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Pseudouridine modifications influence binding of aminoglycosides to helix 69 of bacterial ribosomes

机译:伪尿苷修饰影响氨基糖苷与细菌核糖体的螺旋69的结合

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摘要

Development of antibiotics that target new regions of functionality is a possible way to overcome antibiotic resistance. In this study, the interactions of aminoglycoside antibiotics with helix 69 of the E. coli 23S rRNA in the context of complete 70S ribosomes or the isolated 50S subunit were investigated by using chemical probing and footprinting analysis. Helix 69 is a dynamic RNA motif that plays major roles in bacterial ribosome activity. Neomycin, paromomycin, and gentamicin interact with the stem region of helix 69 in complete 70S ribosomes, but have diminished binding to the isolated 50S subunit. Pseudouridine modifications in helix 69 were shown to impact the aminoglycoside interactions. These results suggest a requirement for a specific conformational state of helix 69 for efficient aminoglycoside binding, and imply that this motif may be a suitable target for mechanism-based therapeutics.
机译:开发针对新功能区域的抗生素是克服抗生素耐药性的一种可能方法。在这项研究中,通过化学探测和足迹分析,研究了氨基糖苷类抗生素与大肠杆菌23S rRNA的螺旋69在完整的70S核糖体或分离的50S亚基中的相互作用。 Helix 69是一种动态RNA主题,在细菌核糖体活性中起主要作用。新霉素,巴龙霉素和庆大霉素与完整的70S核糖体中的螺旋69的茎区域相互作用,但与分离的50S亚基的结合减少。螺旋69中的假尿苷修饰被显示影响氨基糖苷相互作用。这些结果表明有效的氨基糖苷结合需要螺旋69的特定构象状态,并且暗示该基序可能是基于机制的治疗的合适靶标。

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  • 来源
    《Organic & biomolecular chemistry》 |2017年第40期|8535-8543|共9页
  • 作者单位

    Department of Chemistry, Wayne State University, Detroit, MI, United States;

    Department of Chemistry, Wayne State University, Detroit, MI, United States;

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  • 正文语种 eng
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