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首页> 外文期刊>Biochimica et Biophysica Acta. Protein Structure and Molecular Enzymology >Kinetic evidence for surface residues influencing the active site of Coprinus cinereus peroxidase: analysis of the pH dependence of G154E, P90H and P90H-G154E substrate entrance mutants
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Kinetic evidence for surface residues influencing the active site of Coprinus cinereus peroxidase: analysis of the pH dependence of G154E, P90H and P90H-G154E substrate entrance mutants

机译:表面残渣影响灰粉鬼伞过氧化物酶活性位点的动力学证据:G154E,P90H和P90H-G154E底物入口突变体的pH依赖性分析

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摘要

Three mutants of Coprinus cinereus peroxidase (CIP) were made to mimic the substrate entrance histidine 82-glutamic acid 146 pair of the substrate channel in lignin peroxidase (LIP). Compound I formation of LIP has a low pH optimum around pH 3, while optimal formation of CIP compound I is obtained at pH 6-11. The mutants were glycine 154 → glutamic acid (G154E), proline 90 → histidine (P90H) and the double mutant P90H-G154E. All three showed kinetics of compound I formation similar to that of wt CIP between pH 3 and 9. However, the stability of compound I was strongly affected by these mutations. In wt CIP compound I is stable for approximately 30 min, while compound I of the mutants were stable for 5 s or less. The P90H and P90H-G154E mutants showed pK_a values for the alkaline transition at least one pH unit lower than for wt CIP and the G154E mutant. We suggest that the changed electrostatic field results in destabilisation of the oxidised heme in compound I and II and that the P90H residue increases the electrostatic potential in the distal cavity thereby decreasing the pK_a for the alkaline transition.
机译:制作了灰粉鬼伞过氧化物酶(CIP)的三个突变体,以模拟木质素过氧化物酶(LIP)中底物通道的底物入口组氨酸82-谷氨酸146对。 LIP的化合物I的形成在pH约为3时具有较低的最佳pH值,而CIP化合物I的最佳形成是在pH 6-11时获得的。突变体是甘氨酸154→谷氨酸(G154E),脯氨酸90→组氨酸(P90H)和双突变体P90H-G154E。所有这三个化合物都显示出与pH 3和9之间的wt CIP相似的化合物I形成动力学。然而,化合物I的稳定性受到这些突变的强烈影响。在wt CIP中,化合物I稳定约30分钟,而突变体的化合物I稳定5秒或更短。 P90H和P90H-G154E突变体的碱性跃迁pK_a值比wt CIP和G154E突变体低至少一个pH单位。我们建议改变的静电场会导致化合物I和II中氧化血红素的不稳定,并且P90H残留物会增加远端腔中的静电势,从而降低碱性转变的pK_a。

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