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首页> 外文期刊>Nature Communications >Structural insights into catalytic mechanism and product delivery of cyanobacterial acyl-acyl carrier protein reductase
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Structural insights into catalytic mechanism and product delivery of cyanobacterial acyl-acyl carrier protein reductase

机译:催化机制的结构见解和蓝藻酰基 - 酰基载体蛋白还原酶的产物递送

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摘要

Long-chain alk(a/e)nes represent the major constituents of conventional transportation fuels. Biosynthesis of alkanes is ubiquitous in many kinds of organisms. Cyanobacteria possess two enzymes, acyl-acyl carrier protein (acyl-ACP) reductase (AAR) and aldehyde-deformylating oxygenase (ADO), which function in a two-step alkane biosynthesis pathway. These two enzymes act in series and possibly form a complex that efficiently converts long chain fatty acyl-ACP/fatty acyl-CoA into hydrocarbon. While the structure of ADO has been previously described, structures of both AAR and AAR-ADO complex have not been solved, preventing deeper understanding of this pathway. Here, we report a ligand-free AAR structure, and three AAR-ADO complex structures in which AARs bind various ligands. Our results reveal the binding pattern of AAR with its substrate/cofactor, and suggest a potential aldehyde-transferring channel from AAR to ADO. Based on our structural and biochemical data, we proposed a model for the complete catalytic cycle of AAR.
机译:长链ALK(A / E)NES代表常规运输燃料的主要成分。烷烃的生物合成在许多种生物中普遍存在。蓝藻具有两种酶,酰基 - 酰基载体蛋白(Acyl-ACP)还原酶(AAR)和醛 - 脱色氧化氧酶(ADO),其在两步烷烃生物合成途径中起作用。这两种酶串联起作用,并且可能形成复合物,可有效地将长链脂肪酰基-ACP /脂肪酰基-COA转化为烃。虽然先前已经描述了ADO的结构,但尚未解决AAR和AAR-ADO复合物的结构,防止对该途径的更深入了解。在这里,我们报告了一种无韧带的AAR结构,以及三种AAR-ADO复杂结构,其中AARS结合各种配体。我们的结果揭示了与其基材/辅因子的AAR的结合图案,并提出了从AAR到ADO的潜在醛转移渠道。基于我们的结构和生化数据,我们提出了AAR完全催化循环的模型。

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