Aminic Organoselenium Compounds as Glutathione Peroxidase Mimics and Inhibitors of Ferroptosis

Author:

Chhillar Babli1ORCID,Kadian Rajni1ORCID,Kumar Manish1ORCID,Yadav Manisha1ORCID,Sodhi Nikhil1ORCID,Xavier da Silva Thamara Nishida2,Friedmann Angeli Jose Pedro2ORCID,Singh Vijay P.1ORCID

Affiliation:

1. Department of Chemistry & Centre of Advanced Studies in Chemistry Panjab University, Sector-14 Chandigarh 160 014 India

2. Rudolf Virchow Zentrum, Centre for Integrative and Translational Bioimaging, Julius-Maximillian University of Wurzburg 97080 Wurzburg Germany

Abstract

AbstractThe synthesis of diarylamine‐based organoselenium compounds via the nucleophilic substitution reactions has been described. Symmetrical monoselenides and diselenides were conveniently synthesized by the reduction of their corresponding selenocyanates using sodium borohydride. Selenocyanates were obtained from 2‐chloro acetamides by the nucleophilic displacement with potassium selenocyanate. Selenides were synthesized by treating the 2‐chloro acetamides with in situ generated sodium butyl selenolate as nucleophile. Further, the newly synthesized organoselenium compounds were evaluated for their glutathione peroxidase (GPx)‐like activity in thiophenol assay. This study revealed that the methoxy‐substituted organoselenium compounds showed significant effect on the GPx‐like activity. The catalytic parameters for the most efficient catalysts were also determined. The anti‐ferroptotic activity for all GPx‐mimics evaluated in a 4−OH‐tamoxifen (TAM) inducible GPx4 knockout cell line using liproxstatin as standard.

Publisher

Wiley

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