AI Article Synopsis

  • Small interfering RNAs (siRNAs) are valuable for gene expression manipulation but face challenges like degradation and limited delivery efficiency.
  • This study tested three lipid-substituted polyethylenimine (PEI) carriers (Leu-Fect A-C) for delivering siRNAs to various organs, including tumors, in mice.
  • The results showed that these carriers effectively delivered siRNAs, especially in lung and spleen tissues, with Leu-Fect A showing the best distribution, suggesting potential for clinical applications in siRNA therapies.

Article Abstract

Small interfering RNAs (siRNAs) have emerged as a powerful tool to manipulate gene expression . However, their potential therapeutic application encounters significant challenges, such as degradation limited cellular uptake, and restricted biodistribution, among others. This study evaluates the siRNA delivery efficiency of three different lipid-substituted polyethylenimine (PEI)-based carriers, named Leu-Fect A-C, to different organs , including xenograft tumors, when injected into the bloodstream of mice. The siRNA analysis was undertaken by stem-loop RT-PCR, followed by qPCR or digital droplet PCR. Formulating siRNAs with a Leu-Fect series of carriers generated nanoparticles that effectively delivered the siRNAs into K652 and MV4-11 cells, both models of leukemia. The Leu-Fect carriers were able to successfully deliver BCR-Abl and FLT3 siRNAs into leukemia xenograft tumors in mice. All three carriers demonstrated significantly enhanced siRNA delivery into organs other than the liver, including the xenograft tumors. Preferential biodistribution of siRNAs was observed in the lungs and spleen. Among the delivery systems, Leu-Fect A exhibited the highest biodistribution into organs. In conclusion, lipid-substituted PEI-based delivery systems offer improvements in addressing pharmacokinetic challenges associated with siRNA-based therapies, thus opening avenues for their potential translation into clinical practice.

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Source
http://dx.doi.org/10.1021/acs.molpharmaceut.3c01077DOI Listing

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