The basis of antigenic operon fragmentation in Bacteroidota and commensalism.
Nicholas C BankVaidhvi SinghBrandon GrubbBlake McCourtAaron BurberryKyle D RobertsAlex Rodriguez-PalaciosPublished in: bioRxiv : the preprint server for biology (2023)
The causes for variability of pro-inflammatory surface antigens that affect gut commensal/opportunistic dualism within the phylum Bacteroidota remain unclear (1, 2). Using the classical lipopolysaccharide/O-antigen ' rfb operon' in Enterobacteriaceae as a surface antigen model (5-gene-cluster rfbABCDX ), and a recent rfbA- typing strategy for strain classification (3), we characterized the architecture/conservancy of the entire rfb operon in Bacteroidota . Analyzing complete genomes, we discovered that most Bacteroidota have the rfb operon fragmented into non-random gene-singlets and/or doublets/triplets, termed 'minioperons'. To reflect global operon integrity, duplication, and fragmentation principles, we propose a five-category (infra/supernumerary) cataloguing system and a Global Operon Profiling System for bacteria. Mechanistically, genomic sequence analyses revealed that operon fragmentation is driven by intra-operon insertions of predominantly Bacteroides -DNA ( thetaiotaomicron/fragilis ) and likely natural selection in specific micro-niches. Bacteroides -insertions, also detected in other antigenic operons (fimbriae), but not in operons deemed essential (ribosomal), could explain why Bacteroidota have fewer KEGG-pathways despite large genomes (4). DNA insertions overrepresenting DNA-exchange-avid species, impact functional metagenomics by inflating gene-based pathway inference and overestimating 'extra-species' abundance. Using bacteria from inflammatory gut-wall cavernous micro-tracts (CavFT) in Crohn's Disease (5), we illustrate that bacteria with supernumerary-fragmented operons cannot produce O-antigen, and that commensal/CavFT Bacteroidota stimulate macrophages with lower potency than Enterobacteriaceae , and do not induce peritonitis in mice. The impact of 'foreign-DNA' insertions on pro-inflammatory operons, metagenomics, and commensalism offers potential for novel diagnostics and therapeutics.
Keyphrases
- circulating tumor
- cell free
- copy number
- single molecule
- genome wide
- multidrug resistant
- pseudomonas aeruginosa
- single cell
- machine learning
- type diabetes
- inflammatory response
- oxidative stress
- gene expression
- escherichia coli
- immune response
- dna methylation
- small molecule
- klebsiella pneumoniae
- climate change
- adipose tissue
- insulin resistance
- circulating tumor cells
- metabolic syndrome