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Detection of host cell microprotein impurities in antibody drug products
Date Issued
2024-10-04
Date Available
2026-01-19T09:52:53Z
Abstract
Chinese hamster ovary (CHO) cells are used to produce almost 90% of therapeutic monoclonal antibodies (mAbs) and antibody fusion proteins (Fc-fusion). The annotation of non-canonical translation events in these cellular factories remains incomplete, limiting our ability to study CHO cell biology and detect host cell protein (HCP) impurities in the final antibody drug product. We utilised ribosome footprint profiling (Ribo-seq) to identify novel open reading frames (ORFs) including N-terminal extensions and thousands of short ORFs (sORFs) predicted to encode microproteins. Mass spectrometry-based HCP analysis of eight commercial antibody drug products (7 mAbs and 1 Fc-fusion protein) using the extended protein sequence database revealed the presence of microprotein impurities. We present evidence that microprotein abundance varies with growth phase and can be affected by the cell culture environment. In addition, our work provides a vital resource to facilitate future studies of non-canonical translation and the regulation of protein synthesis in CHO cell lines.
Sponsorship
Science Foundation Ireland
Type of Material
Journal Article
Publisher
Springer
Journal
Nature Communications
Volume
15
Issue
1
Copyright (Published Version)
2024 the Authors
Subjects
Language
English
Status of Item
Peer reviewed
ISSN
2041-1723
This item is made available under a Creative Commons License
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Name
Detection of host cell microprotein impurities in antibody drug products.pdf
Size
2.55 MB
Format
Adobe PDF
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