Characterization of Diverse Subvariants of the Meningococcal Factor H (fH) Binding Protein for Their Ability To Bind fH, To Mediate Serum Resistance, and To Induce Bactericidal Antibodies

Kate L. Seib; Brunella Brunelli; Barbara Brogioni; Emmanuelle Palumbo; Stefania Bambini; Alessandro Muzzi; Federica Dimarcello; Sara Marchi; Arie van der Ende; Beatrice Aricó; Silvana Savino; Maria Scarselli; Maurizio Comanducci; Rino Rappuoli; Marzia M. Giuliani; Mariagrazia Pizza

doi:https://doi.org/10.1128/IAI.00891-10

Characterization of Diverse Subvariants of the Meningococcal Factor H (fH) Binding Protein for Their Ability To Bind fH, To Mediate Serum Resistance, and To Induce Bactericidal Antibodies

Kate L. Seib, Brunella Brunelli, Barbara Brogioni, Emmanuelle Palumbo, Stefania Bambini, Alessandro Muzzi, Federica Dimarcello, Sara Marchi, Arie van der Ende, Beatrice Aricó, Silvana Savino, Maria Scarselli, Maurizio Comanducci, Rino Rappuoli, Marzia M. Giuliani, Mariagrazia Pizza

Research output: Contribution to journal › Article › Academic › peer-review

64 Citations (Scopus)

Abstract

Neisseria meningitidis is a commensal of the human nasopharynx but is also a major cause of septicemia and meningitis. The meningococcal factor H binding protein (fHbp) binds human factor H (fH), enabling down-regulation of complement activation on the bacterial surface. fHbp is a component of two serogroup B meningococcal vaccines currently in clinical development. Here we characterize 12 fHbp subvariants for their level of surface exposure and ability to bind fH, to mediate serum resistance, and to induce bactericidal antibodies. Flow cytometry and Western analysis revealed that all strains examined expressed fHbp on their surface to different extents and bound fH in an fHbp-dependent manner. However, differences in fH binding did not always correlate with the level of fHbp expression, indicating that this is not the only factor affecting the amount of fH bound. To overcome the issue of strain variability in fHbp expression, the MC58 Delta fHbp strain was genetically engineered to express different subvariants from a constitutive heterologous promoter. These recombinant strains were characterized for fH binding, and the data confirmed that each subvariant binds different levels of fH. Surface plasmon resonance revealed differences in the stability of the fHbp-fH complexes that ranged over 2 orders of magnitude, indicating that differences in residues between and within variant groups can influence fH binding. Interestingly, the level of survival in human sera of recombinant MC58 strains expressing diverse subvariants did not correlate with the level of fH binding, suggesting that the interaction of fHbp with fH is not the only function of fHbp that influences serum resistance. Furthermore, cross-reactive bactericidal activity was seen within each variant group, although the degree of activity varied, suggesting that amino acid differences within each variant group influence the bactericidal antibody response

Original language	English
Pages (from-to)	970-981
Journal	Infection and immunity
Volume	79
Issue number	2
DOIs	https://doi.org/10.1128/IAI.00891-10
Publication status	Published - 2011

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Cite this

Seib, K. L., Brunelli, B., Brogioni, B., Palumbo, E., Bambini, S., Muzzi, A., Dimarcello, F., Marchi, S., van der Ende, A., Aricó, B., Savino, S., Scarselli, M., Comanducci, M., Rappuoli, R., Giuliani, M. M., & Pizza, M. (2011). Characterization of Diverse Subvariants of the Meningococcal Factor H (fH) Binding Protein for Their Ability To Bind fH, To Mediate Serum Resistance, and To Induce Bactericidal Antibodies. Infection and immunity, 79(2), 970-981. https://doi.org/10.1128/IAI.00891-10

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title = "Characterization of Diverse Subvariants of the Meningococcal Factor H (fH) Binding Protein for Their Ability To Bind fH, To Mediate Serum Resistance, and To Induce Bactericidal Antibodies",

abstract = "Neisseria meningitidis is a commensal of the human nasopharynx but is also a major cause of septicemia and meningitis. The meningococcal factor H binding protein (fHbp) binds human factor H (fH), enabling down-regulation of complement activation on the bacterial surface. fHbp is a component of two serogroup B meningococcal vaccines currently in clinical development. Here we characterize 12 fHbp subvariants for their level of surface exposure and ability to bind fH, to mediate serum resistance, and to induce bactericidal antibodies. Flow cytometry and Western analysis revealed that all strains examined expressed fHbp on their surface to different extents and bound fH in an fHbp-dependent manner. However, differences in fH binding did not always correlate with the level of fHbp expression, indicating that this is not the only factor affecting the amount of fH bound. To overcome the issue of strain variability in fHbp expression, the MC58 Delta fHbp strain was genetically engineered to express different subvariants from a constitutive heterologous promoter. These recombinant strains were characterized for fH binding, and the data confirmed that each subvariant binds different levels of fH. Surface plasmon resonance revealed differences in the stability of the fHbp-fH complexes that ranged over 2 orders of magnitude, indicating that differences in residues between and within variant groups can influence fH binding. Interestingly, the level of survival in human sera of recombinant MC58 strains expressing diverse subvariants did not correlate with the level of fH binding, suggesting that the interaction of fHbp with fH is not the only function of fHbp that influences serum resistance. Furthermore, cross-reactive bactericidal activity was seen within each variant group, although the degree of activity varied, suggesting that amino acid differences within each variant group influence the bactericidal antibody response",

author = "Seib, {Kate L.} and Brunella Brunelli and Barbara Brogioni and Emmanuelle Palumbo and Stefania Bambini and Alessandro Muzzi and Federica Dimarcello and Sara Marchi and {van der Ende}, Arie and Beatrice Aric{\'o} and Silvana Savino and Maria Scarselli and Maurizio Comanducci and Rino Rappuoli and Giuliani, {Marzia M.} and Mariagrazia Pizza",

year = "2011",

doi = "https://doi.org/10.1128/IAI.00891-10",

language = "English",

volume = "79",

pages = "970--981",

journal = "Infection and immunity",

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Seib, KL, Brunelli, B, Brogioni, B, Palumbo, E, Bambini, S, Muzzi, A, Dimarcello, F, Marchi, S, van der Ende, A, Aricó, B, Savino, S, Scarselli, M, Comanducci, M, Rappuoli, R, Giuliani, MM & Pizza, M 2011, 'Characterization of Diverse Subvariants of the Meningococcal Factor H (fH) Binding Protein for Their Ability To Bind fH, To Mediate Serum Resistance, and To Induce Bactericidal Antibodies', Infection and immunity, vol. 79, no. 2, pp. 970-981. https://doi.org/10.1128/IAI.00891-10

Characterization of Diverse Subvariants of the Meningococcal Factor H (fH) Binding Protein for Their Ability To Bind fH, To Mediate Serum Resistance, and To Induce Bactericidal Antibodies. / Seib, Kate L.; Brunelli, Brunella; Brogioni, Barbara et al.
In: Infection and immunity, Vol. 79, No. 2, 2011, p. 970-981.

Research output: Contribution to journal › Article › Academic › peer-review

TY - JOUR

T1 - Characterization of Diverse Subvariants of the Meningococcal Factor H (fH) Binding Protein for Their Ability To Bind fH, To Mediate Serum Resistance, and To Induce Bactericidal Antibodies

AU - Seib, Kate L.

AU - Brunelli, Brunella

AU - Brogioni, Barbara

AU - Palumbo, Emmanuelle

AU - Bambini, Stefania

AU - Muzzi, Alessandro

AU - Dimarcello, Federica

AU - Marchi, Sara

AU - van der Ende, Arie

AU - Aricó, Beatrice

AU - Savino, Silvana

AU - Scarselli, Maria

AU - Comanducci, Maurizio

AU - Rappuoli, Rino

AU - Giuliani, Marzia M.

AU - Pizza, Mariagrazia

PY - 2011

Y1 - 2011

N2 - Neisseria meningitidis is a commensal of the human nasopharynx but is also a major cause of septicemia and meningitis. The meningococcal factor H binding protein (fHbp) binds human factor H (fH), enabling down-regulation of complement activation on the bacterial surface. fHbp is a component of two serogroup B meningococcal vaccines currently in clinical development. Here we characterize 12 fHbp subvariants for their level of surface exposure and ability to bind fH, to mediate serum resistance, and to induce bactericidal antibodies. Flow cytometry and Western analysis revealed that all strains examined expressed fHbp on their surface to different extents and bound fH in an fHbp-dependent manner. However, differences in fH binding did not always correlate with the level of fHbp expression, indicating that this is not the only factor affecting the amount of fH bound. To overcome the issue of strain variability in fHbp expression, the MC58 Delta fHbp strain was genetically engineered to express different subvariants from a constitutive heterologous promoter. These recombinant strains were characterized for fH binding, and the data confirmed that each subvariant binds different levels of fH. Surface plasmon resonance revealed differences in the stability of the fHbp-fH complexes that ranged over 2 orders of magnitude, indicating that differences in residues between and within variant groups can influence fH binding. Interestingly, the level of survival in human sera of recombinant MC58 strains expressing diverse subvariants did not correlate with the level of fH binding, suggesting that the interaction of fHbp with fH is not the only function of fHbp that influences serum resistance. Furthermore, cross-reactive bactericidal activity was seen within each variant group, although the degree of activity varied, suggesting that amino acid differences within each variant group influence the bactericidal antibody response

AB - Neisseria meningitidis is a commensal of the human nasopharynx but is also a major cause of septicemia and meningitis. The meningococcal factor H binding protein (fHbp) binds human factor H (fH), enabling down-regulation of complement activation on the bacterial surface. fHbp is a component of two serogroup B meningococcal vaccines currently in clinical development. Here we characterize 12 fHbp subvariants for their level of surface exposure and ability to bind fH, to mediate serum resistance, and to induce bactericidal antibodies. Flow cytometry and Western analysis revealed that all strains examined expressed fHbp on their surface to different extents and bound fH in an fHbp-dependent manner. However, differences in fH binding did not always correlate with the level of fHbp expression, indicating that this is not the only factor affecting the amount of fH bound. To overcome the issue of strain variability in fHbp expression, the MC58 Delta fHbp strain was genetically engineered to express different subvariants from a constitutive heterologous promoter. These recombinant strains were characterized for fH binding, and the data confirmed that each subvariant binds different levels of fH. Surface plasmon resonance revealed differences in the stability of the fHbp-fH complexes that ranged over 2 orders of magnitude, indicating that differences in residues between and within variant groups can influence fH binding. Interestingly, the level of survival in human sera of recombinant MC58 strains expressing diverse subvariants did not correlate with the level of fH binding, suggesting that the interaction of fHbp with fH is not the only function of fHbp that influences serum resistance. Furthermore, cross-reactive bactericidal activity was seen within each variant group, although the degree of activity varied, suggesting that amino acid differences within each variant group influence the bactericidal antibody response

U2 - https://doi.org/10.1128/IAI.00891-10

DO - https://doi.org/10.1128/IAI.00891-10

M3 - Article

C2 - 21149595

SN - 0019-9567

VL - 79

SP - 970

EP - 981

JO - Infection and immunity

JF - Infection and immunity

IS - 2

ER -