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Bringing functions together with fusion enzymes-from nature's inventions to biotechnological applications

机译:将功能与融合酶融合-从自然界的发明到生物技术应用

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摘要

It is a mammoth task to develop a modular protein toolbox enabling the production of posttranslational organized multifunctional enzymes that catalyze reactions in complex pathways. However, nature has always guided scientists to mimic evolutionary inventions in the laboratory and, nowadays, versatile methods have been established to experimentally connect enzymatic activities with multiple advantages. Among the oldest known natural examples is the linkage of two or more juxtaposed proteins catalyzing consecutive, non-consecutive, or opposing reactions by a native peptide bond. There are multiple reasons for the artificial construction of such fusion enzymes including improved catalytic activities, enabled substrate channelling by proximity of biocatalysts, higher stabilities, and cheaper production processes. To produce fused proteins, it is either possible to genetically fuse coding open reading frames or to connect proteins in a posttranslational process. Molecular biology techniques that have been established for the production of end-to-end or insertional fusions include overlap extension polymerase chain reaction, cloning, and recombination approaches. Depending on their flexibility and applicability, these methods offer various advantages to produce fusion genes in high throughput, different orientations, and including linker sequences to maximize the flexibility and performance of fusion partners. In this review, practical techniques to fuse genes are highlighted, enzymatic parameters to choose adequate enzymes for fusion approaches are summarized, and examples with biotechnological relevance are presented including a focus on plant biomass-degrading glycosyl hydrolases.
机译:开发模块化蛋白质工具箱是一项艰巨的任务,该工具箱能够产生可催化复杂途径反应的翻译后组织化多功能酶。然而,自然界一直在引导科学家在实验室中模仿进化发明,如今,已经建立了多种方法来通过实验将酶活性与多种优势联系起来。在最古老的已知自然实例中,有两个或多个并列的蛋白质通过天然肽键催化连续,非连续或相反的反应。人工构建此类融合酶的原因有很多,包括改善的催化活性,通过生物催化剂的接近而实现的底物通道化,更高的稳定性和更便宜的生产工艺。为了产生融合蛋白,有可能在遗传上融合编码开放阅读框,或者在翻译后过程中连接蛋白。已建立用于产生端对端或插入融合的分子生物学技术,包括重叠延伸聚合酶链反应,克隆和重组方法。根据它们的灵活性和适用性,这些方法具有产生高通量,不同方向的融合基因的各种优点,并且包括使融合伴侣的灵活性和性能最大化的接头序列。在这篇综述中,着重介绍了融合基因的实用技术,总结了用于选择适合融合酶的酶参数,并列举了与生物技术相关的实例,其中包括对植物生物质降解糖基水解酶的关注。

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