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首页> 外文期刊>Journal of bacteriology >Elongation Factor Tu3 (EF-Tu3) from the Kirromycin Producer Streptomyces ramocissimus Is Resistant to Three Classes of EF-Tu-Specific Inhibitors
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Elongation Factor Tu3 (EF-Tu3) from the Kirromycin Producer Streptomyces ramocissimus Is Resistant to Three Classes of EF-Tu-Specific Inhibitors

机译:来自基罗霉素生产商链霉菌的延伸因子Tu3(EF-Tu3)对三类EF-Tu特异性抑制剂有抵抗力

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摘要

The antibiotic kirromycin inhibits prokaryotic protein synthesis by immobilizing elongation factor Tu (EF-Tu) on the elongating ribosome. Streptomyces ramocissimus, the producer of kirromycin, contains three tuf genes. While tuf1 and tuf2 encode kirromycin-sensitive EF-Tu species, the function of tuf3 is unknown. Here we demonstrate that EF-Tu3, in contrast to EF-Tu1 and EF-Tu2, is resistant to three classes of EF-Tu-targeted antibiotics: kirromycin, pulvomycin, and GE2270A. A mixture of EF-Tu1 and EF-Tu3 was sensitive to kirromycin and resistant to GE2270A, in agreement with the described modes of action of these antibiotics. Transcription of tuf3 was observed during exponential growth and ceased upon entry into stationary phase and therefore did not correlate with the appearance of kirromycin in stationary phase; thus, it is unlikely that EF-Tu3 functions as a resistant alternative for EF-Tu1. EF-Tu3 from Streptomyces coelicolor A3(2) was also resistant to kirromycin and GE2270A, suggesting that multiple antibiotic resistance is an intrinsic feature of EF-Tu3 species. The GE2270A-resistant character of EF-Tu3 demonstrated that this divergent elongation factor is capable of substituting for EF-Tu1 in vivo.
机译:抗生素奇霉素通过将伸长因子Tu(EF-Tu)固定在伸长的核糖体上来抑制原核蛋白的合成。奇异霉素的生产者 rameptossimus ,包含三个 tuf 基因。虽然 tuf1 tuf2 编码对奇霉素敏感的EF-Tu物种,但 tuf3 的功能尚不清楚。在这里,我们证明与EF-Tu1和EF-Tu2相比,EF-Tu3对以EF-Tu为靶标的三类抗生素具有耐药性:奇霉素,普尔霉素和GE2270A。 EF-Tu1和EF-Tu3的混合物对奇异霉素敏感,对GE2270A具有耐药性,与这些抗生素的作用方式一致。在指数生长过程中观察到 tuf3 的转录,并在进入固定相时停止转录,因此与固定相中奇罗霉素的出现无关。因此,EF-Tu3不太可能充当EF-Tu1的抗性替代品。 Streptomyces coelicolor A3(2)的EF-Tu3也对奇罗霉素和GE2270A具有抗性,这表明多种抗生素抗性是EF-Tu3种的固有特征。 EF-Tu3的GE2270A耐药特性表明,这种不同的延伸因子能够在体内替代EF-Tu1。

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