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[摘要]:Sil1 functions as a NEF (nucleotide-exchange factor) for the ER (endoplasmic reticulum) Hsp70 (heat-shock protein of 70 kDa) Bip in eukaryotic cells. Sill may catalyse the ADP release from Bip by interacting directly with the ATPase domain of Bip. In the present study we show the complex crystal structure of the yeast Bip and the NEF Sil1 at the resolution of 2.3 angstrom (1 angstrom = 0.1 nm). In the Sil1-Bip complex structure, the Sil1 molecule acts as a 'clamp' which binds lobe IIb of the Bip ATPase domain. The binding of Sil1 causes the rotation of lobe Ilb similar to 13.5 degrees away from the ADP-binding pocket. The complex formation also induces lobe Ib to swing in the opposite direction by similar to 3.7 degrees. These conformational changes open up the nucleotide-binding pocket in the Bip ATPase domain and disrupt the hydrogen bonds between Bip and bound ADP, which may catalyse ADP release. Mutation of the Sill residues involved in binding the Bip ATPase domain compromise the binding affinity of Sill to Bip, and these Sil1 mutants also abolish the ability to stimulate the ATPase activity of Bip. |
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