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6EQ6

MTH1 in complex with fragment 1

Summary for 6EQ6
Entry DOI10.2210/pdb6eq6/pdb
Descriptor7,8-dihydro-8-oxoguanine triphosphatase, 3-pyrrolidin-1-ylquinoxalin-2-amine, ACETATE ION, ... (5 entities in total)
Functional Keywordsinhibitor, complex, hydrolase, dna repair, fragment
Biological sourceHomo sapiens (Human)
Total number of polymer chains1
Total formula weight21474.30
Authors
Wiedmer, L.,Sledz, P.,Caflisch, A. (deposition date: 2017-10-12, release date: 2018-10-31, Last modification date: 2024-05-08)
Primary citationWiedmer, L.,Scharer, C.,Spiliotopoulos, D.,Hurzeler, M.,Sledz, P.,Caflisch, A.
Ligand retargeting by binding site analogy.
Eur.J.Med.Chem., 175:107-113, 2019
Cited by
PubMed Abstract: The DNA-repair enzyme MutT homolog 1 (MTH1) is a potential target for a broad range of tumors. Its substrate binding site features a non-catalytical pair of aspartic acids which resembles the catalytic dyad of aspartic proteases. We hypothesized that inhibitors of the latter might be re-targeted for MTH1 despite the two enzyme classes having different substrates and catalyze different reactions. We selected from the crystal structures of holo aspartic proteases a library of nearly 350 inhibitors for in silico screening. Three fragment hits were identified by docking and scoring according to a force field-based energy with continuum dielectric solvation. These fragments showed good ligand efficiency in a colorimetric assay (MW <300 Da and IC<50μM). Molecular dynamics simulations were carried out for determining the most favorable interaction patterns. On the basis of the simulation results we evaluated in vitro seven commercially available compounds, two of which showed submicromolar potency for MTH1. To obtain definitive evidence of the predicted binding modes we solved the crystal structures of five of the 10 inhibitors predicted in silico. The final step of hit optimization was guided by protein crystallography and involved the synthesis of a single compound, the lead 11, which shows nanomolar affinity for MTH1 in two orthogonal binding assays, and selectivity higher than 2000-fold against its original target (BACE1). The high rate of fragment-hit identification and the fast optimization suggest that ligand retargeting by binding site analogy is an efficient strategy for drug design.
PubMed: 31077996
DOI: 10.1016/j.ejmech.2019.04.037
PDB entries with the same primary citation
Experimental method
X-RAY DIFFRACTION (2.002 Å)
Structure validation

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数据于2024-11-06公开中

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