Journal of Nanobiotechnology (Jun 2021)

Fe-doped chrysotile nanotubes containing siRNAs to silence SPAG5 to treat bladder cancer

  • Jianye Liu,
  • Yi Zhang,
  • Hongliang Zeng,
  • Long Wang,
  • Qun Zhang,
  • Pei Wu,
  • Xiaoming Liu,
  • Hongyi Xie,
  • Wei Xiang,
  • Biao Liu,
  • Jiahao Liu,
  • Xuewen Liu,
  • Jianfei Xie,
  • Jin Tang,
  • Zhi Long,
  • Leye He,
  • Mengqing Xiao,
  • Liang Xiang,
  • Ke Cao

DOI
https://doi.org/10.1186/s12951-021-00935-z
Journal volume & issue
Vol. 19, no. 1
pp. 1 – 20

Abstract

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Abstract Background For certain human cancers, sperm associated antigen 5 (SPAG5) exerts important functions for their development and progression. However, whether RNA interference (RNAi) targeting SPAG5 has antitumor effects has not been determined clinically. Results The results indicated that Fe-doped chrysotile nanotubes (FeSiNTs) with a relatively uniform outer diameter (15–25 nm) and inner diameter (7–8 nm), and a length of several hundred nanometers, which delivered an siRNA against the SPAG5 oncogene (siSPAG5) efficiently. The nanomaterials were designed to prolong the half-life of siSPAG5 in blood, increase tumor cell-specific uptake, and maximize the efficiency of SPAG5 silencing. In vitro, FeSiNTs carrying siSPAG5 inhibited the growth, migration, and invasion of bladder cancer cells. In vivo, the FeSiNTs inhibited growth and metastasis in three models of bladder tumors (a tail vein injection lung metastatic model, an in-situ bladder cancer model, and a subcutaneous model) with no obvious toxicities. Mechanistically, we showed that FeSiNTs/siSPAG5 repressed PI3K/AKT/mTOR signaling, which suppressed the growth and progression of tumor cells. Conclusions The results highlight that FeSiNTs/siSPAG5 caused no activation of the innate immune response nor any systemic toxicity, indicating the possible therapeutic utility of FeSiNTs/siSPAG5 to deliver siSPAG5 to treat bladder cancer. Graphic abstract

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