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

Giuntini, Stefano; Reason, Donald C.; Granoff, Dan M.

doi:10.1128/iai.05956-11

Cited by 59 publications

(85 citation statements)

References 38 publications

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“…The ability of human IgG1, IgG2, and IgG3 to activate human complement has been well documented, and our data (Fig. 7) are in agreement with those of previous studies (49,50). In contrast, studies of the interaction of human antibody with the mouse complement system have been quite limited.…”

Section: Discussionsupporting

confidence: 83%

Influence of IgG Subclass on Human Antimannan Antibody-Mediated Resistance to Hematogenously Disseminated Candidiasis in Mice

et al. 2016

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bCandida albicans is a yeast-like pathogen and can cause life-threatening systemic candidiasis. Its cell surface is enriched with mannan that is resistant to complement activation. Previously, we developed the recombinant human IgG1 antimannan antibody M1g1. M1g1 was found to promote complement activation and phagocytosis and protect mice from systemic candidiasis. Here, we evaluate the influence of IgG subclass on antimannan antibody-mediated protection. Three IgG subclass variants of M1g1 were constructed: M1g2, M1g3, and M1g4. The IgG subclass identity for each variant was confirmed with DNA sequence and subclass-specific antibodies. These variants contain identical M1 Fabs and exhibited similar binding affinities for C. albicans yeast and purified mannan. Yeast cells and hyphae recovered from the kidney of antibody-treated mice with systemic candidiasis showed uniform binding of each variant, indicating constitutive expression of the M1 epitope and antibody opsonization in the kidney. All variants promoted deposition of both murine and human C3 onto the yeast cell surface, with M1g4 showing delayed activation, as determined by flow cytometry and immunofluorescence microscopy. M1g4-mediated complement activation was found to be associated with its M1 Fab that activates the alternative pathway in an Fc-independent manner. Treatment with each subclass variant extended the survival of mice with systemic candidiasis (P < 0.001). However, treatment with M1g1, M1g3, or M1g4, but not with M1g2, also reduced the kidney fungal burden (P < 0.001). Thus, the role of human antimannan antibody in host resistance to systemic candidiasis is influenced by its IgG subclass.

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Section: Discussionsupporting

confidence: 83%

Influence of IgG Subclass on Human Antimannan Antibody-Mediated Resistance to Hematogenously Disseminated Candidiasis in Mice

et al. 2016

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“…After the binding of anti-FHbp antibodies, the Fc density on the bacterial surface may be too low to permit sufficient C3b deposition by the classical complement pathway alone for the formation of a membrane attack complex without alternative pathway amplification (27,39). Since FH downregulates the alternative pathway, the ability of anti-FHbp antibodies to block FH binding can be critical for eliciting anti-FHbp bacteriolysis (25,27,39,40). We investigated whether resistance to anti-FHbp bactericidal activity might be explained by binding of FH to ligands other than FHbp (16).…”

Section: Discussionmentioning

confidence: 99%

Binding of Complement Factor H to PorB3 and NspA Enhances Resistance of Neisseria meningitidis to Anti-Factor H Binding Protein Bactericidal Activity

Giuntini¹,

Pajón²,

Ram

et al. 2015

Infect Immun

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T wo meningococcal serogroup B vaccines contain factor H binding protein (FHbp) (1, 2). One of the vaccines, Bexsero (Novartis Vaccines), is licensed in Europe, Australia, and Canada for use in infants, older children, and adults. This vaccine also contains three other antigens capable of eliciting bactericidal antibodies (2) and is referred to as "4CMenB" (four component meningococcal B). The second vaccine, Trumenba (Pfizer), was licensed in the United States on 29 October 2014 for use with the age group from 10 to 25 years. This vaccine contains FHbp (see below).As of October 2014, there were 758 distinct amino acid sequence variants of FHbp, each assigned a unique "peptide" identifier (ID) as designated on a public database (http://pubmlst.org /neisseria/fHbp/). Based on amino acid sequence relatedness, FHbp sequence variants can be subdivided into two subfamilies, A and B (3, 4), or into three variant groups (5). There is general agreement that protection conferred by anti-FHbp antibody is subfamily (3) or variant group (5) specific. There is also general agreement that isolates with very low FHbp expression are resistant to anti-FHbp bactericidal activity and that isolates with relatively high expression are susceptible as long as there is an antigenic match between the FHbp sequence variant expressed by the isolate and that of the vaccine used to raise the antibody (6-8).The Pfizer FHbp vaccine contains two FHbp sequence variants, one from each subfamily. The Novartis 4CMenB vaccine contains only a subfamily B FHbp sequence variant. Antibodies elicited by the three other antigens in 4CMenB provide coverage against the majority of meningococci with subfamily A FHbp sequence variants. To date, defining threshold levels of FHbp expression and/or cross-reactivity that are sufficient for predicting susceptibility of an isolate to anti-FHbp bactericidal activity has largely been done empirically by correlating FHbp expression of isolates from different strain collections with susceptibility to bactericidal activity of serum pools from vaccinated infants or adolescents (9-11).In the present study, we identified four disease-causing serogroup B isolates with relatively high expression of FHbp that were resistant to complement-mediated bactericidal activity of sera from mice immunized with FHbp sequence variants that matched those of the isolates. As described below, two of the four isolates had evidence of human FH-dependent complement evasion independent of FHbp. We report the results of investigations of the basis for the anti-FHbp bactericidal resistance in these two isolates.

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“…The AP acting in isolation is insufficient to kill meningococci (15, 19); however, the AP is required for maximal classical pathway-initiated killing (7, 19, 47). We investigated the role of PorB2 in mediating resistance to infant rat serum (all complement pathways functional) by comparing the isogenic strain pair in a bactericidal assay.…”

Section: Downloaded Frommentioning

confidence: 99%

“…The AP is characterized by a positive-feedback loop that amplifies C3b deposition on microbial surfaces (5,6). The AP works in concert with the classical pathway and plays an important role in maximizing the killing activity of select antibodies, including those directed against the vaccine antigen, factor H binding protein (fHbp) (7). Factor H (fH), a host complement control protein, plays a key role in limiting unwanted activation of the AP (8,9) by assisting with factor I-mediated cleavage of C3b to iC3b (10,11) and by irreversibly dissociating the AP C3 convertase (C3bBb) (12,13).…”

mentioning

confidence: 99%

Inhibition of the Alternative Pathway of Nonhuman Infant Complement by Porin B2 Contributes to Virulence of Neisseria meningitidis in the Infant Rat Model

Lewis

Vu²,

Granoff³

et al. 2014

Infect Immun

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bNeisseria meningitidis utilizes capsular polysaccharide, lipooligosaccharide (LOS) sialic acid, factor H binding protein (fHbp), and neisserial surface protein A (NspA) to regulate the alternative pathway (AP) of complement. Using meningococcal mutants that lacked all four of the above-mentioned molecules (quadruple mutants), we recently identified a role for PorB2 in attenuating the human AP; inhibition was mediated by human fH, a key downregulatory protein of the AP. Previous studies showed that fH downregulation of the AP via fHbp or NspA is specific for human fH. Here, we report that PorB2-expressing quadruple mutants also regulate the AP of baby rabbit and infant rat complement. Blocking a human fH binding region on PorB2 of the quadruple mutant of strain 4243 with a chimeric protein that comprised human fH domains 6 and 7 fused to murine IgG Fc enhanced AP-mediated baby rabbit C3 deposition, which provided evidence for an fH-dependent mechanism of nonhuman AP regulation by PorB2. Using isogenic mutants of strain H44/76 that differed only in their PorB molecules, we confirmed a role for PorB2 in resistance to killing by infant rat serum. The PorB2-expressing strain also caused higher levels of bacteremia in infant rats than its isogenic PorB3-expressing counterpart, thus providing a molecular basis for increased survival of PorB2 isolates in this model. These studies link PorB2 expression with infection of infant rats, which could inform the choice of meningococcal strains for use in animal models, and reveals, for the first time, that PorB2-expressing strains of N. meningitidis regulate the AP of baby rabbits and rats. N eisseria meningitidis is an important cause of bacterial meningitis worldwide (1, 2). The complement system contributes to innate immune defenses against this pathogen, and individuals with defects in the terminal complement components (C5 through C9) or in components of the alternative pathway (AP) are at an increased risk of meningococcal disease (3, 4). The AP is characterized by a positive-feedback loop that amplifies C3b deposition on microbial surfaces (5, 6). The AP works in concert with the classical pathway and plays an important role in maximizing the killing activity of select antibodies, including those directed against the vaccine antigen, factor H binding protein (fHbp) (7). Factor H (fH), a host complement control protein, plays a key role in limiting unwanted activation of the AP (8, 9) by assisting with factor I-mediated cleavage of C3b to iC3b (10,11) and by irreversibly dissociating the AP C3 convertase (C3bBb) (12,13).N. meningitidis employs several distinct mechanisms to limit AP activation. Capsular polysaccharides elaborated by meningococci are important determinants of meningococcal serum resistance; group B and C capsules serve to inhibit the AP and limit C3 deposition on the bacterial surface (14, 15). Sialylation of lacto-Nneotetraose (LNT) lipooligosaccharide (LOS) inhibits the AP by enhancing the interactions of fH with C3 fragments bound to the bacterial surf...

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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

Cited by 59 publications

References 38 publications

Influence of IgG Subclass on Human Antimannan Antibody-Mediated Resistance to Hematogenously Disseminated Candidiasis in Mice

Influence of IgG Subclass on Human Antimannan Antibody-Mediated Resistance to Hematogenously Disseminated Candidiasis in Mice

Binding of Complement Factor H to PorB3 and NspA Enhances Resistance of Neisseria meningitidis to Anti-Factor H Binding Protein Bactericidal Activity

Inhibition of the Alternative Pathway of Nonhuman Infant Complement by Porin B2 Contributes to Virulence of Neisseria meningitidis in the Infant Rat Model

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