Published August 10, 2020 | Version v1
Dataset Open

HLA Class II specificity assessed by high-density peptide microarray interactions

  • 1. University of Copenhagen
  • 2. Technical University of Denmark
  • 3. Monash University
  • 4. Schafer-N (Denmark)

Description

The ability to predict and/or identify MHC binding peptides is an essential component of T cell epitope discovery; something that ultimately should benefit the development of vaccines and immunotherapies. In particular, MHC class I (MHC-I) prediction tools have matured to a point where accurate selection of optimal peptide epitopes is possible for virtually all MHC-I allotypes; in comparison, current MHC class II (MHC-II) predictors are less mature. Since MHC-II restricted CD4+ T cells control and orchestrate most immune responses, this shortcoming severely hampers the development of effective immunotherapies. The ability to generate large panels of peptides and subsequently large bodies of peptide-MHC-II interaction data is key to the solution of this problem; a solution that also will support the improvement of bioinformatics predictors, which critically relies on the availability of large amounts of accurate, diverse and representative data. Here, we have used recombinant HLA-DRB1*01:01 and HLA-DRB1*03:01 molecules to interrogate high-density peptide arrays, in casu containing 70,000 random peptides in triplicates. We demonstrate that the binding data acquired contains systematic and interpretable information reflecting the specificity of the HLA-DR molecules investigated. Collectively, with a cost per peptide reduced to a few cents combined with the flexibility of recombinant HLA technology, this poses an attractive strategy to generate vast bodies of MHC-II binding data at an unprecedented speed and for the benefit of generating peptide-MHC-II binding data as well as improving MHC-II prediction tools.

Notes

Funding provided by: European Commission
Crossref Funder Registry ID: http://dx.doi.org/10.13039/501100000780
Award Number: HIPAD project no. 278832

Funding provided by: Det Frie Forskningsråd
Crossref Funder Registry ID: http://dx.doi.org/10.13039/501100004836
Award Number: DFF – 6110-00644

Funding provided by: Scleroseforeningen
Crossref Funder Registry ID: http://dx.doi.org/10.13039/100008361
Award Number: A31444

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