Lipopeptide nanoparticles for potent and selective siRNA delivery in rodents and nonhuman primates

Yizhou Dong; Kevin T. Love; J. Robert Dorkin; Sasilada Sirirungruang; Yunlong Zhang; Delai Chen; Roman L. Bogorad; Hao Yin; Yi Chen; Arturo J. Vegas; Christopher A. Alabi; Gaurav Sahay; Karsten Olejnik; Weiheng Wang; Avi Schroeder; Abigail K. R. Lytton‐Jean; Daniel J. Siegwart; Akin Akinc; Carmen Barnes; Scott Barros; Mary Carioto; Kevin Fitzgerald; Julia Hettinger; Varun Kumar; Tatiana I. Novobrantseva; June Qin; William Querbes; Victor Koteliansky; Róbert Langer; Daniel G. Anderson

doi:10.1073/pnas.1322937111

Lipopeptide nanoparticles for potent and selective siRNA delivery in rodents and nonhuman primates

Yizhou Dong(Boston Children's Hospital), Kevin T. Love(Boston Children's Hospital), J. Robert Dorkin(Massachusetts Institute of Technology), Sasilada Sirirungruang(Massachusetts Institute of Technology), Yunlong Zhang(Massachusetts Institute of Technology), Delai Chen(Boston Children's Hospital), Roman L. Bogorad(Massachusetts Institute of Technology), Hao Yin(Massachusetts Institute of Technology), Yi Chen(Massachusetts Institute of Technology), Arturo J. Vegas(Boston Children's Hospital), Christopher A. Alabi(Massachusetts Institute of Technology), Gaurav Sahay(Massachusetts Institute of Technology), Karsten Olejnik(Massachusetts Institute of Technology), Weiheng Wang(Boston Children's Hospital), Avi Schroeder(Massachusetts Institute of Technology), Abigail K. R. Lytton‐Jean(Massachusetts Institute of Technology), Daniel J. Siegwart(Massachusetts Institute of Technology), Akin Akinc(Alnylam Pharmaceuticals (United States)), Carmen Barnes(Alnylam Pharmaceuticals (United States)), Scott Barros(Alnylam Pharmaceuticals (United States)), Mary Carioto(Alnylam Pharmaceuticals (United States)), Kevin Fitzgerald(Alnylam Pharmaceuticals (United States)), Julia Hettinger(Alnylam Pharmaceuticals (United States)), Varun Kumar(Alnylam Pharmaceuticals (United States)), Tatiana I. Novobrantseva(Alnylam Pharmaceuticals (United States)), June Qin(Alnylam Pharmaceuticals (United States)), William Querbes(Alnylam Pharmaceuticals (United States)), Victor Koteliansky(Alnylam Pharmaceuticals (United States)), Róbert Langer(Massachusetts Institute of Technology), Daniel G. Anderson(Boston Children's Hospital)

Proceedings of the National Academy of Sciences

February 10, 2014

10.1073/pnas.1322937111

Cited by 478Open Access

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Abstract

siRNA therapeutics have promise for the treatment of a wide range of genetic disorders. Motivated by lipoproteins, we report lipopeptide nanoparticles as potent and selective siRNA carriers with a wide therapeutic index. Lead material cKK-E12 showed potent silencing effects in mice (ED50 ∼ 0.002 mg/kg), rats (ED50 < 0.01 mg/kg), and nonhuman primates (over 95% silencing at 0.3 mg/kg). Apolipoprotein E plays a significant role in the potency of cKK-E12 both in vitro and in vivo. cKK-E12 was highly selective toward liver parenchymal cell in vivo, with orders of magnitude lower doses needed to silence in hepatocytes compared with endothelial cells and immune cells in different organs. Toxicity studies showed that cKK-E12 was well tolerated in rats at a dose of 1 mg/kg (over 100-fold higher than the ED50). To our knowledge, this is the most efficacious and selective nonviral siRNA delivery system for gene silencing in hepatocytes reported to date.

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