Self assembling nanoparticle enzyme clusters provide access to substrate channeling in multienzymatic cascades

自组装纳米颗粒酶簇为多酶级联中的底物通道提供了途径

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作者:Joyce C Breger #, James N Vranish #, Eunkeu Oh, Michael H Stewart, Kimihiro Susumu, Guillermo Lasarte-Aragonés, Gregory A Ellis, Scott A Walper, Sebastián A Díaz, Shelby L Hooe, William P Klein, Meghna Thakur, Mario G Ancona, Igor L Medintz

Abstract

Access to efficient enzymatic channeling is desired for improving all manner of designer biocatalysis. We demonstrate that enzymes constituting a multistep cascade can self-assemble with nanoparticle scaffolds into nanoclusters that access substrate channeling and improve catalytic flux by orders of magnitude. Utilizing saccharification and glycolytic enzymes with quantum dots (QDs) as a model system, nanoclustered-cascades incorporating from 4 to 10 enzymatic steps are prototyped. Along with confirming channeling using classical experiments, its efficiency is enhanced several fold more by optimizing enzymatic stoichiometry with numerical simulations, switching from spherical QDs to 2-D planar nanoplatelets, and by ordering the enzyme assembly. Detailed analyses characterize assembly formation and clarify structure-function properties. For extended cascades with unfavorable kinetics, channeled activity is maintained by splitting at a critical step, purifying end-product from the upstream sub-cascade, and feeding it as a concentrated substrate to the downstream sub-cascade. Generalized applicability is verified by extending to assemblies incorporating other hard and soft nanoparticles. Such self-assembled biocatalytic nanoclusters offer many benefits towards enabling minimalist cell-free synthetic biology.

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