A Combined Computer-Aided Approach to Drive the Identification of Potential Epitopes in Protein Therapeutics

Authors

  • Bárbara Athayde Vaz Galvão da Silva Molecular Biology Laboratory – Unit of Innovation and Development, Butantan Institute and Centre of Excellence in New Target Discovery – CENTD, Butantan Institute, Sao Paulo, Brazil.
  • Ana Marisa Chudzinski-Tavassi Molecular Biology Laboratory – Unit of Innovation and Development, Butantan Institute and Centre of Excellence in New Target Discovery – CENTD, Butantan Institute, Sao Paulo, Brazil.
  • Kerly Fernanda Mesquita Pasqualoto Molecular Biology Laboratory – Unit of Innovation and Development, Butantan Institute and Centre of Excellence in New Target Discovery – CENTD, Butantan Institute, Sao Paulo, Brazil.

DOI:

https://doi.org/10.18433/jpps29800

Abstract

Background: The identification of fragment sequences, or motifs, within a therapeutic protein that may elicit an immune response when processed by T-cells can be provided by computer-aided approaches. Immunogenicity is a significant problem associated with protein therapeutics and should be investigated in the early stage of protein-based drug development to avoid treatment resistance and potentially life-threatening immune responses. Purpose: To provide a combined computer-aided protocol for investigating the immunogenic profile of a recombinant Kunitz-type inhibitor, which has been reported as promising antitumor agent by our research group. Methods: The combination of databases searching (IEDB and SYFPEITHI) and molecular docking simulations was exploited, herein. This combined protocol has allowed the identification of potential epitopes before in vitro/in vivo evaluation. Predictors of human proteasome cleavage transport and major histocompatibility complex (MHC) binding were considered as overall score assigning the corresponding intrinsic potential of being a T cell epitope to each fragment sequence. The peptides or motifs better classified in the two databases were docked into the three-dimensional (3D) structure of MHC (class I and II) complex to verify the calculated binding affinity.  The binding interactions regarding the molecular recognition process by T-cells were also exploited through the MHC:ligand:T-cell complexes. Results: Regarding the Kunitz-type sequence, four motifs were identified as potentially epitopes for MHC-I and three motifs were found for MHC-II. But, those motifs were classified as moderately immunogenic. Final remarks: The combined computer-aided protocol has significantly reduced the number of potential epitopes to be considered for further analysis and could be useful to identify immunogenic fragments (high, moderate and low) in protein pharmaceutics before in vitro/in vivo experimentation.

Downloads

Download data is not yet available.

Downloads

Published

2018-07-14

How to Cite

Galvão da Silva, B. A. V., Chudzinski-Tavassi, A. M., & Pasqualoto, K. F. M. (2018). A Combined Computer-Aided Approach to Drive the Identification of Potential Epitopes in Protein Therapeutics. Journal of Pharmacy & Pharmaceutical Sciences, 21(1), 268–285. https://doi.org/10.18433/jpps29800

Issue

Vol. 21 (2018): Pages 143 - 304

Section

Pharmaceutical Sciences; Original Research Articles

License

This is an open access journal with free of charge non-commercial download. At the time of submission, authors will be asked to transfer the copyright to the accepted article to the Journal of Pharmacy and Pharmaceutical Sciences. The author may purchase the copyright for $500 upon which he/she will have the exclusive copyright to the article. Nevertheless, acceptance of a manuscript for publication in the Journal is with the authors' approval of the terms and conditions of the Creative Commons copyright license Creative Common license (Attribution-ShareAlike) License for non-commercial uses.

CLOCKSS system has permission to collect, preserve, and serve this Archival Unit.