Folate Receptor-Mediated Small Interfering RNA Delivery: Recent Developments and Future Directions for RNA Interference Therapeutics

被引:36
作者
Gangopadhyay, Sumit [1 ]
Nikam, Rahul R. [2 ]
Gore, Kiran R. [1 ]
机构
[1] Indian Inst Technol Kharagpur, Dept Chem, Kharagpur 721302, W Bengal, India
[2] Univ Mumbai, Dept Chem, Mumbai, Maharashtra, India
关键词
RNA interference; siRNA; gene silencing; targeted delivery; folate receptor; folic acid; MESOPOROUS SILICA NANOPARTICLES; LIPID-BASED NANOPARTICLES; IRON-OXIDE NANOPARTICLES; LIGAND-TARGETED DELIVERY; GENE-SILENCING ACTIVITY; SIRNA DELIVERY; FOLIC-ACID; IN-VITRO; SYSTEMIC DELIVERY; CHEMICAL-MODIFICATIONS;
D O I
10.1089/nat.2020.0882
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
RNA interference (RNAi), a gene regulatory process mediated by small interfering RNAs (siRNAs), has made remarkable progress as a potential therapeutic agent against various diseases. However, RNAi is associated with fundamental challenges such as poor systemic delivery and susceptibility to the nucleases. Targeting ligand-bound delivery vehicles has improved the accumulation of drug at the target site, which has resulted in high transfection efficiency and enhanced gene silencing. Recently, folate receptor (FR)-mediated targeted delivery of siRNAs has garnered attention due to their enhanced cellular uptake and high transfection efficiency toward tumor cells. Folic acid (FA), due to its small size, low immunogenicity, high in vivo stability, and high binding affinity toward FRs, has attracted much attention for targeted siRNA delivery. FRs are overexpressed in a large number of tumors, including ovarian, breast, kidney, and lung cancer cells. In this review, we discuss recent advances in FA-mediated siRNA delivery to treat cancers and inflammatory diseases. This review summarizes various FA-conjugated nanoparticle systems reported so far in the literature, including liposome, silica, metal, graphene, dendrimers, chitosan, organic copolymers, and RNA nanoparticles. This review will help in the design and development of potential delivery vehicles for siRNA drug targeting to tumor cells using an FR-mediated approach.
引用
收藏
页码:245 / 270
页数:26
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