Pereira Humberto M, Rezende Martha M, Castilho Marcelo Santos, Oliva Glaucius, Garratt Richard C
Instituto de Física de São Carlos, Universidade de São Paulo, Avenida Trabalhador Sãocarlense 400, São Carlos, SP 13560-970, Brazil.
Acta Crystallogr D Biol Crystallogr. 2010 Jan;66(Pt 1):73-9. doi: 10.1107/S0907444909045715. Epub 2009 Dec 21.
Schistosomes are unable to synthesize purines de novo and depend exclusively on the salvage pathway for their purine requirements. It has been suggested that blockage of this pathway could lead to parasite death. The enzyme purine nucleoside phosphorylase (PNP) is one of its key components and molecules designed to inhibit the low-molecular-weight (LMW) PNPs, which include both the human and schistosome enzymes, are typically analogues of the natural substrates inosine and guanosine. Here, it is shown that adenosine both binds to Schistosoma mansoni PNP and behaves as a weak micromolar inhibitor of inosine phosphorolysis. Furthermore, the first crystal structures of complexes of an LMW PNP with adenosine and adenine are reported, together with those with inosine and hypoxanthine. These are used to propose a structural explanation for the selective binding of adenosine to some LMW PNPs but not to others. The results indicate that transition-state analogues based on adenosine or other 6-amino nucleosides should not be discounted as potential starting points for alternative inhibitors.
血吸虫无法从头合成嘌呤,其嘌呤需求完全依赖于补救途径。有人提出,阻断该途径可能导致寄生虫死亡。嘌呤核苷磷酸化酶(PNP)是该途径的关键组成部分之一,旨在抑制低分子量(LMW)PNP的分子,包括人类和血吸虫的酶,通常是天然底物肌苷和鸟苷的类似物。在此表明,腺苷既能与曼氏血吸虫PNP结合,又能作为肌苷磷酸解的微弱微摩尔级抑制剂。此外,还报道了LMW PNP与腺苷、腺嘌呤以及与肌苷、次黄嘌呤形成的复合物的首个晶体结构。这些结构被用于对腺苷与某些LMW PNP选择性结合而与其他LMW PNP不结合的现象提出结构上的解释。结果表明,基于腺苷或其他6-氨基核苷的过渡态类似物作为替代抑制剂的潜在起始点不应被忽视。
