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의료용 고분자 부문위원회(I)

  • Sep 30(Tue), 2025, 09:00 - 12:00
  • 포스터장
  • Chair : 박민주,박정태
09:00 - 10:30
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[1PS-108]

Urease-powered nanomotor containing STING agonist for bladder cancer immunotherapy

발표자서예원 (포항공과대학교)

연구책임자한세광 (포항공과대학교)

공동저자서예원 (포항공과대학교), 최현식 (포항공과대학교), 한세광 (포항공과대학교)

Abstract

Most non-muscle invasive bladder cancers have been treated by transurethral resection and following intravesical injection of immunotherapeutic agents. However, the delivery efficiency of therapeutic agents into bladder wall is low due to frequent urination, which leads to the failure of treatment with side effects. Here, we report a urease-powered nanomotor containing the agonist of stimulator of interferon genes (STING) for the efficient activation of immune cells in the bladder wall. After characterization, we perform in vitro motion analysis and assess in vivo swarming behaviors of nanomotors. The intravesical instillation results in the effective penetration and retention of nanomotors in the bladder. In addition, we confirm the anti-tumor effect of nanomotor containing the STING agonist (94.2% of inhibition), with recruitment of CD8+ T cells (11.2-fold compared with PBS) and enhanced anti-tumor immune responses in bladder cancer model in female mice. Furthermore, we demonstrate the better anti-tumor effect of nanomotor containing the STING agonist than those of the gold standard Bacille Calmette-Guerin therapy and the anti-PD-1 inhibitor pembrolizumab in bladder cancer model. Taken together, the urease-powered nanomotor would provide a paradigm as a next-generation platform for bladder cancer immunotherapy.

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