Major Histocompatibility Complex Binding, Eluted Ligands, and Immunogenicity: Benchmark Testing and Predictions

Paul, Sinu; Grifoni, Alba; Peters, Bjoern; Sette, Alessandro

doi:10.3389/fimmu.2019.03151

Cited by 25 publications

(21 citation statements)

References 34 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…These studies suggested that 1,000 nM is a generally applicable threshold for biologically relevant binding in the context of HLA class II. This threshold was also confirmed in a recent analysis which found that 83.3% of HLA class II restricted epitopes are predicted to bind their corresponding restricting allele with an affinity of 1,000 nM, or better (19). Of note, optimal thresholds for MHC class II are still unclear and are being discussed in the community.…”

Section: Hla Class II Reported Eluted Ligands Are In General Predicsupporting

confidence: 52%

See 1 more Smart Citation

Comparison of HLA ligand elution data and binding predictions reveals varying prediction performance for the multiple motifs recognized by HLA-DQ2.5

Yalcin

Sidney

Chronister

et al. 2020

Preprint

Self Cite

View full text Add to dashboard Cite

Binding prediction tools are commonly used to identify peptides presented on MHC class II molecules. Recently, a wealth of data in the form of naturally eluted ligands has become available and discrepancies between ligand elution data and binding predictions have been reported. Quantitative metrics for such comparisons are currently lacking. In this study, we assessed how efficiently MHC class II binding predictions can identify naturally eluted peptides, and investigated instances with discrepancies between the two methods in detail. We found that, in general, MHC class II eluted ligands are predicted to bind to their reported restriction element with high affinity. But, for several studies reporting an increased number of ligands that were not predicted to bind, we found that the reported MHC restriction was ambiguous. Additional analyses determined that most of the ligands predicted to not bind are either weak binders or predicted to bind other co-expressed MHC class II molecules. For selected alleles, we addressed discrepancies between elution data and binding predictions by experimental measurements, and found that predicted and measured affinities correlate well. For DQA1*05:01/DQB1*02:01 (DQ2.5) however, binding predictions did miss several peptides that were determined experimentally to be binders. For these peptides and several known DQ2.5 binders we determined key residues for conferring DQ2.5 binding capacity, which revealed that DQ2.5 utilizes two different binding motifs, of which only one is predicted effectively. These findings have important implications for the interpretation of ligand elution data and for the improvement of MHC class II binding predictions.

show abstract

Section: Hla Class II Reported Eluted Ligands Are In General Predicsupporting

confidence: 52%

“…Peptides with predicted binding affinities of >1,000nM were considered predicted nonbinders. This threshold was selected based on previous studies analyzing the binding affinity of HLA class II restricted T cell epitopes (16)(17)(18)(19).…”

Section: Hla Binding Predictionsmentioning

confidence: 99%

Comparison of HLA ligand elution data and binding predictions reveals varying prediction performance for the multiple motifs recognized by HLA-DQ2.5

Yalcin

Sidney

Chronister

et al. 2020

Preprint

Self Cite

View full text Add to dashboard Cite

show abstract

“…Peptides with predicted percentile ranks of >20% were considered predicted non‐binders. This threshold was selected based on previous studies analysing the binding affinity of HLA class II‐restricted T‐cell epitopes 20‐23 …”

Section: Methodsmentioning

confidence: 99%

Comparison of HLA ligand elution data and binding predictions reveals varying prediction performance for the multiple motifs recognized by HLA‐DQ2.5

et al. 2020

Self Cite

View full text Add to dashboard Cite

SummaryBinding prediction tools are commonly used to identify peptides presented on MHC class II molecules. Recently, a wealth of data in the form of naturally eluted ligands has become available and discrepancies between ligand elution data and binding predictions have been reported. Quantitative metrics for such comparisons are currently lacking. In this study, we assessed how efficiently MHC class II binding predictions can identify naturally eluted peptides, and investigated instances with discrepancies between the two methods in detail. We found that, in general, MHC class II eluted ligands are predicted to bind to their reported restriction element with high affinity. But, for several studies reporting an increased number of ligands that were not predicted to bind, we found that the reported MHC restriction was ambiguous. Additional analyses determined that most of the ligands predicted to not bind, are predicted to bind other co‐expressed MHC class II molecules. For selected alleles, we addressed discrepancies between elution data and binding predictions by experimental measurements and found that predicted and measured affinities correlate well. For DQA1*05:01/DQB1*02:01 (DQ2.5) however, binding predictions did miss several peptides that were determined experimentally to be binders. For these peptides and several known DQ2.5 binders, we determined key residues for conferring DQ2.5 binding capacity, which revealed that DQ2.5 utilizes two different binding motifs, of which only one is predicted effectively. These findings have important implications for the interpretation of ligand elution data and for the improvement of MHC class II binding predictions.

show abstract

“…Overall, the 49 most dominant epitopes showed significantly higher binding promiscuity (number of alleles bound at the 1,000 nM or better threshold) (Paul et al, 2019;Southwood et al, 1998) for the panel of common HLA class II than a control group of 49 non-epitopes derived from the same proteins (Average number of HLA predicted to be bind ± SD epitopes = 10.8 ± 6.5; non-epitopes = 5.7 ± 6; p=0.0001 by Mann-Whitney; Fig. S3C-D).…”

Section: Hla Binding Capacity Of Dominant Epitopesmentioning

confidence: 99%

Comprehensive analysis of T cell immunodominance and immunoprevalence of SARS-CoV-2 epitopes in COVID-19 cases

Tarke

Sidney

Kidd

et al. 2020

Preprint

Self Cite

158

View full text Add to dashboard Cite

SUMMARYT cells are involved in control of SARS-CoV-2 infection. To establish the patterns of immunodominance of different SARS-CoV-2 antigens, and precisely measure virus-specific CD4+ and CD8+ T cells, we studied epitope-specific T cell responses of approximately 100 convalescent COVID-19 cases. The SARS-CoV-2 proteome was probed using 1,925 peptides spanning the entire genome, ensuring an unbiased coverage of HLA alleles for class II responses. For HLA class I, we studied an additional 5,600 predicted binding epitopes for 28 prominent HLA class I alleles, accounting for wide global coverage. We identified several hundred HLA-restricted SARS-CoV-2-derived epitopes. Distinct patterns of immunodominance were observed, which differed for CD4+ T cells, CD8+ T cells, and antibodies. The class I and class II epitopes were combined into new epitope megapools to facilitate identification and quantification of SARS-CoV-2-specific CD4+ and CD8+ T cells.

show abstract

Major Histocompatibility Complex Binding, Eluted Ligands, and Immunogenicity: Benchmark Testing and Predictions

Cited by 25 publications

References 34 publications

Comparison of HLA ligand elution data and binding predictions reveals varying prediction performance for the multiple motifs recognized by HLA-DQ2.5

Comparison of HLA ligand elution data and binding predictions reveals varying prediction performance for the multiple motifs recognized by HLA-DQ2.5

Comparison of HLA ligand elution data and binding predictions reveals varying prediction performance for the multiple motifs recognized by HLA‐DQ2.5

Comprehensive analysis of T cell immunodominance and immunoprevalence of SARS-CoV-2 epitopes in COVID-19 cases

Contact Info

Product

Resources

About