Exp Clin Endocrinol Diabetes 2020; 128(06/07): 375-378
DOI: 10.1055/a-1022-9916
Mini-Review

Structure and Mechanism of Iodothyronine Deiodinases – What We Know, What We Don’t Know, and What Would Be Nice to Know

Clemens Steegborn
1   Lehrstuhl Biochemie, Universität Bayreuth, Bayreuth, Germany
,
Ulrich Schweizer
2   Institut für Biochemie und Molekularbiologie, Rheinische Friedrich-Wilhelms-Universität Bonn, Bonn, Germany
› Author Affiliations

Abstract

Deiodinases catalyze the specific removal of iodine atoms from one of the two iodinated phenyl rings in iodothyronines. They thereby fine-regulate local thyroid hormone concentrations in organs or cells. The chemical reaction is unique in the sense that in metazoans the reductive elimination of iodide depends on the rare amino acid selenocysteine in the enzymes’ active centers. While there is no prokaryotic homologue of such deiodinases, the solution of the crystal structure of a catalytic domain of mouse deiodinase 3 has revealed that the ancient peroxiredoxin structure has been repurposed, and improved using selenocysteine, as a deiodinase during metazoan evolution. Likewise, many biochemical findings obtained over decades can now be interpreted in light of the molecular structure. Despite this leap in our understanding of deiodinase structure, there are still several open questions that need to be addressed in order to fully understand substrate binding, catalytic mechanism, and regulation of deiodinases. We surmise that these issues as well as differences between the three highly homologous isoenzymes must be understood in order to develop modulators of deiodinases that could be valuable in clinical use.



Publication History

Received: 27 August 2019
Received: 25 September 2019

Accepted: 07 October 2019

Article published online:
07 November 2019

© Georg Thieme Verlag KG
Stuttgart · New York

 
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