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细菌素样肽类细菌素免疫机制的结构基础。

Structural Basis of the Immunity Mechanisms of Pediocin-like Bacteriocins.

机构信息

State Key Laboratory of Membrane Biology, Beijing Frontier Research Center for Biological Structure, Beijing Advanced Innovation Center for Structural Biology, School of Life Sciences, Tsinghua University, Beijing, P. R. China.

出版信息

Appl Environ Microbiol. 2022 Jul 12;88(13):e0048122. doi: 10.1128/aem.00481-22. Epub 2022 Jun 15.

Abstract

Pediocin-like bacteriocins, also designated class IIa bacteriocins, are ribosomally synthesized antimicrobial peptides targeting species closely related to the producers. They act on the cytoplasmic membrane of Gram-positive cells by dissipating the transmembrane electrical potential through pore formation with the mannose phosphotransferase system (man-PTS) as the target/receptor. Bacteriocin-producing strains also synthesize a cognate immunity protein that protects them against their own bacteriocins. Herein, we report the cryo-electron microscopy structure of the bacteriocin-receptor-immunity ternary complex from Lactobacillus sakei. The complex structure reveals that pediocin-like bacteriocins bind to the same position on the Core domain of man-PTS, while the C-terminal helical tails of bacteriocins delimit the opening range of the Core domain away from the Vmotif domain to facilitate transmembrane pore formation. Upon attack of bacteriocins from the extracellular side, man-PTS exposes its cytosolic side for recognition of the N-terminal four-helix bundle of the immunity protein. The C-terminal loop of the immunity protein then inserts into the pore and blocks leakage induced by bacteriocins. Elucidation of the toxicity and immunity mechanisms of pediocin-like bacteriocins could support the design of novel bacteriocins against antibiotic-resistant pathogenic bacteria. Pediocin-like bacteriocins, ribosomally synthesized antimicrobial peptides, are generally co-expressed with cognate immunity proteins to protect the bacteriocin-producing strain from its own bacteriocin. Bacteriocins are considered potential alternatives to conventional antibiotics in the context of the bacterial resistance crisis, but the immunity mechanism is unclear. This study uncovered the mechanisms of action and immunity of class IIa bacteriocins.

摘要

类肠肮菌素细菌素,也称为 IIa 类细菌素,是一类核糖体合成的抗菌肽,针对与产生菌密切相关的物种发挥作用。它们通过在细胞质膜上形成孔来破坏跨膜电势,从而作用于革兰氏阳性细胞,其中甘露糖磷酸转移酶系统 (man-PTS) 是靶标/受体。产生细菌素的菌株还合成一种同源免疫蛋白,以保护它们免受自身细菌素的侵害。在此,我们报告了从清酒乳杆菌中获得的细菌素-受体-免疫三元复合物的冷冻电子显微镜结构。该复合物结构揭示了类肠肮菌素细菌素结合到 man-PTS 的 Core 结构域的相同位置,而细菌素的 C 端螺旋尾巴限定了 Core 结构域远离 Vmotif 结构域的开口范围,以促进跨膜孔的形成。当来自细胞外的细菌素攻击时,man-PTS 暴露其胞质侧,以便识别免疫蛋白的 N 端四螺旋束。然后,免疫蛋白的 C 端环插入孔中,并阻止细菌素引起的渗漏。阐明类肠肮菌素细菌素的毒性和免疫机制可以支持设计针对抗药性病原菌的新型细菌素。

类肠肮菌素细菌素是一类核糖体合成的抗菌肽,通常与同源免疫蛋白共同表达,以保护产生菌免受自身细菌素的侵害。在细菌耐药性危机的背景下,细菌素被认为是传统抗生素的潜在替代品,但免疫机制尚不清楚。本研究揭示了 IIa 类细菌素的作用机制和免疫机制。

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Structural Basis of the Immunity Mechanisms of Pediocin-like Bacteriocins.细菌素样肽类细菌素免疫机制的结构基础。
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