ACS APPL BIO MATER. 2022; 5, 4: 1489-1500 DOI:10.1021/acsabm.1c01226

Influence of Hydrophobicity in the Hydrophilic Region of Cationic Lipids on Enhancing Nucleic Acid Delivery and Gene Editing

Rapaka, H; Manturthi, S; Arjunan, P; Venkatesan, V; Thangavel, S; Marepally, S; Patri, SV

Abstract

Intracellular delivery of biomolecules using non-viral vectors critically depends on the vectors' ability to allow the escape and release of the contents from the endosomes. Prior findings demonstrated that aromatic/hydrophobic group-containing amino acids such as phenylalanine (F) and tryptophan (W) destabilize cellular membranes by forming pores in the lipid bilayer. Taking cues from these findings, we have developed four alpha-tocopherol-based cationic amphiphiles by varying the aromatic/hydrophobic amino acids such as glycine (G), proline (P), phenylalanine (F), and tryptophan (W) as head groups and triazole in the linker region to study their impact on endosomal escape for the enhanced transfection efficacy. The lipids tocopherol-triazole-phenylalanine (TTF) and tocopherol-triazole-tryptophan (TTW) exhibited similar potential to commercial transfecting reagents, Lipofectamine (LF) 3000 and Lipofectamine Messenger Max (LFMM), respectively, in transfecting plasmid DNA and messenger RNA in multiple cultured cell lines. The TTW liposome was also found to be effective in delivering Cas9 mRNA and demonstrated equal efficiency of gene editing AAVS1 locus compared to LFMM in CHO, Neuro-2a, and EA.HY926 cell lines. In this current investigation, it is shown that the synthesized cationic lipids with aromatic hydrophobic R group-containing amino acids are safe, economic, and actually more efficient in nucleic acid delivery and genome-editing applications. These findings can be further explored in the genome-editing approach for treating genetic disorders.

Keywords: cationic lipids; alpha-tocopherol; endosomal escape; non-viral nucleic acid delivery; gene editing

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Liposomes for DNA/RNA Delivery

Liposomes represent a category of biological nanocarriers extensively employed for transporting DNA and RNA. Their composition comprises an aqueous core enveloped by a hydrophobic lipid layer, forming a protective enclosure for DNA or RNA molecules. Liposomes establish connections with nucleic acids either through charge interactions or lipid membrane fusion. These interactions extend to the cell membrane, fostering liposome-cell interactions and facilitating the internal release of nucleic acids. The liposome delivery system boasts excellent biocompatibility and minimal toxicity, proving proficient in guiding DNA and RNA across biological barriers like cell membranes. This method exhibits promise in diverse fields such as gene therapy and vaccine development, offering a viable approach for targeted therapy. Nevertheless, challenges persist in liposome delivery systems, including issues like insufficient local concentration and immune activation. Ongoing research endeavors concentrate on refining liposome design to enhance delivery efficiency and biological stability, with the ultimate goal of expanding their utilization in gene delivery within various applications.

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