4.7 Article

Advance of structural modification of nucleosides scaffold

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ELSEVIER FRANCE-EDITIONS SCIENTIFIQUES MEDICALES ELSEVIER
DOI: 10.1016/j.ejmech.2021.113233

关键词

Nucleosides scaffold; Antiviral; Anti-tumor; Triazoles; Prodrugs

资金

  1. National Natural Science Foundation of China [21967003]
  2. basic ability improvement project for young and middle-aged teachers in colleges and universities in Guangxi [2017KY1226]

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Different modifications of the sugar and base in nucleoside drugs can affect their bioactivity, with certain groups enhancing anti-tumor or antiviral effects. Macromolecule-modified nucleosides can improve bioavailability and bioactivity, while reducing toxicity.
With Remdesivir being approved by FDA as a drug for the treatment of Corona Virus Disease 2019 (COVID-19), nucleoside drugs have once again received widespread attention in the medical community. Herein, we summarized modification of traditional nucleoside framework (sugar + base), traizole nucleosides, nucleoside analogues assembled by other drugs, macromolecule-modified nucleosides, and their bioactivity rules. 2'-Ara-substituted by -F or -CN group, and 3'-ara substituted by acetylenyl group can greatly influence their anti-tumor activities. Dideoxy dehydrogenation of 2',3'-sites can enhance antiviral efficiencies. Acyclic nucleosides and L-type nucleosides mainly represented antiviral capabilities. 5-F Substituted uracil analogues exihibit anti-tumor effects, and the substrates substituted by -I, -CF3, bromovinyl group usually show antiviral activities. The sugar coupled with 1-N of triazolid usually displays anti-tumor efficiencies, while the sugar coupled with 2-N of triazolid mainly represents antiviral activities. The nucleoside analogues assembled by cholesterol, polyethylene glycol, fatty acid and phospholipid would improve their bioavailabilities and bioactivities, or reduce their toxicities. (C) 2021 Elsevier Masson SAS. All rights reserved.

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