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4DRT

Three dimensional structure of de novo designed serine hydrolase OSH26, Northeast Structural Genomics Consortium (NESG) target OR89

Summary for 4DRT
Entry DOI10.2210/pdb4drt/pdb
Related3MZF
Descriptorde novo designed serine hydrolase, OR89, SODIUM ION, CHLORIDE ION, ... (4 entities in total)
Functional Keywordsstructural genomics, psi-biology, northeast structural genomics consortium, nesg, de novo protein
Biological sourceartificial gene
Total number of polymer chains1
Total formula weight40146.67
Authors
Primary citationRajagopalan, S.,Wang, C.,Yu, K.,Kuzin, A.P.,Richter, F.,Lew, S.,Miklos, A.E.,Matthews, M.L.,Seetharaman, J.,Su, M.,Hunt, J.F.,Cravatt, B.F.,Baker, D.
Design of activated serine-containing catalytic triads with atomic-level accuracy.
Nat.Chem.Biol., 10:386-391, 2014
Cited by
PubMed Abstract: A challenge in the computational design of enzymes is that multiple properties, including substrate binding, transition state stabilization and product release, must be simultaneously optimized, and this has limited the absolute activity of successful designs. Here, we focus on a single critical property of many enzymes: the nucleophilicity of an active site residue that initiates catalysis. We design proteins with idealized serine-containing catalytic triads and assess their nucleophilicity directly in native biological systems using activity-based organophosphate probes. Crystal structures of the most successful designs show unprecedented agreement with computational models, including extensive hydrogen bonding networks between the catalytic triad (or quartet) residues, and mutagenesis experiments demonstrate that these networks are critical for serine activation and organophosphate reactivity. Following optimization by yeast display, the designs react with organophosphate probes at rates comparable to natural serine hydrolases. Co-crystal structures with diisopropyl fluorophosphate bound to the serine nucleophile suggest that the designs could provide the basis for a new class of organophosphate capture agents.
PubMed: 24705591
DOI: 10.1038/nchembio.1498
PDB entries with the same primary citation
Experimental method
X-RAY DIFFRACTION (2.002 Å)
Structure validation

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