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最小化 α-羧化体衍生外壳的结构及其在酶稳定化中的应用。

Structure of a Minimal α-Carboxysome-Derived Shell and Its Utility in Enzyme Stabilization.

机构信息

Department of Biochemistry, Yong Loo Lin School of Medicine, National University of Singapore (NUS), 8 Medical Drive, Singapore 117597.

NUS Synthetic Biology for Clinical and Technological Innovation, 28 Medical Drive, Singapore 117456.

出版信息

Biomacromolecules. 2021 Oct 11;22(10):4095-4109. doi: 10.1021/acs.biomac.1c00533. Epub 2021 Aug 12.

Abstract

Bacterial microcompartments are proteinaceous shells that encase specialized metabolic processes in bacteria. Recent advances in simplification of these intricate shells have encouraged bioengineering efforts. Here, we construct minimal shells derived from the α-carboxysome, which we term Cso-shell. Using cryogenic electron microscopy, the atomic-level structures of two shell forms were obtained, reinforcing notions of evolutionarily conserved features in bacterial microcompartment shell architecture. Encapsulation peptide sequences that facilitate loading of heterologous protein cargo within the shells were identified. We further provide a first demonstration in utilizing minimal bacterial microcompartment-derived shells for hosting heterologous enzymes. Cso-shells were found to stabilize enzymatic activities against heat shock, presence of methanol co-solvent, consecutive freeze-thawing, and alkaline environments. This study yields insights into α-carboxysome assembly and advances the utility of synthetic bacterial microcompartments as nanoreactors capable of stabilizing enzymes with varied properties and reaction chemistries.

摘要

细菌微室是一种蛋白质外壳,将细菌中的特殊代谢过程包裹在其中。最近对这些复杂外壳进行简化的进展鼓励了生物工程方面的努力。在这里,我们构建了源自 α-羧化体的最小外壳,我们称之为 Cso-壳。使用低温电子显微镜,获得了两种壳形式的原子级结构,这加强了细菌微室壳结构中进化保守特征的概念。确定了封装肽序列,这些序列有助于将异源蛋白货物加载到壳内。我们进一步首次展示了利用最小细菌微室衍生的壳来容纳异源酶。发现 Cso-壳能够稳定酶的活性,使其能够抵抗热冲击、甲醇共溶剂的存在、连续的冻融循环和碱性环境。这项研究深入了解了 α-羧化体的组装,并推进了合成细菌微室作为纳米反应器的应用,这些纳米反应器能够稳定具有不同性质和反应化学性质的酶。

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