Molecular characterization of a family 5 glycoside hydrolase suggests an induced-fit enzymatic mechanism

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作者
Marcelo V. Liberato
Rodrigo L. Silveira
Érica T. Prates
Evandro A. de Araujo
Vanessa O. A. Pellegrini
Cesar M. Camilo
Marco A. Kadowaki
Mario de O. Neto
Alexander Popov
Munir S. Skaf
Igor Polikarpov
机构
[1] São Carlos Institute of Physics,
[2] University of São Paulo,undefined
[3] Institute of Chemistry,undefined
[4] University of Campinas,undefined
[5] Institute of Bioscience,undefined
[6] State University of São Paulo,undefined
[7] European Synchrotron Radiation Facility,undefined
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Glycoside hydrolases (GHs) play fundamental roles in the decomposition of lignocellulosic biomaterials. Here, we report the full-length structure of a cellulase from Bacillus licheniformis (BlCel5B), a member of the GH5 subfamily 4 that is entirely dependent on its two ancillary modules (Ig-like module and CBM46) for catalytic activity. Using X-ray crystallography, small-angle X-ray scattering and molecular dynamics simulations, we propose that the C-terminal CBM46 caps the distal N-terminal catalytic domain (CD) to establish a fully functional active site via a combination of large-scale multidomain conformational selection and induced-fit mechanisms. The Ig-like module is pivoting the packing and unpacking motions of CBM46 relative to CD in the assembly of the binding subsite. This is the first example of a multidomain GH relying on large amplitude motions of the CBM46 for assembly of the catalytically competent form of the enzyme.
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