level of P-gp proteins. It overcomes drug resistance because it is not a substrate of P-gp. Therefore, the use of Cu(DDC)2 NP will not affect the normal function of P-gp and avoid the toxic side effects associated with P-gp inhibitors. It will be a promising therapeutic agent for treating drug-resistant prostate cancers or other solid tumors.en_US
dc.rightsEMBARGO_GLOBALen_US
dc.subjectInterdepartmental Pharmacyen_US
dc.titleDetermine the Anticancer Activity and Mechanism of Overcoming Drug Resistance by Cu(DDC)2 NPs in Prostate Cancersen_US
dc.typeMaster's Thesisen_US
dc.embargo.lengthMONTHS_WITHHELD:60en_US
dc.embargo.statusEMBARGOEDen_US
dc.embargo.enddate2026-07-14en_US
dc.contributor.committeeRamapuram, Jayachandra
dc.contributor.committeeArnold, Robert

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