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The identification of an integral membrane cytochrome c urate oxidase completes the catalytic repertoire of a therapeutic enzyme

机译:完整的膜细胞色素尿酸氧化酶的鉴定完成了治疗性酶的催化库

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摘要

In living organisms, the conversion of urate into allantoin requires three consecutive enzymes. The pathway was lost in hominid, predisposing humans to hyperuricemia and gout. Among other species, the genomic distribution of the two last enzymes of the pathway is wider than that of urate oxidase (Uox), suggesting the presence of unknown genes encoding Uox. Here we combine gene network analysis with association rule learning to identify the missing urate oxidase. In contrast with the known soluble Uox, the identified gene (puuD) encodes a membrane protein with a C-terminal cytochrome c. The 8-helix transmembrane domain corresponds to DUF989, a family without similarity to known proteins. Gene deletion in a PuuD-encoding organism (Agrobacterium fabrum) abolished urate degradation capacity; the phenotype was fully restored by complementation with a cytosolic Uox from zebrafish. Consistent with H2O2 production by zfUox, urate oxidation in the complemented strain caused a four-fold increase of catalase. No increase was observed in the wild-type, suggesting that urate oxidation by PuuD proceeds through cytochrome c-mediated electron transfer. These findings identify a missing link in purine catabolism, assign a biochemical activity to a domain of unknown function (DUF989), and complete the catalytic repertoire of an enzyme useful for human therapy.
机译:在活生物体中,尿酸盐转化为尿囊素需要三个连续的酶。该途径在人猿中丢失,使人易患高尿酸血症和痛风。在其他物种中,该途径的最后两种酶的基因组分布比尿酸氧化酶(Uox)的基因组分布更宽,表明存在编码Uox的未知基因。在这里,我们将基因网络分析与关联规则学习结合起来,以识别缺失的尿酸氧化酶。与已知的可溶性Uox相比,已鉴定的基因(puuD)编码具有C端细胞色素c的膜蛋白。 8螺旋跨膜结构域对应于DUF989,DUF989是与已知蛋白质没有相似性的一个家族。编码PuuD的有机体(法氏农杆菌)中的基因缺失消除了尿酸盐的降解能力。该表型通过与来自斑马鱼的胞质Uox互补而完全恢复。与zfUox生产H2O2一致,互补菌株中的尿酸盐氧化导致过氧化氢酶增加了4倍。在野生型中未观察到增加,表明由PuuD引起的尿酸盐氧化通过细胞色素c介导的电子转移进行。这些发现确定了嘌呤分解代谢中的缺失环节,将生化活性分配给功能未知的区域(DUF989),并完成了可用于人类治疗的酶的催化库。

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