Al-Rashid_2015_Bioorg.Med.Chem.Lett_25_4848

Reference

Title : A computational view on the significance of E-ring in binding of (+)-arisugacin A to acetylcholinesterase - Al-Rashid_2015_Bioorg.Med.Chem.Lett_25_4848
Author(s) : Al-Rashid ZF , Hsung RP
Ref : Bioorganic & Medicinal Chemistry Lett , 25 :4848 , 2015
Abstract :

A computational docking study of a series of de novo structural analogs of the highly potent, non-nitrogen containing, acetylcholinesterase inhibitor (+)-arisugacin A is presented. In direct comparison to the recently reported X-ray single-crystal structure of (+)-territrem B bound hAChE, the modeling suggests that there is a unique conformational preference for the E-ring that is responsible for the superior inhibitory activity of (+)-arisugacin A against hAChE relative to (+)-territrem B, and that substitutions on the E-ring also play an important role in the protein-ligand interaction.

PubMedSearch : Al-Rashid_2015_Bioorg.Med.Chem.Lett_25_4848
PubMedID: 26159481

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Citations formats

Al-Rashid ZF, Hsung RP (2015)
A computational view on the significance of E-ring in binding of (+)-arisugacin A to acetylcholinesterase
Bioorganic & Medicinal Chemistry Lett 25 :4848

Al-Rashid ZF, Hsung RP (2015)
Bioorganic & Medicinal Chemistry Lett 25 :4848