Exploring sample preparation and data evaluation strategies for enhanced identification of host cell proteins in drug products of therapeutic antibodies and Fc-fusion proteins

Esser‐Skala, Wolfgang; Segl, Marius; Wohlschlager, Therese; Reisinger, Veronika; Holzmann, Johann; Huber, Christian G.

doi:10.1007/s00216-020-02796-1

Cited by 9 publications

(5 citation statements)

References 55 publications

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“…It is known that Peroxiredoxin-1 is difficult to remove and has been reported previously. [30][31][32] Cornifin-A, another commonly observed HCP, has also been identified frequently. 8,33 Nine HCP were identified in 20% or more of the drugs analyzed.…”

Section: Host Cell Proteins In Commercial Biotherapeuticsmentioning

confidence: 99%

Host cell protein profiling of commercial therapeutic protein drugs as a benchmark for monoclonal antibody-based therapeutic protein development

Molden

et al. 2021

mAbs

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Therapeutic proteins including monoclonal antibodies (mAbs) are usually produced in engineered host cell lines that also produce thousands of endogenous proteins at varying levels. A critical aspect of the development of biotherapeutics manufacturing processes is the removal of these host cell proteins (HCP) to appropriate levels in order to minimize risk to patient safety and drug efficacy. During the development process and associated analytical characterization, mass spectrometry (MS) has become an increasingly popular tool for HCP analysis due to its ability to provide both relative abundance and identity of individual HCP and because the method does not rely on polyclonal antibodies, which are used in enzyme-linked immunosorbent assays. In this study, HCP from 29 commercially marketed mAb and mAbbased therapeutics were profiled using liquid chromatography (LC)-MS/MS with the identification and relative quantification of 79 individual HCP in total. Excluding an outlier drug, the relative levels of individual HCP determined in the approved therapeutics were generally low, with an average of 20 ppm (µmol HCP/mol drug) measured by LC-MS/MS, and only a few (<7 in average) HCP were identified in each drug analyzed. From this analysis, we also gained knowledge about which HCP are frequently identified in mAb-based products and their typical levels relative to the drugs for the identified individual HCP. In addition, we examined HCP composition from antibodies produced in house and found our current development process brings HCP to levels that are consistent with marketed drugs. Finally, we described a specific case to demonstrate how the HCP information from commercially marketed drugs could inform future HCP analyses.

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Section: Host Cell Proteins In Commercial Biotherapeuticsmentioning

confidence: 99%

Host cell protein profiling of commercial therapeutic protein drugs as a benchmark for monoclonal antibody-based therapeutic protein development

Molden

et al. 2021

mAbs

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“…However, while the global HCP titer may be below the threshold mandated by regulatory agencies, individual HCPs that persist into the drug product can cause specific challenges to product stability or patient safety (Jones et al, 2021; Krutzke et al, 2022; Rane et al, 2019; Valente et al, 2018). Among the potential mechanisms of HCP persistence, product association and co‐elution have received the most attention (Aboulaich et al, 2014; Esser‐Skala et al, 2020; Gilgunn et al, 2019; Levy et al, 2014; Valente et al, 2018). An additional mechanism that has been reported is nonspecific binding of chromatin‐derived complexes, composed of DNA, histones, HCPs, and mAbs, to protein A resins and subsequent co‐elution with the mAb product (Gagnon et al, 2014; Gagnon et al, 2015).…”

Section: Introductionmentioning

confidence: 99%

Characterization and implications of host‐cell protein aggregates in biopharmaceutical processing

Becker

Mendola

et al. 2023

Biotech & Bioengineering

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In the production of biopharmaceuticals such as monoclonal antibodies (mAbs) and vaccines, the residual amounts of host-cell proteins (HCPs) are among the critical quality attributes. In addition to overall HCP levels, individual HCPs may elude purification, potentially causing issues in product stability or patient safety. Such HCP persistence has been attributed mainly to biophysical interactions between individual HCPs and the product, resin media, or residual chromatin particles. Based on measurements on process streams from seven mAb processes, we have found that HCPs in aggregates, not necessarily chromatin-derived, may play a significant role in the persistence of many HCPs. Such aggregates may also hinder accurate detection of HCPs using existing proteomics methods. The findings also highlight that certain HCPs may be difficult to remove because of their functional complementarity to the product; specifically, chaperones and other proteins involved in the unfolded protein response (UPR) are disproportionately present in the aggregates. The methods and findings described here expand our understanding of the origins and potential behavior of HCPs in cell-based biopharmaceutical processes and may be instrumental in improving existing techniques for HCP detection and clearance.

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“…Accordingly, anti-HIV protease as a therapeutic agent invalidates further research [31]. Hence, the present study intended to introduce the Fc tag of the IgG1 antibody as a cell-mediated inducer by selective targeting of the APCs [21,25,[32][33][34][35].…”

Section: Discussionmentioning

confidence: 99%

“…Amongst them, the Fc fusion protein with the receptor binding domain fragment of the virus demonstrated significant immunogenicity and clinical development for the induction and augmentation of neutralising IgG titres [39,40]. Nevertheless, from some studies of FDA-approved Fc fusion drugs [25,29,35] and suitable vaccines against infectious diseases such as Ebola [41], HIV [42], and influenza [43], there have been no efforts to construct Fc fusion vaccines against HTLV-1.…”

Section: Discussionmentioning

confidence: 99%

Development of a Novel HTLV-1 Protease: Human Fcγ1 Recombinant Fusion Molecule in the CHO Eukaryotic Expression System

Ghezeldasht

Heravi

Valizadeh

et al. 2022

Appl Biochem Biotechnol

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Human T-cell leukaemia virus type 1 (HTLV-1) is the causative agent of two life-threatening diseases, adult T cell leukaemia/lymphoma (ATLL), and HTLV-1-associated myelopathy/tropical spastic (HAM/TSP). HTLV-1 protease (HTLV-1-PR) is an aspartic protease that represents a promising target for therapeutic purposes like human immunodeficiency virus-PR inhibitors (HIV-PR). Therefore, in this study, the human Fc fusion recombinant-PR (HTLV-1-PR:hFcγ1) was designed and expressed for two applications, finding a blocking substrate as a potential therapeutic or a potential subunit peptide vaccine. The PCR amplified DNA sequences encoding the HTLV-1-PR from the MT2-cell line using specific primers with restriction enzyme sites of Not1 and Xba1. The construct was then cloned to pTZ57R/T TA plasmid and, after confirming the PR sequence, subcloned into the pDR2ΔEF1α Fc-expression vector to create pDR2ΔEF1α.HTLV-1-PR:hFcγ1. The integrity of recombinant DNA was confirmed by sequencing to ensure that the engineered construct was in the frame. The recombinant fusion protein was then produced in the Chinese hamster ovary cell (CHO) system and was purified from its supernatant using HiTrap-rPA column affinity chromatography. Then, the immunofluorescence assay (IFA) co-localisation method showed that HTLV-1-PR:hFc recombinant fusion protein has appropriate folding as it binds to the anti-Fcγ antibody; the Fcγ1 tag participates to have HTLV-1-PR:hFcγ1 as a dimeric secretory protein. The development and production of HTLV-1-PR can be used to find a blocking substrate as a potential therapeutic molecule and apply it in an animal model to assess its immunogenicity and potential protection against HTLV-1 infection. KeywordsAdult T cell leukaemia/lymphoma (ATLL) • Chinese hamster ovary cell (CHO) expression system • HTLV-1 protease • Human T-cell leukaemia virus type 1 (HTLV-1) • Recombinant Fc-fusion protein * Arman Mosavat

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Exploring sample preparation and data evaluation strategies for enhanced identification of host cell proteins in drug products of therapeutic antibodies and Fc-fusion proteins

Cited by 9 publications

References 55 publications

Host cell protein profiling of commercial therapeutic protein drugs as a benchmark for monoclonal antibody-based therapeutic protein development

Host cell protein profiling of commercial therapeutic protein drugs as a benchmark for monoclonal antibody-based therapeutic protein development

Characterization and implications of host‐cell protein aggregates in biopharmaceutical processing

Development of a Novel HTLV-1 Protease: Human Fcγ1 Recombinant Fusion Molecule in the CHO Eukaryotic Expression System

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