Reduced Susceptibility of Recombinant Polyclonal Antibodies to Inhibitory Anti-Variable Domain Antibody Responses

Klitgaard, Josephine L.; Coljee, Vincent W.; Andersen, Peter S.; Rasmussen, Lone K.; Nielsen, Lene; Haurum, John S.; Bregenholt, Søren

doi:10.4049/jimmunol.177.6.3782

Cited by 18 publications

(6 citation statements)

References 21 publications

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“…In contrast, previous studies using interferon a2b transgenic mice showed that tolerance could be broken in response to administration of aggregated protein. 21 Important differences between the current study and the previous studies may be related to the natural function and abundance of the respective proteins, 5 as well as the mouse strains 60 used to generate the transgenic mice. The current study used the strain B6.SJL-Tg(HBB-GH1)420King/J, which results from the cross breeding of C57BL/6J with SJL strains, whereas the interferon a2b study was based on the strain FVB/N.…”

Section: Activated Dendritic Cells Can In Turn Activate T Cells Into mentioning

confidence: 93%

Immunogenicity of aggregates of recombinant human growth hormone in mouse models

Fradkin

Carpenter

Randolph

2009

Journal of Pharmaceutical Sciences

147

121

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Section: Activated Dendritic Cells Can In Turn Activate T Cells Into mentioning

confidence: 93%

Immunogenicity of aggregates of recombinant human growth hormone in mouse models

Fradkin

Carpenter

Randolph

2009

Journal of Pharmaceutical Sciences

147

121

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“…Although the use of the respective animal proteins might help elucidate basic immunological properties of the molecules studied, animal and human MHC are not equivalent because they can have different amino acid side-chain restrictions. This is best illustrated by the variability of immune response to chimeric antibodies in different strains of inbred mice [38]. For human homologs, standard animal models are even less predictive because the induction of immunogenicity in humans is based on breaking B and T cell tolerance, although such models do allow comparison of relative immunogenicity of different preparations of the same protein.…”

Section: Animal Studiesmentioning

confidence: 99%

Immunogenicity of protein therapeutics

Groot¹,

Scott²

2007

Trends in Immunology

434

314

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“…Plasmablast cells were isolated by flow cytometry and sorted into single wells of 96-well plates (50 plates per donor), and the antibody-containing supernatants were screened by a custom Luminex assay for PTx reactivity (see Table S1 in the supplemental material). The antibody variable heavy chain (V H ) and variable light chain (V L ) sequences were then amplified from PTx-reactive wells by use of established methodologies ( 14 , 15 ), resulting in identification of five unique antibody sequences ( Fig. 1 ).…”

Section: Resultsmentioning

confidence: 99%

Characterization of Individual Human Antibodies That Bind Pertussis Toxin Stimulated by Acellular Immunization

Acquaye-Seedah

Reczek²,

Russell³

et al. 2018

Infect Immun

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Despite high vaccination rates, the incidence of whooping cough has steadily been increasing in developing countries for several decades. The current acellular pertussis (aP) vaccines all include the major protective antigen pertussis toxin (PTx) and are safer, but they appear to be less protective than infection or older, whole-cell vaccines. To better understand the attributes of individual antibodies stimulated by aP, we isolated plasmablast clones recognizing PTx after booster immunization of two donors. Five unique antibody sequences recognizing native PTx were recovered and expressed as recombinant human IgG1 antibodies. The antibodies all bind different epitopes on the PTx S1 subunit, B oligomer, or S1-B subunit interface, and just one clone neutralized PTx in an in vitro assay. To better understand the epitopes bound by the nonneutralizing S1-subunit antibodies, comprehensive mutagenesis with yeast display provided a detailed map of the epitope recognized by antibodies A8 and E12. Residue R76 is required for antibody A8 binding and is present on the S1 surface but is only partially exposed in the holotoxin, providing a structural explanation for A8's inability to neutralize holotoxin. The B-subunit-specific antibody D8 inhibited PTx binding to a model receptor and neutralized PTx in vitro as well as in an in vivo leukocytosis assay. This is the first study, to our knowledge, to identify individual human antibodies stimulated by the acellular pertussis vaccine and demonstrates the feasibility of using these approaches to address outstanding issues in pertussis vaccinology, including mechanisms of accelerated waning of protective immunity despite repeated aP immunization.

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Reduced Susceptibility of Recombinant Polyclonal Antibodies to Inhibitory Anti-Variable Domain Antibody Responses

Cited by 18 publications

References 21 publications

Immunogenicity of aggregates of recombinant human growth hormone in mouse models

Immunogenicity of aggregates of recombinant human growth hormone in mouse models

Immunogenicity of protein therapeutics

Characterization of Individual Human Antibodies That Bind Pertussis Toxin Stimulated by Acellular Immunization

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