Electron-rich anilines as cleavable linkers for peptides

Andrew M Watts; Caitlyn J Hughes; Gavin A Clausen; Pamira Yanar; Evan J Wolff; Phoebe R Rubio; Natalie M Stuart; Christopher R Shugrue

doi:10.1016/j.bioorg.2024.108084

Electron-rich anilines as cleavable linkers for peptides

Bioorg Chem. 2025 Jan:154:108084. doi: 10.1016/j.bioorg.2024.108084. Epub 2024 Dec 25.

Authors

Andrew M Watts¹, Caitlyn J Hughes¹, Gavin A Clausen¹, Pamira Yanar¹, Evan J Wolff¹, Phoebe R Rubio¹, Natalie M Stuart¹, Christopher R Shugrue²

Affiliations

¹ Department of Chemistry, University of Richmond, Gottwald Science Center, B-100 138 UR Drive, Richmond, VA 23173, United States.
² Department of Chemistry, University of Richmond, Gottwald Science Center, B-100 138 UR Drive, Richmond, VA 23173, United States. Electronic address: [email protected].

PMID: 39753039
DOI: 10.1016/j.bioorg.2024.108084

Abstract

We report the development of a new electron-rich aniline (ERA)-based cleavable linker. Anilines can be incorporated into peptides during SPPS and are stable to most reaction conditions. ERA-containing peptides can be cleaved rapidly in the presence of oxidants, such as DDQ, CAN, and NaIO₄, in 30 min at room temperature. The compatibility of these conditions is demonstrated on peptides containing natural and unnatural amino acids. While the cleavages of other oxidatively labile linkers is known to cause decomposition of Tyr and Trp, these sensitive residues are stable to DDQ oxidations. An ERA-linker also enables the capture and release of a biotinylated peptide from immobilized streptavidin. ERA-linkers may serve as an excellent tool for peptide library screening applications.

Keywords: Affinity capture; Aniline; Cleavable linker; Oxidation; Peptides.

MeSH terms

Aniline Compounds* / chemical synthesis
Aniline Compounds* / chemistry
Electrons*
Molecular Structure
Peptides* / chemical synthesis
Peptides* / chemistry

Substances

Aniline Compounds
Peptides
aniline