A broadly distributed toxin family mediates contact-dependent antagonism between gram-positive bacteria.
John C WhitneyS Brook PetersonJungyun KimManuel PazosAdrian J VersterMatthew C RadeyHemantha D KulasekaraMary Q ChingNathan P BullenDiane BryantYoung Ah GooMichael G SuretteElhanan BorensteinWaldemar VollmerJoseph D MougousPublished in: eLife (2017)
The Firmicutes are a phylum of bacteria that dominate numerous polymicrobial habitats of importance to human health and industry. Although these communities are often densely colonized, a broadly distributed contact-dependent mechanism of interbacterial antagonism utilized by Firmicutes has not been elucidated. Here we show that proteins belonging to the LXG polymorphic toxin family present in Streptococcus intermedius mediate cell contact- and Esx secretion pathway-dependent growth inhibition of diverse Firmicute species. The structure of one such toxin revealed a previously unobserved protein fold that we demonstrate directs the degradation of a uniquely bacterial molecule required for cell wall biosynthesis, lipid II. Consistent with our functional data linking LXG toxins to interbacterial interactions in S. intermedius, we show that LXG genes are prevalent in the human gut microbiome, a polymicrobial community dominated by Firmicutes. We speculate that interbacterial antagonism mediated by LXG toxins plays a critical role in shaping Firmicute-rich bacterial communities.
Keyphrases
- cell wall
- escherichia coli
- human health
- risk assessment
- endothelial cells
- single cell
- healthcare
- climate change
- mental health
- cell therapy
- biofilm formation
- electronic health record
- gene expression
- candida albicans
- gram negative
- fatty acid
- multidrug resistant
- machine learning
- cystic fibrosis
- induced pluripotent stem cells
- small molecule
- transcription factor
- artificial intelligence
- pluripotent stem cells