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级联酶的微观共定位可提高活性。

Microscale Colocalization of Cascade Enzymes Yields Activity Enhancement.

作者信息

Xiong Yan, Tsitkov Stanislav, Hess Henry, Gang Oleg, Zhang Yifei

机构信息

Department of Chemical Engineering, Columbia University, New York, New York 10027, United States.

Department of Biomedical Engineering, Columbia University, New York, New York 10027, United States.

出版信息

ACS Nano. 2022 Jul 26;16(7):10383-10391. doi: 10.1021/acsnano.2c00475. Epub 2022 May 12.

Abstract

Colocalization of cascade enzymes is broadly discussed as a phenomenon that can boost the cascade reaction throughput, although a direct experimental verification is often challenging. This is mainly due to difficulties in establishing proper size regimes and in the analytical quantification of colocalization effect with adequate experimental systems and simulations. In this study, by taking advantage of reversible DNA-directed colocalization of enzymes on microspheres, we established a cascade system that can be used to directly evaluate the colocalization effect with exactly the same experimental settings except for the state of enzyme dispersion. In the regime of highly dilute microspheres of particular sizes, the colocalized cascade shows enhanced activity compared with the freely diffusing cascade, as evidenced by a shortened lag phase in the time-course production. Reaction-diffusion modeling reveals that the enhancement can be ascribed to the initial accumulation of intermediate substrate around the colocalized enzymes and is found to be carrier-size-dependent. This work demonstrates the dependence of the colocalization effect of enzyme cascades on an interplay of nano- and microscales, lending theoretical support to the rational design of highly efficient multienzyme catalysts.

摘要

级联酶的共定位作为一种能够提高级联反应通量的现象被广泛讨论,尽管直接的实验验证往往具有挑战性。这主要是由于难以建立合适的尺寸范围,以及难以用适当的实验系统和模拟对共定位效应进行分析定量。在本研究中,通过利用酶在微球上的可逆DNA定向共定位,我们建立了一个级联系统,该系统可用于在除酶分散状态外完全相同的实验设置下直接评估共定位效应。在特定尺寸的高度稀释微球体系中,与自由扩散的级联相比,共定位级联显示出增强的活性,这在时间进程生产中缩短的延迟阶段得到了证明。反应扩散模型表明,这种增强可归因于共定位酶周围中间底物的初始积累,并且发现其与载体尺寸有关。这项工作证明了酶级联共定位效应依赖于纳米和微米尺度的相互作用,为高效多酶催化剂的合理设计提供了理论支持。

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