標題: | Identification of Essential Residues of Human alpha-L-Fucosidase and Tests of Its Mechanism |
作者: | Liu, Sheng-Wen Chen, Chao-Sheng Chang, Shih-Shen Mong, Kwok-Kong Tony Lin, Chun-Hung Chang, Cheng-Wen Tang, Chuan Yi Li, Yaw-Kuen 應用化學系 Department of Applied Chemistry |
公開日期: | 13-Jan-2009 |
摘要: | Fucosylated glycoconjugates have critical roles in biological processes, but a limited availability Of alpha-L-fucosidase has hampered research on this human enzyme (h-Fuc) at a molecular level. After overexpressing h-Fuc in Escherichia coli as an active form, we investigated the catalytic function of this recombinant enzyme. Based on sequence alignment and structural analysis of close homologues of h-Fuc, nine residues of glutamate and aspartate in h-Fuc were selected for mutagenic tests to determine the essential residues. Among the mutants, D225N, E289Q, and E289G lost catalytic activity significantly; their k(cat) values are 1/5700, 1/430, and 1/340, respectively, of that of the wild-type enzyme. The Bronsted plot for k(cat)/K(m) for the E289G mutant is linear with beta(1g) = -0.93, but that for k(cat) is biphasic, with beta(1g) for poor substrates being -0.88 and for activated substrates being -0.11. The small magnitude of Pig for the activated substrates may indicate that the rate-limiting step of the reaction is defucosylation, whereas the large magnitude of the latter Pig value for the poor substrates indicates that the rate-limiting step of the reaction becomes fucosylation. The kinetic outcomes support an argument that ASp(225) functions as a nucleophile and Glu(289) as a general acid/base catalyst. As further evidence, azide significantly reactivated D225G and E289G, and (1)H NMR spectral analysis confirmed the formation of beta-fucosyl azide and alpha-fucosyl azide in the azide rescues of D225G and E289G catalyses, respectively. As direct evidence to prove the function of Glu(289), an accumulation of fucosyl-enzyme intermediate was detected directly through ESI/MS analysis. |
URI: | http://dx.doi.org/10.1021/bi801529t http://hdl.handle.net/11536/7749 |
ISSN: | 0006-2960 |
DOI: | 10.1021/bi801529t |
期刊: | BIOCHEMISTRY |
Volume: | 48 |
Issue: | 1 |
起始頁: | 110 |
結束頁: | 120 |
Appears in Collections: | Articles |
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