Improving the Stability of Maleimide-Thiol Conjugation for Drug Targeting

Marianne Lahnsteiner; Alexander Kastner; Josef Mayr; Alexander Roller; Bernhard K Keppler; Christian R Kowol

doi:10.1002/chem.202003951

Improving the Stability of Maleimide-Thiol Conjugation for Drug Targeting

Chemistry. 2020 Dec 4;26(68):15867-15870. doi: 10.1002/chem.202003951. Epub 2020 Oct 27.

Authors

Marianne Lahnsteiner¹, Alexander Kastner¹, Josef Mayr¹, Alexander Roller¹, Bernhard K Keppler^{1

2}, Christian R Kowol^{1

2}

Affiliations

¹ Faculty of Chemistry, Institute of Inorganic Chemistry, University of Vienna, Waehringer Strasse 42, 1090, Vienna, Austria.
² Research Cluster "Translational Cancer Therapy Research", Waehringer Strasse 42, 1090, Vienna, Austria.

Abstract

Maleimides are essential compounds for drug conjugation reactions via thiols to antibodies, peptides and other targeting units. However, one main drawback is the occurrence of thiol exchange reactions with, for example, glutathione resulting in loss of the targeting ability. A new strategy to overcome such retro-Michael exchange processes of maleimide-thiol conjugates by stabilization of the thiosuccinimide via a transcyclization reaction is presented. This reaction enables the straightforward synthesis of stable maleimide-thiol adducts essential in drug-conjugation applications.

Keywords: bioconjugation; bioorganic chemistry; drug delivery; maleimide; retro-Michael reactions.

MeSH terms

Cyclization
Drug Delivery Systems
Drug Stability
Immunoconjugates* / chemistry
Maleimides* / chemistry
Succinimides / chemistry
Sulfhydryl Compounds* / chemistry

Substances

Immunoconjugates
Maleimides
Succinimides
Sulfhydryl Compounds

Grants and funding

AP32886/Austrian Science Fund