Steric and stereoscopic disulfide construction for cross-linkage via N-dithiophthalimides

Wen-Chao Gao; Jun Tian; Yu-Zhu Shang; Xuefeng Jiang

doi:10.1039/d0sc01060j

Steric and stereoscopic disulfide construction for cross-linkage via N-dithiophthalimides

Chem Sci. 2020 Mar 20;11(15):3903-3908. doi: 10.1039/d0sc01060j.

Authors

Wen-Chao Gao^{1

2}, Jun Tian², Yu-Zhu Shang², Xuefeng Jiang^{1

3}

Affiliations

¹ Shanghai Key Laboratory of Green Chemistry and Chemical Process, Department of Chemistry, East China Normal University Shanghai 200062 P. R. China xfjiang@chem.ecnu.edu.cn.
² College of Biomedical Engineering, Taiyuan University of Technology Taiyuan 030024 P. R. China.
³ State Key Laboratory of Organometallic Chemistry, Shanghai Institute of Organic Chemistry Shanghai 200032 P. R. China.

Abstract

Disulfide bonds are a significant motif in life and drug-delivery systems. In particular, steric hindrance and stereoscopic disulfide linkers are closely associated with the stability of antibody-drug conjugates, which affects the potency, selectivity, and pharmacokinetics of drugs. However, limited availability and diversity of tertiary thiols impede the construction of steric and stereoscopic disulfides for cross-linkage in biochemistry and pharmaceuticals. Through modulating the mask effect of disulfurating reagents, we develop a facile and robust strategy for construction of diverse steric and stereoscopic disulfides via N-dithiophthalimides. The practical cross-linkage of biomolecules including amino acids, saccharides, and nucleosides with different drugs and fluorescent molecules is successfully established through hindered disulfide linkers.