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Cancerous pH-responsive polycarboxybetaine-coated lipid nanoparticle for smart delivery of siRNA against subcutaneous tumor model in mice.

Yi-Jung SungHaochen GuoAria GhasemizadehXin ShenWanphiwat ChintrakulchaiMotoaki KobayashiMasahiro ToyodaKoichi OgiJunya MichinishiTomoyuki OhtakeMakoto MatsuiYuto HondaTakahiro NomotoHiroyasu TakemotoYutaka MiuraNobuhiro Nishiyama
Published in: Cancer science (2022)
Lipid nanoparticles (LNPs) have been commonly used as a vehicle for nucleic acids, such as small interfering RNA (siRNA); the surface modification of LNPs is one of the determinants of their delivery efficiency especially in systemic administration. However, the applications of siRNA-encapsulated LNPs are limited due to a lack effective systems to deliver to solid tumors. Here, we report a smart surface modification using a charge-switchable ethylenediamine-based polycarboxybetaine for enhancing tumor accumulation via interaction with anionic tumorous tissue constituents due to selective switching to cationic charge in response to cancerous acidic pH. Our polycarboxybetaine-modified LNP could enhance cellular uptake in cancerous pH, resulting in facilitated endosomal escape and gene knockdown efficiency. After systemic administration, the polycarboxybetaine-modified LNP accomplished high tumor accumulation in SKOV3-luc and CT 26 subcutaneous tumor models. The siPLK-1-encapsulated LNP thereby accomplished significant tumor growth inhibition. This study demonstrates a promising potential of the pH-responsive polycarboxybetaine as a material for modifying the surface of LNPs for efficient nucleic acid delivery.
Keyphrases
  • copy number
  • genome wide
  • nucleic acid
  • cancer therapy
  • computed tomography
  • fatty acid
  • adipose tissue
  • metabolic syndrome
  • image quality
  • skeletal muscle
  • genome wide identification