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Infect. Immun., May 1995, 1906-1913, Vol 63, No. 5
FH Azmi, AH Lucas, HL Spiegelberg and DM Granoff
Three hundred fifty-nine serum samples from patients with immunoglobulin M
(IgM) or IgG monoclonal gammopathies were tested for binding to the
capsular polysaccharide (PS) of Neisseria meningitidis group B (MenB PS,
poly-alpha[2-->8]-N-acetylneuraminic acid). Of 159 IgM paraproteins, 7
(4.4%) were positive, compared with 0 of 200 IgG paraproteins (P <
0.05). Since MenB PS reactivity was limited to the IgM paraproteins, the
159 IgM paraproteins were tested by enzyme-linked immunosorbent assay
(ELISA) for reactivity with seven other bacterial PSs. None reacted with
meningococcal A or C, Haemophilus influenzae type b, or Streptococcus
pneumoniae type 3, 6, 14, or 23 PS. The specificity of the MenB PS-reactive
antibodies was confirmed by demonstration of binding to N. meningitidis
group B cells but not to a capsular PS-deficient mutant and by specific
inhibition of binding to solid-phase MenB PS by soluble MenB PS in an
ELISA. Five of five antibodies tested protected infant rats from bacteremia
caused by Escherichia coli K1, an organism with a PS capsule that also is
composed of poly-alpha[2-->8]-N-acetylneuraminic acid. Each of the seven
MenB PS-reactive paraproteins had autoantibody activity as defined by
binding to homogenates of calf brain in a radioimmunoassay. For six of the
seven antibodies, binding to calf brain was inhibited by the addition of
soluble MenB PS. Thus, approximately 4% of human IgM paraproteins have
autoantibody activity to poly-alpha[2-->8]-N- acetylneuraminic acid, an
antigen expressed in fetal brain and cross- reactive with the MenB capsular
PS. The reason for this skewing of the IgM paraprotein repertoire toward
reactivity with poly-alpha[2-->8]-N- acetylneuraminic acid antigenic
determinants is unknown.
Copyright © 1995, American Society for Microbiology
Human immunoglobulin M paraproteins cross-reactive with Neisseria meningitidis group B polysaccharide and fetal brain
Children's Hospital Oakland Research Institute, CA 94609, USA.
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