A combination of spin diffusion methods for the determination of protein-ligand 
complex structural ensembles.

Pilger, J.; Mazur, A.; Monecke, P.; Schreuder, H.; Elshorst, B.; Bartoschek, S.; Langer, T; Schiffer, A.; Krimm, I.; Wegstroht, M.; Lee, D.; Hessler, G.; Wendt, K. U.; Becker, S.; Griesinger, C.

doi:10.1002/anie.201500671

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A combination of spin diffusion methods for the determination of protein-ligand complex structural ensembles.

MPS-Authors

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Pilger, J.
Department of NMR Based Structural Biology, MPI for biophysical chemistry, Max Planck Society;

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Mazur, A.
Department of NMR Based Structural Biology, MPI for biophysical chemistry, Max Planck Society;

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Wegstroht, M.
Department of NMR Based Structural Biology, MPI for biophysical chemistry, Max Planck Society;

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Lee, D.
Department of NMR Based Structural Biology, MPI for biophysical chemistry, Max Planck Society;

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Becker, S.
Department of NMR Based Structural Biology, MPI for biophysical chemistry, Max Planck Society;

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Griesinger, C.
Department of NMR Based Structural Biology, MPI for biophysical chemistry, Max Planck Society;

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2149624_Suppl.pdf
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Citation

Pilger, J., Mazur, A., Monecke, P., Schreuder, H., Elshorst, B., Bartoschek, S., et al. (2015). A combination of spin diffusion methods for the determination of protein-ligand complex structural ensembles. Angewandte Chemie International Edition, 54(22), 6511-6515. doi:10.1002/anie.201500671.

Cite as: https://hdl.handle.net/11858/00-001M-0000-0026-C6DA-1

Abstract

Structure-based drug design (SBDD) is a powerful and widely used approach to optimize affinity of drug candidates. With the recently introduced INPHARMA method, the binding mode of small molecules to their protein target can be characterized even if no spectroscopic information about the protein is known. Here, we show that the combination of the spin-diffusion-based NMR methods INPHARMA, trNOE, and STD results in an accurate scoring function for docking modes and therefore determination of protein-ligand complex structures. Applications are shown on the model system protein kinase A and the drug targets glycogen phosphorylase and soluble epoxide hydrolase (sEH). Multiplexing of several ligands improves the reliability of the scoring function further. The new score allows in the case of sEH detecting two binding modes of the ligand in its binding site, which was corroborated by X-ray analysis.