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首页> 外文期刊>Bioorganic and medicinal chemistry >Exploiting translational stalling peptides in an effort to extend azithromycin interaction within the prokaryotic ribosome nascent peptide exit tunnel
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Exploiting translational stalling peptides in an effort to extend azithromycin interaction within the prokaryotic ribosome nascent peptide exit tunnel

机译:利用翻译失速肽以扩大阿奇霉素在原核核糖体新生肽出口通道内的相互作用

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摘要

The ribosome is the primary protein synthesis machine in the cell and is a target for treatment of a variety of diseases including bacterial infection and cancer. The ribosomal peptide exit tunnel, the route of egress for the nascent peptide, is an inviting site for drug design. Toward a rational engagement of the nascent peptide components for the design of small molecule inhibitors of ribosome function, we designed and disclosed herein a set of N-10 indole functionalized azithromycin analogs. The indole moiety of these compounds is designed to mimic the translation stalling interaction of SecM W155 side-chain with the prokaryotic (Escherichia coli) ribosome A751 residue. Many of these N-10 functionalized compounds have enhanced translation inhibition activities against E. coli ribosome relative to azithromycin while a subset inhibited the growth of representative susceptible bacteria strains to about the same extent as azithromycin. Moreover, the inclusion of bovine serum in the bacterial growth media enhanced the anti-bacterial potency of the N-10 functionalized azithromycin analogs by as high as 10-fold. Published by Elsevier Ltd.
机译:核糖体是细胞中主要的蛋白质合成机器,是治疗包括细菌感染和癌症在内的多种疾病的靶标。核糖体肽出口通道是新生肽的出口途径,是药物设计的诱人场所。为了合理设计新生肽成分以设计核糖体功能的小分子抑制剂,我们在本文中设计并公开了一组N-10吲哚官能化的阿奇霉素类似物。这些化合物的吲哚部分被设计为模拟SecM W155侧链与原核(大肠杆菌)核糖体A751残基的翻译停滞相互作用。相对于阿奇霉素,许多这些N-10官能化化合物具有增强的针对大肠杆菌核糖体的翻译抑制活性,而其中一个子集抑制代表性易感细菌菌株的生长的程度与阿奇霉素大致相同。此外,在细菌生长培养基中加入牛血清可将N-10功能化的阿奇霉素类似物的抗菌能力提高多达10倍。由Elsevier Ltd.发布

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