Cyclic 5-membered disulfides are not selective substrates of thioredoxin reductase, but are opened nonspecifically

Author:

Felber Jan G.ORCID,Poczka Lena,Scholzen Karoline C.ORCID,Zeisel LukasORCID,Maier Martin S.,Busker Sander,Theisen UlrikeORCID,Brandstädter Christina,Becker Katja,Arnér Elias S. J.ORCID,Thorn-Seshold JuliaORCID,Thorn-Seshold OliverORCID

Abstract

AbstractThe cyclic five-membered disulfide 1,2-dithiolane has been widely used in chemical biology and in redox probes. Contradictory reports have described it either as nonspecifically reduced in cells, or else as a highly specific substrate for thioredoxin reductase (TrxR). Here we show that 1,2-dithiolane probes, such as “TRFS” probes, are nonspecifically reduced by thiol reductants and redox-active proteins, and their cellular performance is barely affected by TrxR inhibition or knockout. Therefore, results of cellular imaging or inhibitor screening using 1,2-dithiolanes should not be interpreted as reflecting TrxR activity, and previous studies may need re-evaluation. To understand 1,2-dithiolanes’ complex behaviour, probe localisation, environment-dependent fluorescence, reduction-independent ring-opening polymerisation, and thiol-dependent cellular uptake must all be considered; particular caution is needed when co-applying thiophilic inhibitors. We present a general approach controlling against assay misinterpretation with reducible probes, to ensure future TrxR-targeted designs are robustly evaluated for selectivity, and to better orient future research.

Funder

Studienstiftung des deutschen Volkes

GRK 2338 PhD scholarship

Kekulé-scholarship of Fond der chemischen Industrie, Germany

Deutsche Forschungsgemeinschaft

Joachim-Hertz Foundation fellowship

Publisher

Springer Science and Business Media LLC

Subject

General Physics and Astronomy,General Biochemistry, Genetics and Molecular Biology,General Chemistry,Multidisciplinary

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