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A smart multiantenna gene theranostic system based on the programmed assembly of hypoxia-related siRNAs

Author

Listed:
  • Xue Gong

    (Wuhan University)

  • Haizhou Wang

    (Wuhan University)

  • Ruomeng Li

    (Wuhan University)

  • Kaiyue Tan

    (Wuhan University)

  • Jie Wei

    (Wuhan University)

  • Jing Wang

    (Wuhan University)

  • Chen Hong

    (Wuhan University)

  • Jinhua Shang

    (Wuhan University)

  • Xiaoqing Liu

    (Wuhan University)

  • Jing Liu

    (Wuhan University)

  • Fuan Wang

    (Wuhan University)

Abstract

The systemic therapeutic utilisation of RNA interference (RNAi) is limited by the non-specific off-target effects, which can have severe adverse impacts in clinical applications. The accurate use of RNAi requires tumour-specific on-demand conditional activation to eliminate the off-target effects of RNAi, for which conventional RNAi systems cannot be used. Herein, a tumourous biomarker-activated RNAi platform is achieved through the careful design of RNAi prodrugs in extracellular vesicles (EVs) with cancer-specific recognition/activation features. These RNAi prodrugs are assembled by splitting and reconstituting the principal siRNAs into a hybridisation chain reaction (HCR) amplification machine. EVs facilitate the specific and efficient internalisation of RNAi prodrugs into target tumour cells, where endogenous microRNAs (miRNAs) promote immediate and autonomous HCR-amplified RNAi activation to simultaneously silence multiantenna hypoxia-related genes. With multiple guaranteed cancer recognition and synergistic therapy features, the miRNA-initiated HCR-promoted RNAi cascade holds great promise for personalised theranostics that enable reliable diagnosis and programmable on-demand therapy.

Suggested Citation

  • Xue Gong & Haizhou Wang & Ruomeng Li & Kaiyue Tan & Jie Wei & Jing Wang & Chen Hong & Jinhua Shang & Xiaoqing Liu & Jing Liu & Fuan Wang, 2021. "A smart multiantenna gene theranostic system based on the programmed assembly of hypoxia-related siRNAs," Nature Communications, Nature, vol. 12(1), pages 1-13, December.
  • Handle: RePEc:nat:natcom:v:12:y:2021:i:1:d:10.1038_s41467-021-24191-9
    DOI: 10.1038/s41467-021-24191-9
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