Link Andreas, Heidler Philipp, Kaiser Marcel, Brun Reto
Institute of Pharmacy, Ernst-Moritz-Arndt-University, Friedrich-Ludwig-Jahn-Strasse 17, 17487 Greifswald, Germany.
Eur J Med Chem. 2009 Sep;44(9):3665-71. doi: 10.1016/j.ejmech.2009.02.010. Epub 2009 Feb 20.
The involvement of purine salvage in the accumulation of current trypanocidal drugs is important for the treatment of African sleeping sickness. The substrate specificity of essential nucleoside transporters is therefore of physiological and pharmacological interest. With the intention to contribute to the knowledge in the field, a series of 16 adenosine derivatives with substituents in N(6)-position were prepared in order to evaluate their potential to inhibit Trypanosoma brucei spp. in vitro. An unmodified ribose moiety was selected to conserve key molecular recognition motifs of the arsenal of integral membrane proteins expressed in large numbers on the protozoan plasma membrane. Two of the new compounds prepared using a polymer-assisted acylation protocol showed antitrypanosomal activities in the single digit micromolar concentration range.
嘌呤补救途径参与当前杀锥虫药物的蓄积对非洲昏睡病的治疗很重要。因此,必需核苷转运体的底物特异性具有生理和药理学意义。为了增进该领域的知识,制备了一系列16种在N(6)位带有取代基的腺苷衍生物,以评估它们在体外抑制布氏锥虫属的潜力。选择未修饰的核糖部分以保留原生动物质膜上大量表达的整合膜蛋白库的关键分子识别基序。使用聚合物辅助酰化方案制备的两种新化合物在个位数微摩尔浓度范围内显示出抗锥虫活性。
