1. Biocatalytic control of site-selectivity and chain length-selectivity in radical amino acid halogenases.
- Author
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Kissman EN, Neugebauer ME, Sumida KH, Swenson CV, Sambold NA, Marchand JA, Millar DC, and Chang MCY
- Subjects
- Halogenation, Ornithine, Amino Acids, Lysine
- Abstract
Biocatalytic C-H activation has the potential to merge enzymatic and synthetic strategies for bond formation. Fe
II /αKG-dependent halogenases are particularly distinguished for their ability both to control selective C-H activation as well as to direct group transfer of a bound anion along a reaction axis separate from oxygen rebound, enabling the development of new transformations. In this context, we elucidate the basis for the selectivity of enzymes that perform selective halogenation to yield 4-Cl-lysine (BesD), 5-Cl-lysine (HalB), and 4-Cl-ornithine (HalD), allowing us to probe how site-selectivity and chain length selectivity are achieved. We now report the crystal structure of the HalB and HalD, revealing the key role of the substrate-binding lid in positioning the substrate for C4 vs C5 chlorination and recognition of lysine vs ornithine. Targeted engineering of the substrate-binding lid further demonstrates that these selectivities can be altered or switched, showcasing the potential to develop halogenases for biocatalytic applications.- Published
- 2023
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