2012.05.16�����,我院陳宇星教授研究組和周叢照教授研究組合作在Journal of Biological Chemistry上在線發(fā)表論文:Structural insights into the substrate specificity of Streptococcus pneumoniae β(1,3) galactosidase BgaC. published May 16, 2012 as doi:10.1074/jbc.M112.367128.
作? 者:成望#�����、王雷#、江永亮�、柏曉輝、儲俊�����、李瓊�、于歌、梁秋玲�����、周叢照*��、陳宇星*����。(#共第一作者)
Abstract:
The surface-exposed β-galactosidase BgaC from Streptococcus pneumoniae was reported to be a virulence factor because of its specific hydrolysis activity towards the β(1,3)-linked galactose and N-acetylglucosamine [Galβ(1,3)NAG] moiety of oligosaccharides on the host molecules. Here we report the crystal structure of BgaC at 1.8 ? and its complex with galactose at 1.95 ?. At pH 5.5 to 8.0, BgaC exists as a stable homodimer, each subunit of which consists of three distinct domains: a catalytic domain of a classic (β/α)8 TIM barrel, followed by two all-β domains (ABDs) of unknown function. The side-walls of the TIM β-barrel and a loop extended from the first ABD constitute the active site. Superposition of the galactose-complexed structure to the apo-form revealed significant conformational changes of residues Trp243 and Tyr455. Simulation of a putative substrate entrance tunnel and modeling of a complex structure with Galβ(1,3)NAG enabled us to assign three key residues to the specific catalysis. Site-directed mutagenesis in combination with activity assays further proved that residues Trp240 and Tyr455 contribute to stabilizing the N-acetylglucosamine moiety, whereas Trp243 is critical for fixing the galactose ring. Moreover, we propose that BgaC and other galactosidases in the GH-35 family share a common domain organization and a conserved substrate-determinant aromatic residue protruding from the second domain.
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