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抑制型内切葡聚糖酶和外切葡聚糖酶在模型纤维素底物上的竞争吸附动力学。

Competitive sorption kinetics of inhibited endo- and exoglucanases on a model cellulose substrate.

机构信息

Department of Chemical and Biomolecular Engineering, University of California-Berkeley, Berkeley, California 94720-1462, USA.

出版信息

Langmuir. 2012 Oct 16;28(41):14598-608. doi: 10.1021/la3024524. Epub 2012 Oct 1.

Abstract

For the first time, the competitive adsorption of inhibited cellobiohydrolase I (Cel7A, an exoglucanase) and endoglucanase I (Cel7B) from T. longibrachiatum is studied on cellulose. Using quartz crystal microgravimetry (QCM), sorption histories are measured for individual types of cellulases and their mixtures adsorbing to and desorbing from a model cellulose surface. We find that Cel7A has a higher adsorptive affinity for cellulose than does Cel7B. The adsorption of both cellulases becomes irreversible on time scales of 30-60 min, which are much shorter than those typically used for industrial cellulose hydrolysis. A multicomponent Langmuir kinetic model including first-order irreversible binding is proposed. Although adsorption and desorption rate constants differ between the two enzymes, the rate at which each surface enzyme irreversibly binds is identical. Because of the higher affinity of Cel7A for the cellulose surface, when Cel7A and Cel7B compete for surface sites, a significantly higher bulk concentration of Cel7B is required to achieve comparable surface enzyme concentrations. Because cellulose deconstruction benefits significantly from the cooperative activity of endoglucanases and cellobiohydrolases on the cellulose surface, accounting for competitive adsorption is crucial to developing effective cellulase mixtures.

摘要

首次研究了来自嗜热纤维单胞菌的抑制型纤维二糖水解酶 I(Cel7A,外切葡聚糖酶)和内切葡聚糖酶 I(Cel7B)在纤维素上的竞争吸附。使用石英晶体微天平(QCM)测量了单独类型的纤维素酶及其混合物在模型纤维素表面上吸附和解吸的吸附历史。我们发现 Cel7A 对纤维素的吸附亲和力高于 Cel7B。两种纤维素酶的吸附在 30-60 分钟的时间尺度内变为不可逆,这比通常用于工业纤维素水解的时间尺度短得多。提出了一个包含一级不可逆结合的多组分 Langmuir 动力学模型。尽管两种酶的吸附和解吸速率常数不同,但每种表面酶不可逆结合的速率是相同的。由于 Cel7A 对纤维素表面的亲和力更高,因此当 Cel7A 和 Cel7B 竞争表面位点时,需要更高的 Cel7B 本体浓度才能达到可比的表面酶浓度。由于纤维素的解构明显受益于内切葡聚糖酶和纤维二糖水解酶在纤维素表面上的协同活性,因此考虑竞争吸附对于开发有效的纤维素酶混合物至关重要。

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