Engineering siRNA therapeutics: challenges and strategies

被引:0
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作者
Syed Saqib Ali Zaidi
Faria Fatima
Syed Aqib Ali Zaidi
Dezhong Zhou
Wuquan Deng
Shuai Liu
机构
[1] Xi’an Jiaotong University,School of Chemical Engineering and Technology
[2] Ziauddin University,College of Medical Technology
[3] Shenzhen University Medical School,Shenzhen Key Laboratory of Anti
[4] Shenzhen University,Aging and Regenerative Medicine
[5] Chongqing University Central Hospital,Department of Endocrinology and Metabolism, Chongqing Diabetic Foot Medical Research Center
[6] Chongqing Emergency Medical Center,College of Pharmaceutical Sciences
[7] Zhejiang University,undefined
关键词
siRNA; Extracellular barriers; Intracellular barriers; siRNA modification; siRNA delivery;
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学科分类号
摘要
Small interfering RNA (siRNA) is a potential method of gene silencing to target specific genes. Although the U.S. Food and Drug Administration (FDA) has approved multiple siRNA-based therapeutics, many biological barriers limit their use for treating diseases. Such limitations include challenges concerning systemic or local administration, short half-life, rapid clearance rates, nonspecific binding, cell membrane penetration inability, ineffective endosomal escape, pH sensitivity, endonuclease degradation, immunological responses, and intracellular trafficking. To overcome these barriers, various strategies have been developed to stabilize siRNA, ensuring their delivery to the target site. Chemical modifications implemented with nucleotides or the phosphate backbone can reduce off-target binding and immune stimulation. Encapsulation or formulation can protect siRNA from endonuclease degradation and enhance cellular uptake while promoting endosomal escape. Additionally, various techniques such as viral vectors, aptamers, cell-penetrating peptides, liposomes, and polymers have been developed for delivering siRNA, greatly improving their bioavailability and therapeutic potential.
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