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Literature DB >> 34366123

Strategies to deliver RNA by nanoparticles for therapeutic potential.

Alysia Cox¹, Siyoung A Lim², Eun Ji Chung³.

Abstract

The use of a variety of RNA molecules, including messenger RNA, small interfering RNA, and microRNA, has shown great potential for prevention and therapy of many pathologies. However, this therapeutic promise has historically been limited by short in vivo half-life, lack of targeted delivery, and safety issues. Nanoparticle (NP)-mediated delivery has been a successful platform to overcome these limitations, with multiple formulations already in clinical trials and approved by the FDA. Although there is a diversity of NPs in terms of material formulation, size, shape, and charge that have been proposed for biomedical applications, specific modifications are required to facilitate sufficient RNA delivery and adequate therapeutic effect. This includes optimization of (i) RNA incorporation into NPs, (ii) specific cell targeting, (iii) cellular uptake and (iv) endosomal escape ability. In this review, we summarize the methods by which NPs can be modified for RNA delivery to achieve optimal therapeutic effects.

Entities: Chemical

Keywords: Cellular uptake; Drug delivery; Endosomal escape; Nanomedicine; RNA therapy; Targeting

Mesh：

Substances：

Year: 2021 PMID： 34366123 PMCID： PMC8792155 DOI： 10.1016/j.mam.2021.100991

Source DB: PubMed Journal: Mol Aspects Med ISSN： 0098-2997

142 in total

1. In vivo application of RNA leads to induction of specific cytotoxic T lymphocytes and antibodies.

Authors: I Hoerr; R Obst; H G Rammensee; G Jung
Journal: Eur J Immunol Date: 2000-01 Impact factor: 5.532

2. Aerosolizable siRNA-encapsulated solid lipid nanoparticles prepared by thin-film freeze-drying for potential pulmonary delivery.

Authors: Jie-Liang Wang; Mahmoud S Hanafy; Haiyue Xu; Jasmim Leal; Yufeng Zhai; Debadyuti Ghosh; Robert O Williams Iii; Hugh David Charles Smyth; Zhengrong Cui
Journal: Int J Pharm Date: 2021-01-21 Impact factor: 5.875

3. Self-assembled peptide nanoparticles with endosome escaping permits for co-drug delivery.

Authors: Yingshu Guo; Yinhua Hu; Xiaofei Zheng; Xiuping Cao; Qiong Li; Zhiyong Wei; Zhenkai Zhu; Shusheng Zhang
Journal: Talanta Date: 2020-09-06 Impact factor: 6.057

4. Advances in delivery systems for doxorubicin.

Authors: Na Zhao; Martin C Woodle; A James Mixson
Journal: J Nanomed Nanotechnol Date: 2018-11-04

5. Multifunctional nanoparticles co-delivering EZH2 siRNA and etoposide for synergistic therapy of orthotopic non-small-cell lung tumor.

Authors: Zhi-Qiang Yuan; Wei-Liang Chen; Ben-Gang You; Yang Liu; Shu-di Yang; Ji-Zhao Li; Wen-Jing Zhu; Xiao-Feng Zhou; Chun Liu; Xue-Nong Zhang
Journal: J Control Release Date: 2017-10-20 Impact factor: 9.776

Strategies to deliver RNA by nanoparticles for therapeutic potential.

1. In vivo application of RNA leads to induction of specific cytotoxic T lymphocytes and antibodies.

2. Aerosolizable siRNA-encapsulated solid lipid nanoparticles prepared by thin-film freeze-drying for potential pulmonary delivery.

3. Self-assembled peptide nanoparticles with endosome escaping permits for co-drug delivery.

4. Advances in delivery systems for doxorubicin.

5. Multifunctional nanoparticles co-delivering EZH2 siRNA and etoposide for synergistic therapy of orthotopic non-small-cell lung tumor.

6. Layer-by-layer assembled gold nanoshells for the intracellular delivery of miR-34a.

7. Effect of complexing lipids on cellular uptake and expression of messenger RNA in human skin explants.

Review 8. Opportunities and Challenges in the Delivery of mRNA-based Vaccines.

Review 9. Cytosolic delivery of nucleic acids: The case of ionizable lipid nanoparticles.

10. Long-term storage of lipid-like nanoparticles for mRNA delivery.

Review 1. Clinical progress of nanomedicine-based RNA therapies.