Binding properties and anti-bacterial activities of V-region identical, human IgG and IgM antibodies, against group B Neisseria meningitidis

Michaelsen, T. E.; Ihle, Øistein; Beckstrøm, Karen Johanne; Herstad, Tove Karin; Sandin, Randi; Kolberg, Jan; Aase, Audun

doi:10.1042/bst0311032

Cited by 14 publications

(13 citation statements)

References 25 publications

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“…At low complement concentrations (Ͻ10%) activation of complement occurs mainly through the classical pathway (59). However, previous studies comparing monoclonal IgG and IgM antibodies against meningococcal surface PorA protein revealed IgM to be more active than IgG in OPA under conditions similar to those used in the present study (29,30). Also, when different concentrations of complement serum were tested with a human monoclonal IgM anti-P1.…”

Section: Discussionmentioning

confidence: 97%

Protection by Natural Human Immunoglobulin M Antibody to Meningococcal Serogroup B Capsular Polysaccharide in the Infant Rat Protection Assay Is Independent of Complement-Mediated Bacterial Lysis

et al. 2005

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Neisseria meningitidis, an important cause of bacterial meningitis and septicemia worldwide, is associated with high mortality and serious sequelae. Natural immunity against meningococcal disease develops with age, but the specificity and functional activity of natural antibodies associated with protection are poorly understood. We addressed this question by using a selected subset of prevaccination sera (n ‫؍‬ 26) with convergent or discrepant serum bactericidal activity (SBA) and infant rat protective activity (

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Section: Discussionmentioning

confidence: 97%

Protection by Natural Human Immunoglobulin M Antibody to Meningococcal Serogroup B Capsular Polysaccharide in the Infant Rat Protection Assay Is Independent of Complement-Mediated Bacterial Lysis

et al. 2005

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“…Thus, a conformational change in this loop may affect the relative orientation of the CH1 domain versus the Fc, thereby influencing effector binding to the Fc. There are now many examples of Abs with identical variable domains but different isotypes that bind the same Ag with a different affinity or specificity (13,(15)(16)(17)(18)(19)(20)(21)(22)(23)(24). Some of these studies suggested that the CH1 domain accounts for the observed changes in binding, because it was identified as the only region with sequence diversity between the tested Abs and because a similar effect was observed using only the Fab instead of the entire Ab scaffold (13,16,19).…”

Section: Discussionmentioning

confidence: 99%

“…However, recent reports provide some evidence for binding-related allosteric effects in Abs. It was demonstrated that Ag binding, as well as the structure of the variable domains, may be influenced by changes in the constant domains (11)(12)(13)(14)(15)(16)(17)(18)(19)(20)(21)(22)(23)(24). For example, Pritsch et al (13) demonstrated that two human mAbs sharing identical variable domains, but expressing different isotypes, bind tubulin with significantly different affinities.…”

mentioning

confidence: 99%

A Systematic Comparison of Free and Bound Antibodies Reveals Binding-Related Conformational Changes

Sela-Culang

Alon

Ofran

2012

The Journal of Immunology

104

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To study structural changes that occur in Abs upon Ag binding, we systematically compared free and bound structures of all 141 crystal structures of the 49 Abs that were solved in these two forms. We found that many structural changes occur far from the Ag binding site. Some of them may constitute a mechanism for the recently suggested allosteric effects in Abs. Within the binding site itself, CDR-H3 is the only element that shows significant binding-related conformational changes; however, this occurs in only one third of the Abs. Beyond the binding site, Ag binding is associated with changes in the relative orientation of the H and L chains in both the variable and constant domains. An even larger change occurs in the elbow angle between the variable and the constant domains, and it is significantly larger for binding of big Ags than for binding of small ones. The most consistent and substantial conformational changes occur in a loop in the H chain constant domain. This loop is implicated in the interaction between the H and L chains, is often intrinsically disordered, and is involved in complement binding. Hence, we suggest that it may have a role in Ab function. These findings provide structural insight into the recently proposed allosteric effects in Abs.

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“…In one study, all three IgG1 anti-PorA MAbs tested had superior bactericidal activity to the respective IgG3 MAbs (28), while in the second study an IgG1 anti-PorA MAb had similar or better activity than the IgG3 MAb (37). The second study also investigated the activity of a chimeric IgG2 anti-PorA MAb, which had less activity than the IgG1 or IgG3 MAbs, while the IgG4 MAb with identical respective V region genes had no activity.…”

Section: Discussionmentioning

confidence: 99%

Combined Roles of Human IgG Subclass, Alternative Complement Pathway Activation, and Epitope Density in the Bactericidal Activity of Antibodies to Meningococcal Factor H Binding Protein

Giuntini¹,

Reason²,

Granoff³

2012

Infect Immun

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Meningococcal vaccines containing factor H binding protein (fHbp) are in clinical development. fHbp binds human fH, which enables the meningococcus to resist complement-mediated bacteriolysis. Previously, we found that chimeric human IgG1 mouse anti-fHbp monoclonal antibodies (MAbs) had human complement-mediated bactericidal activity only if the MAb inhibited fH binding. Since IgG subclasses differ in their ability to activate complement, we investigated the role of human IgG subclasses on antibody functional activity. We constructed chimeric MAbs in which three different murine fHbp-specific binding domains were each paired with human IgG1, IgG2, or IgG3. Against a wild-type group B isolate, all three IgG3 MAbs, irrespective of their ability to inhibit fH binding, had bactericidal activity that was >5-fold higher than the respective IgG1 MAbs, while the IgG2 MAbs had the least activity. Against a mutant with increased fHbp expression, the anti-fHbp MAbs elicited greater C4b deposition (classical pathway) and greater bactericidal activity than against the wild-type strain, and the IgG1 MAbs had similar or greater activity than the respective IgG3 MAbs. The bactericidal activity against both wild-type and mutant strains also was dependent, in part, on activation of the alternative complement pathway. Thus, at lower epitope density in the wild-type strain, the IgG3 anti-fHbp MAbs had the greatest bactericidal activity. At a higher epitope density in the mutant, the IgG1 MAbs had similar or greater bactericidal activity than the IgG3 MAbs, and the activity was less dependent on the inhibition of fH binding than at a lower epitope density.

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Binding properties and anti-bacterial activities of V-region identical, human IgG and IgM antibodies, against group B Neisseria meningitidis

Cited by 14 publications

References 25 publications

Protection by Natural Human Immunoglobulin M Antibody to Meningococcal Serogroup B Capsular Polysaccharide in the Infant Rat Protection Assay Is Independent of Complement-Mediated Bacterial Lysis

Protection by Natural Human Immunoglobulin M Antibody to Meningococcal Serogroup B Capsular Polysaccharide in the Infant Rat Protection Assay Is Independent of Complement-Mediated Bacterial Lysis

A Systematic Comparison of Free and Bound Antibodies Reveals Binding-Related Conformational Changes

Combined Roles of Human IgG Subclass, Alternative Complement Pathway Activation, and Epitope Density in the Bactericidal Activity of Antibodies to Meningococcal Factor H Binding Protein

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