Literature DB >> 26514585

Rational design of therapeutic mAbs against aggregation through protein engineering and incorporation of glycosylation motifs applied to bevacizumab.

Fabienne Courtois1, Neeraj J Agrawal1, Timothy M Lauer1, Bernhardt L Trout1.   

Abstract

The aggregation of biotherapeutics is a major hindrance to the development of successful drug candidates; however, the propensity to aggregate is often identified too late in the development phase to permit modification to the protein's sequence. Incorporating rational design for the stability of proteins in early discovery has numerous benefits. We engineered out aggregation-prone regions on the Fab domain of a therapeutic monoclonal antibody, bevacizumab, to rationally design a biobetter drug candidate. With the purpose of stabilizing bevacizumab with respect to aggregation, 2 strategies were undertaken: single point mutations of aggregation-prone residues and engineering a glycosylation site near aggregation-prone residues to mask these residues with a carbohydrate moiety. Both of these approaches lead to comparable decreases in aggregation, with an up to 4-fold reduction in monomer loss. These single mutations and the new glycosylation pattern of the Fab domain do not modify binding to the target. Biobetters with increased stability against aggregation can therefore be generated in a rational manner, by either removing or masking the aggregation-prone region or crowding out protein-protein interactions.

Entities:  

Keywords:  aggregation; bevacizumab; biobetter; glycosylation; monoclonal antibody; protein engineering; spatial aggregation propensity; stability

Mesh:

Substances:

Year:  2016        PMID: 26514585      PMCID: PMC4966521          DOI: 10.1080/19420862.2015.1112477

Source DB:  PubMed          Journal:  MAbs        ISSN: 1942-0862            Impact factor:   5.857


  69 in total

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2.  Glycosylation influences on the aggregation propensity of therapeutic monoclonal antibodies.

Authors:  Veysel Kayser; Naresh Chennamsetty; Vladimir Voynov; Kurt Forrer; Bernhard Helk; Bernhardt L Trout
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6.  Capability measurement of size-exclusion chromatography with a light-scattering detection method in a stability study of bevacizumab using the process capability indices.

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Review 5.  Technological Microbiology: Development and Applications.

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Journal:  Front Microbiol       Date:  2017-05-10       Impact factor: 5.640

6.  Variable Domain N-Linked Glycans Acquired During Antigen-Specific Immune Responses Can Contribute to Immunoglobulin G Antibody Stability.

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7.  Web-based display of protein surface and pH-dependent properties for assessing the developability of biotherapeutics.

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8.  Aggrescan3D (A3D) 2.0: prediction and engineering of protein solubility.

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9.  De Novo Sequencing and Resurrection of a Human Astrovirus-Neutralizing Antibody.

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10.  Predicting B cell receptor substitution profiles using public repertoire data.

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Journal:  PLoS Comput Biol       Date:  2018-10-17       Impact factor: 4.475

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