Litcius/Paper detail

Exhaustive search of the configurational space of heat‐shock protein 90 with its inhibitor by multicanonical molecular dynamics based dynamic docking

Gert‐Jan Bekker, Mitsugu Araki, Kanji Oshima, Yasushi Okuno, Narutoshi Kamiya

2020Journal of Computational Chemistry31 citationsDOI

Abstract

Multicanonical molecular dynamics based dynamic docking was used to exhaustively search the configurational space of an inhibitor binding to the N-terminal domain of heat-shock protein 90 (Hsp90). The obtained structures at 300 K cover a wide structural ensemble, with the top two clusters ranked by their free energy coinciding with the native binding site. The representative structure of the most stable cluster reproduced the experimental binding configuration, but an interesting conformational change in Hsp90 could be observed. The combined effects of solvation and ligand binding shift the equilibrium from a preferred loop-in conformation in the unbound state to an α-helical one in the bound state for the flexible lid region of Hsp90. Thus, our dynamic docking method is effective at predicting the native binding site while exhaustively sampling a wide configurational space, modulating the protein structure upon binding.

Topics & Concepts

Molecular dynamicsDocking (animal)ChemistrySolvationBinding siteImplicit solvationBinding energyComputational chemistryPhysicsMoleculeBiochemistryMedicineNuclear physicsNursingOrganic chemistryProtein Structure and DynamicsHeat shock proteins researchEnzyme Structure and Function