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Increased PIP3 activity blocks nanoparticle mRNA delivery.

Kalina PaunovskaAlejandro Da Silva SanchezMatthew T FosterDavid LoughreyEmmeline L BlanchardFatima Z IslamZubao GanAthanasios MantalarisPhilip J SantangeloJames E Dahlman
Published in: Science advances (2020)
The biological pathways that affect drug delivery in vivo remain poorly understood. We hypothesized that altering cell metabolism with phosphatidylinositol (3,4,5)-triphosphate (PIP3), a bioactive lipid upstream of the metabolic pathway PI3K (phosphatidylinositol 3-kinase)/AKT/ mTOR (mammalian target of rapamycin) would transiently increase protein translated by nanoparticle-delivered messenger RNA (mRNA) since these pathways increase growth and proliferation. Instead, we found that PIP3 blocked delivery of clinically-relevant lipid nanoparticles (LNPs) across multiple cell types in vitro and in vivo. PIP3-driven reductions in LNP delivery were not caused by toxicity, cell uptake, or endosomal escape. Interestingly, RNA sequencing and metabolomics analyses suggested an increase in basal metabolic rate. Higher transcriptional activity and mitochondrial expansion led us to formulate two competing hypotheses that explain the reductions in LNP-mediated mRNA delivery. First, PIP3 induced consumption of limited cellular resources, "drowning out" exogenously-delivered mRNA. Second, PIP3 triggers a catabolic response that leads to protein degradation and decreased translation.
Keyphrases
  • single cell
  • drug delivery
  • binding protein
  • cell therapy
  • signaling pathway
  • cell proliferation
  • protein kinase
  • mesenchymal stem cells
  • protein protein
  • high glucose
  • cancer therapy
  • stress induced
  • walled carbon nanotubes