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- W2981188561 endingPage "5106" @default.
- W2981188561 startingPage "5106" @default.
- W2981188561 abstract "The spatiotemporal control of enzymes by light is of growing importance for industrial biocatalysis. Within this context, the photo-control of allosteric interactions in enzyme complexes, common to practically all metabolic pathways, is particularly relevant. A prominent example of a metabolic complex with a high application potential is tryptophan synthase from Salmonella typhimurium (TS), in which the constituting TrpA and TrpB subunits mutually stimulate each other via a sophisticated allosteric network. To control TS allostery with light, we incorporated the unnatural amino acid o-nitrobenzyl-O-tyrosine (ONBY) at seven strategic positions of TrpA and TrpB. Initial screening experiments showed that ONBY in position 58 of TrpA (aL58ONBY) inhibits TS activity most effectively. Upon UV irradiation, ONBY decages to tyrosine, largely restoring the capacity of TS. Biochemical characterization, extensive steady-state enzyme kinetics, and titration studies uncovered the impact of aL58ONBY on the activities of TrpA and TrpB and identified reaction conditions under which the influence of ONBY decaging on allostery reaches its full potential. By applying those optimal conditions, we succeeded to directly light-activate TS(aL58ONBY) by a factor of ~100. Our findings show that rational protein design with a photo-sensitive unnatural amino acid combined with extensive enzymology is a powerful tool to fine-tune allosteric light-activation of a central metabolic enzyme complex." @default.
- W2981188561 created "2019-10-25" @default.
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- W2981188561 date "2019-10-15" @default.
- W2981188561 modified "2023-09-23" @default.
- W2981188561 title "Light-Regulation of Tryptophan Synthase by Combining Protein Design and Enzymology" @default.
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- W2981188561 doi "https://doi.org/10.3390/ijms20205106" @default.
- W2981188561 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6829457" @default.
- W2981188561 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/31618845" @default.