Predicting 19F NMR Chemical Shifts: A Combined Computational and Experimental Study of a Trypanosomal Oxidoreductase

6533b7d5fe1ef96bd12648a4

RESEARCH PRODUCT

Predicting 19F NMR Chemical Shifts: A Combined Computational and Experimental Study of a Trypanosomal Oxidoreductase–Inhibitor Complex

Annika Wagner Annika Wagner Johannes C. B. Dietschreit Bernd Engels Ute A. Hellmich Ute A. Hellmich Hermann Schindelin Christian Ochsenfeld Christian Ochsenfeld T. Anh Le Till Opatz Philipp Klein

subject

Trypanosoma brucei brucei Protozoan Proteins Context (language use)Pyrimidinones Thiophenes 010402 general chemistry 01 natural sciences Catalysis quantum chemistry Thioredoxins NMR spectroscopy Computational chemistry Oxidoreductase structural biology Enzyme Inhibitors Nuclear Magnetic Resonance Biomolecular chemistry.chemical_classification African sleeping sickness 010405 organic chemistry Chemistry Chemical shift Communication General Chemistry Nuclear magnetic resonance spectroscopy Fluorine Oxidoreductase inhibitor Ligand (biochemistry)Trypanocidal Agents Communications 0104 chemical sciences Structural biology Covalent bond ddc:540 Mutation covalent inhibitors Protein Binding

description

Abstract The absence of fluorine from most biomolecules renders it an excellent probe for NMR spectroscopy to monitor inhibitor–protein interactions. However, predicting the binding mode of a fluorinated ligand from a chemical shift (or vice versa) has been challenging due to the high electron density of the fluorine atom. Nonetheless, reliable 19F chemical‐shift predictions to deduce ligand‐binding modes hold great potential for in silico drug design. Herein, we present a systematic QM/MM study to predict the 19F NMR chemical shifts of a covalently bound fluorinated inhibitor to the essential oxidoreductase tryparedoxin (Tpx) from African trypanosomes, the causative agent of African sleeping sickness. We include many protein–inhibitor conformations as well as monomeric and dimeric inhibitor–protein complexes, thus rendering it the largest computational study on chemical shifts of 19F nuclei in a biological context to date. Our predicted shifts agree well with those obtained experimentally and pave the way for future work in this area.

year	journal	country	edition	language
2020-05-25	Angewandte Chemie (International Ed. in English)

10.1002/anie.202000539 http://europepmc.org/articles/PMC7496126