首页> 外文期刊>The Journal of biological chemistry >Cellulose Surface Degradation by a Lytic Polysaccharide Monooxygenase and Its Effect on Cellulase Hydrolytic Efficiency
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Cellulose Surface Degradation by a Lytic Polysaccharide Monooxygenase and Its Effect on Cellulase Hydrolytic Efficiency

机译:纤维素表面通过裂解多糖单氧化酶降解其对纤维素酶水解效率的影响

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Lytic polysaccharide monooxygenase (LPMO) represents a unique principle of oxidative degradation of recalcitrant insoluble polysaccharides. Used in combination with hydrolytic enzymes, LPMO appears to constitute a significant factor of the efficiency of enzymatic biomass depolymerization. LPMO activity on different cellulose substrates has been shown from the slow release of oxidized oligosaccharides into solution, but an immediate and direct demonstration of the enzyme action on the cellulose surface is lacking. Specificity of LPMO for degrading ordered crystalline and unordered amorphous cellulose material of the substrate surface is also unknown. We show by fluorescence dye adsorption analyzed with confocal laser scanning microscopy that a LPMO (from Neurospora crassa) introduces carboxyl groups primarily in surface-exposed crystalline areas of the cellulosic substrate. Using time-resolved in situ atomic force microscopy we further demonstrate that cellulose nano-fibrils exposed on the surface are degraded into shorter and thinner insoluble fragments. Also using atomic force microscopy, we show that prior action of LPMO enables cellulases to attack otherwise highly resistant crystalline substrate areas and that it promotes an overall faster and more complete surface degradation. Overall, this study reveals key characteristics of LPMO action on the cellulose surface and suggests the effects of substrate morphology on the synergy between LPMO and hydrolytic enzymes in cellulose depolymerization.
机译:Lytic多糖单氧化酶(LPMO)代表了顽固性不溶性多糖的氧化降解的独特原理。与水解酶组合使用,LPMO似乎构成了酶生物量解聚的效率的显着因素。已经从氧化寡糖的缓慢释放到溶液中显示出不同纤维素基材的LPMO活性,但缺乏酶表面上的酶作用的即时和直接证明。 LPMO用于降解底物表面的有序结晶和无序无定形纤维素材料的特异性也是未知的。我们通过共聚焦激光扫描显微镜进行荧光染料吸附,即LPMO(来自神经孢子Crassa),主要在纤维素基材的表面暴露的表面暴露的结晶区域中引入羧基。使用沿原位原子力显微镜的时间分辨,我们进一步证明暴露在表面上的纤维素纳米原纤维降解到更短且较薄的不溶性片段中。同样使用原子力显微镜,我们表明LPMO的前提作用使纤维素酶能够攻击另外的高度抗性结晶衬底区域,并且它促进整体更快,更完整的表面劣化。总体而言,该研究揭示了纤维素表面对LPMO作用的关键特征,并提出了底物形态对纤维素解聚中LPMO与水解酶的协同作用的影响。

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