Institute of Pharmaceutical Chemistry, Philipps-University Marburg, Marbacher Weg 6, 35032, Marburg, Germany.
Mol Divers. 2010 May;14(2):307-20. doi: 10.1007/s11030-009-9176-2. Epub 2009 Jun 26.
A series of 30 adenosine derivatives with three different substituents at the N(6)-position were prepared in order to evaluate their potential to inhibit the pathogenic protozoa Plasmodium falciparum and Trypanosoma brucei in vitro. The rationale for synthesis of these structures was the high probability of interactions with multiple adenosine associated targets and the assumption that N(6)-substitutents should increase stability against adenosine deaminases and allow the molecules to diffuse across parasite membranes. Starting from inosine, the new compounds were prepared as single isomers using a polymer-assisted acylation protocol enabling the straightforward isolation of the target compounds in pure form. Three of the compounds displayed anti-plasmodial and one anti-trypanosomal activity in the single digit micromolar concentration range.
为了评估一系列 30 种具有三种不同取代基的腺嘌呤衍生物在体外抑制致病原生动物疟原虫和布氏锥虫的潜力,我们进行了这些结构的合成。这些结构合成的依据是与多个腺嘌呤相关靶标发生相互作用的高概率,以及假设 N(6)取代基应该增加对腺嘌呤脱氨酶的稳定性,并允许分子扩散穿过寄生虫膜。从肌苷开始,使用聚合物辅助酰化方案制备新的化合物,这些方案能够以单一异构体的形式制备,从而可以以纯形式直接分离目标化合物。其中三种化合物在个位数微摩尔浓度范围内表现出抗疟原虫活性,一种化合物具有抗锥虫活性。
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