Genes and Diseases (Sep 2023)

Identification of new aptamer BC-3 targeting RPS7 from rapid screening for bladder carcinoma

  • Yunyi Liu,
  • Juan Li,
  • Hailong Ou,
  • Dan Qi,
  • Bei Hu,
  • Yuxi Xu,
  • Jian Hu,
  • Yi Xiong,
  • Luling Xia,
  • Jason H. Huang,
  • Xiaoxiao Hu,
  • Erxi Wu

Journal volume & issue
Vol. 10, no. 5
pp. 2137 – 2150

Abstract

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Aptamers, short single DNA or RNA oligonucleotides, have shown immense application potential as molecular probes for the early diagnosis and therapy of cancer. However, conventional cell-SELEX technologies for aptamer discovery are time-consuming and laborious. Here we discovered a new aptamer BC-3 by using an improved rapid X-Aptamer selection process for human bladder carcinoma, for which there is no specific molecular probe yet. We show that BC-3 exhibited excellent affinity in bladder cancer cells but not normal cells. We demonstrate that BC-3 displayed high selectivity for tumor cells over their normal counterparts in vitro, in mice, and in patient tumor tissue specimens. Further endocytosis pathway analysis revealed that BC-3 internalized into bladder cancer cells via clathrin-mediated endocytosis. Importantly, we identified ribosomal protein S7 (RPS7) as the binding target of BC-3 via an integrated methodology (mass spectrometry, colocalization assay, and immunoblotting). Together, we report that a novel aptamer BC-3 is discovered for bladder cancer and its properties in the disease are unearthed. Our findings will facilitate the discovery of novel diagnostic and therapeutic strategies for bladder cancer.

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