Neisseria gonorrhoeae and Neisseria meningitidis have evolved intricate mechanisms to evade complement-mediated killing. Sialylation of gonococcal lipooligosaccharide (LOS) results in conversion of previously serum sensitive strains to unstable serum resistance, which is mediated by factor H binding. Porin (Por) is also instrumental in mediating stable serum resistance in gonococci. The 5th loop of certain gonococcal PorlAs binds factor H, which efficiently inactivates C3b to iC3b. Factor H glycan residues may be essential for factor H binding to certain Por1A strains. Por1A strains can also regulate the classical pathway by binding to C4b-binding protein (C4bp) probably via the 1st loop of the Por molecule. Certain serum resistant Por1 B strains can also regulate complement by binding C4bp through a loop other than loop 1. Purified C4b can inhibit binding of C4bp to Por 1B, but not Por1A, suggesting different binding sites on C4bp for the two Por types. Unlike serum resistant gonococci, resistant meningococci have abundant C3b on their surface, which is only partially processed to iC3b. The main mechanism of complement evasion by group B meningococci is inhibition of membrane attack complex (MAC) insertion by their polysaccharide capsule. LOS structure may act in concert with capsule to prevent MAC insertion. Meningococcal strains with Class 3 Por preferentially bind factor H, suggesting Class 3 Por acts as a receptor for factor H.
%0 Journal Article
%1 ram_contrasting_1999
%A Ram, S
%A Mackinnon, F G
%A Gulati, S
%A McQuillen, D P
%A Vogel, U
%A Frosch, M
%A Elkins, C
%A Guttormsen, H K
%A Wetzler, L M
%A Oppermann, M
%A Pangburn, M K
%A Rice, P A
%D 1999
%J Molecular Immunology
%K Activity, Bactericidal Blood Complement Humans, Lipopolysaccharides, Neisseria Porins, Proteins, Species Specificity System gonorrhoeae, meningitidis,
%N 13-14
%P 915--928
%T The contrasting mechanisms of serum resistance of Neisseria gonorrhoeae and group B Neisseria meningitidis
%U http://www.ncbi.nlm.nih.gov/pubmed/10698346
%V 36
%X Neisseria gonorrhoeae and Neisseria meningitidis have evolved intricate mechanisms to evade complement-mediated killing. Sialylation of gonococcal lipooligosaccharide (LOS) results in conversion of previously serum sensitive strains to unstable serum resistance, which is mediated by factor H binding. Porin (Por) is also instrumental in mediating stable serum resistance in gonococci. The 5th loop of certain gonococcal PorlAs binds factor H, which efficiently inactivates C3b to iC3b. Factor H glycan residues may be essential for factor H binding to certain Por1A strains. Por1A strains can also regulate the classical pathway by binding to C4b-binding protein (C4bp) probably via the 1st loop of the Por molecule. Certain serum resistant Por1 B strains can also regulate complement by binding C4bp through a loop other than loop 1. Purified C4b can inhibit binding of C4bp to Por 1B, but not Por1A, suggesting different binding sites on C4bp for the two Por types. Unlike serum resistant gonococci, resistant meningococci have abundant C3b on their surface, which is only partially processed to iC3b. The main mechanism of complement evasion by group B meningococci is inhibition of membrane attack complex (MAC) insertion by their polysaccharide capsule. LOS structure may act in concert with capsule to prevent MAC insertion. Meningococcal strains with Class 3 Por preferentially bind factor H, suggesting Class 3 Por acts as a receptor for factor H.
@article{ram_contrasting_1999,
abstract = {Neisseria gonorrhoeae and Neisseria meningitidis have evolved intricate mechanisms to evade complement-mediated killing. Sialylation of gonococcal lipooligosaccharide {(LOS)} results in conversion of previously serum sensitive strains to unstable serum resistance, which is mediated by factor H binding. Porin {(Por)} is also instrumental in mediating stable serum resistance in gonococci. The 5th loop of certain gonococcal {PorlAs} binds factor H, which efficiently inactivates C3b to {iC3b.} Factor H glycan residues may be essential for factor H binding to certain {Por1A} strains. {Por1A} strains can also regulate the classical pathway by binding to C4b-binding protein {(C4bp)} probably via the 1st loop of the Por molecule. Certain serum resistant Por1 B strains can also regulate complement by binding C4bp through a loop other than loop 1. Purified C4b can inhibit binding of C4bp to Por {1B}, but not {Por1A}, suggesting different binding sites on C4bp for the two Por types. Unlike serum resistant gonococci, resistant meningococci have abundant C3b on their surface, which is only partially processed to {iC3b.} The main mechanism of complement evasion by group B meningococci is inhibition of membrane attack complex {(MAC)} insertion by their polysaccharide capsule. {LOS} structure may act in concert with capsule to prevent {MAC} insertion. Meningococcal strains with Class 3 Por preferentially bind factor H, suggesting Class 3 Por acts as a receptor for factor H.},
added-at = {2011-06-24T11:21:47.000+0200},
author = {Ram, S and Mackinnon, F G and Gulati, S and {McQuillen}, D P and Vogel, U and Frosch, M and Elkins, C and Guttormsen, H K and Wetzler, L M and Oppermann, M and Pangburn, M K and Rice, P A},
biburl = {https://www.bibsonomy.org/bibtex/2cd1c4cce26d900ef64ba85d7b554c811/ag_vogel},
interhash = {4b67db2fd78dd11f00096d5f8fbc9136},
intrahash = {cd1c4cce26d900ef64ba85d7b554c811},
issn = {0161-5890},
journal = {Molecular Immunology},
keywords = {Activity, Bactericidal Blood Complement Humans, Lipopolysaccharides, Neisseria Porins, Proteins, Species Specificity System gonorrhoeae, meningitidis,},
month = oct,
note = {{PMID:} 10698346},
number = {13-14},
pages = {915--928},
timestamp = {2011-06-24T11:21:54.000+0200},
title = {The contrasting mechanisms of serum resistance of Neisseria gonorrhoeae and group B Neisseria meningitidis},
url = {http://www.ncbi.nlm.nih.gov/pubmed/10698346},
volume = 36,
year = 1999
}