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Additional Role of Nicotinic Acid Hydroxylase for the Transformation of 3-Succinoyl-Pyridine by Pseudomonas sp. Strain JY-Q

机译:烟碱酸羟化酶通过假鼠SP的3-琥珀酰吡啶转化的额外作用。 菌株JY-Q

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Nicotine and nicotinic acid (NA) are both considered to be representatives of N -heterocyclic aromatic compounds, and their degradation pathways have been revealed in Pseudomonas species. However, the cooccurrence of these two pathways has only been observed in Pseudomonas sp. strain JY-Q. The nicotine pyrrolidine catabolism pathway of strain JY-Q consists of the functional modules Nic1, Spm, and Nic2. The module enzyme, 3-succinoylpyridine monooxygenase (Spm), catalyzes transformation of 3-succinoyl-pyridine (SP) to 6-hydroxy-3-succinoyl-pyridine (HSP). There exist two homologous but not identical Spm enzymes (namely, Spm1 and Spm2) in JY-Q. However, when spm1 and spm2 were both in-frame deleted, the mutant still grew well in basic salt medium (BSM) supplemented with nicotine as the sole carbon/nitrogen nutrition, suggesting that there exists an alternative pathway responsible for SP catabolism in JY-Q. NicAB, an enzyme accounting for NA hydroxylation, contains reorganized domains similar to those of Spm. When the JY-Q_ nicAB gene ( nicAB in strain JY-Q) was introduced into another Pseudomonas strain, one that is unable to degrade NA, the resultant recombinant strain exhibited the ability to transform SP to HSP, but without the ability to metabolize NA. Here, we conclude that NicAB in strain JY-Q exhibits an additional role in SP transformation. The other genes in the NA cluster, NicXDFE (Nic2 homolog), then also exhibit a role in subsequent HSP metabolism for energy yield. This finding also suggests that the cooccurrence of nicotine and NA degradation genes in strain JY-Q represents an advantage for JY-Q, making it more effective and flexible for the degradation of nicotine.IMPORTANCE 3-Succinoyl-pyridine (SP) and 6-hydroxy-3-succinoyl-pyridine (HSP) are both valuable chemical precursors to produce insecticides and hypotensive agents. SP and HSP could be renewable through the nicotine microbial degradation pathway, in which 3-succinoylpyridine monooxygenases (Spm) account for transforming SP into HSP in Pseudomonas sp. strain JY-Q. However, when two homologous Spm genes ( spm1 and spm2 ) were knocked out, the mutant retained the ability to degrade nicotine. Thus, in addition to Spm, JY-Q should have an alternative pathway for SP conversion. In this research, we showed that JY-Q_NicAB was responsible for this alternative SP conversion. Both of the primary functions for nicotinic acid dehydrogenation and the additional function for SP metabolism were detected in a recombinant strain harboring JY-Q_NicAB. As a result, both nicotinic acid and nicotine degradation pathways in JY-Q contribute to its remarkable nicotine tolerance and nicotine degradation availability. These findings also provide one more metabolic engineering strategy for accumulation for value-added intermediates.
机译:尼古丁和烟酸(Na)被认为是N-丙酰芳族芳族化合物的代表,并且它们在假单胞菌种类中揭示了它们的降解途径。然而,在Pseudomonas SP中才观察到这两种途径的共同电流。菌株JY-Q。菌株JY-Q的尼古丁吡咯烷分解代谢途径由功能模块NIC1,SPM和NIC2组成。模块酶,3-琥珀酰吡啶单氧化酶(SPM),催化3-琥珀酰吡啶(SP)转化为6-羟基-3-琥珀酰吡啶(HSP)。在JY-Q中存在两种同源但不是相同的SPM酶(即SPM1和SPM2)。然而,当SPM1和SPM2均缺失时,突变体仍然很好地在补充有尼古丁作为唯一碳/氮营养的碱性盐培养基(BSM)中,这表明存在替代途径,其负责SP分解代谢在JY中问: Nicab是Na羟基化的酶核算,含有与SPM类似的重组结构域。当将JY-Q_NICAB基因(NiCAB在菌株JY-Q)中引入另一个假单胞菌菌株时,不能降解NA的一种,所得的重组菌株表现出转化SP至HSP的能力,但没有代谢NA的能力。在这里,我们得出结论,乳腺菌株JY-Q在SP变换中表现出额外的作用。 NICXDFE(NIC2同源物)中的其他基因,然后在随后的HSP代谢中表现出用于能量产率的作用。该发现还表明,烟碱和Na降解基因在菌株JY-Q中的结合代表了JY-Q的优势,使尼古丁的降解更有效和灵活。分析3-琥珀酰基 - 吡啶(SP)和6-羟基-3-琥珀酰吡啶(HSP)都是有价值的化学前体,用于生产杀虫剂和低血压剂。可以通过尼古丁微生物降解途径可再生SP和HSP,其中3-琥珀酰吡啶单氧基酶(SPM)在假单胞菌SP中将SP转化为HSP。菌株JY-Q。然而,当敲除两种同源SPM基因(SPM1和SPM2)时,突变体保留降解尼古丁的能力。因此,除了SPM之外,JY-Q还应具有SP转换的替代路径。在这项研究中,我们表明,JY-Q_NICAB是对这种替代的SP转换负责。在储存JY-Q_NICAB的重组菌株中检测到烟酸脱氢的主要功能和SP代谢的附加功能。结果,JY-Q中的烟酸和尼古丁降解途径均有助于其显着的尼古丁耐受性和尼古丁降解可用性。这些调查结果还提供了一种用于积累增值中间体的一种代谢工程战略。

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