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Cell-based high-throughput screening of polysaccharide biosynthesis hosts

机译:基于细胞的多糖生物合成宿主的高通量筛选

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摘要

Schematic view of cell-based high-throughput screening strategies based on fluorescently-labeled substrates. In the original strategy, a single fluorescent substrate was used to screen a library of mutant sialyltransferases. First, fluorescently-labeled monosaccharides are transported into the cell by a transmembrane sugar transport protein (step 1). After an incubation period during which the fluorescently-labeled substrates may be modified enzymatically (step 2), unreacted substrates are removed using a washing step (step 3). Cells containing catalytically-active glycosyltransferases retain the fluorescent product inside the cell, now as part of a polysaccharide. Finally, desired cells (with high fluorescence, hence high-level polysaccharide production) are screened by rapid sorting techniques such as fluorescence activated cell sorting (FACS) (step 4), followed by sequencing (step 5)
机译:基于荧光标记基底的细胞基高通量筛选策略的示意图。在原始策略中,使用单个荧光基底筛选突变唾液酸盐库文库。首先,通过跨膜糖转运蛋白将荧光标记的单糖转运到细胞中(步骤1)。在诱导荧光标记的基材的孵育时间之后(步骤2),使用洗涤步骤(步骤3)去除未反应的底物(步骤3)。含有催化活性糖基转移酶的细胞在细胞内保留荧光产物,现在作为多糖的一部分。最后,通过快速分选技术(例如荧光活化的细胞分选(FACS)(步骤4),通过快速分选技术筛选所需的细胞(具有高荧光,因此高级多糖产生)(步骤4)(步骤5)

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