Brunschweiger Andreas, Iqbal Jamshed, Umbach Frank, Scheiff Anja B, Munkonda Mercedes N, Sévigny Jean, Knowles Aileen F, Müller Christa E
PharmaCenter Bonn, Pharmaceutical Institute, Pharmaceutical Chemistry I, Pharmaceutical Sciences Bonn, University of Bonn, An der Immenburg 4, D-53121 Bonn, Germany.
J Med Chem. 2008 Aug 14;51(15):4518-28. doi: 10.1021/jm800175e. Epub 2008 Jul 17.
Ecto-nucleoside triphosphate diphosphohydrolases (E-NTPDases, subtypes 1, 2, 3, 8 of NTPDases) dephosphorylate nucleoside tri- and diphosphates to the corresponding di- and monophosphates. In the present study we synthesized adenine and uracil nucleotide mimetics, in which the phosphate residues were replaced by phosphonic acid esters attached to the nucleoside at the 5'-position by amide linkers. Among the synthesized uridine derivatives, we identified the first potent and selective inhibitors of human NTPDase2. The most potent compound was 19a (PSB-6426), which was a competitive inhibitor of NTPDase2 exhibiting a K i value of 8.2 microM and selectivity versus other NTPDases. It was inactive toward uracil nucleotide-activated P2Y 2, P2Y 4, and P2Y 6 receptor subtypes. Compound 19a was chemically and metabolically highly stable. In contrast to the few known (unselective) NTPDase inhibitors, 19a is an uncharged molecule and may be perorally bioavailable. NTPDase2 inhibitors have potential as novel cardioprotective drugs for the treatment of stroke and for cancer therapy.
胞外核苷三磷酸二磷酸水解酶(E-NTPDases,NTPDases的1、2、3、8亚型)将核苷三磷酸和二磷酸去磷酸化为相应的二磷酸和一磷酸。在本研究中,我们合成了腺嘌呤和尿嘧啶核苷酸类似物,其中磷酸残基被通过酰胺连接子连接在核苷5'-位的膦酸酯取代。在合成的尿苷衍生物中,我们鉴定出了首个有效的、选择性的人NTPDase2抑制剂。最有效的化合物是19a(PSB-6426),它是NTPDase2的竞争性抑制剂,K i值为8.2 microM,对其他NTPDases具有选择性。它对尿嘧啶核苷酸激活的P2Y 2、P2Y 4和P2Y 6受体亚型无活性。化合物19a在化学和代谢方面高度稳定。与少数已知的(非选择性的)NTPDase抑制剂不同,19a是不带电荷的分子,可能具有口服生物利用度。NTPDase2抑制剂有潜力作为新型心脏保护药物用于治疗中风和癌症。
