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Ultrasound mediated delivery of oxygen and LLL12 loaded stimuli responsive microdroplets for the treatment of hypoxic cancer cells. | LitMetric

AI Article Synopsis

  • LLL12 specifically inhibits the phosphorylation and dimerization of STAT3 in cancer cells, inducing apoptosis without harming normal cells.
  • Its clinical use is limited by low bioavailability and resistance in low-oxygen environments, which is addressed by encapsulating LLL12 and oxygen in stimuli responsive microdroplets (SRMs) through a novel gas-driven process.
  • In vitro studies show that these SRMs effectively release their contents under ultrasound, enhancing anticancer effects in pancreatic cancer cells under hypoxic conditions.

Article Abstract

LLL12 exhibits high specificity for inhibiting STAT3 phosphorylation and dimerization, and inducing apoptosis to constitutively activated STAT3 cancer cells without cytotoxicity to normal cells with dormant STAT3. However, clinical deployment of LLL12 in cancer treatment is hindered by its low bioavailability and hypoxia-induced resistance. To overcome these limitations, we encapsulate both oxygen and LLL12 in stimuli responsive microdroplets (SRMs) by a gas-driven coaxial flow focusing (CFF) process for ultrasound mediated treatment of hypoxic cancer cells. Our benchtop experiments demonstrate that the CFF process is able to produce SRMs with uniform size distribution, large oxygen loading capacity, high LLL12 encapsulation efficiency, well protection of bioactivity, and steadily long shelf time. The in vitro therapeutic studies in pancreatic cancer cells (PANC-1 and CAPAN-1) demonstrate the immediate release of oxygen and LLL12 in exposure to therapeutic ultrasound pulses as well as the improved anticancer effects under hypoxic conditions. The findings suggest that the proposed oxygen and LLL12 loaded SRMs provide a promising drug delivery strategy for more effective treatment of hypoxic cancer cells.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC5359616PMC
http://dx.doi.org/10.1038/srep44908DOI Listing

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