1. Academic Validation
  2. A Combinatorial Library of Lipid Nanoparticles for RNA Delivery to Leukocytes

A Combinatorial Library of Lipid Nanoparticles for RNA Delivery to Leukocytes

  • Adv Mater. 2020 Mar;32(12):e1906128. doi: 10.1002/adma.201906128.
Srinivas Ramishetti 1 2 3 Inbal Hazan-Halevy 1 2 3 Ramesh Palakuri 1 2 3 Sushmita Chatterjee 1 2 3 Somu Naidu Gonna 1 2 3 Niels Dammes 1 2 3 Inbar Freilich 4 Luba Kolik Shmuel 4 Dganit Danino 4 Dan Peer 1 2 3
Affiliations

Affiliations

  • 1 Laboratory of Precision NanoMedicine, School of Molecular Cell Biology and Biotechnology, George S. Wise Faculty of Life Sciences, Tel Aviv University, Tel Aviv, 69978, Israel.
  • 2 Department of Materials Sciences and Engineering, Faculty of Engineering, Tel Aviv University, Tel Aviv, 69978, Israel.
  • 3 Center for Nanoscience and Nanotechnology and Cancer Biology Research Center, Tel Aviv University, Tel Aviv, 69978, Israel.
  • 4 CryoEM Laboratory of Soft Matter, Faculty of Biotechnology and Food Engineering, Technion, Haifa, 3200003, Israel.
Abstract

Lipid nanoparticles (LNPs) are the most advanced nonviral platforms for small interfering RNA (siRNA) delivery that are clinically approved. These LNPs, based on ionizable lipids, are found in the liver and are now gaining much attention in the field of RNA therapeutics. The previous generation of ionizable lipids varies in linker moieties, which greatly influences in vivo gene silencing efficiency. Here novel ionizable amino lipids based on the linker moieties such as hydrazine, hydroxylamine, and ethanolamine are designed and synthesized. These lipids are formulated into LNPs and screened for their efficiency to deliver siRNAs into leukocytes, which are among the hardest to transfect cell types. Two potent lipids based on their in vitro gene silencing efficiencies are also identified. These lipids are further evaluated for their biodistribution profile, efficient gene silencing, liver toxicity, and potential immune activation in mice. A robust gene silencing is also found in primary lymphocytes when one of these lipids is formulated into LNPs with a pan leukocyte selective targeting agent (β7 Integrin). Taken together, these lipids have the potential to open new avenues in delivering RNAs into leukocytes.

Keywords

T-lymphocytes; gene silencing; lipid nanoparticles; synthetic small interfering RNA; targeted delivery.

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