Departamento de Farmacia, Facultad de Ciencias Químicas, Universidad Nacional de Córdoba, 5000 Córdoba, Argentina.
Eur J Med Chem. 2013 Nov;69:455-64. doi: 10.1016/j.ejmech.2013.08.045. Epub 2013 Sep 13.
Chagas disease is caused by Trypanosoma cruzi (T. cruzi) leading to a huge number of infections and deaths per year, because in addition to many sufferers only having limited access to health services only an inefficient chemotherapy is available using drugs such as benznidazole and nifurtimox. Here, C6-alkyl (2a-c) and N1-acyl (3a-c) derivatives of Allopurinol (Allop, compound with activity against T. cruzi) were synthesized in good yields and their structures were unambiguously characterized. Only 2a, 2b and 3c showed inhibitory activity against the proliferative stages of the parasite when tested at 1 μg mL(-1) with the 3c derivative exhibiting an IC50 value similar to that of Allop and not being toxic for mammalian cells. Relevant pharmaceutical physicochemical properties (pKa, stability, solubility, lipophilicity) were also determined as well by using Lipinski's rule, polar surface area and molecular rigidity. Taken together, the results demonstrated that the studied derivatives had optimal properties for bioavailability and oral absorption. For the stability studies, Micellar Liquid Chromatography was used as the analytical method which was fully validated according to the FDA guidelines and shown to be a suitable, sensitive and simple method for routine analysis of these Allop derivatives.
恰加斯病是由克氏锥虫(T. cruzi)引起的,每年导致大量感染和死亡,因为除了许多患者只能有限地获得医疗服务外,目前仅有一种低效的化疗方法,即使用苯并咪唑和硝呋替莫等药物。在这里,我们合成了别嘌醇(Allop,对 T. cruzi 具有活性的化合物)的 C6-烷基(2a-c)和 N1-酰基(3a-c)衍生物,产率良好,其结构明确。只有 2a、2b 和 3c 在 1 μg mL(-1)浓度下对寄生虫的增殖阶段表现出抑制活性,其中 3c 衍生物的 IC50 值与 Allop 相似,且对哺乳动物细胞没有毒性。还通过使用 Lipinski 规则、极性表面积和分子刚性来确定相关的药物物理化学性质(pKa、稳定性、溶解度、亲脂性)。总的来说,研究结果表明,所研究的衍生物具有最佳的生物利用度和口服吸收特性。对于稳定性研究,我们使用胶束液相色谱作为分析方法,该方法完全按照 FDA 指南进行了验证,被证明是一种适合、灵敏和简单的常规分析这些 Allop 衍生物的方法。
