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Small activating RNA delivery in vivo:Challenges,prospects,and lessons learned from siRNA delivery
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作者 Shalini Pandey Patrick T.Bednarz +1 位作者 matthias a.oberli Omid Veiseh 《Nano Research》 SCIE EI CSCD 2024年第10期8990-9002,共13页
Over the last two decades,small activating RNAs(saRNAs)have quickly moved from discovery to clinical trials.Characterized as 20 nucleotide long,double stranded RNA,saRNAs have the unique ability to increase gene trans... Over the last two decades,small activating RNAs(saRNAs)have quickly moved from discovery to clinical trials.Characterized as 20 nucleotide long,double stranded RNA,saRNAs have the unique ability to increase gene transcription at the chromatin level.This therapeutic modality has great potential as a safe and redosable alternative to gene therapy by increasing target protein expression without changing the genetic sequence.We describe the successful in vivo saRNA delivery vectors and found that similar to small interfering RNA(siRNA)and mRNA targeting tissues outside the liver works best at the end of a needle.We highlight nanoparticle vectors and RNA-conjugates,where some success has been reported for non-hepatic delivery of saRNAaptamers. 展开更多
关键词 small activating RNA hepatic bias lipid nanoparticles RNA-conjugates
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