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具有聚乙二醇修饰的治疗性寡核苷酸。

Therapeutic oligonucleotides with polyethylene glycol modifications.

作者信息

Winkler Johannes

机构信息

Department of Pharmaceutical Chemistry, University of Vienna, Althanstraße 14, 1090 Vienna, Austria.

出版信息

Future Med Chem. 2015;7(13):1721-31. doi: 10.4155/fmc.15.94. Epub 2015 Sep 29.

Abstract

In the field of oligonucleotide drugs, the attachment of PEG is a well-established strategy to prevent enzymatic degradation and avoid renal elimination. Pegaptanib and other oligonucleotides in clinical development utilize the attachment of linear or branched high molecular weight PEG chains for increase of accumulation and duration of the effect after local or systemic application. The length of PEG chains is decisive for the pharmacokinetic and pharmacodynamic effects. Longer chains increase circulation times, but generally decrease gene-silencing efficiencies for antisense and siRNA agents and binding affinities for aptamers. Shorter chains are less efficient in preventing renal filtration, but have also less impact on the gene-silencing machinery and binding kinetics.

摘要

在寡核苷酸药物领域,连接聚乙二醇(PEG)是一种成熟的策略,可防止酶降解并避免肾脏清除。培加他尼及其他处于临床开发阶段的寡核苷酸药物利用连接线性或分支状高分子量PEG链,以增加局部或全身给药后的蓄积量和作用持续时间。PEG链的长度对药代动力学和药效学效应起决定性作用。较长的链可延长循环时间,但通常会降低反义核酸和小干扰RNA(siRNA)药物的基因沉默效率以及适体的结合亲和力。较短的链在防止肾脏滤过方面效率较低,但对基因沉默机制和结合动力学的影响也较小。

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