Northern Institute for Cancer Research, Bedson Building, Newcastle University, Newcastle Upon Tyne, UK NE1 7RU.
Org Biomol Chem. 2010 May 21;8(10):2397-407. doi: 10.1039/b925481a. Epub 2010 Mar 18.
CDK2 inhibitory structure-activity relationships have been explored for a range of 5-substituted O(4)-alkylpyrimidines. Variation of the 5-substituent in the 2,6-diaminopyrimidine series confirmed the 5-nitroso substituent as optimal, and showed that 5-formyl and 5-acetyl substituents were also tolerated at this position. A series of O(4)-alkyl-N(2)-aryl-5-substituted-6-aminopyrimidines revealed interesting structure-activity relationships. In the 5-nitroso series, the optimum O(4)-alkyl substituents were cyclohexylmethyl or sec-butyl, combined with a 2-sulfanilyl group. By contrast, in the N(2)-arylsulfonamido-5-formyl series, the cyclohexylmethyl compound showed relatively poor activity compared with the sec-butyl derivative (22j, (R)-4-(4-amino-6-sec-butoxy-5-formylpyrimidin-2-ylamino)benzenesulfonamide; CDK2 IC(50) = 0.8 nM). Similarly, in the N(2)-arylsulfonamido-5-(hydroxyiminomethyl) series the O(4)-sec-butyl substituent conferred greater potency than the cyclohexylmethyl (23c, (rac)-4-(4-amino-6-sec-butoxy-5-(hydroxyiminomethyl)pyrimidin-2-ylamino)benzenesulfonamide; CDK2 IC(50) = 7.4 nM). The 5-formyl derivatives show selectivity for CDK2 over other CDK family members, and are growth inhibitory in tumour cells (e.g. 22j, GI(50) = 0.57 microM).
已针对一系列 5-取代的 O(4)-烷基嘧啶研究了 CDK2 抑制结构-活性关系。在 2,6-二氨基嘧啶系列中改变 5-取代基证实 5-亚硝基取代基为最佳,并且表明 5-甲酰基和 5-乙酰基取代基在此位置也可耐受。一系列 O(4)-烷基-N(2)-芳基-5-取代-6-氨基嘧啶揭示了有趣的结构-活性关系。在 5-亚硝基系列中,最佳的 O(4)-烷基取代基是环己基甲基或仲丁基,与 2-磺胺酰基结合。相比之下,在 N(2)-芳基磺酰胺基-5-甲酰基系列中,与仲丁基衍生物(22j,(R)-4-(4-氨基-6-仲丁氧基-5-甲酰基嘧啶-2-基氨基)苯磺酰胺;CDK2 IC(50) = 0.8 nM)相比,环己基甲基化合物的活性相对较差。同样,在 N(2)-芳基磺酰胺基-5-(羟亚氨基甲基)系列中,O(4)-仲丁基取代基比环己基甲基赋予更大的效力(23c,(rac)-4-(4-氨基-6-仲丁氧基-5-(羟亚氨基甲基)嘧啶-2-基氨基)苯磺酰胺;CDK2 IC(50) = 7.4 nM)。5-甲酰基衍生物对 CDK2 具有选择性,并且对其他 CDK 家族成员具有抑制作用,并且在肿瘤细胞中具有生长抑制作用(例如 22j,GI(50) = 0.57 microM)。
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