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核糖体结合的唑修饰肽 phazolicin 的结构解释了其对细菌翻译的抑制作用具有种属特异性的模式。

Structure of ribosome-bound azole-modified peptide phazolicin rationalizes its species-specific mode of bacterial translation inhibition.

机构信息

Center of Life Sciences, Skolkovo Institute of Science and Technology, Moscow, Russia.

Institute of Gene Biology, Russian Academy of Science, Moscow, Russia.

出版信息

Nat Commun. 2019 Oct 8;10(1):4563. doi: 10.1038/s41467-019-12589-5.

Abstract

Ribosome-synthesized post-translationally modified peptides (RiPPs) represent a rapidly expanding class of natural products with various biological activities. Linear azol(in)e-containing peptides (LAPs) comprise a subclass of RiPPs that display outstanding diversity of mechanisms of action while sharing common structural features. Here, we report the discovery of a new LAP biosynthetic gene cluster in the genome of Rhizobium Pop5, which encodes the precursor peptide and modification machinery of phazolicin (PHZ) - an extensively modified peptide exhibiting narrow-spectrum antibacterial activity against some symbiotic bacteria of leguminous plants. The cryo-EM structure of the Escherichia coli 70S-PHZ complex reveals that the drug interacts with the 23S rRNA and uL4/uL22 proteins and obstructs ribosomal exit tunnel in a way that is distinct from other compounds. We show that the uL4 loop sequence determines the species-specificity of antibiotic action. PHZ expands the known diversity of LAPs and may be used in the future as biocontrol agent for agricultural needs.

摘要

核糖体合成的翻译后修饰肽(RiPPs)是一类快速发展的天然产物,具有多种生物活性。线性含唑(in)肽(LAPs)是 RiPPs 的一个子类,它们具有不同的作用机制,同时具有共同的结构特征。在这里,我们在 Rhizobium Pop5 的基因组中发现了一个新的 LAP 生物合成基因簇,该基因簇编码了 phazolicin(PHZ)的前体肽和修饰机制 - 一种对一些豆科植物共生细菌具有窄谱抗菌活性的广泛修饰肽。Cryo-EM 结构的大肠杆菌 70S-PHZ 复合物表明,该药物与 23S rRNA 和 uL4/uL22 蛋白相互作用,并以不同于其他化合物的方式阻碍核糖体出口隧道。我们表明,uL4 环序列决定了抗生素作用的物种特异性。PHZ 扩展了已知的 LAP 多样性,将来可能被用作农业需求的生物防治剂。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4464/6783444/7071cad7f142/41467_2019_12589_Fig1_HTML.jpg

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