A general approach for predicting protein epitopes targeted by antibody repertoires using whole proteomes

A general approach for predicting protein epitopes targeted by antibody repertoires using whole proteomes

Antibodies are essential to functional immunity, yet the epitopes targeted by antibody repertoires remain largely uncharacterized. To aid in characterization, we developed a generalizable strategy to predict antibody-binding epitopes within individual proteins and entire proteomes. Specifically, we...

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Veröffentlicht in:PloS one 2019-09, Vol.14 (9), p.e0217668-e0217668
Hauptverfasser: Paull, Michael L, Johnston, Tim, Ibsen, Kelly N, Bozekowski, Joel D, Daugherty, Patrick S
Format: Artikel
Sprache:eng
Schlagworte:
Adolescent
Adult
Aged
AIDS vaccines
Algorithms
Amino acids
Antibodies
Antibodies - chemistry
Antibodies - immunology
Antigenic determinants
Antigens
Antigens, Bacterial - chemistry
Antigens, Bacterial - immunology
Antigens, Viral - chemistry
Antigens, Viral - immunology
Binding
Bioinformatics
Biological markers
Biology and Life Sciences
Biomarkers
Chemical engineering
Child
Datasets
Diagnostic systems
Enterovirus - immunology
Enteroviruses
Epitopes
Epitopes - chemistry
Epitopes - immunology
Epstein-Barr virus
Experiments
Humans
Immunity
Immunoglobulins
Immunology
Infections
Libraries
Medical research
Medicine and Health Sciences
Methods
Middle Aged
Monoclonal antibodies
Next-generation sequencing
Novels
Peptides
Product development
Protein binding
Proteins
Proteome - chemistry
Proteome - immunology
Proteomics
Proteomics - methods
Research and Analysis Methods
Researchers
Rhinovirus
Rhinoviruses
Sequence Analysis, Protein - methods
Staphylococcus - immunology
Streptococcus - immunology
Therapeutic applications
Tiling
Vaccines
Viral infections
Viruses
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Zusammenfassung:Antibodies are essential to functional immunity, yet the epitopes targeted by antibody repertoires remain largely uncharacterized. To aid in characterization, we developed a generalizable strategy to predict antibody-binding epitopes within individual proteins and entire proteomes. Specifically, we selected antibody-binding peptides for 273 distinct sera out of a random library and identified the peptides using next-generation sequencing. To predict antibody-binding epitopes and the antigens from which these epitopes were derived, we tiled the sequences of candidate antigens into short overlapping subsequences of length k (k-mers). We used the enrichment over background of these k-mers in the antibody-binding peptide dataset to predict antibody-binding epitopes. As a positive control, we used this approach, termed K-mer Tiling of Protein Epitopes (K-TOPE), to predict epitopes targeted by monoclonal and polyclonal antibodies of well-characterized specificity, accurately recovering their known epitopes. K-TOPE characterized a commonly targeted antigen from Rhinovirus A, predicting four epitopes recognized by antibodies present in 87% of sera (n = 250). An analysis of 2,908 proteins from 400 viral taxa that infect humans predicted seven enterovirus epitopes and five Epstein-Barr virus epitopes recognized by >30% of specimens. Analysis of Staphylococcus and Streptococcus proteomes similarly predicted 22 epitopes recognized by >30% of specimens. Twelve of these common viral and bacterial epitopes agreed with previously mapped epitopes with p-values < 0.05. Additionally, we predicted 30 HSV2-specific epitopes that were 100% specific against HSV1 in novel and previously reported antigens. Experimentally validating these candidate epitopes could help identify diagnostic biomarkers, vaccine components, and therapeutic targets. The K-TOPE approach thus provides a powerful new tool to elucidate the organisms, antigens, and epitopes targeted by human antibody repertoires.
ISSN:1932-6203
1932-6203
DOI:10.1371/journal.pone.0217668