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      Disulfide-crosslinked nanomicelles confer cancer-specific drug delivery and improve efficacy of paclitaxel in bladder cancer

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          Abstract

          Chemotherapy commonly used in the treatment of advanced bladder cancer is only moderately effective and associated with significant toxicity. There has been no appreciable improvement in overall survival over the last three decades. The goal of this project is to develop and characterize bladder cancer-specific nanometer-scale micelles loaded with the chemotherapeutic drug paclitaxel (PTX) and determine the anti-tumor activity and toxicity. Micelle-building-material telodendrimers were synthesized through the stepwise conjugation of eight cholic acid units at one terminus of polyethylene glycol (PEG) and a bladder cancer-specific targeting peptide named PLZ4 at the other terminus. To synthesize disulfide-crosslinked PLZ4 nanomicelles (DC-PNM), cysteine was introduced between the cholic acid and PEG. DC-PNM-PTX was synthesized through the evaporation method by loading PTX in the core. The loading capacity of PTX in DC-PNM was 25% (W/W). The loading efficiency was over 99%. DC-PNM-PTX was spherical with the median size of 25 nm. The stability of DC-PNM-PTX was determined in a solution containing sodium docecyl sulfate (SDS). It was stable in a SDS solution, but dissolved within 5 min after the addition of glutathione at the physiological intracellular concentration of 10 mM. In vivo targeting and anti-tumor activity were determined in immunodeficient mice carrying patient-derived bladder cancer xenografts (PDXs). After intravenous administration, DC-PNM specifically targeted the bladder cancer PDXs, but very little to the lung cancer xenografts in the same mice (p < 0.001). DC-PNM loaded with PTX overcame cisplatin resistance, and improved the median survival from 55 d with free PTX to 69.5 d (p = 0.03) of mice carrying PDXs. In conclusion, DC-PNM remained stable in the SDS solution, specifically targeted the bladder cancer xenografts in vivo, and improved the anti-cancer efficacy of PTX.

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          Author and article information

          Journal
          101241272
          32564
          Nanotechnology
          Nanotechnology
          Nanotechnology
          0957-4484
          1361-6528
          8 May 2019
          19 September 2016
          21 October 2016
          16 May 2019
          : 27
          : 42
          : 425103
          Affiliations
          [1 ]Department of Biochemistry and Molecular Medicine, School of Medicine, University of California-Davis, Sacramento, CA 95817, USA
          [2 ]Division of Hematology and Oncology, Department of Internal Medicine, School of Medicine, University of California-Davis, Sacramento, CA 95817, USA
          [3 ]Jackson Laboratory, 4910 Raley Blvd, Sacramento, CA 95838, USA
          [4 ]Department of Urology, University of California-Davis Cancer Center, Sacramento, CA 95817, USA
          [5 ]VA Northern California Health Care System, 10535 Hospital Way, Mather, CA 95655, USA
          [6 ]These two authors contributed equally to this article.
          [7 ]Current address: Department of Psychology, University of California San Diego, La Jolla, CA, USA.
          [8 ]Current address: Department of Urology, The Four Military Medical School, Xi’an, People’s Republic of China.
          Article
          PMC6522262 PMC6522262 6522262 nihpa1020344
          10.1088/0957-4484/27/42/425103
          6522262
          27640312
          7ae1406e-c3bf-444c-b8a3-c40dd7af79d7
          History
          Categories
          Article

          paclitaxel,bladder cancer,nanomicelle,targeted delivery
          paclitaxel, bladder cancer, nanomicelle, targeted delivery

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