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F-NMR reveals substrate specificity of CYP121A1 in Mycobacterium tuberculosis

J Biol Chem. 2021-10; 
Christopher S Campomizzi, George E Ghanatios, D Fernando Estrada
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摘要

Cytochromes P450 are versatile enzymes that function in endobiotic and xenobiotic metabolism and undergo meaningful structural changes that relate to their function. However, the way in which conformational changes inform the specific recognition of the substrate is often unknown. Here, we demonstrate the utility of fluorine (F)-NMR spectroscopy to monitor structural changes in CYP121A1, an essential enzyme from Mycobacterium tuberculosis. CYP121A1 forms functional dimers that catalyze the phenol-coupling reaction of the dipeptide dicyclotyrosine. The thiol-reactive compound 3-bromo-1,1,1-trifluoroacetone was used to label an S171C mutation of the enzyme FG loop, which is located adjacent to the homodimer inter... More

关键词

CYP121A1, Cytochrome P450, NMR