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硫肽类抗生素刺激枯草芽孢杆菌生物膜的形成。

Thiopeptide antibiotics stimulate biofilm formation in Bacillus subtilis.

作者信息

Bleich Rachel, Watrous Jeramie D, Dorrestein Pieter C, Bowers Albert A, Shank Elizabeth A

机构信息

Division of Chemical Biology and Medicinal Chemistry, School of Pharmacy, University of North Carolina, Chapel Hill, NC 27599;

Departments of Pharmacology and Chemistry and Biochemistry, University of California at San Diego, La Jolla, CA 92093; Skaggs School of Pharmacy and Pharmaceutical Sciences, University of California at San Diego, La Jolla, CA 92093;

出版信息

Proc Natl Acad Sci U S A. 2015 Mar 10;112(10):3086-91. doi: 10.1073/pnas.1414272112. Epub 2015 Feb 23.

Abstract

Bacteria have evolved the ability to produce a wide range of structurally complex natural products historically called "secondary" metabolites. Although some of these compounds have been identified as bacterial communication cues, more frequently natural products are scrutinized for antibiotic activities that are relevant to human health. However, there has been little regard for how these compounds might otherwise impact the physiology of neighboring microbes present in complex communities. Bacillus cereus secretes molecules that activate expression of biofilm genes in Bacillus subtilis. Here, we use imaging mass spectrometry to identify the thiocillins, a group of thiazolyl peptide antibiotics, as biofilm matrix-inducing compounds produced by B. cereus. We found that thiocillin increased the population of matrix-producing B. subtilis cells and that this activity could be abolished by multiple structural alterations. Importantly, a mutation that eliminated thiocillin's antibiotic activity did not affect its ability to induce biofilm gene expression in B. subtilis. We go on to show that biofilm induction appears to be a general phenomenon of multiple structurally diverse thiazolyl peptides and use this activity to confirm the presence of thiazolyl peptide gene clusters in other bacterial species. Our results indicate that the roles of secondary metabolites initially identified as antibiotics may have more complex effects--acting not only as killing agents, but also as specific modulators of microbial cellular phenotypes.

摘要

细菌已经进化出产生多种结构复杂的天然产物的能力,这些天然产物在历史上被称为“次级”代谢产物。尽管其中一些化合物已被确定为细菌通讯信号,但天然产物更常因其与人类健康相关的抗生素活性而受到仔细研究。然而,人们很少关注这些化合物可能会以其他方式影响复杂群落中相邻微生物的生理机能。蜡样芽孢杆菌分泌的分子可激活枯草芽孢杆菌中生物膜基因的表达。在此,我们使用成像质谱法鉴定出硫霉素,这是一类噻唑基肽抗生素,是蜡样芽孢杆菌产生的生物膜基质诱导化合物。我们发现硫霉素增加了产生基质的枯草芽孢杆菌细胞的数量,并且这种活性可以通过多种结构改变而消除。重要的是,消除硫霉素抗生素活性的突变并不影响其在枯草芽孢杆菌中诱导生物膜基因表达的能力。我们接着表明,生物膜诱导似乎是多种结构多样的噻唑基肽的普遍现象,并利用这种活性来确认其他细菌物种中噻唑基肽基因簇的存在。我们的结果表明,最初被鉴定为抗生素的次级代谢产物的作用可能具有更复杂的影响——不仅作为杀伤剂,还作为微生物细胞表型的特定调节剂。

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