School of Biotechnology, Dublin City University, Glasnevin, Dublin, Ireland.
Mol Biol Evol. 2012 Aug;29(8):2039-46. doi: 10.1093/molbev/mss073. Epub 2012 Feb 21.
Myeloperoxidase (MPO) is a member of the mammalian heme peroxidase (MHP) multigene family. Whereas all MHPs oxidize specific halides to generate the corresponding hypohalous acid, MPO is unique in its capacity to oxidize chloride at physiologic pH to produce hypochlorous acid (HOCl), a potent microbicide that contributes to neutrophil-mediated host defense against infection. We have previously resolved the evolutionary relationships in this functionally diverse multigene family and predicted in silico that positive Darwinian selection played a major role in the observed functional diversities (Loughran NB, O'Connor B, O'Fagain C, O'Connell MJ. 2008. The phylogeny of the mammalian heme peroxidases and the evolution of their diverse functions. BMC Evol Biol. 8:101). In this work, we have replaced positively selected residues asparagine 496 (N496), tyrosine 500 (Y500), and leucine 504 (L504) with the amino acids present in the ancestral MHP and have examined the effects on the structure, biosynthesis, and activity of MPO. Analysis in silico predicted that N496F, Y500F, or L504T would perturb hydrogen bonding in the heme pocket of MPO and thus disrupt the structural integrity of the enzyme. Biosynthesis of the mutants stably expressed in human embryonic kidney 293 cells yielded apoproMPO, the heme-free, enzymatically inactive precursor of MPO, that failed to undergo normal maturation or proteolytic processing. As a consequence of the maturational arrest at the apoproMPO stage of development, cells expressing MPO with mutations N496F, Y500F, L504T, individually or in combination, lacked normal peroxidase or chlorinating activity. Taken together, our data provide further support for the in silico predictions of positive selection and highlight the correlation between positive selection and functional divergence. Our data demonstrate that directly probing the functional importance of positive selection can provide important insights into understanding protein evolution.
髓过氧化物酶 (MPO) 是哺乳动物血红素过氧化物酶 (MHP) 多基因家族的成员。虽然所有的 MHPs 都能氧化特定的卤化物生成相应的次卤酸,但 MPO 是独特的,它能够在生理 pH 值下氧化氯离子生成次氯酸 (HOCl),次氯酸是一种有效的杀菌剂,有助于中性粒细胞介导的宿主抗感染防御。我们之前已经确定了这个功能多样的多基因家族的进化关系,并通过计算机预测,正达尔文选择在观察到的功能多样性中发挥了主要作用 (Loughran NB、O'Connor B、O'Fagain C、O'Connell MJ. 2008. 哺乳动物血红素过氧化物酶的系统发育及其不同功能的进化。BMC 进化生物学。8:101)。在这项工作中,我们用祖先 MHP 中的氨基酸取代了正选择的残基天冬酰胺 496 (N496)、酪氨酸 500 (Y500) 和亮氨酸 504 (L504),并研究了这些突变对 MPO 的结构、生物合成和活性的影响。计算机分析预测,N496F、Y500F 或 L504T 将扰乱 MPO 血红素口袋中的氢键,从而破坏酶的结构完整性。在人胚肾 293 细胞中稳定表达的突变体的生物合成产生了 apoMPO,即 MPO 的无血红素、无酶活性前体,它不能正常成熟或蛋白水解加工。由于在 apoMPO 发育阶段的成熟停滞,单独或组合表达 MPO 突变 N496F、Y500F、L504T 的细胞缺乏正常的过氧化物酶或氯化活性。总之,我们的数据为正选择的计算机预测提供了进一步的支持,并强调了正选择和功能分化之间的相关性。我们的数据表明,直接探测正选择的功能重要性可以为理解蛋白质进化提供重要的见解。
