Structure-Activity Relationship of the Dimeric and Oligomeric Forms of a Cytotoxic Biotherapeutic Based on Diphtheria Toxin

Marcin Mielecki; Marcin Ziemniak; Magdalena Ozga; Radosław Borowski; Jarosław Antosik; Angelika Kaczyńska; Beata Pająk

doi:10.3390/biom12081111

Structure-Activity Relationship of the Dimeric and Oligomeric Forms of a Cytotoxic Biotherapeutic Based on Diphtheria Toxin

Biomolecules. 2022 Aug 12;12(8):1111. doi: 10.3390/biom12081111.

Authors

Marcin Mielecki¹, Marcin Ziemniak¹, Magdalena Ozga¹, Radosław Borowski¹, Jarosław Antosik¹, Angelika Kaczyńska¹, Beata Pająk¹

Affiliation

¹ WPD Pharmaceuticals, Żwirki and Wigury 101, 02-089 Warsaw, Poland.

Abstract

Protein aggregation is a well-recognized problem in industrial preparation, including biotherapeutics. These low-energy states constantly compete with a native-like conformation, which is more pronounced in the case of macromolecules of low stability in the solution. A better understanding of the structure and function of such aggregates is generally required for the more rational development of therapeutic proteins, including single-chain fusion cytotoxins to target specific receptors on cancer cells. Here, we identified and purified such particles as side products of the renaturation process of the single-chain fusion cytotoxin, composed of two diphtheria toxin (DT) domains and interleukin 13 (IL-13), and applied various experimental techniques to comprehensively understand their molecular architecture and function. Importantly, we distinguished soluble purified dimeric and fractionated oligomeric particles from aggregates. The oligomers are polydisperse and multimodal, with a distribution favoring lower and even stoichiometries, suggesting they are composed of dimeric building units. Importantly, all these oligomeric particles and the monomer are cystine-dependent as their innate disulfide bonds have structural and functional roles. Their reduction triggers aggregation. Presumably the dimer and lower oligomers represent the metastable state, retaining the native disulfide bond. Although significantly reduced in contrast to the monomer, they preserve some fraction of bioactivity, manifested by their IL-13RA2 receptor affinity and selective cytotoxic potency towards the U-251 glioblastoma cell line. These molecular assemblies probably preserve structural integrity and native-like fold, at least to some extent. As our study demonstrated, the dimeric and oligomeric cytotoxin may be an exciting model protein, introducing a new understanding of its monomeric counterpart's molecular characteristics.

Keywords: IL-13; LC/MS; MALS; SAXS; biotherapeutics; cytotoxin; diphtheria toxin; disulfide bond; inclusion bodies; protein oligomerization; refolding.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Antineoplastic Agents*
Cytotoxins
Diphtheria Toxin* / chemistry
Diphtheria Toxin* / metabolism
Diphtheria Toxin* / toxicity
Disulfides
Macromolecular Substances
Structure-Activity Relationship

Substances

Antineoplastic Agents
Cytotoxins
Diphtheria Toxin
Disulfides
Macromolecular Substances

Grants and funding

This research was co-financed by the European Union from the European Regional Development Fund under the Smart Growth Operational Program 2014-2020. Project is implemented as part of the National Center for Research and Development: Proposal No 5/1.1.1/2017—“Fast track”, Priority I: Support for conducting R&D works by Medium and Small companies and Microenterprises, Sub-measure 1.1.1. Industrial research projects and Experimental development work projects carried out by companies. Contract No: POIR.01.01.01-00-0912/17-00.