Torpedo californica acetylcholinesterase with bifunctional inhibitor
From Proteopedia
Conformational flexibility in the peripheral site of Torpedo californica acetylecholinesterase revealed by the complex structure with a bifunctional inhibitor
Contents |
Overview
The X-ray crystallographic structure of Torpedo californica acetylcholinesterase (TcAChE) in complex with the bifunctional inhibitor NF595, a potentially new anti-Alzheimer drug, has been solved. For the first time in TcAChE, a major conformational change in the peripheral-site tryptophan residue is observed upon complexation. The observed conformational flexibility highlights the dynamic nature of protein structures and is of importance for structure-based drug design.
About this Structure
2CEK is a Single protein structure of sequence from Torpedo californica with , , , and as ligands. Active as acetylcholinesterase, with EC number 3.1.1.7 Known structural/functional Site: . Full crystallographic information is available from OCA.
Down the gorge
binds both the active and peripheral sites. It is mainly bound to through pi-pi interactions. The n-carbon long linker spans the gorge.
Reference
Conformational flexibility in the peripheral site of Torpedo californica acetylcholinesterase revealed by the complex structure with a bifunctional inhibitor., Colletier JP, Sanson B, Nachon F, Gabellieri E, Fattorusso C, Campiani G, Weik M, J Am Chem Soc. 2006 Apr 12;128(14):4526-7. PMID:16594661
Created with the participation of Eran Hodis, Jaime Prilusky.
Categories: Acetylcholinesterase | Single protein | Torpedo californica | Campiani, G. | Colletier, J P. | Fattorusso, C. | Gabellieri, E. | Nachon, F. | Sanson, B. | Weik, M. | MES | N8T | NAG | NDG | PGE | Alpha/beta hydrolase | Alternative splicing | Alzheimer disease | Conformational flexibility | Glycoprotein | Gpi-anchor | Hydrolase | Lipoprotein | Neurotransmitter cleavage | Neurotransmitter degradation | Serine esterase | Synapse | Synapse membrane
