寡核苷酸
前药
化学
转染
组合化学
核酸酶
试剂
立体化学
生物化学
生物物理学
DNA
生物
有机化学
基因
作者
Norihito Sugimoto,Junsuke Hayashi,Ryohei Funaki,Shun‐ichi Wada,Fumito Wada,Mariko Harada‐Shiba,Hidehito Urata
出处
期刊:ChemBioChem
[Wiley]
日期:2023-10-16
卷期号:24 (24)
被引量:4
标识
DOI:10.1002/cbic.202300526
摘要
Various chemical modifications have been developed to create new antisense oligonucleotides (AONs) for clinical applications. Our previously designed prodrug-type phosphotriester-modified oligonucleotide with cyclic disulfides (cyclic SS PTE ON) can be converted into unmodified ON in an intracellular-mimetic reducing environment. However, the conversion rate of the cyclic SS PTE ON was very low, and the AON with cyclic SS PTE modifications showed much weaker antisense activity than corresponding to the fully phosphorothioate-modified AON. In this study, we synthesized several types of PTE ONs containing linear disulfides (linear SS PTE ONs) and evaluated their conversion rates under reducing conditions. From the results, the structural requirements for the conversion of the synthesized linear SS PTE ONs were elucidated. Linear SS PTE ON with promising promoieties showed a nuclease resistance up to 4.8-fold compared to unmodified ON and a cellular uptake by endocytosis without any transfection reagent. In addition, although the knockdown activity of the linear SS PTE gapmer AON is weaker than that of the fully phosphorothioate-modified gapmer AON, the knockdown activity is slightly stronger than that of the cyclic SS PTE gapmer AON. These results suggest that the conversion rates may be related to the expression of the antisense activity.
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