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Immunoinformatic Risk Assessment of Host Cell Proteins During Process Development for Biologic Therapeutics

Kirk Haltaufderhyde, Brian Roberts, Sundos Khan, Frances Terry, Christine M. Boyle, Mitchell McAllister, William Martin, Amy S. Rosenberg, Anne S. De Groot

2023The AAPS Journal16 citationsDOIOpen Access PDF

Abstract

The identification and removal of host cell proteins (HCPs) from biologic products is a critical step in drug development. Despite recent improvements to purification processes, biologics such as monoclonal antibodies, enzyme replacement therapies, and vaccines that are manufactured in a range of cell lines and purified using diverse processes may contain HCP impurities, making it necessary for developers to identify and quantify impurities during process development for each drug product. HCPs that contain sequences that are less conserved with human homologs may be more immunogenic than those that are more conserved. We have developed a computational tool, ISPRI-HCP, that estimates the immunogenic potential of HCP sequences by evaluating and quantifying T cell epitope density and relative conservation with similar T cell epitopes in the human proteome. Here we describe several case studies that support the use of this method for classifying candidate HCP impurities according to their immunogenicity risk.

Topics & Concepts

EpitopeImmunogenicityMonoclonal antibodyComputational biologyProteomeHuman proteome projectProcess developmentHuman proteinsDrug developmentIdentification (biology)BiologyCellAntibodyDrugBioinformaticsImmunologyProteomicsBiochemistryGenePharmacologyBusinessBotanyProcess managementvaccines and immunoinformatics approachesMonoclonal and Polyclonal Antibodies ResearchCAR-T cell therapy research