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. 2019 Jun 13;21(11):e13063. doi: 10.1111/cmi.13063

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© 2019 The Authors Cellular Microbiology Published by John Wiley & Sons Ltd

This is an open access article under the terms of the http://creativecommons.org/licenses/by/4.0/ License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.

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Neisseria meningitidis, a commensal and pathogenic bacterium. A. N. meningitidis grow in the mucus in nasopharynx where it encounters a poor nutritive medium and a rich microbiota. Meningococci survive by expressing capsule, LOS, the MtrCDE efflux pump, and factors that capture nutrients. N. meningitidis also express two families of polymorphic toxins: MafB and CdiA. A1 depicts the domain organisation found in CdiA and MafB polymorphic toxins constituted by a conserved N‐terminal domain (blue boxes) apposed to a toxic domain in the variable C‐terminal region (green boxes). Many toxic activities have been reported for toxic domains (Zhang et al., 2012). SP, signal peptide; Hemag activity, hemagglutination activity domain, also called a “TPS domain” (PF05860); fil hemag repeats, filamentous hemagglutinin repeats (PF13332); PT‐VENN, pre‐toxin domain with a VENN motif; DUF1020, domain of unknown function 1020. A2: Simplified genomic organisations of maf and cdi loci. Full‐length toxin genes cdiA and mafB are depicted in blue with their extremity encoding the toxic activity depicted in green. Genes encoding immunity proteins are depicted in red (cdiI and mafI). Open Reading Frame (ORF) encoding alternative C‐terminal toxic domains of CdiA and MafB are depicted in green surrounded with dotted lines. cdiB encodes the dedicated transporter of CdiA toxin, whereas the role of mafA in MafB secretion is unknown. Black boxes indicate regions potentially involved in recombination. Left panel: aggregates harvested from the biomass covering a monolayer of FaDu cells infected by the meningococcal Z5463 strain (Bille et al., 2017) and labelled by the anti‐MDA polyclonal antibody coupled to 8 nm‐diameter gold particles. Representative picture of meningococcal MDAΦ phage‐dependant aggregates. Bar: 1 μm. B. For an unknown reason, meningococci cross the epithelial layer and enter the bloodstream where bacteria adhere to the vascular wall. Adhesive bacteria proliferate and induce an active signalling that leads to better adhesion and opening of the vascular barrier, vessel leakage, and massive thrombosis