Bioorthogonal Delivery of Carbon Disulfide in Living Cells

Author:

Zhao Ruohan1,Chen Yinghan1,Liang Yong1ORCID

Affiliation:

1. State Key Laboratory of Coordination Chemistry Jiangsu Key Laboratory of Advanced Organic Materials Chemistry and Biomedicine Innovation Center School of Chemistry and Chemical Engineering Nanjing University Nanjing 210023 China

Abstract

AbstractCarbon disulfide (CS2) is an environmental contaminant, which is deadly hazardous to the workers under chronic or acute exposure. However, the toxicity mechanisms of CS2 are still unclear due to the scarcity of biocompatible donors, which can release CS2 in cells. Here we developed the first bioorthogonal CS2 delivery system based on the “click‐and‐release” reactions between mesoionic 1,3‐thiazolium‐5‐thiolates (TATs) and strained cyclooctyne exo‐BCN‐OH. We successfully realized intracellular CS2 release and investigated the causes of CS2‐induced hepatotoxicity, including oxidative stress, proteotoxic stress and copper‐dependent cell death. It is found that CS2 can be copper vehicles bypassing copper transporters after reacting with nucleophiles in cytoplasm, and extra copper supplementation will exacerbate the loss of homeostasis of cells and ultimately cell death. These findings inspired us to explore the anticancer activity of CS2 in combination with copper by introducing a copper chelating group in our CS2 delivery system.

Funder

National Natural Science Foundation of China

Publisher

Wiley

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