首页> 美国卫生研究院文献>Journal of Bacteriology >The biosynthetic gene cluster for coronamic acid an ethylcyclopropyl amino acid contains genes homologous to amino acid-activating enzymes and thioesterases.
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The biosynthetic gene cluster for coronamic acid an ethylcyclopropyl amino acid contains genes homologous to amino acid-activating enzymes and thioesterases.

机译:冠氨酸(一种乙基环丙基氨基酸)的生物合成基因簇包含与氨基酸激活酶和硫酯酶同源的基​​因。

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摘要

Coronamic acid (CMA), an ethylcyclopropyl amino acid derived from isoleucine, functions as an intermediate in the biosynthesis of coronatine, a chlorosis-inducing phytotoxin produced by Pseudomonas syringae pv. glycinea PG4180. The DNA required for CMA biosynthesis (6.9 kb) was sequenced, revealing three distinct open reading frames (ORFs) which share a common orientation for transcription. The deduced amino acid sequence of a 2.7-kb ORF designated cmaA contained six core sequences and two conserved motifs which are present in a variety of amino acid-activating enzymes, including nonribosomal peptide synthetases. Furthermore, CmaA contained a spatial arrangement of histidine, aspartate, and arginine residues which are conserved in the ferrous active site of some nonheme iron(II) enzymes which catalyze oxidative cyclizations. The deduced amino acid sequence of a 1.2-kb ORF designated cmaT was related to thioesterases of both procaryotic and eucaryotic origins. These data suggest that CMA assembly is similar to the thiotemplate mechanism of nonribosomal peptide synthesis. No significant similarities between a 0.9-kb ORF designated cmaU and other database entries were found. The start sites of two transcripts required for CMA biosynthesis were identified in the present study. pRG960sd, a vector containing a promoterless glucuronidase gene, was used to localize and study the promoter regions upstream of the two transcripts. Data obtained in the present study indicate that CMA biosynthesis is regulated at the transcriptional level by temperature.
机译:冠状动脉酸(CMA),一种衍生自异亮氨酸的乙基环丙基氨基酸,在冠状动脉的生物合成中发挥着中间体的作用。冠状动脉是丁香假单胞菌PV产生的一种引起绿化的植物毒素。甘氨酸PG4180。对CMA生物合成所需的DNA(6.9 kb)进行了测序,揭示了三个不同的开放阅读框(ORF),它们具有共同的转录方向。推定为cmaA的2.7-kb ORF的推导氨基酸序列包含六个核心序列和两个保守基序,这些基序存在于多种氨基酸激活酶中,包括非核糖体肽合成酶。此外,CmaA包含组氨酸,天冬氨酸和精氨酸残基的空间排列,这些残基在催化氧化环化作用的某些非血红素铁(II)酶的亚铁活性位点保守。推定为cmaT的1.2-kb ORF的氨基酸序列与原核和真核来源的硫酯酶有关。这些数据表明,CMA组装与非核糖体肽合成的硫模板机制相似。在0.9kb ORF指定的cmaU与其他数据库条目之间未发现明显相似之处。在本研究中确定了CMA生物合成所需的两个转录本的起始位点。 pRG960sd,一种包含无启动子的葡萄糖醛酸酶基因的载体,用于定位和研究两个转录本上游的启动子区域。在本研究中获得的数据表明,CMA生物合成在转录水平受温度调节。

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