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The use of Group 3 LEA proteins as fusion partners in facilitating recombinant expression of recalcitrant proteins in E. coli

机译:第3组LEA蛋白作为融合伴侣在促进大肠杆菌中顽calc蛋白的重组表达中的用途

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Late embryogenesis abundant (LEA) proteins are intrinsically disordered proteins that accumulate in organisms during the development of dehydration stress tolerance and cold acclimation. Group 3 LEA proteins have been implicated in the prevention of cellular protein denaturation and membrane damage during desiccation and anhydrobiosis. We tested the ability of LEA proteins to facilitate recombinant expression of recalcitrant and intrinsic membrane proteins. Two Brassica napus Group 3 LEA proteins, BN115m and a truncated fragment of BNECP63, were fused to two target proteins identified as recalcitrant to overexpression in soluble form or outside of inclusion bodies. Fusion of a truncated peptide of BNECP63 is sufficient to provide soluble and high levels of recombinant overexpression of BNPsbS (an intrinsic membrane chlorophyll-binding protein of photosystem II light harvesting complex) and a peptide of the Hepatitis C viral polyprotein. Furthermore, fusion of the recombinant target proteins to BNECP63 or BN115 prevented irreversible heat- and freeze-induced precipitation. These experiments not only underscore the exploitation of LEA-type peptides in facilitating protein overexpression and protection, but also provide insights into the mechanism of LEA proteins in cellular protection.
机译:晚期胚胎发生丰富(LEA)蛋白是在脱水胁迫耐受性和冷驯化过程中在生物体中积累的内在无序的蛋白。在干燥和脱水生物过程中,第3组LEA蛋白与细胞蛋白变性和膜损伤的预防有关。我们测试了LEA蛋白促进重组顽固和内在膜蛋白表达的能力。将两个甘蓝型油菜第3组LEA蛋白BN115m和一个截短的BNECP63片段融合到两个靶蛋白上,这些靶蛋白被确定为难以以可溶形式或在包涵体外部表达。 BNECP63的截短肽的融合足以提供可溶性和高水平的BNPsbS(光系统II光收集复合物的固有膜叶绿素结合蛋白)和丙型肝炎病毒多蛋白肽重组过表达。此外,重组靶蛋白与BNECP63或BN115的融合防止了不可逆的热和冷冻诱导的沉淀。这些实验不仅强调了LEA型肽在促进蛋白质过表达和保护中的应用,而且还提供了LEA蛋白在细胞保护中的作用机理的见解。

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