4.8 Article

Aerosol delivery of star polymer-siRNA nanoparticles as a therapeutic strategy to inhibit lung tumor growth

Journal

BIOMATERIALS
Volume 285, Issue -, Pages -

Publisher

ELSEVIER SCI LTD
DOI: 10.1016/j.biomaterials.2022.121539

Keywords

siRNA; Aerosol drug delivery; Star polymers; Lung cancer; PLK1; ?III-tubulin

Funding

  1. Children's Cancer Institute
  2. Sydney Children's Hospital Network
  3. NHMRC project grant [APP1144113]
  4. NHMRC Program Grant [APP1091261]
  5. Cancer Australia [1141485]
  6. Cancer Australia/Kids Cancer Project [APP1184840]
  7. University International Postgraduate Award (University of New South Wales)
  8. NHMRC Principal Research Fellowship [APP1119152]
  9. Australian Research Council Future Fellowship [170100144]
  10. Olivia Lambert Foundation
  11. Alexander von Humboldt Foundation

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The study demonstrated that star-shaped siRNA nanoparticles can effectively inhibit target gene expression in lung cancer cells and delay tumor growth in mouse lung tumors. This provides a proof-of-concept for aerosol delivery of star-siRNA nanoparticles as a novel therapeutic strategy to inhibit lung tumor growth.
Lung cancer is a major contributor to cancer-related death worldwide. siRNA nanomedicines are powerful tools for cancer therapeutics. However, there are challenges to overcome to increase siRNA delivery to solid tumors, including penetration of nanoparticles into a complex microenvironment following systemic delivery while avoiding rapid clearance by the reticuloendothelial system, and limited siRNA release from endosomes once inside the cell. Here we characterized cell uptake, intracellular trafficking, and gene silencing activity of miktoarm star polymer (PDMAEMA-POEGMA) nanoparticles (star nanoparticles) complexed to siRNA in lung cancer cells. We investigated the potential of nebulized star-siRNA nanoparticles to accumulate into orthotopic mouse lung tumors to inhibit expression of two genes [beta III-tubulin, Polo-Like Kinase 1 (PLK1)] which: 1) are upregulated in lung cancer cells; 2) promote tumor growth; and 3) are difficult to inhibit using chemical drugs. StarsiRNA nanoparticles internalized into lung cancer cells and escaped the endo-lysosomal pathway to inhibit target gene expression in lung cancer cells in vitro. Nebulized star-siRNA nanoparticles accumulated into lungs and silenced the expression of beta III-tubulin and PLK1 in mouse lung tumors, delaying aggressive tumor growth. These results demonstrate a proof-of-concept for aerosol delivery of star-siRNA nanoparticles as a novel therapeutic strategy to inhibit lung tumor growth.

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