The ability to specifically label the sulphide ions of protein-bound iron-sulphur (FeS) clusters with S isotope greatly facilitates structure-function studies. In particular, it provides insight when using either spectroscopic techniques that probe cluster-associated vibrations, or non-denaturing mass spectrometry, where the ∼+2 Da average increase per sulphide enables unambiguous assignment of the FeS cluster and, where relevant, its conversion/degradation products. Here, we employ a thermostable homologue of the -acetyl-l-serine sulfhydrylase CysK to generate S-substituted l-cysteine and subsequently use it as a substrate for the l-cysteine desulfurase NifS to gradually supply S for FeS cluster assembly in an otherwise standard cluster reconstitution protocol.
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| http://dx.doi.org/10.1093/biomethods/bpy015 | DOI Listing |
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