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首页> 外文期刊>Bioengineered >Engineering of N-acetylglucosamine metabolism for improved antibiotic production in Streptomyces coelicolor A3(2) and an unsuspected role of NagA in glucosamine metabolism
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Engineering of N-acetylglucosamine metabolism for improved antibiotic production in Streptomyces coelicolor A3(2) and an unsuspected role of NagA in glucosamine metabolism

机译:N-乙酰氨基葡萄糖代谢的工程,以改善链霉菌A3(2)中的抗生素生产,以及NagA在氨基葡萄糖代谢中的作用毋庸置疑

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N -acetylglucosamine (GlcNAc), the monomer of chitin and constituent of bacterial peptidoglycan, is a preferred carbon and nitrogen source for streptomycetes. Recent studies have revealed new functions of GlcNAc in nutrient signaling of bacteria. Exposure to GlcNAc activates development and antibiotic production of Streptomyces coelicolor under poor growth conditions (famine) and blocks these processes under rich conditions (feast). Glucosamine-6-phosphate (GlcN-6P) is a key molecule in this signaling pathway and acts as an allosteric effector of a pleiotropic transcriptional repressor DasR, the regulon of which includes the GlcNAc metabolic enzymes N -actetylglucosamine-6-phosphate (GlcNAc-6P) deacetylase (NagA) and GlcN-6P deaminase (NagB). Intracellular accumulation of GlcNAc-6P and GlcN-6P enhanced production of the pigmented antibiotic actinorhodin. When the nag B mutant was challenged with GlcNAc or GlcN, spontaneous second-site mutations that relieved the toxicity of the accumulated sugar phosphates were obtained. Surprisingly, deletion of nagA also relieved toxicity of GlcN, indicating novel linkage between the GlcN and GlcNAc utilization pathways. The strongly enhanced antibiotic production observed for many suppressor mutants shows the potential of the modulation of GlcNAc and GlcN metabolism as a metabolic engineering tool toward the improvement of antibiotic productivity or even the discovery of novel compounds.
机译:N-乙酰氨基葡糖(GlcNAc)是几丁质的单体和细菌肽聚糖的成分,是链霉菌的优选碳和氮源。最近的研究揭示了GlcNAc在细菌营养信号传递中的新功能。在不良生长条件下(饥荒),暴露于GlcNAc会激活天蓝色链霉菌的发育和抗生素生产,而在富营养条件下(盛宴)会阻止这些过程。氨基葡萄糖-6-磷酸酯(GlcN-6P)是该信号传导途径中的关键分子,并作为多效转录抑制因子DasR的变构效应物,其调节子包括GlcNAc代谢酶N-乙酰基葡糖胺-6-磷酸酯。 (GlcNAc-6P)脱乙酰酶(NagA)和GlcN-6P脱氨酶(NagB)。 GlcNAc-6P和GlcN-6P在细胞内的积累增强了有色抗生素放线菌丝蛋白的产生。当nag B突变体用GlcNAc或GlcN攻击时,获得了自发的第二位点突变,其减轻了积累的糖磷酸酯的毒性。令人惊讶地,nagA的缺失也减轻了GlcN的毒性,表明GlcN和GlcNAc利用途径之间存在新的联系。在许多抑制突变体中观察到的抗生素产生的强烈增强显示出调节GlcNAc和GlcN代谢作为代谢工程工具的潜力,从而可以提高抗生素的生产率甚至发现新的化合物。

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