前药
生物利用度
药理学
部分
药品
核苷酸
药物输送
化学
组合化学
生物化学
医学
立体化学
有机化学
基因
作者
Larryn W. Peterson,Charles E. McKenna
标识
DOI:10.1517/17425240902824808
摘要
Nucleotide analogues have been well accepted as therapeutic agents active against a number of viruses. However, their use as antiviral agents is limited by the need for phosphorylation by endogenous enzymes, and if the analogue is orally administered, by low bioavailability due to the presence of an ionizable diacid group. To circumvent these limitations, a number of prodrug approaches have been proposed. The ideal prodrug achieves delivery of a parent drug by attachment of a non-toxic moiety that is stable during transport and delivery, but is readily cleaved to release the parent drug once at the target. Here, a brief overview of several promising prodrug strategies currently under development is given.
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