首页> 美国卫生研究院文献>Antimicrobial Agents and Chemotherapy >Identification and Characterization of the Anti-Methicillin-Resistant Staphylococcus aureus WAP-8294A2 Biosynthetic Gene Cluster from Lysobacter enzymogenes OH11
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Identification and Characterization of the Anti-Methicillin-Resistant Staphylococcus aureus WAP-8294A2 Biosynthetic Gene Cluster from Lysobacter enzymogenes OH11

机译:耐溶杆菌酶金黄色葡萄球菌WAP-8294A2生物合成基因簇的鉴定与表征

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摘要

Lysobactor enzymogenes strain OH11 is an emerging biological control agent of fungal and bacterial diseases. We recently completed its genome sequence and found it contains a large number of gene clusters putatively responsible for the biosynthesis of nonribosomal peptides and polyketides, including the previously identified antifungal dihydromaltophilin (HSAF). One of the gene clusters contains two huge open reading frames, together encoding 12 modules of nonribosomal peptide synthetases (NRPS). Gene disruption of one of the NRPS led to the disappearance of a metabolite produced in the wild type and the elimination of its antibacterial activity. The metabolite and antibacterial activity were also affected by the disruption of some of the flanking genes. We subsequently isolated this metabolite and subjected it to spectroscopic analysis. The mass spectrometry and nuclear magnetic resonance data showed that its chemical structure is identical to WAP-8294A2, a cyclic lipodepsipeptide with potent anti-methicillin-resistant Staphylococcus aureus (MRSA) activity and currently in phase I/II clinical trials. The WAP-8294A2 biosynthetic genes had not been described previously. So far, the Gram-positive Streptomyces have been the primary source of anti-infectives. Lysobacter are Gram-negative soil/water bacteria that are genetically amendable and have not been well exploited. The WAP-8294A2 synthetase represents one of the largest NRPS complexes, consisting of 45 functional domains. The identification of these genes sets the foundation for the study of the WAP-8294A2 biosynthetic mechanism and opens the door for producing new anti-MRSA antibiotics through biosynthetic engineering in this new source of Lysobacter.
机译:溶菌酶酶原菌株OH11是真菌和细菌性疾病的新兴生物防治剂。我们最近完成了其基因组序列,发现其中包含大量基因簇,这些基因簇可能与非核糖体肽和聚酮化合物的生物合成有关,包括先前鉴定的抗真菌二氢麦芽糖蛋白(HSAF)。其中一个基因簇包含两个巨大的开放阅读框,它们一起编码12个模块的非核糖体肽合成酶(NRPS)。 NRPS之一的基因破坏导致野生型产生的代谢产物消失,并消除了其抗菌活性。代谢和抗菌活性也受到一些侧翼基因破坏的影响。我们随后分离了该代谢物,并对其进行了光谱分析。质谱和核磁共振数据表明,其化学​​结构与WAP-8294A2相同,WAP-8294A2是一种具有强抗甲氧西林抗性金黄色葡萄球菌(MRSA)活性的环状脂肽,目前处于I / II期临床试验。 WAP-8294A2生物合成基因以前没有描述过。迄今为止,革兰氏阳性链霉菌一直是抗感染药的主要来源。溶菌属革兰氏阴性土壤/水细菌,在遗传上可修正,尚未得到充分利用。 WAP-8294A2合成酶代表最大的NRPS复合物之一,由45个功能域组成。这些基因的鉴定为WAP-8294A2生物合成机制的研究奠定了基础,并为在这种新型溶菌来源中通过生物合成工程生产新的抗MRSA抗生素打开了大门。

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