Function and contribution of two putative Enterococcus faecalis glycosaminoglycan degrading enzymes to bacteremia and catheter-associated urinary tract infection.
Alexandra O JohnsonBraden M ShipmanBenjamin C HuntBrian S LearmanAimee L BrauerSerena P ZhouRachael Hageman BlairNicole J De NiscoChelsie E ArmbrusterPublished in: bioRxiv : the preprint server for biology (2024)
Enterococcus faecalis is a common cause of healthcare acquired bloodstream infections and catheter associated urinary tract infections (CAUTI) in both adults and children. Treatment of E. faecalis infection is frequently complicated by multi-drug resistance. Based on protein homology, E. faecalis encodes two putative hyaluronidases, EF3023 (HylA) and EF0818 (HylB). In other Gram-positive pathogens, hyaluronidases have been shown to contribute to tissue damage and immune evasion, but function in E. faecalis has yet to be explored. Here, we show that both hylA and hylB contribute to E. faecalis pathogenesis. In a CAUTI model, Δ hylA exhibited defects in bladder colonization and dissemination to the bloodstream, and Δ hylB exhibited a defect in kidney colonization. Furthermore, a Δ hylA Δ hylB double mutant exhibited a severe colonization defect in a model of bacteremia while the single mutants colonized to a similar level as the wild-type strain, suggesting potential functional redundancy within the bloodstream. We next examined enzymatic activity, and demonstrate that HylB is capable of digesting both HA and CS in vitro while HylA exhibits only a very modest activity against heparin. Importantly, HA degradation by HylB provided a modest increase in cell density during stationary phase and also contributed to dampening of LPS-mediated NF-Bκ activation. Overall, these data demonstrate that glycosaminoglycan degradation is important for E. faecalis pathogenesis in the urinary tract and during bloodstream infection.
Keyphrases
- urinary tract infection
- gram negative
- wild type
- multidrug resistant
- urinary tract
- healthcare
- oxidative stress
- klebsiella pneumoniae
- signaling pathway
- single cell
- inflammatory response
- lps induced
- machine learning
- young adults
- venous thromboembolism
- stem cells
- cell therapy
- risk assessment
- growth factor
- big data
- ultrasound guided
- mass spectrometry
- combination therapy
- binding protein
- human health
- escherichia coli
- bone marrow
- replacement therapy