Author/Authors :
Jinzhi Tan، نويسنده , , Koen HG Verschueren، نويسنده , , Kanchan Anand، نويسنده , , Jianhua Shen، نويسنده , , Maojun Yang، نويسنده , , Yechun Xu، نويسنده , , Zihe Rao، نويسنده , , Janna Bigalke، نويسنده , , Burkhard Heisen، نويسنده , , Jeroen R. Mesters، نويسنده , , KaiXian Chen، نويسنده , , Xu Shen، نويسنده , , Hualiang Jiang and Helmut Grubmüller، نويسنده , , Rolf Hilgenfeld، نويسنده ,
Abstract :
The SARS coronavirus main proteinase (Mpro) is a key enzyme in the processing of the viral polyproteins and thus an attractive target for the discovery of drugs directed against SARS. The enzyme has been shown by X-ray crystallography to undergo significant pH-dependent conformational changes. Here, we assess the conformational flexibility of the Mpro by analysis of multiple crystal structures (including two new crystal forms) and by molecular dynamics (MD) calculations. The MD simulations take into account the different protonation states of two histidine residues in the substrate-binding site and explain the pH-activity profile of the enzyme. The low enzymatic activity of the Mpro monomer and the need for dimerization are also discussed.
Keywords :
SARS-CoV Mpro , Molecular dynamics simulation , conformational flexibility , new crystal forms , multiple X-ray structures
