| Literature DB >> 31901519 |
Franz G Zingl1, Paul Kohl1, Fatih Cakar1, Deborah R Leitner1, Fabian Mitterer1, Katherine E Bonnington2, Gerald N Rechberger3, Meta J Kuehn2, Ziqiang Guan4, Joachim Reidl5, Stefan Schild6.
Abstract
Gram-negative bacteria release outer membrane vesicles into the external milieu to deliver effector molecules that alter the host and facilitate virulence. Vesicle formation is driven by phospholipid accumulation in the outer membrane and regulated by the phospholipid transporter VacJ/Yrb. We use the facultative human pathogen Vibrio cholerae to show that VacJ/Yrb is silenced early during mammalian infection, which stimulates vesiculation that expedites bacterial surface exchange and adaptation to the host environment. Hypervesiculating strains rapidly alter their bacterial membrane composition and exhibit enhanced intestinal colonization fitness. This adaptation is exemplified by faster accumulation of glycine-modified lipopolysaccharide (LPS) and depletion of outer membrane porin OmpT, which confers resistance to host-derived antimicrobial peptides and bile, respectively. The competitive advantage of hypervesiculation is lost upon pre-adaptation to bile and antimicrobial peptides, indicating the importance of these adaptive processes. Thus, bacteria use outer membrane vesiculation to exchange cell surface components, thereby increasing survival during mammalian infection.Entities:
Keywords: Alm pathway; Mla pathway; OMV; OmpT; OmpU; antimicrobial peptides; bile; glycination; lipid A; porin
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Year: 2019 PMID: 31901519 PMCID: PMC7155939 DOI: 10.1016/j.chom.2019.12.002
Source DB: PubMed Journal: Cell Host Microbe ISSN: 1931-3128 Impact factor: 21.023