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Repurposed HisC Aminotransferases Complete the Biosynthesis of Some Methanobactins

机译:改组的HisC氨基转移酶完成了一些甲烷菌素的生物合成

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摘要

Methanobactins (Mbns) are ribosomally produced, post-translationally modified bacterial natural products with a high affinity for copper. MbnN, a pyridoxal 5′-phosphate (PLP) dependent aminotransferase, performs a transamination reaction that is the last step in the biosynthesis of Mbns produced by several Methylosinus (Ms.) species. Our bioinformatic analyses indicate that MbnNs likely derive from histidinol-phosphate aminotransferases (HisCs), which play a key role in histidine biosynthesis. A comparison of the HisC active site with the predicted MbnN structure suggests that MbnN’s active site is altered to accommodate the larger and more hydrophobic substrates necessary for Mbn biosynthesis. Moreover, we have confirmed that MbnN is capable of catalyzing the final transamination step in Mbn biosynthesis in vitro and in vivo. We also demonstrate that without this final modification, Mbn would exhibit significantly decreased stability under physiological conditions. An examination of other Mbns and Mbn operons suggests that N-terminal protection of this family of natural products is of critical importance, and that several different means of N-terminal stabilization have evolved independently in Mbn subfamilies.
机译:甲烷菌素(Mbns)是核糖体产生的,翻译后修饰的细菌天然产物,对铜具有高度亲和力。 MbnN是一种吡ido醛5'-磷酸(PLP)依赖性氨基转移酶,它发生转氨反应,这是由几种甲基肌球菌(Ms.)物种产生的Mbns生物合成的最后一步。我们的生物信息学分析表明,MbnNs可能来源于组氨酸磷酸氨基转移酶(HisCs),后者在组氨酸的生物合成中起关键作用。 HisC活性位点与预测的MbnN结构的比较表明,MbnN的活性位点发生了变化,以容纳Mbn生物合成所需的更大,更疏水的底物。此外,我们已经证实,MbnN能够在体外和体内催化Mbn生物合成中的最终转氨步骤。我们还证明,如果不进行最终修饰,Mbn在生理条件下的稳定性会大大降低。对其他Mbn和Mbn操纵子的检查表明,该天然产物家族的N末端保护至关重要,而且Mbn亚家族已经独立发展了几种不同的N末端稳定方式。

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